STG and Nemlt 2021

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THE UNITED REPUBLIC OF TANZANIA

MINISTRY OF HEALTH, COMMUNITY DEVELOPMENT,


GENDER, ELDERLY AND CHILDREN

STANDARD TREATMENT GUIDELINES AND


NATIONAL ESSENTIAL MEDICINES LIST FOR
TANZANIA MAINLAND

SIXTH EDITION 2021


THE UNITED REPUBLIC OF TANZANIA

MINISTRY OF HEALTH, COMMUNITY DEVELOPMENT,


GENDER, ELDERLY AND CHILDREN

STANDARD TREATMENT GUIDELINES AND


NATIONAL ESSENTIAL MEDICINES LIST FOR
TANZANIA MAINLAND

SIXTH EDITION 2021


FOREWORD
The Government is committed to ensure adequate availability and accessibility of safe, efficacious
and affordable essential medicines at all times to all Tanzanians. To realize this objective, the
development and implementation of Standard Treatment Guidelines (STG) and National Essential
Medicines List (NEMLIT) is an important step in the health care system for quality diagnosis,
treatment and prevention of diseases as well as procurement and supply of essential medicnes.
The 2017 edition of STG/NEMLIT has been updated to reflect new therapeutic options and changing
therapeutic needs, the need to ensure drug quality, safety issues, medicines for emerging diseases,
medicines to meet changing resistance pattern and to reconsider levels of care. A new chapter
“approach to patients with emergency conditions” has been added to guide clinicians in the
management of patients with emergency conditions and provide initial resuscitation and
stabilization. In addition, under notifiable diseases, guidance for the management of COVID-19 has
been addressed.

The list of medicines has been selected with due regard to disease prevalence and public health
relevance, evidence of clinical efficacy and safety, comparative costs, availability and treatment
facilities. The review considered the ongoing expansion of services in primary health facilities;
hence, levels of some medicines have been lowered to be available at that level. Inparticular,
special attention has been paid to medicines used to manage non-communicable diseases, such as
diabetes and cardiovascular diseases. Also, this new version of STG/NEMLIT adopted the World
Health Organization classification of antibiotics into Access, Watch, Reserve (AWaRe) groups,
aiming to improve the rational use of antimicrobial agents and minimize the burden of antimicrobial
resistance.

The Standard Treatment Guidelines comprise statements to assist practitioners in making decisions
about appropriate treatment for specific clinical conditions. Hence, this is a key tool, which should be
used to effectively promote access to essential medicines, to achieve maximum therapeutic benefit
and optimize patient outcomes. Further, the document will guide the procurement and supply of
medicines at the Medical Stores Department (MSD)prescribing and dispensing of medicines in
public health facilities as well as the reimbursements of medicines at the National Health Insurance
Fund (NHIF).

I therefore urge all responsible institutions and experts to adhere to STG/NEMLIT and to ensure
availability of essential medicines at all times, in adequate amounts, in appropriate dosage forms,
with assured quality and adequate information, and at a price the individual and the community can
afford. Comments and suggestions that may help us to improve a next edition of STG/NEMLIT are
welcome and much appreciated. I am confident that health care workers and responsible institutions
will find this document very useful.

Hon. Dr. Dorothy O. Gwajima (MP)


MINISTER FOR HEALTH, COMMUNITY DEVELOPMENT, GENDER, ERLDERLY AND
CHILDREN

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ACKNOWLEDGEMENTS
This document was developed through a co-creation process that engaged a broad range of
stakeholders. This participatory approach permits ownership of the Standard Treatment Guidelines
and Essential Medicines List of Tanzania (STG/NEMLIT)and facilitatesits successful implementation.
The development process was initiated in December 2019 by identifying key stakeholders.
Thereafter, all key stakeholders, including all hospitals were asked to provide their inputs on
essential medicines to be added or deleted based on scientific evidence. In addition, stakeholders
were asked to recommend stratification forlevels of use for specific medicines. I highly appreciate
support fromMuhimbili National Hospital, Bugando and Mbeya Zonal Referral hospitals as well as
Bukoba, Katavi, Njombe and Sekou Toure Regional Referral Hospitals who provided inputs. Your
comments were valuable and were incorporated in this STG/NEMLIT edition.

Further, the Ministry in collaboration with Health Promotion and System Strengthening (HPSS)
project conducted a surveyfor the collection of recommendations regardingthe review of
STG/NEMLIT in 26 health facilities in six regions of Dodoma, Singida, Manyara, Morogoro, Pwani
and Dar es Salaam. I thank all health care workers who provided recommendations for
STG/NEMLIT improvements; your contributions were consolidated and used to enrich this
document.

In a further step, Lead Reviewers for individual chapters were nominated. We thank all Professional
Associations who participated in the review through their professional peer reviewersrendering the
process fully participatory. I acknowledge the Association of Physicians of Tanzania (APHYTA),
Association of Gynecologists and Obstetricians of Tanzania (AGOTA), Association of
Pulmonologists-Chest Tanzania, Emergency Medicine Association of Tanzania (EMAT), Nephrology
Society of Tanzania (NESOT), Pediatric Association of Tanzania (PAT), Pharmaceutical Society of
Tanzania (PST), Tanzania Association for Respiratory Diseases (TARD), Tanzania Cardiac Society
(TCS), Tanzania Dental Association (TDA), Tanzania Diabetes Association (TDA), Tanzania Ear
Nose & Throat Society (TENTS), Tanzania Gastroenterology and Endoscopy Society (TGES),
Tanzania Oncology Society (TOS), Tanzania Ophthalmology Society (TOS), Tanzania Orthopedic
Association (TOA), Tanzania Society for Dermatovenereology (TASOD) and Tanzania Surgical
Associations (TSA). I also acknowledge the Holistic Approach to Unravel Antibacterial Resistance in
East Africa (HATUA-MR/S004785/1)-Tanzania for their preliminary results of patients with urinary
tract infections (UTI) which provided insight of the susceptibility patterns of common isolates causing
UTI in Tanzania, which was useful to update the relevant chapter. I trust that in the future review you
will continue providing technical support.

I sincerely thank the National Medicines and Therapeutic Committee (NMTC), all Lead Reviewers
and the NMTC Secretariat who made this a reality. Their names are annexed. Finally, I would like to
gratefully acknowledgethe financial support provided by the USAID Medicines, Technologies and
Pharmaceutical Services (MTaPS) program implemented by Management Science for Health, the
Swiss Agency for Development and Cooperation (SDC) through the Health Promotion and System
Strengthening (HPSS) project, the Global Fund for AIDS, TB and Malaria (GFATM) and the National
Health Insurance (NHIF).

Prof. Abel N. Makubi


PERMANENT SECRETARY (HEALTH)

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TABLE OF CONTENTS

FOREWORD ............................................................................................................................ i

ACKNOWLEDGEMENTS ....................................................................................................... ii

PART I ..................................................................................................................................... 1

THE NATIONAL ESSENTIAL MEDICINES LIST (NEMLIT) .................................................. 1

PART II .................................................................................................................................. 30

THE STANDARD TREATMENT GUIDELINE (STG) ............................................................ 30

CHAPTER ONE ..................................................................................................................... 31

APPROACH TO PATIENTS WITH EMERGENCY CONDITIONS ....................................... 31

1.1 The Concept of Emergency Care and Resuscitation ................................................. 31

1.2 Cardiac Arrest and Cardiopulmonary Resuscitation ................................................. 32

1.3 Approach to Stridor ....................................................................................................... 33

1.4 Approach to Upper Gastrointestinal Bleeding ............................................................ 34

1.5 Approach to Seizure and Status Epilepticus .............................................................. 35

1.6 Approach to Altered Mental Status .............................................................................. 36

1.7 Approach to Difficult in Breathing ............................................................................... 36

1.8 Anaphylaxis .................................................................................................................... 37

1.9 Cardiac Tamponade ...................................................................................................... 38

1.10 Pulmonary Edema ....................................................................................................... 38

1.11 Approach to Shock ...................................................................................................... 39

1.12 Sepsis and Septic Shock..................................................................................... 41

1.13 Approach to Pain ................................................................................................. 43

1.13.1 Approach to chest pain ............................................................................................ 43

1.13.2 Approach to Abdominal Pain .................................................................................. 44

1.13. 3 Headache .................................................................................................................. 45

1.13.4 Other Pains ................................................................................................................ 46

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1.14 Approach to Fever (Pyrexia) ............................................................................... 46

1.15 Cough .................................................................................................................... 47

1.16 . Approach to the Trauma Patient....................................................................... 48

1.17 Approach to Dehydrated Patient ........................................................................ 48

1.18 Hyponatremia ....................................................................................................... 50

1.19 Hypokalaemia ....................................................................................................... 51

1.20 Triage Overview ................................................................................................... 52

CHAPTER TWO .................................................................................................................... 55

ANAESTHESIA ..................................................................................................................... 55

2.1 General Anaesthesia ................................................................................................... 55

2.2 Local Anaesthesia ....................................................................................................... 57

2.3 Sedation .......................................................................................................................... 58

2.4 Anaesthesia in Special Conditions .............................................................................. 59

2.4.1 Surgery in Diabetic Patient ........................................................................................ 59

2.4.2 Surgery in Hypertensive Patient ............................................................................... 60

2.4.3 Surgery in Asthmatic Patient ..................................................................................... 60

2.4.4 Surgery in Sickle Cell Patient .................................................................................... 61

CHAPTER THREE ................................................................................................................ 62

HAEMATOLOGY AND BLOOD TRANSFUSION ................................................................. 62

3.1 Anaemia .......................................................................................................................... 62

3.1.1 Iron Deficiency Anaemia ............................................................................................ 62

3.1.2 Megaloblastic Anemia ................................................................................................ 63

3.1.3 Haemolytic Anaemia ................................................................................................... 64

3.1.4 Sickle Cell Disease (SCD) ........................................................................................ 64

3.1.4 G6PD Deficiency ......................................................................................................... 68

3.1.5 Aplastic Anaemia (Bone Marrow Failure) ............................................................... 68

3.1.6 Myelodysplastic syndrome (MDS) ............................................................................ 69

3.2 Bleeding Disorders ..................................................................................................... 69

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3.2.1 Hereditary Bleeding Disorders .................................................................................. 69

3.2.3Acquired Bleeding Disorders/Platelet Disorders ...................................................... 71

3.3 Coagulation Disorders .................................................................................................. 72

3.3.1 Deep Vein Thrombosis (DVT) .................................................................................... 72

3.3.2 Pulmonary Embolism (PE) ......................................................................................... 73

3.4 Blood Transfusion ......................................................................................................... 73

CHAPTER FOUR .................................................................................................................. 77

NOTIFIABLE DISEASES ...................................................................................................... 77

4.1 Bacterial Infections ........................................................................................................ 77

4. 1.1 Cholera ....................................................................................................................... 77

4.1.2 Anthrax ........................................................................................................................ 80

4.1.3 Plague .......................................................................................................................... 82

4.1.4Bacterial Cerebro-Spinal Meningitis .......................................................................... 84

4.1.6 Tick-Borne Relapsing Fever (TBRF) ......................................................................... 87

4.2 Viral Infections ............................................................................................................... 88

4.2.1 Viral Haemorrhaghic Fevers (VHF) ........................................................................... 88

4.2.2 Measles (Rubeola) ...................................................................................................... 98

4.2.3 Rabies .......................................................................................................................... 99

4.2.4 Zika Virus Disease .................................................................................................. 101

4.2.5 COVID-19 ................................................................................................................... 103

CHAPTER FIVE .................................................................................................................. 109

MALARIA ............................................................................................................................ 109

5.1 Asymptomatic Malaria Case ....................................................................................... 109

5.2 Symptomatic Malaria Case ......................................................................................... 109

5.2.1 Uncomplicated Malaria .......................................................................................... 109

5.2.2 Severe Malaria ........................................................................................................ 111

5.3 Management of Malaria in Special Groups ............................................................... 114

5.3.1 Malaria in Pregnancy (MIP) ................................................................................... 114

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5.3.2 Management of Malaria in Neonates ....................................................................... 115

5.3.3 Management of Malaria in HIV and AIDS patients ................................................. 116

CHAPTER SIX ..................................................................................................................... 117

HIVAND AIDS ..................................................................................................................... 117

6.1 Treatment of HIV and AIDS in Adults and Adolescents ........................................... 117

6.1.1 First-Line Regimens for Adults and Adolescents ................................................. 117

6.1.2 ART in women of childbearing potential or pregnant women .............................. 117

6.1.3 Prevention of Mother to Child Transmission ......................................................... 118

6.1.4 Second-line ART in Adults and Adolescents ......................................................... 119

6.1.5 Third-line Antiretroviral Therapy ............................................................................. 119

6.2 Changing Antiretroviral Therapy ................................................................................ 120

6.2.1 Drug Specific Adverse Events-Toxicities ............................................................... 120

6.2.2 Changing ART due to Treatment Failure ................................................................ 123

6.3 Monitoring Patients on Antiretroviral Therapy ......................................................... 123

6.4 Immune Reconstitution Inflammatory Syndrome (IRIS) .......................................... 124

6.5 Antiretroviral Therapy in Children and Adolescents Living with HIV ................... 125

6.6. Changing ART in Children Under 15 Years .............................................................. 128

6.7 HIV Prevention ........................................................................................................... 132

6.7.1 Post Exposure Prophylaxis (PEP) ........................................................................... 132

6.7.2 Pre-Exposure Prophylaxis (PrEP) ........................................................................... 133

CHAPTER SEVEN .............................................................................................................. 135

TUBERCULOSIS AND LEPROSY ..................................................................................... 135

7.1General Management of Tuberculosis ........................................................................ 135

7.1.1 Drug Resistance Tuberculosis (DR-TB) ................................................................. 136

7.1.2 Treatment of Tuberculosis in Special Cases ......................................................... 138

Treatment of TB/HIV co-infected patients ....................................................................... 138

7.2 General Treatment of Leprosy .................................................................................... 139

7.2.1 Treatment of Leprosy in Special Cases .................................................................. 139

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CHAPTER EIGHT ............................................................................................................... 141

NERVOUS SYSTEM DISEASE CONDITIONS ................................................................... 141

8.1 Infections of the Nervous System .............................................................................. 141

8.1.1 Bacterial infections ................................................................................................... 141

8.1.2 Fungal Infections ...................................................................................................... 144

8.1.3 Protozoa infections .................................................................................................. 145

8.1.4 Helminthic infections ............................................................................................... 146

8.1.5 Viral infections .......................................................................................................... 147

8.2 Initial Management of Stroke ...................................................................................... 148

8.2.1 Management of acute hemorrhagic stroke ............................................................ 148

8.2.2 Initial Management of Acute Subarachnoid Hemorrhage from Ruptured Cerebral


Aneurysm ........................................................................................................................... 149

8.2.3 Initial management of Acute Ischemic Stroke ....................................................... 150

8.3 Management of Epilepsy ............................................................................................. 153

8.4. Parkinson’s disease ................................................................................................... 155

8.5 Congenital Pediatric Nervous System Diseases ...................................................... 155

8.5.1 Pediatric Hydrocephalus .......................................................................................... 155

8.5.2 Management of Pediatric CSF shunt infections .................................................... 156

8.5.3 Congenital Spina Bifida ........................................................................................... 157

8.6 Cranial Nerve Disorders .............................................................................................. 157

8.6.1 Trigeminal Neuralgia ................................................................................................ 157

8.6.2 Bell’s palsy ................................................................................................................ 158

8.7 Spinal Cord and Peripheral Nerve Disorders ............................................................ 158

8.7.1 Acute Transverse Myelitis (TM) ............................................................................... 158

8.7.2 Guillan Barre syndrome ........................................................................................... 159

8.7.3 Peripheral neuropathy .............................................................................................. 160

CHAPTER NINE .................................................................................................................. 162

RESPIRATORY DISEASE CONDITIONS .......................................................................... 162

9.1 Acute Respiratory Infections (ARI) ............................................................................ 162


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9.1.1 Pneumonia ................................................................................................................ 162

9.2 Obstructive Lung Diseases ........................................................................................ 166

9.2.1 Asthma ....................................................................................................................... 166

9.2.2 Chronic Asthma in Adults ........................................................................................ 168

9.3 Bronchitis ..................................................................................................................... 170

9.3.1 Acute Bronchitis ....................................................................................................... 170

9.3.2 Chronic Bronchitis ................................................................................................... 171

9.4 Emphysema .................................................................................................................. 172

9.5 COPD Exacerbation ..................................................................................................... 173

9.6 Other Respiratory Infections ...................................................................................... 173

9.6.1 Acute Laryngo-tracheobronchitis ........................................................................... 173

9.6.2 Laryngeal Diphtheria ................................................................................................ 174

9.6.3 Whooping Cough ...................................................................................................... 174

9.6.4 Bronchiectasis .......................................................................................................... 175

9.6.5 Lung Abscess ........................................................................................................... 176

9.6.6 Aspergilosis .............................................................................................................. 176

9.6.7 Pneumocystis Pneumonia (PCP) ............................................................................ 177

9.6.8 Silicosis ..................................................................................................................... 177

9.6.11 Obstructive sleep apnea syndrome (OSA ............................................................ 178

9.6.12 Cor Pulmonale ........................................................................................................ 179

9.6.13 Pleural effusion ....................................................................................................... 180

9.6.14 Respiratory Failure ................................................................................................. 182

10.1.1 Amoebiasis .............................................................................................................. 183

10.1.2 Amoebic Liver Abscess ......................................................................................... 183

10.1.3. Giardiasis ............................................................................................................... 183

10.1.4 Ascariasis ................................................................................................................ 184

10.1.5 Ancylostomiasis ..................................................................................................... 184

10.1.6 Strongyloidiasis ...................................................................................................... 185

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10.1.7 Taeniasis ................................................................................................................. 185

10.1.8 Echinococcosis ...................................................................................................... 186

10.1.9 Schistosomiasis ..................................................................................................... 186

10.1.10 Typhoid and Paratyphoid ..................................................................................... 187

10.1.11 Shigellosis ............................................................................................................. 187

10.2. Disorders of Gastrointestinal Tract ........................................................................ 188

10.2.1 Peptic Ulcer Disease .............................................................................................. 188

10.2.2 Ulcer Related Conditions ....................................................................................... 190

10.2.3 Gastrointestinal (GI) Bleeding ............................................................................... 191

10.3 Diseases of the Intestine ........................................................................................... 194

10.3.1 Inflammatory Bowel Diseases ............................................................................... 194

10.3.2 Pseudomembranous Colitis .................................................................................. 195

10.3.3 Radiation Proctitis .................................................................................................. 196

10.3.4 Irritable Bowel Syndrome ...................................................................................... 197

10.3.5 Diverticulosis .......................................................................................................... 197

10.3.6 Diverticulitis ............................................................................................................ 197

10.3.7 Polyps and Adenomas ........................................................................................... 198

10.3.8 Hemorrhoids ........................................................................................................... 199

10.3.9 Anal Fissures .......................................................................................................... 199

10.3.10 Fistula in ano ......................................................................................................... 200

10.3.11 Appendicitis .......................................................................................................... 200

10.4 Pancreatitis ................................................................................................................ 201

10.4.1 Acute Pancreatitis .................................................................................................. 201

10.4.2 Chronic Pancreatitis ............................................................................................... 201

10.4 Disorders of The Liver and Biliary Tract ............................................................... 202

10.4.1 Hepatitis ................................................................................................................... 202

10.4.2 Portal Hypertension ................................................................................................ 209

10.4.3 Biliary Tract Diseases ............................................................................................ 212

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CHAPTER ELEVEN ............................................................................................................ 217

OBSTETRICS, GYNECOLOGY AND CONTRACEPTION ................................................. 217

11.1 Bleeding in Pregnancy .............................................................................................. 217

11.1.1 Abortion ................................................................................................................... 217

11.2 Ectopic Pregnancy .................................................................................................... 222

11.2.1 Un-ruptured ectopic pregnancy ............................................................................ 222

11.2.2 Ruptured ectopic pregnancy ................................................................................. 222

11.3 Antepartum Hemorrhage .......................................................................................... 223

11.3.1 Placenta Praevia ..................................................................................................... 223

11.3.2. Placental Abruption ............................................................................................... 223

11.4 Obstructed Labour .................................................................................................... 224

11.5 Postpartum Hemorrhage (PPH) ................................................................................ 225

11.6 Prelabour Rupture of Membranes (PROM) .............................................................. 226

11.7 Antenatal Care ........................................................................................................... 227

11.7.1 Anaemia in Pregnancy ........................................................................................... 227

11.7.2 Hypertensive Disorders in Pregnancy .................................................................. 228

11.7.3 Pre-eclampsia ......................................................................................................... 228

11.7.4 HELLP syndrome .................................................................................................... 229

11.7.5 Eclampsia ................................................................................................................ 230

11.7.6 Antiphospholipid Syndrome (APS) in Pregnancy ............................................... 231

11.7.7 Deep Vein Thrombosis in Pregnancy ................................................................... 232

11.7.8 Pulmonary Embolism in Pregnancy ..................................................................... 232

11.7.9 Vomiting in Pregnancy and Hyperemesis Gravidarum ....................................... 233

11.7.10 Heartburn in Pregnancy ....................................................................................... 234

11.7.11 Other Medical Disorders in Pregnancy ............................................................... 234

11.7.12 Stimulation of labour and Myometrial Relaxation ............................................. 234

11.7.13 Rhesus Incompatibility ........................................................................................ 236

11.8 Postpartum care ........................................................................................................ 236

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11.8.1 Mastitis .................................................................................................................... 236

11.8.2 Puerperal Sepsis ..................................................................................................... 237

11.8.4 Dysmenorrhea ......................................................................................................... 239

11.8.5 Endometriosis ......................................................................................................... 240

11.9 Contraception ............................................................................................................ 240

11.9.1 Short term Contraceptive Methods ....................................................................... 240

11.9.2 Long term methods ................................................................................................ 241

11.9.3 Permanent (surgical) contraceptive methods ...................................................... 242

11.8.4 Infertility ................................................................................................................... 242

CHAPTER TWELVE ........................................................................................................... 244

SEXUALLY TRANSMITTED INFECTIONS ........................................................................ 244

12.1 STIs/RTIs Management Approaches ........................................................................ 244

12.2 Urethral Discharge Syndrome (UDS) ....................................................................... 245

12.3 Vaginal Discharge Syndrome (VDS) ........................................................................ 245

12.4 Lower Abdominal Pain Syndrome or Pelvic Inflammatory Disease (PID) ............ 246

12.5 Painful Scrotal Swelling (PSS) ................................................................................. 247

12.6 Ano-rectal Syndrome (ARS) ..................................................................................... 247

12.7 Oropharyngeal Syndrome ......................................................................................... 248

12.8 Genital Ulcer Disease (GUD) ..................................................................................... 249

12.9 Neonatal Conjunctivitis (Ophthalmia Neonatorum) ............................................... 249

12.10 Inguinal Bubo (IB) .................................................................................................... 249

12.11STI/RTI flow charts ................................................................................................... 250

12.8 Management of other common STI Conditions .................................................... 260

CHAPTER THIRTEEN ........................................................................................................ 262

SKIN DISEASES AND ALLERGIC REACTIONS ............................................................... 262

13.1 Bacterial Skin Infections ........................................................................................... 262

13.1.1 Impetigo ................................................................................................................... 262

13.1.2 Folliculitis ................................................................................................................ 262

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13.1.3 Abscess ................................................................................................................... 263

13.1.4 Erysipelas and Cellulitis ........................................................................................ 264

13.1.5 Paronychia .............................................................................................................. 264

13.2 Fungal Skin Infections .............................................................................................. 265

13.2.1 Tinea Corporis (Body Ringworm) ......................................................................... 265

13.2.2 Tinea Capitis ........................................................................................................... 265

13.2.3 Pityriasis Versicolor ............................................................................................... 265

13.2.4 Tinea Pedis (Athlete’s Foot) and Tinea Cruris ..................................................... 266

13.2.5 Candidiasis .............................................................................................................. 266

13.2.6 Onychomycosis ...................................................................................................... 267

13.2.7 Chromoblastomycosis ........................................................................................... 267

13.2.8 Mycetoma (Madura Foot) ....................................................................................... 268

13.3 Parasitic Infestations ................................................................................................. 268

13.3.1 Scabies .................................................................................................................... 268

13.4 Viral Infections ........................................................................................................... 269

13.4.1 Herpes Simplex ....................................................................................................... 269

13.4.2 Chickenpox ............................................................................................................. 269

13.4.3 Herpes Zoster (Shingles) ....................................................................................... 269

13.4.4 Post-herpetic Neuralgia ......................................................................................... 270

13.4.5 Molluscum Contagiosum ....................................................................................... 270

13.4.6 Viral warts ................................................................................................................ 271

13.5 Eczema (Dermatitis) Conditions ............................................................................... 271

13.5.1 Contact Dermatitis .................................................................................................. 271

13.5.2 Atopic Eczema ........................................................................................................ 272

13.5.3 Seborrheic Dermatitis ............................................................................................ 273

13.6 Anaphylaxis ................................................................................................................ 273

13.7 Papulosquamous Disorder ....................................................................................... 273

13.7.1. Psoriasis ................................................................................................................. 273

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13.7.2. Lichen Planus ........................................................................................................ 274

13.7.3 Acne ......................................................................................................................... 275

13.8 Drug Reactions .......................................................................................................... 275

13.8.1 Fixed Drug Eruption (FDE) ..................................................................................... 276

13.8.3 Stevens Johnson Syndrome (SJS) and Toxic Epidermal Necrolysis (TEN) ..... 276

13.10 Pellagra ..................................................................................................................... 277

13.11 Vitiligo ....................................................................................................................... 277

13.12 Pruritic Papular Eruption (PPE) .............................................................................. 278

13.13 Oculo-cutaneous Albinism and Xeroderma Pigmentosum ................................. 278

13.14 Urticaria and Angioedema ...................................................................................... 279

13.15 Connective Tissue Diseases .................................................................................. 279

13:16 Autoimmune Blistering Disease ............................................................................ 281

13.17 Keloids ...................................................................................................................... 281

13.18 Folliculitis Decalvans .............................................................................................. 281

13.19 Infantile Haemangioma ........................................................................................... 282

13.20 Cysts ......................................................................................................................... 282

13.21 Skin Lightening ........................................................................................................ 282

CHAPTER FOURTEEN ....................................................................................................... 284

EYE DISEASES AND CONDITIONS .................................................................................. 284

14.1 Major Blinding Eye Diseases .................................................................................... 284

14.1.1 Cataract ................................................................................................................... 284

14.1.2 Glaucoma ................................................................................................................ 286

14.1.3 Trachoma ................................................................................................................. 289

14.1.4 Diseases of the Retina ........................................................................................... 290

14.1.5 Refractive Errors ..................................................................................................... 294

14.2 Painful Red Eyes ........................................................................................................ 296

14.2.1 Ocular Trauma ........................................................................................................ 296

14.2.2 Herpes Simplex Keratitis ....................................................................................... 299

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14.2.3 Corneal Ulcer .......................................................................................................... 299

14.2.4 Uveitis ...................................................................................................................... 300

14.2.5 Conjunctivitis .......................................................................................................... 301

14.3 Structural Abnormalities of the Eye ......................................................................... 305

14.4 Ocular Oncology ........................................................................................................ 305

14.4.1 Retinoblastoma ....................................................................................................... 305

14.4.2 Squamous Cell Carcinoma of Conjunctiva .......................................................... 307

14.5 Dry Eye ....................................................................................................................... 308

14.6 Herpes Zoster Ophthalmicus .................................................................................... 309

14.7 Endophthalmitis ......................................................................................................... 309

14.8 Retinitis ....................................................................................................................... 310

14.9 Orbital Cellulitis ......................................................................................................... 310

14.10 Visual Problems ....................................................................................................... 312

14.11 Onchocerciasis (River Blindness) ......................................................................... 313

CHAPTER FIFTEEN .......................................................................................................... 315

EAR, NOSE AND THROAT DISEASES ........................................................................... 315

15.1 Ear Condition ............................................................................................................. 315

15.1.1 Circumscript otitis Externa (Furunculosis) .......................................................... 315

15.1.2 Diffusewer Otitis Externa (Swimmer’s ear) .......................................................... 315

15.1.3 Necrotizing Otitis Externa ...................................................................................... 316

15.1.4 Herpes Zoster Oticus (Ramsay Hunt syndrome) ................................................. 317

15.1.5 Pre-auricular sinus tract infection ........................................................................ 318

15.2 Trauma of the pinna .................................................................................................. 319

15.2.1 Hematoma of the pinna ........................................................................................... 319

15.2.2 Laceration of the Pinna .......................................................................................... 319

15.2.3 Ear Keloid ................................................................................................................ 319

15.2.4 Cerumen Impaction ................................................................................................ 320

15.2.5 Foreign Body in the Ear ......................................................................................... 320

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15.2.6 Traumatic Tympanic Membrane/ Ear Drum Perforation. .................................... 320

15.3 Otitis Media (Acute or Chronic) ................................................................................ 321

15.3.1 Acute Otitis Media .................................................................................................. 321

15.3.2 Chronic Suppurative Otitis Media ......................................................................... 322

15.3.3 Mastoditis with Sub-Periosteal Abscess .............................................................. 323

15.3.4Otitis Media with Effusion ....................................................................................... 323

15.4 Hearing Loss .............................................................................................................. 324

15.4.1 Sensorineural hearing loss (SNHL) ...................................................................... 324

15.4.2 Sudden Sensorineural Hearing Loss .................................................................... 324

15.4.3 Otosclerosis ............................................................................................................ 325

15.4.4 Peripheral Vertigo (Meniere’s disease and Benign Paroxysmal Positional


Vertigo(BPPV) .................................................................................................................... 325

15.4.5 Vestibular Neuritis /Vestibular Neuronitis and Labyrinthitis .............................. 325

15.4.6 Vestibular Migraine ................................................................................................. 326

15.4.7 Tinnitus .................................................................................................................... 326

15.4.8 Glomus tumours ..................................................................................................... 326

15.4.9 Vestibular schwannomas ....................................................................................... 327

15.5 Nose/Paranasal Sinuses Conditions ....................................................................... 327

15.5.1 Acute Rhinitis .......................................................................................................... 327

15.5.2 Acute Non-Allergic Rhinitis ................................................................................... 327

15.5.3 Allergic Rhinitis ...................................................................................................... 328

15.6 Granulomatous diseases of the nose ...................................................................... 328

15.6.1 Rhinoscleroma ........................................................................................................ 328

15.6.2 Tuberculosis of the nose ....................................................................................... 329

15.6.3 Syphilis of the nose ................................................................................................ 329

15.6.4 Rhinosporiodiosis .................................................................................................. 329

15.6.5 Mucormycosis ........................................................................................................ 330

15.7 Other Conditions of the Nose ................................................................................... 330

15.7.1 Nasal septal abscess and Hematoma ................................................................... 330


xv
15.7.2 Choanal atresia ...................................................................................................... 331

15.7.3 Nasal Turbinate hypertrophy ................................................................................. 331

15.7.4 Nasal bone fracture ................................................................................................ 331

15.7.5 Nasal Septal deviation(non-traumatic) ................................................................. 331

15.7.6 Adenoid Hypertrophy ............................................................................................. 332

15.7.7 Acute Rhinosinusitis ............................................................................................ 332

15.7.8 Chronic Rhinosinusitis .......................................................................................... 334

15.7.9 Nasal polyposis ...................................................................................................... 334

15.7.10 Nose Bleeding (Epistaxis) .................................................................................... 335

15.7.11 Foreign Bodies in the Nose ................................................................................ 336

15.8 Throat Conditions ...................................................................................................... 336

15.8.1 Pharyngotonsilitis ................................................................................................... 336

15.8.2 Laryngitis ................................................................................................................. 337

15.8.3 Acute Laryngitis ...................................................................................................... 337

15.8.4 Chronic Laryngitis .................................................................................................. 338

15.8.5 Acute Epiglottitis (AE) ............................................................................................ 338

15.8.6 Non-infectious Chronic Laryngitis ........................................................................ 338

15.8.7 Recurrent Respiratory Papillomatosis (Laryngeal Papillomas) ......................... 339

15.8.8 Foreign Bodies in the Throat ................................................................................ 339

15.8.9 Subglottic hemangioma ......................................................................................... 340

15.8.9 Laryngomalacia ...................................................................................................... 340

15.8.10 Vocal cords paralysis ........................................................................................... 341

15.8.11 Infection of Thyroglossal duct cyst, dermoid cyst, branchial cleft cysts ....... 341

15.8.12 Deep neck spaces infections ............................................................................... 342

15.8.13 Peritonsillar Abscess (Quincy) ............................................................................ 342

15.9 ENT Neoplasms ......................................................................................................... 343

15.9.1 Juvenile nasopharyngeal angiofibromas (JNA) .................................................. 343

15.9.2 Salivary Gland Tumors ........................................................................................... 343

xvi
15.9.3 Parapharyngeal tumours ....................................................................................... 344

15.9.4 Cancer of the Larynx .............................................................................................. 344

15.9.5 Sino-Nasal Malignancy ........................................................................................... 344

15.9.6 Naso-Pharyngeal Malignancy ................................................................................ 345

15.9.7 Oropharyngeal Malignancy .................................................................................... 346

15.9.8 Hypo-Pharyngeal Malignancy ................................................................................ 346

15.9.9 Metastatic Lymphadenopathy &Neck Masses ..................................................... 347

15.10 Speech Disorders ................................................................................................... 347

16.1 Periodontal Conditions ............................................................................................. 348

16.1.1 Gingivitis ................................................................................................................. 348

16.1.2 Periodontitis ............................................................................................................ 348

16.1.3 Acute Necrotizing Ulcerative Gingivitis (ANUG) .................................................. 349

16.1.4 Stomatitis ................................................................................................................ 349

16.2 Dental Caries .............................................................................................................. 349

16.3 Odontogenic and Non-Odontogenic Orofacial Infections ..................................... 350

16.3.1 Periapical abscess ................................................................................................. 350

16.3.2 Dental Abscess (Odontogenic Abscess) .............................................................. 351

16.3.3 Ludwig’s Angina ..................................................................................................... 352

16.3.4 Pericoronitis ............................................................................................................ 352

16.3.5 Osteomyelitis of the jaw ......................................................................................... 353

16.4 Fungal Infections ...................................................................................................... 353

16.4.1 Oral Candidiasis ..................................................................................................... 353

16.5 Viral Infections ........................................................................................................... 354

16.5.1 Herpes Simplex Virus ............................................................................................. 354

16.6 Aphthous Ulceration ................................................................................................. 355

16.7 Post Extraction Complications ................................................................................. 355

16.7.1 Bleeding socket ...................................................................................................... 355

16.7.2 Infected Socket ....................................................................................................... 356

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16.7.3 Dry Socket ............................................................................................................... 356

16.7.4 Oro-Antral communication .................................................................................... 357

16.8 Tooth Sensitivities ..................................................................................................... 357

16.9 Tooth Eruption, Shedding and Edentulousness .................................................... 357

16.9.1 Eruption of Teeth .................................................................................................... 357

16.9.2 Shedding of Deciduous Teeth ............................................................................... 358

16.9.3 Edentulousness ...................................................................................................... 358

16.10 Malocclusions .......................................................................................................... 359

16.11 Management of Maxillofacial Trauma .................................................................... 359

16.11.1 Traumatic Dental Injuries ..................................................................................... 359

16.11.2 Facial Bones Injuries ............................................................................................ 360

16.12 Tumours and Tumour-Like Conditions of Oral Cavity and Facial Region ......... 362

16.12.1 Benign Odontogenic Tumors .............................................................................. 362

16.12.2 Non Odontogenic Benign Tumours .................................................................... 363

16.12.3 Benign Soft Tissues Non-Odontogenic Tumours ............................................. 364

16.12.4 Malignant Soft and Bone Tumours ..................................................................... 364

16.12.5 Odontogenic and Non- Odontogenic Cysts ...................................................... 365

16:13 Management of Oral Conditions during Pregnancy ............................................. 367

16.14 Temporal Mandibular Disorder and Chronic Orofacial Pain ............................... 367

16.14.1 Chronic Orofacial Pain other than Temporomandibular disorders ................. 367

16.14.2 Temporomandibular Disorders (TMDs) .............................................................. 368

16.14.3 Osteoarthritis and Rheumatoid arthritis of TMJ ................................................ 369

CHAPTER SEVENTEEN ................................................................................................... 370

MUSCULOSKELETAL DISORDERS ............................................................................... 370

17.1 Infections .................................................................................................................... 370

17.1.1 Osteomyelitis ........................................................................................................ 370

17.1.2 Septic arthritis ....................................................................................................... 371

17.1.3 Gonococcal arthritis .............................................................................................. 371

xviii
17.1.4 Post Open reduction and internal fixation or arthroplasty infection ................ 371

17.1.5 Tropical Pyomyositis ............................................................................................ 372

17.1.6 Necrotizing fasciitis ............................................................................................... 373

17.2 Inflammatory Conditions .......................................................................................... 374

17.2.1 Rheumatoid Arthritis .............................................................................................. 374

17.2.2 Juvenile Idiopathic Arthritis ................................................................................. 376

17.2.3. Gout ........................................................................................................................ 377

17.2.4 Osteoarthritis .......................................................................................................... 378

17.2.5 Heterotopic Ossification ........................................................................................ 380

17.2.6 Tendinopathies ....................................................................................................... 380

17.2.7 Plantar Fasciitis ...................................................................................................... 381

17.3 Metabolic Bone Diseases ........................................................................................ 382

17.3.1 Osteoporosis and Brittle Bone Diseases ............................................................. 382

17.3.2 Hypocholecalciferolemia (Vitamin D Deficiency) ............................................... 383

17.4.1 Diabetic Foot Ulcers .............................................................................................. 384

17.5 Affection of the Brain and Spine ..............................................................................385

17.51 Low Back Pain.......................................................................................................385

17.5.2 Cervical Degenerative Disorders ......................................................................... 388

17.5.3 Pyogenic spondylodiscitis .................................................................................... 390

17.5.4 Tuberculous spondylodiscitis .............................................................................. 391

17.5.5 Osteoporotic vertebral compression fractures (VCFs) ...................................... 392

17.6 Common Congenital Anomalies of Musculoskeletal System .............................. 394

17.6.1 Talipes equinovarus (congenital clubfoot) .......................................................... 394

17.8 Angular Deformity of Limbs ..................................................................................... 395

17.8.1 Rickets ..................................................................................................................... 395

17.8.2 Physiological Bowing/Knocked Knees ................................................................. 396

CHAPTER NINETEEN ........................................................................................................ 397

19.1 Diabetes Mellitus ....................................................................................................... 397

xix
19.2 Management of Diabetes During Religious Fasting ............................................... 403

19.3 Hyperglycaemia in Pregnancy .................................................................................. 404

19.4 Diabetes and HIV ....................................................................................................... 405

19.5 Diabetes and Tuberculosis ....................................................................................... 406

19.6 Hypoglycaemia .......................................................................................................... 406

19.7 Diabetic Ketoacidosis and Hyperosmolar Hyperglycemic States ........................ 407

19..8 Diabetes and Cardiovascular Diseases .................................................................. 410

19.9 Diabetic Peripheral Neuropathy ............................................................................... 411

19.10 Diabetic Nephropathy .............................................................................................. 412

19.11 Diabetic Retinopathy ............................................................................................... 413

19.12 Thyroid Disorders .................................................................................................... 414

19.12.1 Hypothyroidism .................................................................................................... 414

19.12.2 Hyperthyroidism ................................................................................................... 415

19.12.3 Toxic Multinodular Goitre or Thyroid Antibody Positive .................................. 415

19.12.4 Grave’s Hyperthyroidism ..................................................................................... 416

19.12.5 Thyroid Storm (Crisis) .......................................................................................... 417

19.13 Cushing's Syndrome ............................................................................................... 434

19.14 Prolactinoma ............................................................................................................ 435

19.15 Diabetic Insipidus (DI) ............................................................................................. 435

19.16 Pheochromocytoma ................................................................................................ 436

19.17 Disorder of Sexual Development (DSD) ................................................................ 436

19.8 Obesity in Adults ....................................................................................................... 437

19.19 Physical Activity ...................................................................................................... 439

CHAPTER TWENTY ........................................................................................................... 441

CARDIOVASCULAR DISEASE CONDITIONS .................................................................. 441

20.1 Prevention of Atherosclerotic Ischaemic Heart Disease and Stroke .................... 441

20.2 Management of Dyslipidemias ................................................................................. 442

20.3 Chronic Stable Coronary Artery Disease (CSCAD) / ISCHAEMIC Heart Disease
(IHD) .................................................................................................................................... 443
xx
20.4 Acute Coronary Syndrome .................................................................................... 444

20.4.1 Unstable Angina (UA) ............................................................................................. 444

20.4.2 Non-ST Elevation Myocardial Infarction (NSTEMI) .............................................. 444

20.4.3 ST Elevation Myocardial Infarction (STEMI) ......................................................... 445

20.5 Hypertension .............................................................................................................. 447

20.6 Resistant (Refractory) Hypertension ..................................................................... 454

20.7 Hypertensive Urgency ............................................................................................... 454

20.8 Hypertensive Emergency .......................................................................................... 454

20.9 Heart Failure ............................................................................................................... 454

20.10 Chronic Heart Failure ............................................................................................ 456

20.11 Pulmonary Oedema ................................................................................................. 457

20.12 Infective Endocarditis (IE) ....................................................................................... 458

20.13 Acute Rheumatic Fever ........................................................................................... 460

20.14 Pulmonary Embolism .............................................................................................. 462

20.14.1 Acute Pulmonary Embolism .............................................................................. 462

20.14.2 Chronic Pulmonary Embolism ............................................................................ 463

20.15 Cardiac Arrhythmias/ Dysrhythmias .................................................................... 464

20.15.1 Tachyarrythmias ................................................................................................... 464

20.15.2 AV Junctional Re-Entry Tachycardias .............................................................. 465

20.15.3 Wide QRS (Ventricular) Tachyarrhythmias (VTs) ............................................ 466

20.16 Heart Block (Second & Third Degree) .................................................................. 467

20.17 Sinus Bradycardia & Sinus Arrest ......................................................................... 468

KIDNEY AND UROLOGICAL DISORDERS ....................................................................... 469

21.1 Chronic Kidney Diseases (CKD) .............................................................................. 469

21.1.1 Diabetic Kidney Disease ......................................................................................... 470

21.1.2 Hypertension and CKD ........................................................................................... 471

21.1.3 Dialysis .................................................................................................................... 473

21.1.4 CKD Associated Metabolic Acidosis .................................................................... 473

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21.1.5 Hyperkalaemia ....................................................................................................... 473

21.1.7 Mineral Bone Disease (MBD) ................................................................................. 475

21.1.8 Haemodialysis (HD) Catheter Related Blood Stream Infection .......................... 475

21.2 Acute Kidney Disease ............................................................................................... 476

21.3 Glomerular Diseases (GD) ........................................................................................ 477

21.3.1 Glomerular disease - Nephritic syndrome ........................................................... 478

21.3.2 Nephrotic syndrome ............................................................................................... 478

21.4 Kidney Transplantation ............................................................................................. 481

21.4.1 Transplant Donor Evaluation ............................................................................... 481

21.4.2 Transplant Candidate ............................................................................................ 483

21.4.3 Transplant Recipient .............................................................................................. 483

21.4.5 Acute Kidney Graft Rejection ............................................................................... 486

21.4. 6 Other Conditions in Transplantation and their Managements .......................... 487

21.5 Cystic Kidney Disease .............................................................................................. 488

21.6 Renal artery stenosis ................................................................................................ 488

21.8 Reflux nephropathy ................................................................................................... 489

21.9 Contrast Induced Nephropathy (CIN) ...................................................................... 490

21.10 Urinary Tract Infection (UTI) ................................................................................... 491

21.10 Urology Disorders ................................................................................................... 493

21.10.1 Prostatitis .............................................................................................................. 493

21.10.2 Benign prostatic hyperplasia (BPH) .................................................................. 493

21.10.3 Prostate cancer .................................................................................................... 494

21.10.4 Urolithiasis ............................................................................................................ 495

21.10.5 Obstructive uropathy ........................................................................................... 496

21.11 Sexual Dysfunction ................................................................................................. 497

21.11.1 Female Sexual Dysfunction ................................................................................. 497

21.11.2 Male sexual dysfunction ...................................................................................... 498

CHAPTER TWENTY-TWO .................................................................................................. 499

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MALIGNANT DISEASE CONDITIONS ............................................................................... 499

22.1 Cancer Prevention, Screening and Early Detection ............................................... 499

22.2 Gynecological Malignancies ..................................................................................... 500

22.2.1 Cancer of the Uterine Cervix ................................................................................. 500

22.2.2 Endometrial Cancer ................................................................................................ 501

22.2.3 Cancer of the Vulva ................................................................................................ 502

22.2.4. Gestational trophoblastic disease .................................................................... 503

22.2.5 Cancer of the Ovary ................................................................................................ 505

22.3 Breast Cancer ............................................................................................................ 506

22.4 Cancer of The Skin .................................................................................................... 508

22.4.1 Non-melanoma Skin Cancers ................................................................................ 508

22.4.2 Malignant Melanoma .............................................................................................. 509

22.4.3 Kaposi’s sarcoma (KS) ........................................................................................... 509

22.5 Head and Neck Cancers ............................................................................................ 510

22.5.1 Nasopharyngeal Cancer ......................................................................................... 510

22.5.2 Laryngeal Cancer .................................................................................................... 511

22.5.3 Hypopharyngeal Cancers: ..................................................................................... 511

22.5.4 Salivary gland cancer ............................................................................................. 512

22.5.5 Nasal Cavity and Paranasal Sinus Cancer ........................................................... 512

22.5.6 Oral Cavity Cancer .................................................................................................. 512

22.5.7 Oropharyngeal Cancer ........................................................................................... 513

22.5.8 Thyroid Carcinoma ................................................................................................. 514

22.6 Gastrointestinal Malignancies .................................................................................. 515

22.6.1 Esophageal Cancer ................................................................................................ 515

22.6.2 Gastric Cancer ........................................................................................................ 515

22.6.3 Hepatocellular Carcinoma ..................................................................................... 516

22.6.4 Rectal Cancer .......................................................................................................... 518

22.6.5 Colon Cancer .......................................................................................................... 519

xxiii
22.6.6 Anal Cancer ............................................................................................................. 519

22.7 Lung Cancer ............................................................................................................... 520

22.7.1 Non-small cell lung Cancer .................................................................................... 520

22.7.2 Small cell lung cancer ............................................................................................ 521

22.8 Genitourinary Malignancies ...................................................................................... 521

22.8.1 Carcinoma of the Prostate ..................................................................................... 521

22.8.2 Urinary Bladder Cancer .......................................................................................... 523

22.9 Haematological Malignancies ................................................................................... 524

22.9.1 Lymphomas ............................................................................................................. 524

22.9.2 Leukemia ................................................................................................................. 526

22.9.3 Multiple myeloma .................................................................................................... 528

22.10 Central Nervous System Maligancies .................................................................... 529

22.10.1 Meningiomas ......................................................................................................... 529

22.10.2 Pituitary tumors .................................................................................................... 530

22.10.3 Gliomas .................................................................................................................. 531

22.11 Oncological Emergencies ....................................................................................... 533

22.11.1 Superior vena cava syndrome (SVCS) ............................................................... 533

22.11.2 Hypercalcaemia .................................................................................................... 534

22.11.3 Spinal–cord Compression ................................................................................... 534

22.11.4 Tumor lysis Syndrome ......................................................................................... 535

20.11.5 Febrile Neutropenia .............................................................................................. 535

CHAPTER TWENTY-THREE .............................................................................................. 537

MENTAL HEALTH CONDITIONS ....................................................................................... 537

23.1 Patients with Aggressive and Disruptive Behaviours ........................................... 537

23.2 Delirium ..................................................................................................................... 538

23.3 Dementia ................................................................................................................... 539

23.4 Schizophrenia ........................................................................................................... 539

23.5 Catatonia ................................................................................................................... 541

xxiv
23.6 Schizoaffective Disorder .......................................................................................... 541

23.7 Brief or Acute/Transient Psychotic Disorder ......................................................... 542

23.8 Bipolar Mood Disorders ........................................................................................... 542

23.9 Major Depressive Disorder ...................................................................................... 543

23.10 Suicide ..................................................................................................................... 544

23.11 Generalized Anxiety Disorder ................................................................................ 544

23.12 Panic Disorder ........................................................................................................ 545

23.13 Obsessive-Compulsive Disorder .......................................................................... 546

23.14 Acute Stress Disorder and Post-Traumatic Stress Disorder ............................ 547

23.15 Substance Related Disorder .................................................................................. 547

23.15.1 Substance Use Disorder ..................................................................................... 547

23.15.2 Substance Induced Disorder ............................................................................... 549

23.16 Psychiatric Disorders Associated with Epilepsy ................................................. 552

23.17 Psychiatric Disorders in Pregnancy ..................................................................... 554

23.17.1 Depression ............................................................................................................ 554

12.17.2 Panic disorder ....................................................................................................... 555

12.17.3 Obsessive-compulsive disorder ......................................................................... 555

12.17.5 Schizophrenia ....................................................................................................... 556

23.18. Autism Spectrum Disorder .................................................................................... 556

23.19 Attention Deficit / Hyperactivity Disorder (ADHD) ............................................... 557

23.20 Enuresis ................................................................................................................... 558

23.21 Neuroleptic Malignant Syndrome (NMS) .............................................................. 558

23.22 Somatic Symptom Disorder ................................................................................... 559

23.24 Conversion Disorder .............................................................................................. 559

CHAPTER TWENTY-FOUR ................................................................................................ 560

NUTRITION DISORDERS ................................................................................................... 560

24.1 Iodine Deficiency Disorders (IDD) ............................................................................ 560

24.2 Vitamin A Deficiency (VAD) ...................................................................................... 561

xxv
24.3 Vitamin B Deficiencies .............................................................................................. 562

24.3.1 Vitamin B1/Thiamine Deficiency (Wernicke Encephalopathy and Beriberi) ...... 562

24.3.3 Vitamin B6/Pyridoxine Deficiency.......................................................................... 562

24.3.4 Vitamin B12 (Cobalamin) Deficiency ...................................................................... 563

24.4 Malnutrition ................................................................................................................ 563

24.5 Growth Faltering/Failure to Thrive ........................................................................... 566

24.6 Obesity and Overweight ............................................................................................ 567

24.7 Nutritional Management in TB, HIV and AIDS ......................................................... 568

24.7.1 Nutrient Requirements and Dietary Management in TB, HIV and AIDS Patients
............................................................................................................................................. 569

24.8 Dumping Syndrome. .................................................................................................. 569

24.9 Dietary Management in Diabetes Mellitus ............................................................... 570

24.10 Nutrition Care and Support in the Intensive Care ................................................ 571

CHAPTER TWENTY-FIVE .................................................................................................. 573

POISONING ........................................................................................................................ 573

25.1 Common poisons ...................................................................................................... 573

25.2 General principles of management of poisoning ................................................... 573

25.2.1 Management Protocol of a poison (specific and non-specific antidotes) ......... 575

25.2.2 Management of Ingested Poisons ......................................................................... 576

25.2.3 Food Poisoning ....................................................................................................... 577

25.2.4 Herbal Poisoning .................................................................................................... 578

25.2.5 Management of Skin contamination ..................................................................... 579

25.2.6 Management of Eye contamination ...................................................................... 579

25.2.7 Management of Inhaled Poisoning ....................................................................... 579

25.3 Specific poisons ........................................................................................................ 580

25.3.1 Corrosive Compounds Poisoning ......................................................................... 580

25.3.2 Petroleum Compounds Poisoning ........................................................................ 580

25.3.3 Organo-Phosphorus and Carbamate Compounds Poisoning ........................... 581

25.3.4 Paracetamol Poisoning .......................................................................................... 584


xxvi
25.3.5 Acetylsalicylic acid and other salicylates poisoning. ......................................... 585

25.3.6 Iron Poisoning ......................................................................................................... 585

25.3.7 Carbon-monoxide Poisoning ................................................................................. 586

25.3.8 Opioid Poisoning .................................................................................................... 586

25.3.9 Heavy Metal poisoning ........................................................................................... 587

25.4 Prevention of poisoning ............................................................................................ 589

25.5 Alcohol Intoxication .................................................................................................. 589

25.6 Bites and stings ......................................................................................................... 589

25.6.1 Management of Specific Bites/Stings ................................................................... 590

CONTRIBUTORS ................................................................................................................ 596

xxvii
ACRONYMS AND ABBREVIATIONS
3D-CRT Three-dimensional Conformal Radio-Therapy
ACS Acute Coronary Syndrome
ACS Acute Chest Syndrome
ACT Artemisinin Combination Therapy
ADA Adenosine Deaminase
ADH Anti-Diuretic Acid
aHUS atypical Hemolytic Uremic Syndrome
AIS Acute Ischaemic Stoke
ALU Artemether Lumefantrine
AMI Acute Myocardial Infarction
Allergies, Medications, Past medical history, Last meal and Events leading
AMPLE
to presentation
bhCG beta human Chorionic Gonadotropin
BMD Bone Mineral Density
BP Blood Pressure
BUN Blood Urea Nitrogen
C/T/L Cervical, Thoracic, Lumbar
cyclophosphamide, doxorubicin hydrochloride (Adriamycin), and
CAF
fluorouracil
CAH Congenital Adrenal Hyperplasia
CAP Community Acquired Pneumonia
CAVE Cavus, Adductus, Varus, Equinus
CEF Cyclophosphamide Epirubicin Fluorouracil
CKD Chronic Kidney Disease
CPP Cerebral perfusion pressure
CRP C Reactive Protein
CVA Cerebral Vascular Accident
CVD Cardiovascular Disease
CVP Central Venous Pressure
DIND Delayed Ischaemic Neurologic Deficit
DKA Diabetic Keto Acidosis
DME Diabetic Macular Edema
DNS Dextrose Normal Saline
DR-TB Drug Resistance Tuberculosis
DSD Disorder of Sexual Development
DSM-5 Diagnostic and Statistical Manual of Mental Disorders vol.5
DST Drug Susceptibility Test
DTLC District Tuberculosis and Leprosy Coordinator
DWMR Diffusion Weighted Magnetic Resonance
xxviii

ECT Electroconvulsive Therapy
EITB Enzyme-linked Immune Transfer Blot
EMD Emergence Medical Department
ENL Erythema Nodosum Leprosum
ERCP Endoscopic Retrograde Cholangiopancreatography
ESA Erythropoietin Stimulating Agent
ESR Erythrocyte Sedimentation Rate
EVD External Ventricular Drainage
FAO Foot Abduction Orthosis
FAST Focus Assessment with Sonography for Trauma
FAST Facial drooping, Arm weakness, Speech difficulties and Time
FEIBA Factor Eight By-passing Agent
FIGO The International Federation of Gynecology and Obstetrics
FNA Fine Needle Aspiration
G6PD Glucose 6 Phosphatase Dehydrogenase
GB Gall Bladder
GCS Glasco comma scale
GUS Genital Ulcer Syndrome
HBA Haemoglobin Adult
HBS Sickle Haemoglobin
HD: Hemo-Dialysis
HDN Haemolytic Disease of New Bone
HDU High Dependency Unit
HEENT Head, Eye, Ear, Nose and Throat
HHS: Hyperglycemic Hyperosmolar Syndrome
HRCT High Resolution Computer Tomograph
HVL HIV Viral Load
IBD Inflammatory Bowel Syndrome
ICH Intra Cerebral Haemorrhage
ICP Intracranial Pressure
ILAE International League Against Epilepsy
IMCI Integrated Management of Childhood Illness
IOP Intraocular Pressure
IPTP intermittent preventive treatment in pregnancy
IRIS Immune Reconstitution Syndrome
ITI Immune Tolerance Induction
ITP Idiopathic Thrombocytopenia Purpura
JIA Juvenile Idiopathic Arthritis
LAMM Labyrinthine Aplasia, Microtia And Microdontia
LAP Lower Abdominal Syndrome

xxix

LFT Liver Function Test
LKW Last Known Well
LLINs Long Lasting Insecticide Nets
LLQ Left Lower Quadrant
LMWH Low Molecular Weight Heparin
LPR Laryngopharyngeal Reflux
MAP Mean Arterial Pressure
MDMA 3,4-MethyleneDioxy-MethAmphetamine
MDR-TB Multi-Drug Resistance Tuberculosis
mRDT malaria Rapid Diagnostics Test
MSM Men who have Sex with Men
MTD Maximum Tolerated Dose
mTOR mammalian Target Of Rapamycin
MUAC Mid-Upper Arm Circumference
NGT Naso Gastric Tube
NIV Non-Invasive Ventilation
ODS Osmotic Demyelination Syndrome
OI Opportunistic Infection
OPG Orthopantomography
OT Occupational Therapy
PAD Peripheral Artery Disease
PCV Pneumococcal Conjugate Vaccine
PDMPs Plasma-derived medicinal products
PEFR Peak Expiratory Flow Rate
PEP Post Exposure Prophylaxis
PI Protease Inhibitor
PID Pelvic Inflammatory Disease
pMDI Pressurised Metered Dose Inhaler
PPS Parapharyngeal Space
PPSV Pneumococcal Polysaccharide Vaccine
PrEP Pre-Exposure Prophylaxis
PSA Prostate Specific Antigen
PT Physio Therapy
PUVA Psoralens + Ultraviolet radiation
RAM Resistance Associated Mutation
RBG Random Blood Glucose
RICE Rest, Ice, Compression, And Elevation
RR Rifampicin Resistance
RRT Renal Replacement Therapy
RTLC Regional Tuberculosis and Leprosy Coordinator

xxx

rtPA recombinant tissue Plasminogen Activator
SAH Subarachnoid Haemorrhage
SBCC Social Behavioural Change
SLE Systemic Lupus Erythematosus
SMBG Self-Monitoring Blood Glucose
SMFE Systemic Marrow Fat Embolism
SpO2 Oxygen Saturation
SSRI Selective Serotonin Reuptake Inhibitor
SSS Scrotal Swelling Syndrome
TBI Traumatic Brain Injury
TFT Thyroid Fuction Test
TIA Transient Ischaemic Attack
TIVA Total Intravenous Anaesthesia
TM Tympanic Membrane
TMD Temporomandibular Disorders
TMJ Temporomandibular Joint
TMP Tympanic Membrane Perforation
TNM Tumor Nodes and Metastases
TPT Tuberculosis Preventive Therapy
TURP Transurethral Resection of the Prostate
UDS Urethral Discharge Syndrome
UDS Urine Drug Screen
VAP Ventilator-Associated Pneumonia
VDS Vaginal Discharge Syndrome
VTE Venous Thrombo-Embolism
VWF Von Willebrand Factor
WfH Weight for Height
WFNS World Federation Neurological Surgeon
WHZ Weight for Height Z score
WPW Wolff-Parkinson-White Syndrome

xxxi

PART I
THE NATIONAL ESSENTIAL MEDICINES LIST (NEMLIT)
Background Information

The National Essential Medicines List (NEMLIT) presents essential medicines, for which health
facilities at all levels requisite for management of priority diseases. The NEMLIT is based on the
concept of essential medicines, defined by the World Health Organization (WHO) as those
medicines that meet priority healthcare needs of the population and intended to be available within
the context of functioning health systems at all times, with assured quality and at a price the
individual and the community can afford. The concept emphasizes carefully and systematically
selection of essential medicines using an evidence-based process with due consideration of clear
evidence of safety and efficacy and comparative cost effectiveness. The rationale for selecting a
limited number of essential medicines is to enhance supply, improve rational use, and lower costs.

Categorization of antibiotics
A new categorization of antibiotics into Access, Watch, Reserve (AWaRe) classification has been
introduced to guide their prudent use and reduce antimicrobial resistance.

Access Group Antibiotics


This group includes antibiotics that have activity against a wide range of commonly encountered
susceptible pathogens while also showing lower resistance potential than antibiotics in the other
groups. Access group antibiotics are recommended as essential first or second choice empiric
treatment options for infectious syndromes. They are essential antibiotics that should be widely
available, affordable and quality assured.

Watch Group Antibiotics


This group includes antibiotic classes that have higher resistance potential. These medicines should
be prioritized as key targets of stewardship programs and monitoring. The selected Watch group
antibiotics are recommended as essential first or second choice empiric treatment options for a
limited number of specific infectious syndromes.

Reserve Group Antibiotics


This group includes antibiotics that should be reserved for treatment of confirmed or suspected
infections due to multi-drug-resistant organisms. Reserve group antibiotics should be treated as “last
resort” options. While they must be accessible when required, their use should be limited to highly
specific patients and clinical settings, when other antibiotic alternatives have failed or are not
suitable. They should be protected and prioritized as key targets of national and international AMR
stewardship programmes, involving monitoring and utilization reporting, to preserve their
effectiveness.

Prescribing of Medicines with Regard to Level of Service Provision and Professional


Expertise
Similar to previous editions, the NEMLIT will be used with regard to levels of care. Additionally, a
new categorization of prescribing medicines with regards to expertise has been introduced to
facilitate reimbursement of medicines by the NHIF. In summary, stocking and prescribing of
medicines as per level of care will be: tertiary hospitals (A, B, C, D & S); Regional Referral Hospitals
(A, B, C & D); District Hospitals (A, B & C); Health Centers (A & B) and dispensaries (A). Additional
category reflects professional expertise; regardless of level of care: Specialists (A, B, C, D & S);
Medical Officers (A, B, C & D); Assistant Medical Officer (A, B & C); Clinical Officers (A & B) and
Assistant Clinical Officers (A).

1

Table 1: Restrictions for Prescribing Medicines Listed in the NEMLIT

Level of Medicines with Regard to Level of Medicines with Regard to Professional


Service Provision Expertise
Tertiary Hospital A,B,C,D,S Specialist A,B,C,D,S
Regional Referral Hospital A,B,C,D Medical Officer (MO) A,B,C,D
District Hospital A,B,C Assistant Medical Officer A,B,C
(AMO)
Health Centre A&B Clinical Officer (CO) A&B
Dispensary A Assistant Clinical Officer (ACO) A

Hence, at tertiary level hospitals (S); the National, Zonal Referral and Specialized hospitals, all
medicines in the NEMLIT may be stocked; as per hospital needs and specialists may prescribe all
medicines listed in the NEMLIT. However, level (S) medicines are restricted to other experts.
Implying that, a Medical Officers at tertiary hospital will be prescribe medicines listed A, B, C and D
and Assistant Medical Officer A, B, & C but not S.
At Regional Referral Hospitals (RRH) level, medicines listed as (A, B, C & D) will be stocked.
Specialists at that level may prescribe medicines at level (A, B, C, D, S) as per their specialty areas
e.g. cardiologist may prescribe cardiovascular diseases medicines at that level. Medical officer at
RRH will prescribe medicines at level (A, B, C, D). If there is an Assistant Medical Officer at RRH
allowed to prescribe medicines listed (A, B, C) and Clinical Officers (A & B).

At District hospitals level, medicines listed as (A, B & C) will be stocked. Specialists prescribe
medicines listed (A, B, C, D, S) as above. Medical Officers will prescribe medicines listed (A, B, C,
D) and AMO (A, B, C). If their Clinical Officers (CO) at that level will be permitted to prescribe
medicines listed A & B only. Health Centers stock medicines listed as A & B and dispensaries A, but
if there is AMO, MO or specialist will prescribe as above.

Note
• Different from previous editions, the arrangement of STG/NEMLIT have changed; the
NEMLIT starts followed by chapters of STG to make easy reference of essential medicines
by users.
• All medicines indicated for treatment of various diseases in the STG are listed in the
NEMLIT.
• Some medicines are listed in some levels for the treatment of specific disease condition
e.g. cefixime is level (D) but, may be prescribed in lower HFs for treatment of STI only.
• Medicines in the NEMLIT are grouped according to pharmacological groups and written
alphabetically, in generic names, with their dosage forms and strengths.
• All health facilities in the public sector will adhere to the NEMLIT in procurement of
medicines from MSD and other sources.
• The NHIF will adhere to the NEMLIT for reimbursement of medicines in both public and
private health facilities.
• Special arrangement to quantify and procure medicines, which are not managed at specific
health facilities but are needed due to presence of expertise as stated above; for that case
the Hospital Pharmacists in collaboration with the Office of Chief Pharmacist shall facilitate
the process.

Further recommendations, advices and clarifications of the use of this document are much welcome;
please, you may communicate with the office of the Director Pharmaceutical Services - Ministry of
Health, Community Development, Gender, Elderly and Children. We believe that all medicines
stocked in our health facilities are of assured quality. However, for recommendations and advices
concerning all aspects of the quality of medicines and any adverse reaction please contact the
Tanzania Medicines and Medical Devices Authority at www.tmda.go.tz .

2
The National Essential Medicines List, 2021 Edition
Name of drug Dosage forms and Strengths Level

1.0 Anasthetics, Preoperative Medicines and Medical Gases

1.1 General Anaesthetics and Oxygen

1.1.1 Inhalational Medicines

Halothane Liquid for inhalation, bottle B


250mL
Isoflurane Liquid for inhalation, 250MmL B

Nitrous oxide Cylinder (F gas) for inhalation C

Oxygen Cylinder (medical gas) for inhalation B

Sevoflurane Inhalation S

1.1.2 Injectable Medicines and Other Pre-Medication

Atropine Injection 1mg (as sulfate in 1mL ampoule) A

Calcium chloride Injection 10mcg/mL D

Clonidine Injection 500mcg/mL S

Dexmedetomidine Injection 100mcg/mL S

Ephedrine injection Injection 30mg/mL B

Flumazenil Injection 0.2mg (IV) A

Etomidate Injection 20mg/mL S

Glycopyrrolate Injection 200mcg/mL in 1mL, 600mcg in 3mL S

Ketamine Injection (hydrochloride), 10mg/mL in 20mL B

Labetalol Injection 10mg/mL C

Lipid emulsion Solution 20% S

Metaraminol Injection 1mg/mL S

Midazolam Injection 1mg/mL, 5mg/mL D

Noradrenaline Injection 2mg/mL S

Ondansetron Injection 2mg/mL S

Phenylephrine Injection 10mg/mL S

Propofol Injection 10mg/mL, 20mg/mL D

Sodium citrate Solution 0.3 moles D

Thiopental Injection (sodium salt), in 20mL C

3
1.2 Local Anaesthetics
Bupivacaine Injection 0.5% (hydrochloride) in 7.5% C
dextrose spinal
Bupivacaine Injection 2.5mg/mL, 5mg/mL, 7.5mg/mL C

Lidocaine Injection hydrochloride 1% & 2%; A

Lidocaine Gel 2% & 5%; Spray 10% B

Lidocaine in Dextrose Injection (hydrochloride), 5% in 7.5% dextrose B

Lidoocaine + epinephrine Injection (hydrochloride) 2% with adrenaline A


(adrenaline) 1:100,000 in 2mL ampoule for dental use

1.3 Muscle Relaxants and Cholinesterase Inhibitors


Atracurium Injection 50mg/5mL S

Baclofen Tablet 10mg S

Neostigmine Injection (hydrochloride or hydrogen B


tartarate),1mg/mL in 1mL ampoule, Injection
(hydrochloride or hydrogen tartarate),
2.5mg/mL in 1mL ampoule

Pancuronium Injection (bromide) 4mg/mL in 2mL ampoule C

Rocuronium Injection 50mg/5mL S

Sugammadex Injection: 100mg/mL S

Suxamethonium Powder for injection (bromide or chloride) C


50mg/mL in 2mL vial

Tizanidine Tablet/Capsule: 2mg; 4mg S

2.0 Medicines for Pain and Palliative Care


2.1 Non-opioids and Non-steroidal Anti-inflammatory Medicines (NSAIMs)
Acetylsalicylic acid Tablet 300mg A

Dexketoprofen Tablet 25mg S

Diclofenac Injection 25mg/mL; Recto caps 100mg A


(slow release); Gel.
Diclofenac Tablet (sodium/potassium salt) 50mg, 100mg; C

Ketoprofen Tablet/Capsule: 50mg, 75mg, 200mg; Gel S


2.5% w/w
Ibuprofen Tablet 200mg; 400mg ; Syrup 100mg/5ml A

Mefenamic Acid Tablet 500mg B

Meloxicam Tablet 7.5mg; 15mg D

Paracetamol Tablet 500mg; Syrup 125mg/5mL, A


suppositories 125mg
10 mg/mL Solution for Infusion D

4
Piroxicam Tablet 20mg A

Sulfasalazine Tablets 500mg D

2.2 Opioid Analgesics/Antagonists


Fentanyl Injection 100mcg/2mL; Patches S

Methadone Tablet: 5mg; 10mg (as hydrochloride); Oral C


liquid: 5mg/5mL; 10mg/5mL (as
hydrochloride); Concentrate for oral liquid:
5mg/mL; 10mg/mL (as hydrochloride)

Morphine Tablet 10mg (morphine hydrochloride or C


morphine sulfate); Granules (slow-release: to
mix with water) 20mg-200mg (morphine
sulfate); Oral liquid: (10mg morphine
hydrochloride or morphine sulfate)/5mL;
Injection: 10mg (morphine hydrochloride or
morphine sulfate) in 1mL ampoule

Naloxone Injection (hydrochloride) 0.4mg/mL in 1mL B


ampoule
Pethidine Injection (hydrochloride) 50mg/mL in 1mL and B
2mL ampoule

Tramadol Tablet 50mg; Injection 50mg/mL in 2mL B

2.3 Medicines for Other Common Symptoms in Palliative Care

Amitriptyline Tablet 25mg A

Haloperidol Injection: 5mg/1mL ampoule; Tablet 5mg B

Hydrocortisone Powder for injection (as sodium succinate) A


100mg in vial
Hyoscine butyl bromide Tablet 10mg A

Hyoscine butyl bromide Injection: 20mg/mL B

Loperamide Tablet 2mg B


Imipramine Tablet 25mg C

3.0 Anti-allergies and Medicines Used in Anaphylaxis

Betahistine Tablet as dihydrochloride 16 mg C

Bethametasone Injection: 4mg/mL D

Cetirizine Oral solution 5mg/5mL; Tablet (hydrochloride) A


10mg
Chlorpheniramine Injection (maleate 10mg/mL in 1mL ampoule); A
Elixir (maleate) 2mg/5mL; Tablet (maleate)
4mg

Desloratadine Tablet: 5 mg film-coated S

5
Dexamethasone Injection: 4mg/mL in 1mL ampoule (as B
disodium phosphate salt);

Epinephrine (Adrenaline) Injection: 1mg (as hydrochloride or hydrogen A


tartrate) in 1mL ampoule

Loratadine C
Syrup 5mg/5mL; Tablet 10mg
Promethazine Injection (hydrochloride) 25mg/mL in 2mL; A
Syrup 5mg/5mL; Tablet (hydrochloride) 25mg

4.0 Antidotes and Other Substances Used in Poisonings

4.1 Antidotes (Non-specific)

Charcoal, activated A
Tablet or Powder, 50g
Magnesium sulfate C
Powder salt, 5g
4.2 Antidotes (Specific)

Acetylcysteine Injection: 200mg/mL in 10mL ampoules C

Atropine Injection 1mg (as sulfate in 1mL ampoule) A

Calcium gluconate A
Injection 100mg/mL in 10mL
Deferoxamine Injection 500mg (mesylate)in vial D

D-penicillamine Tablet 250mg D

Dimercaprol Injectable 50mg/mL in 2mL ampoule D

Ethylenediaminetetra-acetic acid Injection 200mg/mL in 5mL D


(EDTA)
Flumazenil D
Injection:100mcg/mL in 5mL
Pralidoxime S
Injection 600mg
Sodium bicarbonate 8.4% C
Injection 10mLs
Sugammadex Injection 100mg/mL S

Succimer Capsule 100mg (2,3-Dimercaptosuccinic acid) D

5.0 Anticonvulsants and Antiepileptics

Carbamazepine Syrup 100mg/5mL; Tablet 100mg; 200mg A

Clonazepam Tablet 0.5mg, 2mg D

Diazepam Tablet 5mg C

Injection 5mg/mL in ampoule 2mL A

Lamotrigine Tablet 100mg, 200mg S

6
Levetiracetam Injection 5mg/mL, 10mg/mL, 15mg/mL, S
100mg/mL, Tablet 250mg, 500mg, 750mg,
1000mg
Lorazepam Injection: 2mg/mL in ampoule; 4mg/mL in C
ampoule, Tablet 1mg/2mg

Magnesium sulfate A
Injection 50mg/mL in 10mL vial
Phenobarbital Injection (as sodium salt), A
100mg in 2mL ampoule;
Tablet (as sodium) 30mg, 100mg A

Phenytoin Suspension (as sodium salt) 30mg/5mL; C


Tablet/Capsule (as sodium salt) 50mg, 100mg,
Injection 100mg/2mL
Pregabalin Tablet/Capsule 75mg, 100mg; 150mg D

Sodium Valproate Tablet 200mg, 500mg C

6.0 Anti-Infective Medicines

6.1 Antihelminthics

6.1.1.Intestinal anthelminthics
Albendazole Suspension 100mg/5mL in 30mL bottle; A
Tablet 200mg, 400mg, chewable

Mebendazole Suspension 100mg/5mL in 30mL bottle; Tablet A


100mg, chewable

6.1.2 Antifilariasis

Ivermectin A
Tablet 3mg, 6mg
6.1.3 Anti-schistosomiasis and Other Anti-trematode Medicines

Praziquantel A
Tablet 600mg
Albendazole Tablet 200mg, 400mg A

6.2 Antibacterial
6.2.1 Access Group Antibiotics
Ampicillin Powder for injection (as sodium salt) 250mg, A
500mg in vial
Ampicilin + cloxacillin B
Capsule 250/250mg, injection
Amoxicillin Capsule (as trihydrate) 250mg; Dispersible A
tablet 250mg, 125mg

Amoxicillin + Clavulanic acid Powder for suspension (as trihydrate) 125mg+ B


31.25mg (as potassium salt) in 5mL AND
250mg amoxicillin + 62.5mg clavulanic
acid/5mL; Tablet (as trihydrate) 500mg +
125mg clavulanic acid (as potassium salt)

Amoxicillin + Clavulanic acid Powder for injection 500mg (as sodium), + C


100mg (as potassium salt) in vial

7
Benzathine benzyl penicillin Powder for injection 1.44g (2,400,000 IU) in A
vial
Benzyl Penicillin Powder for injection (as sodium or potassium A
salt) 3g (5,000,000 IU) in vial

Cephalexin Capsule 250mg (as monohydrate); Powder for B


reconstitution 125/5mi; 250mg/mL

Cloxacillin Powder for injection (as sodium salt) 250mg, B


500mg in vial

Doxycycline Capsule (as hydrochloride), 100mg A

Erythromycin Powder for suspension (as ethylsuccinate), A


125mg/5mL in 100mL bottle; Tablet (as
stearate or ethyl succinate), 250mg, film
coated
Flucloxacillin + Amoxicillin Tablet 500mg (as combination) ; C

Flucloxacillin Injection (sodium) 250mg; 125mg/5mL Oral C


solution
Metronidazole Suspension as (benzoate) 200mg/5mL in A
100mL; Tablet 200mg
Injection (I.V) 5mg/mL in 100mL bottle; B

Nitrofurantoin Tablet 100mg A

Phenoxymethylpenicillin Powder for suspension 125mg/5mL; (as A


potassium salt), Tablet 250mg

Tetracycline Capsule 250mg S

Oxytetracycline Eye ointment 1% (hydrochloride) A

6.2.2 Watch Group Antibiotics

Ampicillin + Sulbactum Powder for injection (ampicillin 1g/sulbactam C


0.5g), (ampicillin 2g/sulbactam 1g), (ampicillin
10g/sulbactam 5g)
Azithromycin Capsule/Tablet (as dihydrate) 250mg, 500mg; B ( level A for
Oral liquid 200mg/5mL STI only)

Clarithromycin C
Tablet 250mg, 500mg
Chloramphenicol Oily injection 0.5g (as sodium succinate)/mL B (Reserved for
in 2mL ampoule; Powder for injection (as meningitis)
sodium succinate) 1g, 125mg/5mL injection
(as Phosphate), 150mg/mL in 2mL ampule
Ceftriaxone Injection 250mg, 500mg, 1g in vial B ( level A for
STI only)
Ceftriaxone+sulbactam D
Injection 1.5g vial
Ciprofloxacin Tablet (as hydrochloride) 250mg, 500mg A

Ciprofloxacin Solution for IV infusion 2mg/mL in 100mL C

8
Gentamicin Injection (as sulfate) 40mg/mL in 2mL A
ampoule, 20mg/mL in 2 mL ampoule

Piperacillin + tazobactam Powder for injection 2g (as sodium salt) + S


250mg (as sodium salt); 4g (as sodium salt) +
500mg (as sodium salt) in vial

Sulfamethoxazole + triemethoprim Suspension (Sulphamethoxazole 200 mg/5mL A


+ trimethoprim 40mg/5mL in 100mL bottle;
Tablet 480mg; Sulphamethoxazole
400mg/trimethoprim 80mg
Ceftazidime Powder for injection (as pentahydrate) 250mg D
in vial
Cefixime Capsule 200mg/ 400mg S (A for STI
and Typhoid)
Cefuroxime D
Powder for Injection 250mg, 750mg, 1.5g (as
sodium salt) in vial
D
Oral suspension 125mg/5mL, 250mg/5mL;
Tablet 250mg, 500mg; injection
6.2.3 Reserve Group Antibiotics

Amikacin Injection 250mg/mL (as sulfate) S

Cefepime Injection 1000mg S

Clindamycin Capsule 150mg (as hydrochloride); S

Injection (as phosphate) 150mg/mL in 2mL S


ampule
Colistin Powder for Injection 1MIU per vial S

Dapsone Tablet 100mg S

Meropenem Injection 500mg, 1000mg S

Vancomycin Capsule: 125mg; 250mg (as hydrochloride) S

Powder for injection 250mg (as hydrochloride) S


in vial
6.2.3 Antileprosy Medicines
Clofazimine Capsule: 50mg; 100mg A

Dapsone Dapsone Tablet 50mg, 100mg A

Rifampicin Tablet 25mg; 50mg; 100mg A

6.2.4 Antituberculosis Medicines


Ethambutol Tablet (as hydrochloride) 400mg A

Ethambutol+Isoniazide Tablet 400mg + 100mg A

Ethionamide Tablet 125mg, 250mg S

9
Isoniazid Tablet 100mg A

Pyrazinamide Tablet 500mg A

Rifampicin+Isoniazid Capsule/Tablet,150mg+75mg, 50mg+150mg A

Rifampicin+Isoniazid+Pyrazinamid Tablet 150mg + 75mg + 400mg + 275mg A


e+Ethambutol

6.2.5 Reserved Second-line for Treatment of Multidrug Resistance


Tuberculosis (MDR-TB)
Cycloserine Tablet 250mg S

Bedaquiline Tablet 100mg S

Capromycine Powder for injection 1g (as sulfate) in a vial S

Delamanide Tablet 50mg S

Kanamycin Powder for injection: 1g (as S


sulfate) in vial
Levofloxacin Tablet 250mg S

Linezolid Injection for intravenous administration: S


2mg/mL in 300mL bag; Tablet 400mg; 600mg

Moxifloxacin Tablet 400mg S

p-Amino salicylic acid (PAS) Granules 4g in a sachet; Tablet 500mg S

6.3 Antifungal Medicines


Amphotericin B Amphotericin B Powder for injection 50mg in S
vial
Clotrimazole Clotrimazole Vaginal cream (nitrate) 1%, A
10%; Clotrimazole Pessaries 100mg; 500mg ;
Topical cream/Ointment
Fluconazole IV infusion 2mg/mL in vial C

Tablet/Capsule 150mg, 200mg A

Flucytosine Isotonic infusion solution containing flucytosine S


(1%)and 0.805% sodium chloride
Tablet 250mg, 500mg S

Griseofulvin Tablet 500mg A

Itraconazole Capsule 100mg D

Miconazole Miconazole Oral gel 2%; Vaginal Pessaries, C


Topical cream/ointment
Nystatin Suspension oral 100,000 IU/mL A

Terbinafine Tablet 250mg ; Topical cream C

6.4 Antiviral Medicines


6.4.1 Antiherpes Medicines

10
Acyclovir Cream 5%; Tablet 200mg, 400mg, B

Injection 500mg/Vial D

Valganciclovir Tablet 450mg S

6.4.2 Antiretrovirals (ARVs)

6.4.2.1 Nucleoside/Nucleotide Reverse Transcriptase Inhibitors

Abacavir (ABC) Tablet: 300mg (as sulfate) A

Lamivudine (3TC) Oral Liquid 50mg/mL; Tablet: 150mg A

Tenofovir disoproxil Tablet: 300mg A


fumarate (TDF)
Zidovuine (AZT) Capsule 250mg; Oral liquid 50mg/5mL A

6.4.2.2 Non-nucleoside Transcriptase Inhibitors

Efavirenz (EFV) Tablet: 200mg; 600mg A

Nevirapine (NVP) Oral liquid: 50mg/5mL; Tablet 50mg A


(dispersible); 200mg
6.4.2.3 Protease Inhibitors

Atazanavir Tablet 100mg; 300mg (as sulfate) C

Atazanavir + Ritonavir Tablet: 300mg (as sulfate) + 100mg C

Lopinavir + Ritonavir (LPV/r) Capsule 40mg + 10mg; Oral liquid 400mg + C


100mg/5mL; Tablet 100mg + 25mg; 200mg +
50mg

Ritonavir Oral liquid 400mg/5mL; Tablet 25mg; 100mg C

Darunavir Tablet 75mg, 400mg, 600mg, 800mg S

6.4.2.4 Integrase Inhibitors

Raltegravir Tablet 25mg, 100mg, 400mg S

6.4.2.5 Fixed Dose Combinations

Abacavir/Lamivudine Dispersible Tablet 60/30mg; Dispersible tablet; A


120/60mg; Tablet 600/300mg Scored

Tenofovir /Emtricitabine Tablet 300/200mg A

Tenofovir/Emtricitabine/Efavirenz Tablet 300/200/600mg A

Tenofovir/Lamivudine/Efavirenz Tablet 300/300/600mg A

Tenofovir/Lamivudine/Dolutegravir Dispersible tablet 60/30mg; Tablet A


300/300/50mg
Zidovudine/Lamivudine Tablet 300/150mg A

11
Zidovudine/Lamivudine/Nevirapine Tablet 300/150/200mg A

6.4.2.6 Medicines for Prevention of Opportunistic Infections

Isoniazide Tablet 300mg A

Pyridoxine Tablet 25mg B

Sulphamethoxazole + trimetoprim Tablet 400mg + 80mg A

6.4.3 Antihepatitis Medicines

6.4.3.1 Medicines for Hepatitis-B

Entecavir Tablet 0.5mg S

Tenofovir disoproxil fumarate Tablet: 300mg A


(TDF)
6.4.3.2 Medicines for Hepatitis-C

Ledipasvir Tablet 90mg S

Ribavirin Tablet 600mg S

Sofosbuvir Tablet 400mg S

6.5 Antiprotozoal Medicines


6.5.1 Antiamoebic and Antigiardiasis Medicines
Metronidazole Suspension 200mg/5mL; Tablet 200mg A

Tinidazole B
Tablet 500mg
6.5.2 Anti-malarial Medicines

Artemether/Lumefantrine (ALU) A
Tablet 20mg/120mg
Artemether B
Injection 80mg/mL ampoules
Artesunate Injection: ampoule, containing 60mg A
anhydrous artesunic acid with separate
ampoule of 5% sodium bicarbonate solution

Dihydroartemisinin+Piperaquine Tablet 40mg+320mg, 20mg+160mg C


(DPQ)
Primaquine Tablet (as phosphates) 2.5mg, 7.5mg, 15mg A (restricted to
few HFs under
the project)
Sulfadiazine 500mg tablet D

Pyrimethamine 25mg tablet D

6.5.3 Malaria Prophylaxis

Sulfadoxine + Pyrimethamine Tablet 500mg + 25mg A

12
7.0 Antimigraine Medicines

7.1 Medicines for Treatment of Acute Attack


Acetylsalicylic acid Tablet 300mg A

Ibuprofen Tablet 200mg; 400mg A

Ergotamine tartarate Tablet 1mg, 2mg C

7.2 Medicines for Prophylaxis

Propranolol Tablet 40mg as hydrochloride) A

8. Antineoplastics, Immunosuppressives and Immunomodulators


5-fluorouracil Injection: 250mg; 500mg; 000mg; S

Abiraterone acetate Tablet 250mg S

Actinomycin D Powder for injection: 500 micrograms in vial S

Alfuzocin Tablet 10mg D

Allopurinol Tablet 100mg; 300mg B

Anastrazole Tablet 1mg S

Antithymocite globulin (ATG) Injection 25mg/mL in 5mL S


(rabbit/horse)
Azacitadine Injection 25mg/mL S (with control)

Azathioprine Tablet 50mg, 75mg, 100mg S

basiliximab Injection 20mg S

Bicalutamide Tablet 150mg, 50mg S

Bleomycin Powder for injection: 15 IU (as sulfate) in vial S

Bortezomib Injection 3.5mg/vial S

Capecitabine Tablet 500mg S

Carboplatin Injection 10mg/mL S

Chlorambucil Tablet 2mg S

Cisplatin Powder for injection 50 mg; 10mg in vial. S

Cyclophosphamide Injection S

Cyclosporine Injection: 50 mg/mL in 1-mL ampoule; S


Capsule: 25 mg; 50mg; 100mg
Dacarbazine Powder for injection: 100 mg in vial; 200mg/; S
500mg
Danazol Capsule 100mg S (hematology
special)
Docetaxel Concentrate for infusion 120mg; 80mg S

Doxorubicin Injection 10mg; 20mg, 50mg S

13
Dutasteride Tablet 0.5mg S

Etoposide Capsule: 100 mg; Injection 100 mg/mL; S


Injection 50mg/5mL
Everolimus Tablet 0.25, 0.5mg S

Febuxostat Tablet 40mg; 80mg S

Filgrastim Injection 5mcg S

Finasteride Tablet 5mg D

Folinic acid Tablet 15mg, injection 6mg S

Gemcitabine Injection 200mg; 500mg; 1000mg S

Goserelin Injection 3.6mg, 10.8mg S

Hydroxychloroquine Tablet 200mg S

Hydroxyurea Capsule 500mg S

Ifosfamide Injection 1g/20mL S

Imatinib Tablet 400mg S

Irinotecan Injection 180mg/mL S

Lenalidomide Tablet 25mg S

Leucovorin Injection 200 mg/mL S

Mesna Injection, 100mg/mL; Tablet 400mg S

Methotrexate Tablet 2.5mg; Injection 50 mg/5mL S

Mycophenolate Sodium Tablet 360mg S

Mycophenolate Mofetil Tablet 500mg S

Oxaliplatin Powder for injection 50mg; 100mg in vial; S

Paclitaxel Injection 260mg vial S

Rituximab Injection 375 mg S

Sirolimus Tablet 1mg, 2mg S

Tacrolimus Tablet 0.5mg; 1mg; 2mg Ointment 0.1% S

Tamsulosin Tablet 0.4mg D

Tamoxifen Tablet 20mg D

Temozolomide Tablet 200mg S

Thalidomide Tablet 200mg S

Trastuzumab Injection 440mg; 150mg; 600mg; 500mg S

Vinblastine Injection 10mg S

Vincristine Powder for injection: 2 mg; 5 mg (sulfate) in S


vial.
Zolendronic acid Injection 4mg; 5mg S

14
9.0 Hormones and Antihormones

9.1 Adrenal Hormones and Synthetic Substitutes

Betamethasone Injection 4mg/mL D

Dexamethasone Tablet 0.5mg; 4mg D

Injection (as sodium phosphate) 10mg/mL B

Powder for Solution for Injection/Infusion 100 A


Hydrocortisone
mg (as sodium succinate)
Methylprednisolone 1000 mg powder and solvent for solution for D
injection/infusion; Tablet 4mg; 8mg;
Metyrapone Tablet 250mg S

Prednisolone Tablet 5mg A

Triamcinolone Injection 40mg/mL; Cream 0.1% S

9.2 Oestrogens

Ethinyloestradiol Tablet 50mcg A

9.3 Ovulation Inducers

Clomiphene Tablet 50mg C

9.4 Progesterone

Dydrogestrone 10mg tablet S

Etonorgestrel Implant 68mg A

Levonorgestrel Tablet 0.03mg, 0.07mg, 0.75mg A

Implant 75mg A

Medroxyprogesterone Injection acetate (depot) 150mg A

Norethisterone Tablet 5mg C

9.5 Androgens

Testosterone Injection, 30 mg/1.5mL;100mg/mL; S


200mg/mL; Cream
9.6 Contraceptives

Ethinyloestradiol + Norgestrel Tablet 0.03mg + 0.3mg A

Ethinylestradiol Levonorgestrel Tablet 0.03mg + 0.15mg A

Ethinylestradiol Desogestrel Tablet 0.03mg + 0.15mg A

9.7 Thyroid, Parathyroid Hormones and Antagonists

Carbimazole Tablet 5mg C

Potassium Iodide Solution Iodine 2mg + Potassium Iodide 4mg/g in B


water (prepare from raw material)

15
Levothyroxine Tablet (sodium salt) 0.05g D

Iodized oil Capsule Iodized oil Capsule with nipple A


240mg/0.5mL and 480mg
iodine/mL
Iodized oil Injection C

Propylthiouracil Tablet 50mg D

10. Antiparkinsonism Medicines and Antiprolactenemia


Benzhexol Tablet (hydrochloride) 5mg B

Bromocriptine Tablet 2.5mg C


Cabergoline Tablet 0.5mg S

Levodopa/Carbidopa Tablet 100mg + 25mg D

Selegiline Tablet 5mg S

11. Medicines Affecting the Blood


11.1 Antianaemia Medicines
Erythropoietin 2000 unit/Ml; 4000 units/mL S

Ferrous 200mg ( sulfate or as fumarate) A

Ferrous salts Oral liquid: Equivalent to 25mg iron (as A


sulfate)/mL; Tablet: Equivalent to 60mg iron

Folic acid Folic acid Tablet 5mg A

Hydroxocobalamin (Vitamin B12) Injection 1mg/mL C

11.2 Medicines Affecting Coagulation


Desmopressin (Move to anti- Injection 4mcg/mL, Tablet 0.2mg S
diuretics)
Etamsylate Tablet 500mg C

Low molecular Weight heparin Injection 100mg/mL S

Phytomenadione (Vit K1) Injection 0.5 mg/mL, 2mg/mL in 2mL ampoule; B

Protamine sulfate Injection 10mg/mL in 5mL ampoule B

Rivaroxaban Tablet 15mg, 20mg S

Unfractionated Heparin Sodium Injection (sodium salt) 1,000 IU/mL in 5mL B (Under
ampoule specialist
supervision)
Tranexamic acid Injection 100mg/mL in 5mL ampoule; Syrup C
500mg/5mL in 300mL bottle; Tablet 500mg
Warfarin Tablet: 1mg; 2mg; 5mg (sodium salt) C

16
12.0 Blood Products of Human Origin and Plasma Substitute

12.1 Blood and Blood Components

Fresh frozen plasma (FFP) Fresh frozen plasma (FFP) Bags D

Platelets Platelets D

Red blood cells. Packed red blood cells. D

Whole blood Whole blood B

12.2 Plasma-Derived Medicines

12.2.1 Human Immunoglobulins

Anti-rabies immunoglobulin A

Anti-tetanus immunoglobulin A

Human Immunoglobulin G S

12.2.2 Blood Coagulation Factors

Eltrombopag Tablet 25mg S

Factor VIII concentrate Factor VIII concentrate 500IU S

Factor IX concentrate Factor IX concentrate500 IU S

12.3 Plasma Substitutes

Albumin Infusion 5%; 25% S

Polygeline Polygeline IV solution 3.5%, 500mL bottles S

13.0 Cardiovascular Medicines

13.1 Antianginal Medicines

Bisoprolol Tablet 5mg; 10mg S

Glyceryl trinitrate Spray 400 micrograms/metered dose, C


sublingual spray
Isosorbide Dinitrate Tablet 10mg, 20mg C

Labetalol Tablet 100mg, 200mg ; Injection 5mg/mL C

Nifedipine Slow-release Capsule/Tablet 10mg; 20mg B

Nitroglycerin Injection/Infusion 25mg/250mL; 50mg/250mL; S


100mg/250mL
Propranolol Tablet 40mg A

13.2 Antiarrhythmic Medicines

Adenosine Injection 3mg/mL in Saline S

Amiodarone Injection 30mg/mL in 10mL ampoule; Tablet S


100mg
Sotalol Tablet 80 mg, 120 mg, 160 mg, 240 mg; Oral S with control
solution 5mg/Ml; Injection 15mg/mL

17
Verapamil Injection 2.5mg/mL, 2mL ampoule; Tablet S
40mg 80mg

13.3 Antihypertensive Medicines

Amlodipine Tablet 5mg, 10mg C

Atenolol Tablet 50mg B

Candesartan Tablet 16mg; Tablet in fixed combination S

Captopril Tablet 12.5mg, 25mg B

Carvedilol Tablet 6.25, 12.5mg C

Clonidine Injection 500mcg/mL; Tablet 0.1 mg, 0.2 mg S


and 0.3 mg
Diltiazem Tablet 60mg D

Doxazosin Tablet 2mg, 4mg S

Enalapril Tablet 2.5mg, 5mg (as hydrogen maleate) C

Esmolol Injection 10g/mL S

Hydralazine Tablet 25mg B

20mg Powder for Injection/Infusion C

Irbesartan Tablet 150mg, 300mg; Tablet in fixed S


combination
Lisinopril Tablet 5mg, 10mg C

Losartan Tablet 50mg; Tablet in fixed combination C

Nimodipine Capsule 30mg S

Methyldopa Tablet 250mg A

Metolazone Tablet 5mg S

Metoprolol Tablet 50mg C

Injection 1mg/mL S

Telmisartan Tablet 40mg, 80mg; Tablet in fixed S


combination
13.4 Medicines Used in Heart Failure

Candesartan Tablet 8mg C

Dobutamine Injection 250mg/5mL S

Dopamine Injection 250mg S

Digoxin Injection 250mg/mL D

Tablet 0.25mg D

18
Ivabradine Tablet 5mg S

13.5 Diuretics

Furosemide Injection 10mg/mL; Tablet 40mg B

Eplerenone Tablet 25mg, 50mg S

Bendrofluazide Tablet 5mg A

Hydrochlorothiazide Tablet 25mg; 12.5mg D

Mannitol Injectable solution: 10%; 20% C

Spironolactone Tablet 12.5mg, 25mg C

Torsemide Tablet 2.5mg, 5mg; 10mg S

13.6 Antithrombotic Medicines

13.6.1 Anti- Platelet Medicines

Acetylsalicylic acid Tablet: 75mg, 100mg A

Clopidogrel Tablet: 75mg; 300mg D

Prasugrel Tablet 10mg S (with special


permission)
Ticagrelor Tablet 60mg, 90mg S (with special
permission)
13.6.2 Thrombolytics

Alteplase Powder for injection: 50mg vial S

Streptokinase Powder for injection: 1.5 million IU in vial. S

13.7 Lipid Lowering Medicines

Atorvastatin Tablet 10mg; 20mg; 40mg B

Fenofibrate Capsule 200mg D

Rosuvastatin Tablet: 10mg ; 20mg S

14.0 Dermatological Medicines

14.1 Antifungal Medicines

3% salicylic acid and 6% benzoic acid


Benzoic acid Compound (whitfied's) ointment A

Clotrimazole Cream 1% A

Miconazole Cream (nitrate) 2% C

Terbinafine Cream 1%, C

19
14.2 Anti-infective Medicines
Fusidic acid Cream 2% C

Gentian Violet 1%, aqueous solution A

Mupirocin Ointment 2% C

Potassium permanganate Potassium permanganate A


Solution 1:4000

Povidone iodine Solution 10% A

Silver Sulfadiazine 1% Cream A

14.3 Anti-nflammatory and Anti-pruritic Medicines

Betamethasone cream or ointment 0.1% ( as valerate) C

Calamine Lotion 15.0% w/v A

Clobetasol propionate Cream 0.05%; 0.1% D

Fludrocortisone Tablets 0.1 mg (as acetate) S

Hydrocortisone Hydrocortisone Cream 0.5% A

Mometasone furoate Ointment/Cream containing 0.1% contains S


mometasone furoate,
Triamcinolone Injection 40mg/mL as Acetonide S

14.4 Medicines Affecting Skin differentiation and Proliferation

All-trans-retinoic acid (ATRA) Tablet 10mg, 20mg, injection S

Benzoyl peroxide Gel 2.5%, 5% and 10% A

Coal tar Solution 5% (prepare from raw materials) C

Isotretinoin 0.05% cream, Capsule 10mg, S


20mg
Podophyllin Solution Solution 10-25% (prepare from raw materials) D

Salicylic acid Topical solution 5% (prepare from raw C


materials)
Silver nitrate pencil Silver nitrate pencil C

Tretinoin cream 2.5% cream S

14.5 Scabicides and Pediculicides

Benzyl benzoate Emulsion Emulsion: 25% A

Lindane Lotion 1% C

14.6 Sunscreen Protector

Sunscreen protecting factor (SPF Sun screen cream 30+ C


30+)

20
15.0 Gastro-Intestinal Medicines
15.1 Antiulcer Medicines

Antiacid Mixture Antiacid Mixture containing magnesium B


trisilicate + aluminium hydroxide and
Simethicone
Bismuth Subgallate Tablet 200mg D
Esomeprazole Tablet 20mg; 40mg S
Lansoprazole Tablet 30mg C
Magnesium trisilicate Tablet Tablet (250mg magnesium trisilicate + 120mg A
dried aluminium hydroxide)
Mesalazine Tablet 400mg, 500mg, 800mg S

Octreotide Injection 50mcg; 100mcg S (Special


permission)
Omeprazole Tablet 20mg A

Pantoprazole Tablet 40mg; Powder for injection 40mg C

Terlipressin 0.12mg/mL solution for S


injection (acetate)
15.2 Drugs affecting Intestinal Secretion and Antispasmodics

Cholestyramine Cholestyramine Powder 4g per S


Sachet
Hyoscine butylbromide Tablet Hyoscine butylbromide Tablet 10mg A

Hyoscine butylbromide Injection Hyoscine butylbromide Injection 20mg/mL; C


1mL ampoule

Inflixmab Injection 100mg S (Special


permit)
Mebeverine Tablet 135mg D

Pancreatic Supplement Enzyme S

Ursodeoxycholic acid Tablet/capsule 300mg S

15.3 Anti-emetics

Domperidone Tablet 10mg D

Doxylamine Tablet 25mg C

Metoclopramide Tablet 10mg; Injection 5mg/mL; Suspension C


5mg/5mL

Promethazine Tablet (hydrochloride/theoclate) 25mg; A


Injection (as hydrochloride) 25mg/mL; Elixir
5mg/5mL (as chloral hydrate)

Ondansetron Tablet 8mg, Injection 2mg/mL S

15.4 Cathartics

Bisacodyl Tablet 5mg A

Lactulose Solution 3.1 - 3.7g/5mL, 200mL bottle C

21
L-Ornithine L-Aspartate Granules; Injection S

15.5 Anti-Haemorrhoids

Local anaesthetic + astringent and Suppositories/ointment (zinc oxide 25mg B


anti-inflammatory + bismuth oxide+ bismuth subgallate
59 mg + balsam Peru)

15.6 Medicines Used in Diarrhoea

Loperamide Tablet/Capsule (hydrochloride) 2mg B

Oral Rehydration Salts (ORS) Low osmolality sachet to make 1 litre of A


solution containing Sodium chloride 2.6g,
Sodium citrate 2.9g, Potassium chloride
1.5g and Glucose 20.5g)

Zinc Tablet dispersible (equivalent to 20mg A


elemental zinc)

16.0 Insulin and Medicines Used for Diabetes and Related Disorders
Empagliflozin Tablet 10mg S (with special
permit)
Glibenclamide Tablet 5mg A

Gliclazide Tablet 40mg; 80mg; 30mg; 60mg A

Glimepiride Tablet 1mg; 2mg C

Glucagon Powder for reconstitution S


10mg/vial
Insulin Rapid acting; Injection: 40 IU/mL; 100
IU/Ml
Short acting; Injection: 40 IU/mL; 100 A
IU/mL
Intermediate acting; Injection: 40 IU/mL; A
100 IU/mL
Long acting; Injection: 40 IU/mL; 100 A
IU/mL
Pre-Mixed Insulin; Injection: 40 IU/mL; S
100 IU/Ml
Metformin Tablet 500mg; 750; 850MG; 1000MG; SR A

Pioglitazone 15mg D

Phenoxybenzamine Tablet 10 mg S

Sitagliptin Tablet 50mg; 100mg S

17.0 Immunologicals

17.1 Sera and Immunoglobulins

Anti D immunoglobulin Injection 150mg; 300mg C

Antirabies immune globulin Injection 400IU/mL; A


10,000IU/5mL

22
Anti-venom immunoglobulin Snake venom polyvalent Antiserum A
injection (|Central African type)

Diphtheria antitoxin Injection: 10,000 IU; 20,000 IU vial A

Tetanus Immunoglobulin Tetanus Immunoglobulin A


(human) – 250 IU/mL,250 IU/2.5mL

17.2 Vaccines

17.2.1 For Immunization

BCG Vaccine Injection 20 doses vial (Bacillus Calmette A


Guerin)

DPT-HepB-Hib Vaccine Diphtheria, Tetanus, Pertussis, Hepatitis A


B and Haemophilus Influenza vaccine in
vials of 10 doses

Hepatitis B Injection 10mcg/mL, 20mcg/mL, B


40mcg/Ml
Human Papilloma Vaccine (HPV) Human Papilloma Vaccine A
(HPV) – 0.5mL per dose
Inactivated Polio Vaccine (IPV) Inactivated Polio Vaccine (IPV) A

Measles-Rubella Vaccine Measles-Rubella Vaccine A


Injection 10 doses in vial
Oral Poliomyelitis Vaccine (OPV) Oral Poliomyelitis Vaccine (Live A
attenuated) Oral solution 20 doses in vial

Pneumococcal Conjugate Vaccine Pneumococcal Conjugate A


(PCV13) Vaccine (PCV13) -4 doses vial
Pneumococcal polysaccharide vaccine Vial S
(PPSV-23)
Rota Vaccine Rota Vaccine Oral solution A

Tetanus (toxoid) Vaccine Tetanus (toxoid) Vaccine A


Injection 20 doses in 10mL vial
17.2.2 For Specific Groups for Individuals

Human Diploid Cell Rabies Freeze Human Diploid Cell Rabies A


dried rabies vaccine Freeze dried rabies vaccine
Meningitis vaccine Injection C

Yellow Fever Vaccine 0.5mL dose C

18.0 Muscle Relaxants (Peripherally-Acting) and Cholinesterase Inhibitors


Neostigmine Injection: 500microgram in 1mL C
ampoule; 2.5 (metilsulfate) in 1mL
ampoule
Suxamethonium Injection: 50mg (chloride/mL in 2mL C
ampoule

23
19.0 Ophthamological Preparations

19.1 Anti-infective Agents


Acyclovir ointment Acyclovir Eye ointment 3% C

Ciprofloxacin Drops 0.3% C

Chloramphenicol Drops 0.5%, 1%; Eye ointment 1% A

Chlorhexidine Drops 0.2% S

Dexamethasone+Chloramphenicol Drops 0.1%, 0.5% C

Dexamethasone +Gentamicin Drops 0.1, 0.3% C

Econazole Drops 5% S

Natamycin Drops 5% S

Ofloxacin Drops 0.3% D

Oxytetracycline t Eye ointment 3% A

Iodine Eye drops, 2.5-5% A

19.2 Anti-allergy, Artificial Tears and Anti-inflammatory Agents


Dexamethasone eye drops Drops 0.1% D

Hydroxypropylmethylcellulose Drops 0.70% C

Methylprednisolone acetate Injection 40mg/mL D

Prednisolone eye drops Drops 0.5%, 1% D

Oxymetazoline Drops 0.025% C

Sodium cromoglycate drops Sodium cromoglycate 2%, 4% eye drops C

Triamcinolone Acetatonide Injection 40mg/mL S

19.3 Local and Topical Ocular Anaesthetic Agents


Amethocaine eye drops Drops 0.5%w/v or 1.0%w/v A

Tetracaine eye drops Drops .5%w/v C

19.4 Miotics and Antiglaucoma

Acetazolamide Tablet 250mg C

Acetylcholine Injection; vial contains 20 mg S


acetylcholine chloride and 56 mg
mannitol
Betaxolol Drops 0.25% -0.5% w/v D

Brimonidine Drops 0.15 – 0.2% w/v D

Dorzolamide Drops 20 mg/ml S

Latanoprost Drops 0.005% w/v D

Pilocarpine hydrochloride Drops 2 or 4% w/v C

Prostamide bimatroprost Drops 0.03% w/v D

Timolol Drops 0.25%, 0.5% w/v C

24
19.5 Mydriatics and Anti-vascular Endothelial

Atropine Drops 0.5%, 1% w/v; Ointment 1% B

Cyclopentolate Drops 0.5%, 1% w/v C

Tropicamide Drops 1% w/v S

Tropicamide with Cyclopentolate Drops 0.5%, 1% w/v C

Tropicamide with Phenylephrine Drops 0.8% / 5% w/v C

19.6 Other Ocular Preparations

5 –Fluoro Uracil 1% eye drops D

Ganciclovir Injection 2mg; ophthalmic gel, 0.15% S

Mitomycin C 5mg/vial, 10 mg/vial D

Silicon Oil 1000 CS, 1500 CS, 5000 CS S

20.0 Oxytocics and Antioxytocics

20.1 Oxytocics

Ergometrine Injection Injection (maleate) 0.5mg/mL (hydrogen C


maleate) in 1mL ampoule

Misoprostol Tablet 200mcg (rectal, A


sublingual)
Oxytocin Injection Injection 10 IU in 1mL ampoule A

20.2 Antioxytocics (tocolytics)

Dicyclomine Tablet 20mg; Injection B

Nifedipine Immediate – release capsule: 10mg, B


20mg
Salbutamol Tablet Tablet 4mg A

21.0 Dialysis Solution and Other Related Medicines

Iron Sucrose Injection 20mg/Ml D

Intraperitoneal dialysis solution Parenteral solution (of appropriate S


composition)

22.0 Psychotherapeutic and Related Medicines


22.1 Medicines used in Psychotic Disorders

Benzhexol Tablet 5mg C

Chlorpromazine Injection (hydrochloride) 25mg/mL in 2mL A


ampoule; Tablet (hydrochloride) 25mg,
100mg
Donepezil Tablet 5mg, 10mg S

Fluphenazine Injection 25mg/mL (decanoate) in 1mL C


ampoule
25
Haloperidol Injection 5mg/mL in 1mL ampoule; B
Tablet 1.5mg
Lorazepam Tablet 1mg, 2mg C

Olanzapine Tablet 5mg; 10mg S

Risperidone Tablet 1mg/2mg S

Zuclopenthixol Injection 50mg/mL (Acetate) S

22.2 Medicines Used in Mood Disorders

22.2.1 Medicines used in Depressive disorders

Amitriptyline Tablet (hydrochloride) 25mg A

Citalopram Tablet 20mg D

Fluoxetine Capsule 20mg S

Imipramine Tablet 25 mg C

Oxybutynin Tablet 5mg S

22.2.2 Medicines in Bipolar Disorders

Carbamazepine Tablet 100mg, 200mg A

Lamotrigine Tablet 100mg, 200mg S

Sodium Valproate Tablet 200mg, 500mg C

22.3 Medicines Used for anxiety Disorders

Diazepam Tablet 5mg C

22.4 Medicines Used for Disorders due to Psychoactive Substance use


Buprenorphine Sublingual Tablets2mg S

Methadone Oral liquid: 5mg/5mL; 10mg/5mL C

Naltrexone Tablet 50mg S

23.0 Medicines Acting on Respiratory Tract


23.1 Anti-asthmatics
Budesonide inhaler Inhalation 100mcg, 200mcg B

Fluticasone propionate Nasal Spray 50mcg D

Ipratropium Bromide Aerosol Inhalation (aerosol): 20 S


microgram/metered dose; Nebulizer 250-
500mcg
Montelucast Tablet 5mg; 10mg D

Salbutamol Tablet (as sulfate) 4mg; syrup (as A


sulfate) 2mg/5mL; Inhalation (as sulfate)
0.1mg per dose (aerosol inhaler)

Nebulizer solution 2.5mg/mL; 5mg/mL; B


Injection 0.5mg/mL; img/mL

26
Salfolinl Inhalation 100mcg, 200mcg C

Tiotropium Inhalation1.25mcg/actuation; S ( with special


2.5mcg/actuation permit)
23.2 Cough Preparations
Cough syrup Containing expectorants/Antitussive A
Lictus
24.0 Solutions, Correcting Water Electrolyte and Acid-Base Disturbances
Dextrose 5%; Dextrose 5%; 500mL, 1000mL A

Dextrose 10%; Dextrose 10%; 500mL C

Dextrose 25%, Dextrose 25%, 50mL, 100mL C

Dextrose 50%, Dextrose 50%; 50mL, 100mL C

Polystyrene sulfonate Solution containing calcium (or sodium) D

Sodium bicarbonate Injection 5%, C

Sodium lactate compound Sodium lactate compound (Ringer's A


solution) 500mL, 1000mL.
Sodium Chloride solution 0.9% Sodium Chloride 500mL, A
1000mL
Sodium Chloride solution 3% Sodium Chloride 500mL, C
1000mL
Sodium chloride+Dextrose Sodium chloride+Dextrose B
0.9%+5%; 500mL, 1000mL
Potassium chloride Solution Potassium chloride Solution C
7.4% 10mL Vial
Water for injection 5mL, 10mL vial A

25.0 Vitamins/Minerals

Ascorbic acid (Vitamin C) Tablet Ascorbic acid (Vitamin C) Tablet 100mg A


and 500mg
Calcium gluconate Injection 100mg/mL in 10mL ampoule A

Calcium Carbonate Tablet 500mg S

Calcium with vitamins C

Calcium with amino acids C

Ergocalciferol (vitamin D) Capsule 1.25mg (50, 000IU); Oral solution C


0.25mg/mL (10,000IU/mL)

Glucosamine +Chondrotin sulphate Tablet S

Iron with vitamins C

Iron with amino acid C

Nicotinamide (Vitamin B3) Tablet 50mg C

Potassium chloride Tablet (slow release) 600mg ; Injections C

27
Pyridoxine (Vitamin B6) Tablet (hydrochloride) 25mg B

Retinol (Vitamin A) Capsule Retinol (Vitamin A) Gelatin Capsule (with A


nipple to allow administration drop by
drop) 50,000IU, 100,000IU 200, 000IU
Sodium Hyaluronate 1% Injection. 1% S

Thiamine (Vitamin B1) Tablet (hydrochloride) 100mg C

Thiamine (Vitamin B1) Injection (hydrochloride) 1000mg/mL in C


1mL ampoule
Vitamin B complex Vitamin B complex Tablet BP (contains A
per Tablet: nicotinamide 15mg, iboflavin
1mg, thiamine 1mg)

Syrup (contains nicotinamide 15mg, A


riboflavin 1mg, thiamine 1mg/5mL)

Vitamin B complex Injection BP in 10mL vial (contains B


icotinamide 200mg, pantothenol 30mg,
pyridoxine 20mg, riboflavine 20mg,
thiamine 50mg per 1 mL)

Vitamin E Tablet/capsule alpha tocopherol acetate D


500 mg/5 mL

26.0 Medicines Used in Ear, Nose & Throat Diseases


26.1 Ear Drops
Betamethasone Ear drops; 0.1% w/v

Boric acid Ear drop; 3% A

Ciprofloxacin Ear drops; 0.3% C

Clotrimazole Ear drops; 1%

Chloramphenicol Ear drops; 5% w/v

Dexamethasone + Neomycin Ear drops: 0.1% + 0.5% C

Lidocaine + Beclometasone + Ear drop D


Clotrimazole + Chloramphenicol
26.2 Oral Antiseptics
Chlorhexidine gluconate Solution Chlorhexidine gluconate Solution B
0.1%;prepare from concentrated solution;
gel
Potassium permanganate Solution Potassium permanganate A
Solution 1:4000; prepare from
powder/crystals
26.3 Nasal Preparations

Ephedrine Nasal drops 0.5% and 1% B

Normal saline Nasal drop 0.9% A

Mometasone Nasal spray 50 micrograms/dose (as S


furoate)
Xylometazoline Nasal spray 0.05% S

28
27.0 Disinfectants and Antiseptics

Chlorhexidine + Cetrimide Solution concentrated containing A


chlorhexidine digluconate 1.5%+ 15%
cetrimide

Chloroxylenol Solution 4.9% BP A

Cresol saponated Solution 3% BP A

Formaldehyde Solution 36 - B
37% stabilized
Glutaraldehyde Activated solution 2% C

Hydrogen peroxide Solution 3% A


Hydrogen peroxide Solution 6% A
Methylated spirit Solution 70% A

Potassium permanganate Potassium permanganate A


Solution 1: 4000
Povidone-Iodine Solution 10% A

Sodium dichloroisocyanurate Tablet, 1.67g (equal to 1g available A


chlorine)
28.0 Miscellaneous

Sildenafil Tabet 50mg S

29
PART II
THE STANDARD TREATMENT GUIDELINE (STG)
Standard Treatment Guidelines provide standardized guidance to health professionals on diagnosis
and treatments. It provides invaluable assistance to practitioners especially those with lower skills or
new in the field. STG are systematically developed statements to assist practitioners/prescribers in
making decisions about appropriate treatment for specific clinical conditions. The statements contain
information on: clinical conditions, diagnosis criteria, non- pharmacological, medicines of choice (and
alternatives) for the medical condition, important prescribing information—dose, duration,
contraindications, side effects, warnings, medicine interactions and the referral criteria.

The STGs should be updated regularly to reflect changes in accepted treatment strategies. The
2021 edition of STG have been updated to reflect new therapeutic options and to include new
emerging diseases. In the development process, the use of evidence-based medicine was
overemphasized and each chapter was revised by a Lead Reviewer, an expert on the specific
disease condition. The STG has covered the priority disease conditions in the country arranged in
twenty-six chapters namely:

• Emergency and Critical Care • Skin Disease and Allergic Reactions


• Anaesthesia • Eye Disease Conditions
• Haematological Disease Conditions • Oral and Dental Conditions
• Notifiable Diseases • Ear, Nose and Throat Diseases
• Malaria • Musculoskeletal Disorders
• HIV/AIDS • Trauma and Injuries
• TB and Leprosy • Metabolic and Endocrine Disease Conditions
• Nervous Disease Conditions • Kidney and Urological Disorders
• Respiratory Disease Conditions • Malignant Disease Conditions
• Gastrointestinal Disease Conditions • Mental Health Conditions
• Obstetrics, Gynaecology and Contraception • Nutrition Disorders
• Sexually Transmitted Infections • Poisoning

Note
• All medicines indicated for treatment of various diseases in the STG are listed in the
NEMLIT.

• The referral criteria in the STG meant to refer the patient to the next level of care; with the
fact that expertise to manage a patient/diagnosis capacity may lack at that level.

30
CHAPTER ONE
APPROACH TO PATIENTS WITH EMERGENCY CONDITIONS
1.1 The Concept of Emergency Care and Resuscitation
Emergency care and Resuscitation involves rapid assessment and early intervention. Approach to
Emergency care and resuscitation needs to be systematic hence the use of the ABCs approach.
The ABCs approach provide the framework for evaluation and treatment of severely ill patients.

Primary survey
I. Airway
Assess the airway to establish patency of the airway. This includes:
• Looking for signs of airway obstruction (signs of trauma, swelling, secretions,
presence of foreign body).
• Listen for abnormal sounds like stridor, snoring.

If there are signs of airway obstruction intervene by positioning, opening and clearing the airway.
Perform chin lift or jaw thrust manoeuvre to open the airway (If suspecting cervical spine injury use
the jaw thrust manoeuvre). Use sunction to remove the secretions. Airway adjuncts like
oropharyngeal or nasopharyngeal airway can be used.

Note
• Remember to reassess the airway after performing interventions
• Some patient may require use of advance airway devices like endotracheal intubation or
surgical airway

II. Breathing
Upon completing airway assessment and intervention, assess for presence of breathing, signs
of respiratory distress such as tachypnea, hypoxia, cyanosis, apnoea and abnormal breath
sounds.Provide oxygen when oxygen saturation is below 92% or the patient is dyspnoeic.
Oxygen can be administered using the nasal prong, simple face mask, non-rebreather mask or
ambubag. Advance interventions include: mechanical ventilation.

III. Circulation
Check for pulse (central pulse) for not more than 10 seconds. If absent start CPR (Refer
cardiopulmonary resuscitation section below). Assess for signs of poor peripheral perfusion
(shock) such as cold extremities, prolonged capillary refill, dry mucous membrane and
hypotension. If there are signs of shock, establish two (2) IV large bore cannula and give IV
fluids (crystalloids) bolus (2lts in adults and 20mls/kg in pediatrics). Limit fluids to individuals
whom you suspect to have heart failure, renal failure or malnourished children.

IV. Disability
This involves rapid assessment of the neurological status. This includes assessment for the
level of consciousness (use of AVPU or Glascow coma scale), signs of convulsions, random
blood glucose level, examination of the pupils and presence of focal neurological
deficit.Interventions that can be performed during the disability assessment include: correction
of hypoglycemia, airway protection, stopping the convulsions by administering anticonvulsant

V. Exposure
This involves fully exposing the patient and rapid assessment of the body for signs of trauma,
rashes or infection.

Secondary survey
After assessment and stabilization of ABCs during the primary survey, focus is turned into
secondary survey. The secondary survey is a systematic assessment of the rest of the body to
identify injuries and illnesses. Common approaches include a head to toe or organ –system based
assessment. It is important to note that the secondary survey is performed after the primary
assessment and interventions. When performing a secondary survey, if the patient condition
changes then you must stop immediately and redo the primary survey and necessary interventions.

31
Note:
All patients with compromised airway, breathing, circulation or disability must be attended in the
resuscitation rooms. (Refer Triage overview section)

1.2 Cardiac Arrest and Cardiopulmonary Resuscitation


Cardiopulmonary resuscitation is an Emergency lifesaving procedure performed when there is
sudden cessation of heart beats. It involves the combination of chest compressions and artificial
ventilation to preserve blood flow to the organs including the brain function. Early initiation of CPR
can double or triple the chances of survival after cardiac arrest.

Note: HIGH QUALITY CPR


• Compressions:
• Infant: 2 finger compression (if alone) or thumb encircling technique (if you have
assistance)
• Child: 1 or 2 hand
• Adult: Two hands
• Compression rate: 100-120/min
• Compression depth: approximately 1/3 antero-posterior diameter of the chest
• Compression/ventilation ratio: 30:2 (adults and children), 30:2 (If alone) and 15:2 (If
you have assistance)
• Allow chest recoil
• Minimize interruptions
• Adequate ventilation

Clinical presentation
• Unresponsiveness (sudden loss of consciousness)
• Absence of central pulse (carotid pulse/femoral pulse or brachial pulse in infants)
• Loss of spontaneous respiration

Investigations
While continuing with CPR, point of care (POC) tests are conducted while looking for the reversible
causes of the cardiac arrest (Hypovolemia, hypoxia, hypo/hyperkalemia, acidosis, hypothermia,
hypoglycemia, tension pneumothorax, toxins, thrombi, cardiac tamponade). These includes:
• POC Blood gases
• POC Bicarbonates
• POC Electrolytes- Potassium, sodium, Calcium, Chloride,
• POC Creatinine, POC urea
• POC RBG
• Bedside ultrasound- looking for pneumothorax, cardiac tamponade or thrombi
• POC Toxicology screens (If available)
• POC ECG (if there is return of spontaneous circulation)
• POC lactate
• POC Troponin

Management
• HAZARDS- ensure safety and use of PPEs
• HELLO- Check for responsiveness, Carotid pulse (not more than 10 seconds) and
breathing
• CPR starts with early recognition (unresponsiveness, loss of spontaneous breathing and
absence of carotid pulse. In infant’s CPR is initiated when the heart rate is below 60
beats/min
• Call for HELP and immediately start chest compression. As more members arrives to help
assign different roles including airway and breathing management, time recording,
documentation, AED/monitor, medications
• Open the airway by performing chin lift or jaw thrust (if suspecting C spine injury). Use
airway adjuncts to open the airway.
• Give 2 breaths using bag valve mask connected to oxygen source and observe for chest
rise

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• Establish IV access for administration of fluids and medications, if failed perform
Intraosseous access
• After FIVE cycles of compressions/ventilation (2 minutes), check for pulse and use
AED/Defibrillator to analyze rhythm if there is a need to deliver shock
• If no need for shocking continue with CPR for another 2 minutes (FIVE cycles)
Pharmacological Treatment
A: adrenaline (IV) Adult: 1mg, Pediatrics0.01mg/kg (repeat every 3-5 minutes)
AND
A: 0.9% sodium chloride (IV):Adult 2000mls, pediatrics 20mls/kg; if suspecting
hypovolemia as a cause of the arrest
AND
A: dextrose 5% (IV) if needed to correct hypoglycemia
OR
C: dextrose 10%, 25% or 50% (IV) if needed to correct hypoglycemia
AND
C: sodium bicarbonate 1mmol/kg (IV) push (if needed to correct acidosis)

*Additional medications maybe required depending on cause of the cardiac arrest (the
reversible cause)
Disposition
Upon achieving return of spontaneous circulation (ROSC), definitive airway is achieved by
performing endotracheal intubation for mechanical ventilation and patient must be admitted to the
ICU or transferred to a facility with an ICU capacity.

1.3 Approach to Stridor


Stridor is an abnormal, high-pitched sound produced by turbulent airflow through a partially
obstructed airway. Stridor is a dangerous finding and may indicate imminent airway obstruction. It
can be inspiratory, expiratory or biphasic.

Clinical presentation:
• Hypoxia
• Respiratory distress
• Altered mental status
• Inability to speak
• Inability to swallow

Differential diagnoses
Infectious causes- croup, epiglottitis, peri-tonsillar abcess, retropharyngeal abcess
Non- infectious causes- Foreign body obstruction, burns, trauma, anaphylaxis, malignancy,
laryngotracheomalacia, stenosis

Investigations
Blood gases analysis, Lateral neck X ray (for foreign body, masses or soft tissue swelling), CXR
(foreign body, evidence of aspiration), CT- scan, Blood Sugar, Lactate, Electrolyte analysis and/or
Serum creatinine and urea

Non pharmacological
Keep the patient calm by allowing the patient to assume their most comfortable position. Give
oxygen if there are signs of increased work of breathing.

Pharmacological treatment
A: adrenaline (nebulization) 0.5mls/kg
AND
A: prednisolone (PO) 1-2mg/kg stat
OR
D: dexamethasone (PO) 0.6mg/kg stat

33
Note
Administer IV fluids (if signs of shock) – refer section on the management of shock

Referral: All patients with stridor whom the cause has not yet been established must be referred to
higher health facilities

1.4 Approach to Upper Gastrointestinal Bleeding


Upper GI bleeding is any GI bleeding originating proximal to the ligament of Treitz.

Clinical Presentation
Hematemesis and coffee-ground emesis suggest a UGI source. On physical examination, vital signs
may reveal obvious hypotension and tachycardia. Cool, clammy skin is an obvious sign of shock.
Abdominal examination may disclose tenderness, masses, ascites, or organomegaly. Perform rectal
examination to detect the presence of blood and its appearance, whether bright red, maroon, or
melanotic. Other findings include, the presence of spider angiomas, palmar erythema, jaundice, and
gynecomastia which may suggest liver disease while petechiae and purpura may suggest an
underlying coagulopathy.

Differential diagnosis
Peptic ulcer disease, upper GI malignancy, oesophageal or gastric varices, esophagitis, Mallory-
Weiss tear, Boerhaave syndrome and arteriovenous malformation

Investigations
ABO Grouping and cross-matching, Complete Blood Count, Hemoglobin Level, Blood Urea Nitrogen
and Creatinine, Electrolytes, (Sodium, Potassium, Calcium Chloride), PT, PTT, INR, Liver Function
Tests, Lactate levels, Obtain an ECG in patients with underlying coronary artery disease and/or
Bedside Ultrasound

Non Pharmacological treatment


Maintain ABCs, give oxygen if needed

Pharmacological Treatment
Give blood If severe pallor, ongoing bleeding, Hb < 5g/dl and Hb < 7g/dl (with active bleeding)
• Adults 2 units within 1hour and Paediatric 20ml/kg 1hour (whole blood) or 10ml/kg (pRBC)
• If ongoing indication for blood, start transfusion in the following ratio: 1unit pRBCs
(20ml/kg in Paediatric): 1unit FFP (20mls/kg in Paediatric): 1unit PLT (20ml/kg in
Paediatric)

Give
A: 0.9% sodium chloride (IV)
OR
A: compound sodium lactate (IV); Adult 2000mls and Paediatrics 20ml/kg
AND
C: pantoprazole (IV); Adult 80mg stat, then infusion 8mg/hour for 3days,
Paediatrics1mg/kg stat (max 80mg) then infusion 1mg/kg/hour for 3days
OR
S: esomeprazole (IV) 40mg 24hourly for 3days

For patients with suspected variceal bleeding give:


S: octreotide (IV) Adult 50mg slow bolus, then infusion 50mcg/hour for 5days;
Paediatrics1mcg/kg/hour (maximum 50mcg/hour) for 5days

If features suggestive of cirrhosis; give


C: ciprofloxacin (IV) 500mg 12hourly for 7days
OR
B: ceftriaxone (IV) 2g 24hourly for 7days

DEFINITIVE CARE: Early Endoscopy and Intensive care unit admission (Refer Gastrointestinal
disease chapter)

34
1.5 Approach to Seizure and Status Epilepticus
Status epilepticus is a single seizure ≥5 minutes in length or two or more seizures without recovery
of consciousness between seizures.Status epilepticus is a neurologic emergency, and treatment
should be initiated in all patients with continuous seizure activity lasting more than 5 minutes.

Clinical presentations
• Abrupt onset seizures
• Altered mental status
• Postictal drowsiness
• Tongue biting

Differential diagnoses
Epilepsy, meningitis, encephalitis, malaria, space occupying lesion, alcohol withdrawal, isoniazid
toxicity, intracranial hemorrhage, metabolic abnormalities- hyponatremia, eclampsia, acute
hydrocephalus.

Investigations:
Blood Glucose, Electrolytes: (Sodium, Potassium, Chloride, Magnesium and Calcium), ECG,
Bedside ultrasound, Blood gases, Malaria Test, Serum creatinine and urea, Lactate levels,
Pregnancy test (females), Toxicology screening and/orCT Head

Non-pharmacological management
• Protect patient from injury (If possible place in left lateral position to reduce aspiration
risks), Don’t place tongue depressor
• Perform both primary and secondary assessment and provide necessary interventions
• Give Oxygen if needed
• Do bedside random blood sugar test
• Establish IV access for administration of anticonvulsants, if unable use the rectal route
• Connect the patient to the cardiac monitor to obtain vital signs

Pharmacological management
I. Active seizure 0-5minutes
Supportive care:
IV access, monitors, maintain airway, oxygen therapy. Check point-of-care glucose and provide:
A: dextrose 5%(IV); if glucose is ≤ 3.5mmol/L
AND
A: diazepam (IV) 0.15-0.2mg/kg. Maximum 10mg (Rectal dose: 0.2-0.5mg/kg) repeat
every 5 minutes up to 3 doses
OR
D: midazolam (IV): 0.1mg/kg repeat every 5 minutes up to 3 doses
II. Established Status Epilepticus 5-10 min
B: phenobarbitone (IV): Adults 20mg/kg slowly (max 50mg/min); Paediatrics 20mg/kg
slowly (max 30mg/min)
OR
C: phenytoin (IV) Adults 20mg/kg slowly (max 50mg/min); Paediatrics 20mg/kg slowly
(max 30mg/min)

Consider INTUBATION if patient still seizing


C: thiopental (IV): Adult 3-6mg/kg loading dose then 25-100mg infusion as needed;
Paediatrics 2-5mg/kg loading dose
OR
D: propofol (IV): Adults 2mg/kg loading dose then 2-10mg/kg/hour; Paediatrics 3mg/kg
loading dose, then 7.5-18mg/kg/hr
OR
D: midazolam (IV): Adult 0.2mg/kg loading dose then 0.1-0.2mg/kg/hour; Paediatrics
0.1mg/kg then infusion 0.06 – 0.4mg/kg/hour
Disposition:Intensive care unit admission or refer to the higher health facility with ICU/HDU
capacity

35
1.6 Approach to Altered Mental Status
This is the acute alteration in brain function and may include alteration of arousal or awareness,
thought content, memory or attention.

Clinical presentation
Depending on the cause but may include: agitated, Restlessness, Hemiparesis, visual deficit,
dysphasia
Differential diagnosis
The mnemonic AEIOU TIPS is widely preferred in the emergency department when considering a
broader differential. Alcohol/acidosis, Epilepsy/Electrolytes, Insulin/Inborn Errors of Metabolism,
Oxygen/Overdose, Uremia, Trauma, Infection, Psychiatric/Poisoning, Stroke/Subarachnoid
Hemorrhage/Shock

Investigations
POC Glucose, Rapid Malaria test, Blood gases, Serum Electrolytes, POC ECG, Bedside ultrasound,
Serum Creatinine and Urea, Lactate, Complete Blood Count, Liver function tests, Head CT-scan,
Chest Xray and/orToxicology screening (If highly suspiciousness of intoxication)
Non pharmacological treatment:
• If aggressive/ restless consider restraining- mechanical or chemical (medications)
• Obtain set of vital signs including random blood glucose
• Perform both primary and secondary assessment and provide necessary interventions.
• Give Oxygen if Hypoxic or dyspnoeic
• Connect the patient to the cardiac monitor to obtain vital signs

Pharmacological treatment
A: diazepam (IV):Adult 5-10mg loading dose, maintenance 0.03-0.1mg/kg every 30
minutes to 6 hours; Paediatrics 0.1-0.15mg/kg stat, may repeat after 3-5 minutes
OR
B: haloperidol (IV): Adult 0.5-10mg *** (If concerned about psychiatric disorder)Child:
safety and effectiveness not established
OR
B: ketamine (IV) 1-2mg/kg and 2-4mg/kg for IM
OR
D: midazolam (IV): Adults 5mg stat, maintenance 20-100mcg/kg/hr. infusion; Paediatrics
0.05-0.1mg/kg stat

Note
Additional pharmacological treatment will depend on the cause of the altered mental status
Consult/refer to a higher center with a psychiatrist if concerned about psychiatric disorder

1.7 Approach to Difficult in Breathing


Shortness of breath or breathlessness may result from a range of pulmonary, cardiac and central
nervous system causes. It is important to look for the underlying cause for immediate intervention.

Clinical presentation
• Increased work of breathing
• Altered mental status
• Diaphoresis
• Additional souds- stridor, wheezes
Differential diagnosis
• Pulmonary embolism
• Pulmonary oedema
• Myocardial infarction
• Asthma
• Anaphylaxis
• Airway obstruction
• Tension pneumothorax

36
• Cardiac tamponade
• Acute chest syndrome
• Pneumonia
• Pericarditis

Investigations
Blood gases, Serum Electrolytes, Serum Creatinine and Urea, Troponins, Chest X-ray, POC ECG,
Bedside Ultrasound, Lactate, Troponin, Random blood glucose

Non pharmacological treatment


• Perform both primary survey (ABCs) and secondary survey and provide necessary
interventions
• Obtain Vital signs
• Position the patient
• Give Oxygen if hypoxic or increased work of breathing
Pharmacological treatment
Pharmacological management will depend on the underlying cause of difficulty in breathing. (Refer
Asthma-respiratory chapter and Acute chest syndrome and Pulmonary embolism-
hematology chapter)
1.8 Anaphylaxis
Anaphylaxis is a severe, life-threatening, generalised or systemic hypersensitivity reaction
characterised by rapidly developing life-threatening airway (pharyngeal or laryngeal edema) and/or
breathing (bronchospasm and tachypnea) and/or circulation (hypotension and tachycardia)
problems usually associated with skin and mucosal changes.

Clinical presentation
• Hives
• angioedema
• wheezes
• Difficult breathing
• Diarrhoea
• Hypotension

Anaphylaxis is a clinical diagnosis and should be suspected when:


• Acute onset involving skin, mucosal tissue with either respiratory compromization or blood
pressure reduction (or syncope)
• Hypotension after exposure to a known allergy for the patient (SBP <90mmHg or >30%
from baseline)
• Respiratory compromise (i.e dyspnoea, stridor, wheeze, hypoxemia)
• Exposure to a likely allergen causing involvement of the skin, mucosal, respiratory
compromization or blood pressure reduction

Investigations
Blood gases, Serum Electrolytes, POC ECG, Troponin, CXR and/or POC USS

Non pharmacological management


• Perform both primary and secondary assessment. If patient has signs of severe respiratory
distress perform early intubation/surgical airway
• Give oxygen if hypoxic (spO2 below 95%) or severe respiratory distress
• Insert TWO large bore IV cannulas or obtain intraoseous access
Pharmacological Management
A: adrenaline (IM): Adult 0.3-0.5mg (maximum 0.5mg) every 5-15min as soon as possible. If
inadequate response, start adrenaline (IV) 2-10mcg/min in 0.9% sodium chloride (IV) OR
Ringer lactate (IV) 1-2 litres. If hypotensive. Repeat IV fluids as needed; Paediatric 0.01mg/kg,
every 5-15min as soon as possible. If inadequate response, start adrenaline (IV) 0.05-
1mcg/kg/min in 0.9% sodium chloride (IV)ORcompound sodium lactate (IV) 20mls/kg if
hypotensive. Repeat IV fluids as needed

37
OR
A: hydrocortisone (IV)200mg stat
OR
B: salbutamol (nebulisation) 10mg and equal volume of water for injection (This is useful to
patients with refractory bronchospasm).
OR
D: methylprednisolone (IV) 1-2mg/kg/day

Disposition
All patient with severe and moderate symptoms which required repeated doses of adrenaline or
didn’t respond to treatment must be admitted or referred to higher health facility. Those with mild
response which responded to IM adrenaline may be discharged after 4 hours’ observation at the
health facility.

1.9 Cardiac Tamponade


Cardiac tamponade is the result of compression of the myocardium by fluid, gas, pus, blood, or a
combination of substances. It occurs in a physiologic continuum reflecting the amount of fluid, the
rate of accumulation, and the nature of the heart.

The result is increased pericardial pressure, which causes decreased ventricle compliance and
decreased flow of blood into the right ventricle which eventually leads to a decreased cardiac output.
Conditions that may predispose a patient to pericardial effusion and tamponade include; trauma,
radiation exposure, Tb pericarditis, renal failure (uremic pericarditis), autoimmune diseases, drugs
that induce a lupus-like syndrome, hypothyroidism, or ovarian hyperstimulation syndrome.

Clinical presentations
• Chest pain and dyspnea
• Pulsus paradoxus >10 mm Hg
• Beck’s triad includes low blood pressure, elevated jugular venous distention, and
decreased heart sounds.
• In the absence of hypotension and tension pneumothorax in a patient with PEA, consider
the diagnosis of cardiac tamponade.

Investigations
Bedside ultrasound, POC ECG, Blood gases, Serum Electrolytes, Troponins, Pericardial fluid
analysis- biochemistry, microbiology and cytology, Serum creatinine and urea and/or Chest Xray

Non pharmacological and pharmacological treatment


• Perform both primary and secondary assessment and provide appropriate interventions.
• Give oxygen if hypoxic or increased work of breathing
• Connect the patient to a cardiac monitor and obtain vital signs
• Pericardiocentesis is the definitive management

Pharmacological treatment
A: 0.9% sodium chloride (IV): Adults 1-2 lts, Paediatrics 20ml/kg) to increase right sided
filling pressure

Disposition
All patients with cardiac tamponade require inpatient management in an intensive care unit
setting/HDU.

1.10 Pulmonary Edema


Life threatening condition that occurs due to abnormal fluid build-up in the lungs leading to impaired
gaseous exchange, acute respiratory distress and may cause respiratory failure. Can be classified
as cardiogenic pulmonary edema; due to increased hydrostatic pulmonary pressure (HF) and Non
cardiogenic pulmonary edema; due to increased permeability (acute lung injury and allergic
alveolitis).

38
Note
Cardiogenic and non-cardiogenic pulmonary edema have no clear cut differences in clinical
presentation, however identifying the specific underlying cause of pulmonary edema is
significant for therapeutic and prognostic purposes.

Clinical presentation
Shortness of breath, use of accessory muscles, diaphoresis, tachypnoea and crepitations

Investigations
Chest X-ray, Blood gases, Serum Creatinine and Urea, POC ECG, POC troponin, Serum
electrolytes and/orBedside Ultrasound

Non Pharmacological management


• Perform both primary and secondary assessment and provide necessary interventions
• Give high flow oxygen therapy
• Put patient on cardiac monitor (if available) and obtain vital signs
• Position patient at 45° angle or sitting upright position
• Perform ECG (rule out ischemia, dysrhythmia)
• Perform bedside ECHO (to rule out cardiac causes- contractility, pericardial effusion)
• Perform chest ultrasound (comet tails and B lines)

Pharmacological management

Control hypertension (for SBP>90mmHg)


S: nitroglycerin (IV): Adult loading 100mcg/min titrate rapidly to 400mcg/min over 2
minutes

CAUTION!
Beware of preload sensitive condition example inferior or right ventricular myocardial infarction,
phosphodiesterase inhibitors use

Reduce intravascular volume if fluid overloaded


B: furosemide (IV/IM): 0.5-1mg/kg over 20minutes (maximum 120mg) or infusion IV 5-10mg/kg
(maximum 120mg)

CAUTION!
Beware of renal insufficiency and volume depleted patients, check size of IVC

Ventilation
Oxygen therapy (target saturation>95%); CPAP or BiPAP (for persistent respiratory distress,
hypoxia or acidosis despite high flow oxygen therapy); Intubation and mechanical ventilation (for
respiratory failure despite CPAP/BiPAP)

Disposition
Goal of treatment - Relieve hypoxemia (improve oxygenation); Reduction of pulmonary capillary
pressure and improve perfusion.Admit all patients with pulmonary edema to HDU/ICU or transfer the
patient to a health facility with ICU/HDU capacity

1.11 Approach to Shock


Shock is a state of acute circulatory failure leading to decreased organ perfusion, with inadequate
delivery of oxygenated blood to tissues and resultant end-organ dysfunction and it is an emergency
condition. Adherence to evidence-based care of the specific causes of shock can enhance a
patient’s chances of surviving.

Clinical presentation
• Low blood pressure (systolic BP below 80 mmHg) is the key sign of shock
• Weak and rapid pulse
• Rapid and shallow breathing
• Restlessness and altered mental state

39
• Weakness
• Low urine output

Table 1.1: Types of shock & Additional Symptoms

Type of Description Additional Initial Management


shock symptoms
Hypovolemic Most common Weak thread -Ensure patency of the airway
type of shock pulse, cold and - assess breathing and administer oxygen if
Primary cause is clammy skin. indicated
loss of fluid from -Place two large bore cannula and initiate 2lts of
circulation due to saline/crystalloids (20mls/kg in pediatrics).
haemorrhage, Reassess after giving fluids
burns, diarrhoea - Assess for mental status
etc. -blood products (RBC,plasma,platelets) 1:1:1 if no
improvent then refer
Cardiogenic Caused by the Distended neck -Ensure patency of the airway
shock failure of heart to veins, weak or - Assess breathing and administer oxygen if
pump effectively absent pulses indicated
e.g. in myocardial -Place two large bore cannula and AVOID giving
infarction, cardiac IV fluids, if needed give small volume (adult:
failure etc. systolic 250mls-500mls and pediatrics: 5mls/kg)
blood pressure - Assess for mental status
less than 80 or - Inotropes (Dobutamine 2-20mcg/kg/min or
90mmhg vasopressor (Dopamine 1-50mcg/kg/min)
- Give blood if needed
Septic shock Caused by an Elevated body -Ensure patency of the airway
overwhelming temperature - Assess breathing and administer oxygen if
infection, leading indicated
to vasodilatation. -Place two large bore cannula and initiate 2lts of
saline/crystalloids (20mls/kg in pediatrics)
- Assess for mental status
-Empirical antibiotic therapy within 1hr
Neurogenic Caused by trauma Warm and dry -Ensure patency of the airway
shock to the spinal cord, skin - Assess breathing and administer oxygen if
resulting in -hypotension indicated
sudden decrease -bradycardia -Place two large bore cannula and initiate 2lts of
in peripheral -hypothermia saline/crystalloids (20mls/kg in pediatrics)
vascular - Assess for mental status
resistance and - Inotropes (Dobutamine 2-20mcg/kg/min or
hypotension. vasopressor (Dopamine 1-50mcg/kg/min)
- Give blood if needed
Anaphylactic Caused by severe Bronchospasm, Refer anaphylaxis section
shock allergic reaction to angioedema
an allergen, or and/or Urticaria
drug.

Investigations
The following investigations can be performed depending on the type of shock
• Basic serum chemistry (including renal function)
• Liver function tests
• Blood culture
• POC Ultrasound- lungs, IVC, Cardiac
• Echocardiography
• CSF analysis if a patient is suspected with meningitis
• Troponins
• Blood gases
• Serum Electrolytes
• Lactate
• Hb Level

40
Non-pharmacological Treatment
Prompt diagnosis of underlying cause is essential to ensure optimal treatment.
• Perform ABCD approach. Intervene when needed
• Maintain open airway
• Administer oxygen with face mask and if needed after intubation with assisted
ventilation
• Check for and manage hypoglycemia

Pharmacological Treatment
Treatment depends on the type of shock. Intravenous fluid therapy is important in the treatment of
all types of shock except for cardiogenic shock.

A: 0.9% sodium chloride (IV): Adultgive 2 litres bolus infusion. Repeat bolus until blood
pressure is improved. Transfuse blood and plasma expanders in hemorrhagic shock.
Paediatrics give 20ml/kg as a slow infusion.

All children with shock which is not obviously due to trauma or simple watery diarrhea should receive
antibiotic cover for probable septicemia.

If the pressure doesn’t improve after two bolus of IV Fluids (4lts in adults and 40mls/kg in
pediatrics), administer Ionotropes/vasopressors (Refer Sepsis and septic shock topic section)

CAUTION!
• Do not administer calcium containing fluids, e.g. Ringer Lactate, within 48 hours of
administering ceftriaxone
• Do not administer IV fluids in case of cardiogenic shock but maintain IV line
• If patient develops respiratory distress, discontinue fluids but maintain IV line
• Ceftriaxone is contra-indicated in neonatal jaundice

Referral: Refer the patient urgently with the escort of a nurse to high level facility to establish
the cause and address all medication given in the referral letter.

1.12 Sepsis and Septic Shock


Septicaemia (Sepsis) is defined as life-threatening organ dysfunction caused by a dysregulated host
response to bacterial infection (commonly) and fungal or viral infections (leastly). Organ dysfunction
can be represented by an increase in the Sequential [Sepsis-related] Organ Failure Assessment
(SOFA) score of 2 points or more, with an in-hospital mortality greater than 10%.

Septic Shock is defined as a subset of sepsis in which particularly profound circulatory, cellular, and
metabolic abnormalities are associated with a greater risk of mortality than 40%.

Clinical presentation
• Temperature of >38oC or <360C; Heart rate of >90/min; Respiratory rate of >20/min or
PaCO2 <32 mm Hg
• Above features plus evidence of organ dysfunction (hypotension, jaundice, oliguria, or
altered state of consciousness from altered sensorium like drowsiness/lethargy

Note
• Septicaemia and septic shock are invariably fatal unless timely investigated and promptly
managed using specific antimicrobial therapies and other supportive management.
• Identification of the primary source/focus of infection is mandatory to eliminate the infection
and ensure favorable treatment outcomes.Neonates may present atypically with inability to
feed, respiratory distress/cyanosis or abdominal distension.

Investigations
Blood gases analysis, Bedside ultrasound- accessing the inferior venacava and the lungs, POC
ECG, Urine dipstick, Chest Xray- if suspecting pneumonia, Complete blood count, Qualitative or
quantitative CRP or Procalcitonin in centres available, Serum Electrolytes, Creatinine and Urea,
Liver function tests- liver enzymes, bilirubin, clotting time, Blood culture and antimicrobial
susceptibility testing. Primary source of infection’s clinical sample culture (e.g. urine, pus, sputum,

41
CSF etc) and antimicrobial susceptibility testing and/or RNA/DNA PCR for viral pathogens (where
indicated)

Diagnostic criteria
Sepsis: Q-SOFA in settings with limited laboratory infrastructures: two or more SOFA score namely:
Respiratory rate ≥22/min, Altered mentation and Systolic blood pressure ≥100 mm Hg) ± bacteria or
fungal proven blood culture and susceptibility testing are recommended to make a definitive
diagnosis.

Septic shock:Sepsis diagnostic criteria above and vasopressor therapy needed to elevate MAP ≥65
mmHg and lactate >2 mmol/L (18 mg/dL) despite adequate fluid resuscitation.

Non-pharmacological Treatment
• Nutritional support
• Control measures focused to the primary focus of infection.
• Perform primary and secondary assessment and provide necessary interventions
• Ensure patency of the airway and give oxygen if hypoxic or increased work of breathing
• Connect the patient to the cardiac monitor and obtain vital signs

Pharmacological Treatments
A: 0.9% sodium chloride (IV) (ADULT: 2litres; CHILD: 20mls/kg)
OR
A: compound sodium lactate (IV): Adult 2litres; paediatrics 20mls/kg) in 20minutes as first
bolus followed by second bolus of 2litres/20mls/kg (use small boluses in CCF).
OR
S: dobutamine (IV) 2-20mcg/kg/min can be given for patients in shock not responding to
fluids or when there is poor cardiac output.
OR
S: noradrenaline (IV) 5-20mcg/min for patients in septic shock not responding after 4litres
of IVF to maintain the mean arterial pressure (MAP) of ≥ 65mm Hg
AND
A: hydrocortisone (IV) 200mg stat.

Note: Transfuse blood (If hemoglobin is < 7g/dl)

Antimicrobial therapies (broad spectrum antibiotics must be started within the first hour):
A: ampicillin (IV) 150-200mg / kg/day divided 6hourly a day
AND
B: cloxacillin (IV) 50-100mg / kg/day 6hourly a day
AND
A: gentamicin (IV) or (IM) 120mg [For children 7.5mg/kg] 24hourly for 5 days.

If no improvement in vital signs within 24 hours (Temp, HR, RR and altered state of consciousness),
give:
B: ceftriaxone (IV) 1 gm [For children 100 mg/kg (IV) or (IM)] 24hourly for 4-14 days
AND
A: gentamicin (IV) or (IM) 120mg [For children 7.5mg/kg] 24hourly for 5 days

Refer immediately.
D: ceftriaxone +salbactum (FDC) (IV) or (IM) 75-120 mg/kg 24hourly for 4-14 days
AND
A: gentamicin (IV) or (IM) 120mg [For children 7.5mg/kg] 24hourly for 5days
OR
S**: piperacillin+tazobactum (FDC) (IV) (4g+0.5g) administered 8hourly [For children 100
mg Piperacillin+12.5mg Tazobactam per kg body weight 8hourly] for 7-10days
AND
A: gentamicin (IV) or (IM) 120mg [For children 7.5mg/kg] 24hourly for 5days.

Alternatively, (for patients who have evidence of not improving on the treatment above and referred
to a zonal/tertiary hospital with judicious decision from a medical specialist or medical super-
specialist):

42
S**: meropenem 2g (IV) 8hourly in adults and adolescents [40 mg/kg 8hourly in children]
for 7-14days
OR
S**: vancomycin (IV) 15 to 20 mg/kg body weight 8 -12hourly (not to exceed 2 g per dose)
for 7-14days.

Note
In renal insufficiency vancomycin can be adjusted for dose and dose interval. These antimicrobial
agents are usually reserved for Gram negative and Gram positive pathogen(s), respectively
supported by culture and antimicrobial susceptibility testing

For suspected co-existing anaerobic infections, an additional to all regimes above of


B: metronidazole (IV) 500mg 8hourly [In children 7.5 mg/kg 8hourly] for 7days
OR
S: clindamycin 600mg-1.2g/day diluted infusion in two or three doses [In children 15-
25mg/kg/day in three equal doses] for 7-10days is recommended.

For the rare cases of sepsis or septic shock due to carbapenem-resistant Gram negative
bacteria or vancomycin-resistant Gram positive bacteria, give:
S**: colistin (IV) 2.5-5mg/kg/day 8-12 hourly for 5days
AND
S**: linezolid (PO/IV) 400-600mg 12hourly for 10-14 days respectively or other non-beta
lactam antibiotics may be considered based on culture and antimicrobial susceptibility
testing results.

In case there is/are risk factors for invasive Candida infections like in immunocompromised
states, prolonged invasive vascular, necrotizing pancreatitis, then antifungal therapies should
be added.
C: fluconazole (IV) 800mg 24hourly on the first day then 400mg 24hourly for 14days [In
children 6-12mg/kg/day for 14days]

1.13 Approach to Pain


Pain is an unpleasant sensation or emotional experience associated with actual or potential tissue
damage, or described in terms of such damage. Any pain of moderate or higher intensity is
accompanied by anxiety and the urge to escape or terminate the feeling. Pain is subjective and
unique perceptual experience with multiple dimensions that may not directly be observed by others
or measured by physiological tests. Assesment is almost entirely self-reported.

Assessment of pain.
Self-report is the key to pain assessment. In non- or pre verbal children, facial expression is the
most valid indicator of pain; therefore, use faces pain scale to assess severity. Pain should be
assessed by:
• Duration
• Severity, e.g. does the patient wake up because of the pain
• Site
• Characteristics, e.g. stabbing, throbbing, crushing, cramp like
• Persistent or intermittent
• Relieving or aggravating factors
• Accompanying symptoms
• Distribution of pain
• In children pain can be assessed by child’s crying voice, posture, movement and colour

1.13.1 Approach to Chest Pain


The approach to non-traumatic chest pain requires early recognition of life threatening conditions.
Patients with life threatening conditions may have stable initial vital signs.
For a patient presenting with chest pain, the following are the list of differential diagnoses
• Acute coronary syndrome • Myocarditis
• Cardiac tamponade • Myocardial infarction
• Pericarditis • Aortic dissection

43

• Pulmonary embolism • Lung infection (pneumonia)
• Tension pneumothorax • Esophageal perforation
• Acute chest syndrome (sickle cell • Reflux Esophagitis
patients) • Musculoskeletal pain

Investigations
Depending on the clinical presentation, the following investigations maybe required:
POC ECG, Bedside USS-(cardiac, lungs, pleural, IVC, Abdominal aorta, kidneys etc),Serum
electrolytes, POC Troponin, Blood gases, Serum creatinine and urea, Urine pregnancy test,
Radiological investigations- Chest X-ray and/or CT scan- chest.
Pharmacological Treatments
Treat the underlying cause as indicated in specific chapters. The following analgesia may be used to
relieve the pain:
A: paracetamol (PO) 1g6hourly for 24hrs
OR
A: ibuprofen (PO )400mg 8hourly for 24hours
OR
A: diclofenac (IM) 50-100mg stat

For those patients who are unable to take oral medications


B: tramadol (IV) 50-100mg stat
OR
C: morphine (IV) 0.1mg/kg stat
OR
D: paracetamol (IV) 1g stat

If myocardial ischemia is highly suspected give:

A: acetylsalicylic acid (PO)325mg stat


AND
D: clopidrogel (PO) 300mg stat

Referral: Refer to higher facility with expertise when failed to establish the cause of the chest pain.

1.13.2 Approach to Abdominal Pain


Abdominal pain is among the common complaints of patients presenting to the Emergency
Department. While majority have benign and self-limited etiology, the goal is to identify those with
serious or life threatening etiologies so as to perform early intervention.

Differential Diagnoses:
Surgical causes:
• Abdominal aortic aneurysm • Lower GI bleeding
• Mesenteric ischemia • Splenic rupture
• Perforation (PUD, bowel, • Acute appendicitis
esophagus, appendix) • Pancreatitis
• Intestinal obstruction • Gallbladder diseases
• Upper GI bleeding

Genito-urinary causes Medical causes


• Ectopic pregnancy • Myocardial infarction
• Torsion (Testicular, ovarian) • Peptic ulcer disease
• Dysmenorrhoea • Gastro esophageal reflux disease
• Endometriosis • Inflammatory bowel syndrome
• Ureteric and kidney stones • Gastritis
• Urinary tract infection • Hepatitis
• Pelvic inflammatory disease

Investigations
Depending on the clinical presentation, the following investigations may be required:

44

ECG, Bedside USS- (gall bladder, liver, lungs, IVC, Abdominal aorta, kidneys etc), Serum
electrolytes, Troponin, Blood gases, Lactate, Serum Creatinine and Urea, Urine pregnancy test,
Radiological investigations (Chest and Abdomen X-ray and/or CT scan- Abdomen).
Pharmacological Treatments
For pain control, the following analgesia maybe used:
A: paracetamol (PO)1g 6hourly for 24hours
OR
A: diclofenac (IM) 50-100mg stat.
OR
A: hyoscine butyl bromide (PO) 10mg 8hourly for 24 hours

For those patients who are unable to take oral medications


B: tramadol (IV) 50-100mg stat
OR
C: morphine (IV) 0.1mg/kg stat
OR
B: hyoscine butyl bromide (IM) 10mg stat
OR
D: paracetamol (IV) 1g stat

1.13. 3 Headache
Approach to acute headache
Headache is a challenging complain as it requires balancing symptomatic control with rapid
assessment for life threatening diagnoses. Headaches can be categorized into primary and
secondary. Primary causes are neurologic and include: tension, cluster and migraine. Secondary
headaches are as a results of an underlying pathological process such as malignancies, infections
and other organic causes.

Differential diagnoses
Sudden onset severe headache
• Subarachnoid hemorrhage
• Cerebral venous thrombosis
• Hypertension emergency
• Adrenal and pituitary emergencies

Altered:
• Meningitis • Hypoglycemia
• Encephalitis • Fever
• Intracranial tumor • Meningitis
• Space occupying lesions • Malaria
• Stroke • Brain abscess
• Subarachnoid hemorrhage

Investigations
Will be specific basing on the clinical presentation of the patient. These may include:
• Malaria test • Bedside USS
• Random blood glucose test • Serum Electrolytes
• Blood Gases • Serum Creatinine and Urea
• POC Urine dipstick • POC Lactate
• Urinalysis • Urine pregnancy test
• CSF analysis • Radiological investigations- X-ray,
• POC ECG CT scan
Pharmacological Treatment
A: paracetamol (PO): Adult 1g 8hourly for 3days; Paediatrics 15mg/kg 6hourly when
required to a maximum of 4doses per 24hours
OR
A: ibuprofen (PO): Adult 400mg 8hourly for 3days; Paediatics 5–10mg/kg 8hourly for
24hours

45

For severe pain or if the patient is unable to take orally, IV/ IM analgesia administration may be
administered. These includes:
For those patients who are unable to take oral medications
B: tramadol (IV) 50-100mg stat
C: morphine (IV) 0.1mg/kg stat
D: paracetamol (IV) 1g stat

1.13.4 Other Pains


Other pains may include:
• Generalized body ache
• Joint pain
• Pain due to local infections
• Pains due to injury
• Eye pains
• Ear pains

Non-pharmacological and Pharmacological Treatments


Perform the primary and secondary assessment with interventions when needed.
For generalized pain give analgesics, advise the patient to rest and make a follow-up. For joint,
infections, injury, eye and ear pains treat as for main disease.

CAUTION!
• Do not use acetlysalicylic acid for abdominal pain or if a patient is vomiting or has nausea
and do not use acetlysalicylic acid in children below 12years. Patients with peptic ulcers
should not be given acetlysalicylic acid tablets.
• Refer the patients when pain persists despite of medication given for pain relief for further
investigation.

Referral:
Refer patients if:
• Children with moderate and acute severe pain
• No response to oral pain control
• Uncertain diagnosis
• All acute abdominal pain accompanied by vomiting and no passing of stool
• Pain requiring definitive treatment for the underlying disease
• Pain requiring opioids
1.14 Approach to Fever (Pyrexia)
Fever is abnormal elevation of body temperature that occurs as part of a specific biologic response
that is mediated and controlled by central nervous system and is usually a symptom of an infection.
It is characterized by an elevation of body temperature above the normal range of 36.5–37.5 0C

Clinical presentation
• Depression • Inability to concentrate
• Lethargy • Feeling cold
• Anorexia • Increased muscle tone
• Sleepiness • Shivering
• Hyperalgesia • Irritability

Note
Fever alone is not a diagnosis

Investigations
Will be specific basing on the clinical presentation. These may include:
• Rapid Malaria test • Bedside USS- Gall bladder, Liver,
• Blood slide for malaria parasites spleen, Abdominal aorta, kidneys
• POC Urine dipstick etc
• POC ECG • Serum Electrolytes
• Serum Creatinine and Urea

46
• Radiological investigations- X-ray, • Lactate
CT scan
• Complete blood count

Non-Pharmacological Treatment
• Perform both primary and secondary assessment. Intervene whenever necessary.
• Advise patient for bed rest
• Ask patient to take plenty of fluids (If able to take orally)

Note
• In children, temperature >400C need urgent lowering. However, lukewarm sponging and
evaporative cooling are not recommended.
• Fevers caused by virus are usually self-limiting but all other fevers need treatments.

Pharmacological Treatment
Give antipyretic medicines:
A: paracetamol (PO): Adult1g 6hourly when required, Paediatrics 15mg/kg 6hourly when
required OR suppository 125mg–250mg, 6hourly
OR
A: ibuprofen (PO): Adult 400mg 8hourly when required; Paediatrics 5-10mg/kg 8hourly
when required

For patient who are unable to take oral medications, give:


D: paracetamol 1gm (IV)

Referral
Refer the patient to the next facility with adequate expertise and facilities.
• If no diagnosis is established
• If no improvement of fever after the use of antibiotics
• Fever that recurs
1.15 Cough
Cough is a common reflex action that clears the throat of mucus, allergens, dusts or other foreign
irritants. A cough can be caused by several conditions both temporary and permanent. Frequently
coughing indicates the presence of disease.

Characteristics of cough/sputum
• If cough is dry without sputum and fever, it is probable an allergic condition or mild
upper respiratory illness (e.g. allergic rhinitis or allergic bronchitis)
• If cough is dry without sputum or fever and is associated with other congestive
symptoms it may be due to Congestive Cardiac Failure (CCF)
• If it is a repeated attack cough with wheezing but without fever, it is likely to be
bronchial asthma
• If it is a cough with fever, rapid breathing and chest in-drawing, it is likely pneumonia
• If it is cough with sputum which is yellowish pus-like and there is fever, it is likely
acute bronchitis or pneumonia
• If it is cough with blood in sputum and/or irregular fever with loss of weight and
appetite, it is a suspected tuberculosis
• If it is cough with large quantity of sputum, very foul smelling it is likely lung abscess
or bronchiectasis

Pharmacological Treatment
Causative/precipitating factors e.g. CCF, asthma; allergies must be established and treated
accordingly. (Refer respiratory disease condition chapter 9)

Note
Refer to high facility with expertise when cough persist and failed to establish the cause or when
association with fever.

47

1.16 . Approach to the Trauma Patient

Table 1.2: Approach to Trauma Patient

PREPARATION
Mobilise medical emergency team High Risk Mechanisms of Injury
Prepare equipment, examples; monitors, • High speed motor vehicle accident
ultrasound, Consider high-risk mechanisms of
injury • Pedestrian accidents
• Ejection
• Fall > 3m in height
• Penetrating injuries
INITIAL RESUSCITATION
Airway: Protect as appropriate and ensure Cervical-spine immobilization.

Breathing: Give oxygen and titrate to SpO2 (above 92%). If no air entry or if hyper-resonance present,
insert chest drain. If patient is showing signs of obstructive shock or deviated trachea, needle
decompression can be used initially before definitive decompression with a chest drain.

Circulation: Insert 2 large bore IV Cannula. Resuscitate with crystalloid solutions according to BP. If not
responding to crystalloids, patient should be resuscitated with blood. Control all external bleeding
immediately.

Disability: Check GCS and document this regularly to check for any changes in conscious state.
Perform a brief neurological examination. Check pupillary response. Check RBG.

Exposure: Expose patient to check for other injuries. Prevent against hypothermia.
SECONDARY SURVEY
HEENT – check for scalp Spine – Must log-roll Chest – look, palpate,
haematomas, depressed patient and palpate auscultate. Check for signs
skull fractures, facial bony spinous processes of of pneumothorax,
tenderness, eye injuries, C/T/L-spine and check haemothorax, ribs fractures,
otorrhea, haemotypanum, for any tenderness or flail chest. If failing to
tracheal deviation. stepping. ventilate or oxygenate,
consider NIV or intubation.
Pelvis – careful Abdomen – careful Extremities – examine all
examination for bony pelvic examination for peripheries for bony injury,
ring movement. If concerns guarding / tenderness / compartment syndrome,
re pelvic fractures, a pelvic bruising in all quadrants. muscular or soft tissue
binder (sheet) must be Ensure FAST damage, neurological
placed on the patient. examination performed changes.
in all trauma patients.

CHECKLIST :( Before patient leaves EMD) make sure:


• Airway is patent/protected
• Tension pneumo-haemothorax? Sp02>92%
• Large-bore IV placed and fluid given
• Control of external bleeding
• Pelvic fracture assessment done
• Assessment for internal bleeding done
• Spinal immobilization done
• Neurovascular status of all limbs assessed
• Does the patient need chest tube, NGT or catheter?

1.17 Approach to Dehydrated Patient


It refers to the loss of body water, with or without salt at a rate greater than the body can replace it.
The cause of dehydration is a combination of physiological and disease processes. Persons at

48

greatest risk for dehydration include persons with diarrhoea, vomiting, fever, diabetes or infections,
impaired level status.

Table 1.3: Types of Dehydration

Mild Moderate Severe


Consciousness Is normal May be irritable but is Unconscious
conscious
Skin pinched up Becomes normal Takes two seconds for Remain in folds for
immediately folds to disappear over two seconds
Eyes Moist and tears are Sunken, tears and/or Sunken and tearless
present absent
Mouth Not dry Is dry Is dry
Urine output Decreased Oliguria Oliguria/anuria
Fontanel Normal Depressed Sunken
Blood Pressure Normal Normal but orthostasis Decreased
Capillary refill 2s 2-4s More than 4s

Investigations
• Blood chemistry (to check • Bedside USS- IVC
electrolytes, especially • Complete blood count
sodium, potassium, and • Urine specific gravity
bicarbonate levels) • Blood Gas analysis
• Blood urea nitrogen (BUN) and • Lactate
creatinine

Other tests may be done to determine the cause of the dehydration (for example, blood sugar level
to check for diabetes).

Non-pharmacological Treatment
• Perform both primary and secondary assessment and provide the necessary interventions.
• Give oxygen if hypoxic or increased work of breathing
• Put TWO large bore IV cannulas for fluid resuscitations

The treatment for minor dehydration often considered the most effective, is drinking water and
stopping fluid loss.

Pharmacological Treatment
In more severe cases, correction of a dehydrated state is accomplished by the replenishment of
necessary water and electrolytes.
A: oral rehydration salt (ORS)
OR
A: 0.9% sodium chloride (IV): Adult 1-2litres; Paediatrics 20mls/kg)
OR
A:compound sodium lactate (IV): Adult 1-2litres; Paediatrics 20ml/kg

Remember to do reassessment after fluids resuscitations. If there is no electrolyte loss; give


A: dextrose (IV) 5%

If the underlying disease condition is diagnosed; treat as per specific condition in guidelines.
Referral: Refer to high center with expertise if no improvement.

Note
• Dehydration in Children refer to Plan A,B and C in IMCI guideline

49
1.18 Hyponatremia
Defined as serum sodium (Na+) levels less than 135mEq/L. It can be classified as: Mild
hyponatremia (130-135 mEq/L), Moderate hyponatremia (125 -129 mEq/L), Severe hyponatremia (<
125mEq/L).

Clinical presentation
Clinical signs generally will occur once levels are <125mEq/L. The following are symptoms related to
hyponatremia:
• Nausea and vomiting • loss of consciousness or coma
• Fatigue • Cramps or muscle spasms
• Dizziness • Irritability and restlessness
• Headache or confusion • Weakness
• Tremulousness or seizures • Thirst and anorexia
Investigations
Based on classification and patients’ clinical findings, the following investigations maybe necessary:
• POC RBG • Urine Osmolality
• Urine dipstick • Thyroid profile
• Electrolytes • CT brain (suspected cerebral
• Creatinine and Urea process)
• LFTs • CXR (suspected pulmonary
• Serum Osmolality infection/edema – related to renal
• Urine Na+ failure, CCF)
Non-pharmacological Treatment: Nutritional measures adjusted to patients need
- Salt containing foods
- Rehydration therapy
- Dietary modification

The goal of acute management is treatment of serious complications and careful restoration of
serum sodium concentration. Management depends on the cause, severity and time course. Based
on duration of development, hyponatremia can be (i) acute or (ii) chronic
Table 1.4: Pharmacological Treatment for Hyponatremia

ACUTE HYPONATREMIA CHRONIC HYPONATREMIA


usually symptomatic and onset <48 hours usually asymptomatic and onset > 48hours
Symptoms: neurologic deficit, seizures,
coma and confusion
Requires immediate treatment No specific treatment if mild and asymptomatic
Give: If moderate to severe:
C: 3% sodium chloride (IV) at rate of 1- Give:
2mEq/L/hr A: 0.9% sodium chloride (IV)
Alternative: Do NOT raise serum Sodium by over 12mmol/L
C: sodium bicarbonate (IV) 8.4% 50ml over in the first 24 hours
5min Stop correction when Sodium reaches
Do NOT raise serum Sodium by > 6mmol/L 130mEq/L
in 6hrs
Stop infusion when symptoms have
resolved
Manage seizures and coma as appropriate

Once symptoms have resolved


Assess volume status using point of care Ultrasound (POCUS) for IVC as well as vitals
assessment and quantify as either (i) Hypovolemic hyponatremia, (ii) Euvolemic hyponatremia
and (iii) Hypervolemic hyponatremia

50
(i) HYPOVOLEMIC (ii) EUVOLEMIC (iii) HYPERVOLEMIC
Possible causes: Possible causes: Possible causes:
-Dehydration (vomiting, -Psychogenic polydipsia -Renal Failure
diarrhea, sweating, third -Iatrogenic -Cirrhosis
spacing, -Syndrome of inappropriate - Nephrotic syndrome
hydration with hyperosmolar ADH secretion) -Congestive Cardiac Failure
fluids) -MDMA (Ecstasy use)
-Hypothyroidism
-Psudohyponatremia
-Give compound sodium -Prevent further -Nil per oral, restrict fluids
lactate or 0.9% sodium exacerbation of - Furosemide (IV) 40mg daily
chloride (IV) 250 – 500mls or hyponatremia until fluid volume is corrected.
0.5-1ml/kg/hour (guided by -Prevent rapid
BP response) overcorrection
-Insert Foleys catheter to
monitor output
Note
• Look for complications of over-correction such as Osmotic demyelination syndrome
(ODS)
• Hyponatremia can also lead to cerebral edema which may lead to increased Intra
cranial pressure (ICP)
• Exercise associated hyponatremia is common in athletes and the cause is over
hydration and not excessive water loss
• Psychogenic polydipsia caused by over ingestion of large quantity of water in
psychiatric patients or those on SSRI’s.

Severe Hyponatremia: (seizures, coma, signs of brainstem herniation), consider treatment for
cerebral edema and elevated ICP; give:

• 3% Sodium Chloride 3-5mls/kg over 15 to 60minutes to increase sodium by 2-4mmol/l


• Close monitoring of Serum sodium initially hourly with target correction rate of no more
than 8-10mmol/l/day and less than 0.5mmol/l/hour over 1-2hours

Hypovolemic Hyponatremia:
• Determine Sodium deficit: Total body Sodium deficit = (Desired sodium – actual plasma
Sodium) x Total body water{0.6 x weight (kg) Men OR 0.5 x weight (kg) women}
• Replace with 0.9% sodium chloride (IV)
• Correct at no more than 0.5mmol/l/ hour

Disposition
Symptomatic Hyponatremia, Severe hyponatremiamust be admitted to the HDU/ ICUfor continuous
biochemical and clinical monitoring. If not available refer the patient to a higher health facility with
HDU/ ICU capabilities.
1.19 Hypokalaemia
Is defined as plasma potassium below 3.5mmol/l. It includes: Weakness, constipation, paralysis,
bradycardiaand reduced tendon reflexes.

Investigations
POC ECG, serum creatinine and urea, serum electrolytes and/or bedside ultrasound

Additional investigations may be required basing on the clinical presentation.


Non-pharmacological Treatment
• Perform both primary and secondary assessment and provide necessary interventions
needed.
• Give oxygen if hypoxic or increased work of breathing
• Connect the patient to the monitor and obtain Vital signs
• Place IV access

51
Pharmacological management
Mild (3.0-3.5mmol/l)
C: potassium chloride (PO): Adult 20-40 mEq 8hourly (dissolved in 100-150mL water);
Paediatrics 2 mEq/kg 8hourly diluted in oral fluids or food. In case of diarrhea, give ORS
(5ml/kg/hr)
Moderate (2.5-2.9mmol/l)
C:potassium chloride (IV): Adult 10mEq/hour; Paediatrics 0.5 mEq/kg/hour diluted in 25-
50mls of 0.9% sodium chloride or DNS or 5% dextrose solutions via peripheral vein. Do
not exceed 10 mEq/hour.

Severe (<2.5mmol/l)
Both IV & Oral Replacement
C: potassium chloride(PO): Adult (28mmol K+) per hour if tolerated (dissolved in 100-
150mL water) dilutedpotassium; Paediatrics (PO) 2mEq/kg 8hourly.
OR
C:potassium chloride (IV): Adult 20 mEq in 100mL fluid over 1 hour via cubital fossa vein.
Continue to measure serum potassium every 1 to 2 hours until K+ > 2.8 mmol/L.
Paediatrics 1mEq/kg/hour.

The calculated hourly dose is multiplied by 12.5ml volume for dilution with NS/DNS/D5%.
Do not exceed 10 mEq/hr

Note
• 20 mEq of Potassium will raise K+ by 0.25 mEq/L. Aim to replace 25% of K+ deficit in 6
hours
• potassium chloride must never be given as IM or IV push
• Oral potassium (Slow K) 600mg tab is equivalent to 8 mEq
• Injection potassium chloride 7.5% 1ml = 1 mEq

Role of Magnesium
Magnesium should be checked. IF LOW, give Magnesium as follows:
A: magnesium sulphate 50% (IV): Adult Initially give 4ml diluted to 10ml with 0.9% sodium
chloride run over 20 minutes, then potassium chloride infusion, then magnesium sulphate
50% (IV) 0.12ml/kg/day; Paediatrics 0.1 ml/kg/dose administered over 2hours

Hypokalemia in CARDIAC ARREST in Adults: KCl 10 mEq IV over 5 min; the dose may be repeated
once

Note: ECG changes in hypokalemia


• Increased P wave amplitude, Prolonged PR interval,
• ST segment depression,
• QT prolongation, flattening or T wave inversion, and prominent U waves.

1.20 Triage Overview


Triage is the process of determining the priority of a patient to medical care based on the acuity
(severity of condition) and capacity of the system to address the condition, so as to
optimizeoutcome.

Importance of triage
Triage enables quick identification of patients who need immediate attention, and can thus
improve patient outcomes by avoiding potentialdelays. It helps in organizing, monitoring,
evaluating and determining the department resources that patientsmight need.

52

Triage system
The triage system is based on recommendation of Emergency Medicine expert’s basic principles of
triage, which uses specific criteria to categorize patients into three main levels of acuity:

• Emergency: all patients with immediate life or limb threats who are deemed
salvageable, but likely to further decompensate without immediate intervention
will be triaged in thislevel. This category can also be labeled as RED
• Priority:those seriously injured/ill patients with potential to decompensate if not
treated within 1 hour are triage as prioritycases. This category can also be
labeled as YELLOW
• Queue: this level includes all the walking wounded or those with less serious
injury/sickness who are unlikely to decompensate. Patients in this category can
safely wait for their turn. However, they should be monitored as their conditions
may change and warrant immediatecare. This category is also labeled as
GREEN.

Figure 1. Summary of triage flow and timelines of care

53
EMERGENCY CRITERIA (Tick here if Yes)
Unresponsive Pregnant with Heavy bleeding
Stridor Pregnant with Severe abdominal pain
SpO2 <90% Pregnant with Seizures
Respiratory distress or cyanosis Pregnant with Severe headache
Weak pulse or Capillary refill>3 sec Pregnant with Visual changes
Hear rate <50 or > 150 Pregnant with SBP≥160 or DBP ≥110
Heavy bleeding Pregnant with Active labour
Active convulsions Pregnant with Trauma
Hypoglycemia Age < 2years with Temp <36oC or > 39oC
High-risk trauma* Child <14 with severe dehydration
Poisoning or dangerous chemical Adult with signs of meningitis
exposure*
Threatened limb* Acute chest or abdominal pain (>50 years
old)
Snake bite ECG with acute ischaemia
Violent or aggressive Other
(state):____________________________
PRIORITY CRITERIA (Tick here if Yes)
Vomits everything or ongoing diarrhoea Severe pain (no Red criteria)
(adult)
Unable to feed or drink Visible acute limb deformity
Severe pallor Open fracture
On-going bleeding (no emergency Suspected dislocation
criteria))
Recent fainting Other trauma/burns (no Red criteria)
Altered mental status (no emergency Sexual assault
criteria))
Acute general weakness Acute testicular/ scrotal pain or priapism
Acute focal neurology Unable to pass urine
Acute visual disturbance Wheezing (no Red criteria)
New rash worsening over hours or peeling Exposure requiring time- sensitive
(no emergency criteria) prophylaxis (example: animal bite,
needle-stick injury)
Any infant 8 days to 2 months old Child below 14 years old with malnutrition
Child below 14 years old with dehydration Child below 14 years old with ongoing
diarrhoea
Referral patient (no emergency criteria) Other, state:
__________________________
QUEUE CRITERIA (Tick here if Yes)
Patient with no Emergency or priority criteria indicated in above tables

54
CHAPTER TWO
ANAESTHESIA
Anaesthesia is a state of controlled reversible loss of consciousness usually accompanied by
analgesia, muscle relaxation, amnesia and areflexia. It is usually induced for the purpose of
facilitating surgery and other therapeutic or diagnostic procedures.

Anaesthesia may be achieved with either:


• Regional anaesthesia alone e.g. spinal/epidural anaesthesia, arm block
• General anaesthesia
• A combination of regional and general anaesthesia
• Regional anaesthesia with sedation
• Local anaesthesia through topical application/spray or infiltration of local anaesthetics

Note
• Anesthetic medicines and sedatives MUST be provided by medical practitioners who are
properly trained and have appropriate experience with their use
• Medicines and equipment for resuscitation should be immediately available whenever
general anaesthesia, regional anaesthesia or sedation is administered.

2.1 General Anaesthesia


Medicines used in general anaesthesia include the following pre-medications:
Sedation and Anxiolytics
A: diazepam (IV) 0.05 – 0.1mg/kg
OR
C: diazepam (PO) 0.5 – 0.75mg/kg
OR
C: lorazepam (IM) 0.05mg/kg or 0.04mg/kg (IV)
OR
D: midazolam (IV) 0.05–0.1mg/kg

If there is an overdose with benzodiazepines use the following antidote:


A: flumazenil (IV): 0.2mg stat over 30 seconds. Repeated dose of 0.2mg may be given at
1minute intervals until desired level of consciousness is achieved; do not exceed
4doses (1mg).

If there is bradycardia, salivary secretion or other muscarinic side effects give


A: atropine (IV) 0.01mg/kg
OR
S: glycopyrrolate (IV) 0.2–0.4mg (0.2mg for every 1mg of neostigmine). Alternatively, a
dose of 10–15 µg/kg (0.01–0.015mg/kg) (IV) with 50 µg/kg (0.05mg/kg) neostigmine or
equivalent dose of pyridostigmine
Antiemetics are indicated for prevention of Post-Operative Nausea and Vomiting (PONV)
B: dexamethasone sodium phosphate (IV) 4–5mg for PONV prevention
OR
C: metoclopramide (IV) 10mg
OR
S: ondansetron (IV)4mg administered over 2–5minutes
Antacidsare given to patients at risk of aspiration, such as pregnant women, before Caesarean
section.
B: sodium citrate (PO) 0.3moles, 30ml. Not more than 30 minutes pre–induction of
anaesthesia
OR

55

C: pantoprazole (IV) 40 mg as soon as the possibility of surgery is known in cases of
emergency procedures
General anaesthetics are used for induction of anaesthesia as boluses or for maintenance of
anaesthesia as continuous infusions in Total Intravenous Anaesthesia (TIVA).
B: ketamine (IV) 1–2mg/kg (Forinduction, however can be used for maintenance under
TIVA, but contraindicated in those who a significant rise in BP/IOP/ICP would constitute a
serious hazard)
OR
C: thiopental (IV) 3–5mg/kg (For induction, however can be used for maintenance under
TIVA)
OR
D: propofol (IV) 1.5–2.5mg/kg for induction of anaesthesia and 6–12mg/kg/hour infusion
for maintenance in TIVA.
propofol is contraindicted to Patients with risk of hypotension, use volatile agent for
maintenance of anaesthesia
OR
S: etomidate (IV) 0.3mg/kg (between 0.2–0.6mg/kg) for induction (cardiostable, it affects
cortisol production)

Inhalational anaesthetic agents (for induction and/or maintenance)


B: halothane 2–4% in air, oxygen or oxygen/nitrous oxide and maintenance 0.5–1.5%
(Nitrous oxide is delivered in a ratio of 70:30 Mix with oxygen, reduce the requirement
of a more toxic anaesthetic/ potent agent)
OR
B: isoflurane1.2–2.5% titrates to desired effect
OR
S: sevoflurane 5–7%
Maintenance: 0.5–3% sevoflurane with or without the concomitant use of nitrous oxide.

Muscle Relaxants
B: suxamethonium (IV) 1–1.5mg/kg for induction
OR
C: pancuronium (IV) 0.04–0.1mg/kg for maintenance.
OR
S: atracurium (IV) 0.4–0.5mg/kg over 60 seconds followed by 0.08–0.1mg/kg 20–
45minutes after initial dose for maintenance or infusion at 0.05–0.1 mg/kg/min (For
patients with renal impairment)
OR
S: rocuronium (IV) 0.6 -1 mg/kg can be used for induction if sugammadex (reversal agent)
is available, it has minimal side effects, can be used in case suxamethonium is
contraindicated.

Contraindications
Suxamethonium is contraindicated in patients with risk for developing hyperkalaemia or with
upper/lower motor neuron defect, prolonged chemical denervation, direct muscle trauma, tumour or
inflammation, thermal trauma, disuse atrophy, severe infection

Medicines for Reversal of Neuromuscular Blockade


B: neostigmine (IV) 50µg/kg with atropine (IV), 20µg/kg (maximum 1.2mg)
OR
S: glycopyrrolate (IV)10 µg/kg
OR
S: sugammadex (IV) 2–4mg/kg

56

Analgesics for Pain Management in Peri–operative Period
Non–Opiod Analgesics
B: paracetamol (IV) 15mg/kg 8hourly
Opioid analgesics
B: tramadol (IM/IV) 50mg 6hourly
OR
C: morphine (IV/IM) 3–5mg as a single dose, then further boluses of 1–2mg/minute.
Maximum dose of morphine 0.1–0.2mg/kg, and monitor vitals closely
OR
B: pethidine (IV/IM) 1–2mg/kg (used for analgesia during anaesthesia, and during labour)
OR
S: fentanyl (IV) 1–2µg/kg

Antagonists of Opioids
For opioid over–dosage
B: naloxone (IV) 0.4mg–2mg, alternatively may be given intramuscularly or
subcutaneously. For reversal of opioid sedation initial dose 0.1–0.2mg (IV) at 2–3
minutes’ intervals to the desired degree of reversal.

2.2 Local Anaesthesia


Medicines used as local anaesthetics cause revisable absence of pain sensation, although other
senses are often affected as well. Also, when it is used on specific nerve pathways, paralysis can
also be achieved.
A: lidocaine (site): Maximum 4.5mg/kg without vasoconstrictors (adrenaline) or 7mg/kg
with vasoconstrictors (Not for Spinal Anaesthesia)
OR
C: bupivacaine (site): 625µg/ml(0.0625%)1.25mg/ml(0.125%)
OR
C: bupivacaine + glucose: bupivacaine hydrochloride 5mg/ml (0.5%) with 80 mg/ml
glucose (specific gravity of 1.026). The addition of glucose produces a hyperbaric
solution relative to cerebrospinal fluid.

Medicines for Local Anaesthetics Overdose


S: Lipid emulsion (intralipid 20% or 30% solution) for severe local anaesthetic toxicity with
cardiovascular or neurological impairment.
Dose: 1.5ml/kg (IV) over 1min, then continuous infusion 0.25ml/kg/min. Repeat bolus 1–2times
for persistent cardiovascular collapse. Double infusion rate to 0.5ml/kg/min if BP remains
low. Continue infusion for at least 10 minutes after cardiovascular stability attained.
Recommended upper limit: approximately 10ml/kg lipid emulsion over the first 30 minutes.
Epidural and combined spinal-epidural anaesthesia Techniques
Epidural anaesthesia is a type of neuraxial anaesthesia; local anaesthetic (LA) is injected into the
epidural space to anaesthetize the spinal nerve roots that traverse the space. Epidural anaesthesia
is used for anaesthesia of abdominal, pelvic, and lower extremity procedures and, less commonly,
thoracic procedures.

A: lidocaine 1 to 2 %(Epidurally)
OR
C: bupivacaine 0.25 to 0.75% (Epidurally)
Epidural Labour Analgesia (Local Anaesthetics, Adjuvant Drugs)
D: bupivacaine 0.1-0.25% with or without Fentanyl 50 – 100µg (Epidurally). e.g.
(Bupivacaine 0.1% Plus Fentanyl 2µg/ml at infusion rate of 0-12mls/hour)
Peripheral nerve blocks
Peripheral nerve blocks are widely used for surgical anaesthesia as well as for both postoperative
and nonsurgical analgesia.

57

Blocks are often used to avoid the effects of alternative anesthetics or analgesics. The most
common rationale for their use is to avoid side effects and complications of general anaesthesia
(GA), particularly respiratory-related effects, and to provide analgesia while minimizing opioid use.

Local Anaesthetics
B: lidocaine (Perineurally) 1 to 2%
OR
C: bupivacaine (Perineurally) 0.25 to 0.75%
OR
C:bupivacaine+glucose(Perineurally) 0.25 to .75%

Adjuvants
A: adrenaline (Perineurally) Typical Concentration 5-10µg
OR
B: dexamethasone (Perineurally) 4-10mg
OR
S: clonidine (perineurally) 0.5-2µg
Topical Anaesthesia
B: lidocaine gel (Topically) 2 to 5%
OR
B: lidocaine topical spray 2% and 10% solutions for topical anaesthesia of the upper
airway (i.e., oropharynx and vocal cords), the trachea, and nasal passages.

2.3 Sedation
The aim of providing sedation is to reduce anxiety, agitation and pain so as to tolerate unpleasant
medical procedures or intervention while the patient retains control of airway, breathing and blood
pressure. This procedural sedation and analgesia is commonly used in emergency units,
radiological /diagnostic units, dentistry and for certain endoscopic and gynaecological procedures.

Minimal Sedation/Anxiolysis (no analgesic effect is required)


A: diazepam (IV) 0.1mg/kg (In a 60kg patient, give boluses of 2mg every minute; may
require up to 10mg)
OR
C: nitrous oxide inhaled 20 to 50%, in oxygen (will also provide some analgesia)
OR
D: midazolam (IV) 0.05mg/kg (In a 60 kg patient, give boluses of 1 mg every minute; may
require up to 3mg)

Medicines for moderate sedation & analgesia


If analgesia is required, one of the above is usually combined with an opiate. However, ketamine
has analgesic activity and can be used on its own or combined with a benzodiazepine.
B: ketamine (IV) 0.5mg/kg. Repeat doses of 0.5mg/kg as required, every 5-10minutes
OR
C: morphine(IV) 0.1mg /kg in increments of 2mg every 5minutes
OR
S: fentanyl (IV) 0.25µg/kg

Alternative medicines
D: propofol (IV) 0.5mg/kg. Repeated as 0.25mg/kg boluses every 5minutes as required
OR
S: etomidate (IV) 0.1mg/kg. Repeat doses of 0.05 mg/kg (IV) every 5minutes, as required.
But it is more likely to cause myoclonus

Medicines for Deep Sedation & Analgesia: This is usually achieved with either higher doses of
medications used for moderate sedation, or by combining an opiate, a benzodiazepine, and either
Propofol or Etomidate. When agents are combined, lower doses may be adequate.

58

Supplemental Analgesia: Simple analgesics can be given before or after the procedure:
A: paracetamol (PO): 1g 4-6 hourly when required to a maximum of 4doses per 24hours.
Maximum dose: 15mg/kg/dose. Maximum dose: 4 g in 24 hours.
OR
A: ibuprofen (PO) 400mg 8hourly with meals after the procedure.

Note
Sedation in intensive care
• Indications for sedation in intensive care needs to be defined for each patient, and may include
one or more of anxiolysis, analgesia, agitation control, or to help patients tolerate
uncomfortable situations or procedures (e.g. intubation and ventilation)
• Sedation requirements fluctuate rapidly so, it warrants regular review
• Adequate pain control is often more efficacious than sedatives for reducing agitation. Delirium
should be considered and managed appropriately.

Short–term and long–term sedation


Medicines for short–term sedation (less than 24 hours)
C: midazolam (IV) 0.05–0.2mg/kg/hour.
OR
D: propofol (IV) 0.5mg/kg/hour.
Due to high fat solubility, midazolam also becomes ‘long acting’ after infusions of more than 24
hours

Medicines for longer–term sedation (72 hours or more)


C: lorazepam (IV) 0.1mg/kg/hour.
OR
D: midazolam (IV) 0.2mg/kg/hour.

Lorazepam (0.1 mg/kg/hour) is as effective (and as easy to wean) as midazolam 0.2 mg/kg/hour) but
more difficult to titrate.

Supplemental analgesia
C: morphine (IV) 0.1–0.2mg/kg/hour.
OR
S: fentanyl (IV) 1 µg/kg/hour (also becomes long acting after prolonged infusion due to fat
solubility)

2.4 Anaesthesiain Special Conditions


2.4.1 Surgery in Diabetic Patient
Diabetes leads to increased surgical morbidity, mortality and length of hospital stay. Perioperative
Hyperglycemia is associated with increased risk of infection, medical complications and death. The
following shall be considered:
• Ideally, the elective patient should have a preoperative glycated haemoglobin less than 9%
or blood glucose fasting 10 mmol/l of random 13 mmol/l.
• Screen for nephropathy, cardiac disease, retinopathy and neuropathy and inform surgical
team.
• If on oral hypoglycemic therapy and well controlled and surgery is minor, omit therapy on
morning of surgery and resume therapy when eating normally.
• If on insulin adjust depending on the type of surgery and expected fasting period as
follows:
Minor surgery (duration < 3hours)
Insulin: in the morning intermediate–acting insulin, 1/2 to 2/3 of total daily dose.
• If blood glucose is above 20 mmol/l, give a small dose short–acting insulin.
• In the evening give intermediate–acting insulin, 1/3 of daily dose.
Fluid: 5% dextrose (IV), volume according to age.

59

Blood glucose monitoring: every 1–2 hours’ values between 10–14 mmol/l.

Major surgery (duration > 3hours) Involve a general anesthesia and therefore a period
of fasting.
• Insulin and fluid: infusion solution containing 5% glucose and 20 mmol/l potassium
chloride (maintenance volume)
• Insulin infusion 0.05 IU/kg/hour.
• Blood glucose monitoring: every 1–2 hours; values between 6–14 mmol/l, if < 5
mmol/l reduce infusion rate, continue infusion therapy intraoperatively.
• Post operatively: give 5–10% dextrose (IV) 1 Litre + 20ml potassium chloride + 2/3 of
total daily dose of insulin over 8hours and repeat to maintain infusion therapy until
food intake is re–established.

2.4.2 Surgery in Hypertensive Patient


• Monitor BP, scan monitors for HR, ECG rhythm, EtCO2, temperature
• Provided the patient is adequately oxygenated & ventilated, deepen anesthetic
• Examine patient:
o Pupils (high ICP)
o Diaphoresis & flushing (carcinoid, pheochromocytoma, hyperthyroidism)
o Rigidity (malignant hyperthermia, serotonin syndrome)
o Bladder distension
o Hot (thyroid storm, malignant hyperthermia, serotonin syndrome)
• Examine drugs & equipment:
o Potential drug error
o Possible TIVA or circuit disconnect (awareness)
o Tourniquet (pain)
o Equipment error (falsely high reading)
Give
C: hydralazine (IV) 5-20mg (max 30mg) slow IV push every 20minutes
OR
C: labetalol (IV) 5-20mg every10min (max total 300mg)
OR
S: esmolol (IV) 0.5mg/kg over 1minute; start infusion at 50mcg/kg/min
OR
S: nitroglycerin (IV) 50-100mcg; start infusion at 10mcg/min
• Treat underlying cause i.e., pain.

2.4.3 Surgery in Asthmatic Patient


Considerations
• Risk of perioperative respiratory complications:
o Bronchospasm, mucous plugging, pneumothorax, atelectasis, pneumonia
• Possible pulmonary hypertension & RV failure
• Need for preoperative optimization:
o Treatment of bronchospasm, infection, atelectasis
• Avoidance of triggers & exacerbating factors:
o Avoid general anesthesia, endotracheal intubation, histamine releasing
medications, light anesthesia
• Medication management:
o Continue usual inhalers pre-operatively
o Stress dose steroids (STEROID COVER) if recent high dose steroid use

Severe Asthma Exacerbation Treatment Options


Refer to asthma section.
Anesthetics
B: ketamine (briochodilator effect)
OR
D: propofol(bronchodilator effect)
• Volatiles all are bronchodilators but sevoflurane is likely best choice
• Always consider noninvasive PPV as rescue before intubation
• If intubation & ventilation:

60

o Use permissive hypercapnia
o Use low respiratory rates: start at 10-12 breaths/minute but may need lower
rates
o Use prolonged expiratory time (e.g. I: E ratios 1:3, 1:4, or even 1:5)
o Tidal volume 6-8cc/kg
o FiO2 to achieve PaO2>60mm Hg

2.4.4 Surgery in Sickle Cell Patient


• Avoid precipitants of sickle cell crisis:
o Hypoxia
o Vascular stasis
o Hypothermia
o Hypovolemia/hypotension
o Acidosis
• Optimize perioperative pain control
• Monitor for:
o Vaso-occlusive crisis
o Acute chest syndrome
o Aplastic crisis
o Splenic sequestration syndrome
o Right upper quadrant syndrome

Optimization (in consultation with hematology)


Risk factors for acute pain crises:
• Age, frequency of hospitalizations &/or transfusions for episodes of crisis, evidence of
organ damage (e.g., low baseline oxygen saturation, elevated creatinine, cardiac
dysfunction), history of central nervous system events, concurrent infection
• Procedural risk for complications:
o Low: minor surgery (e.g., inguinal hernia & extremity surgery)
o Intermediate: intra-abdominal operations (e.g., cholecystectomy)
o High: intracranial & intrathoracic procedures, hip surgery
• Hematology consult, optimize treatment:
o Hydroxyurea to ↑ fetal hemoglobin production
o Cancel non-emergent cases if patient experiencing a crisis
o IV fluid to avoid dehydration while NPO
• Preoperative transfusion therapy:
o Controversial without good evidence
o Purpose is to correct pre-existing anemia, ↓ hemoglobin S concentration
& ↑ adult hemoglobin
o Consider target hemoglobin 6 -10 for surgery & always have blood available for
any surgery
o Exchange transfusions are not routinely recommended
• Treatment of Pain:
o Rest, warmth, reassurance, analgesia, fluid replacement:
o Oral analgesics may be sufficient for minor attacks
o Opioids (IM, SC, IV, PO)
o PCA opioids with baseline analgesia provided by background infusion or fentanyl
patch
o Paracetamol & NSAIDs
o NSAIDS particularly good for bone pain
o Ketamine as adjunct
o Regional blocks as appropriate, epidural use has been reported

61

CHAPTER THREE
HAEMATOLOGY AND BLOOD TRANSFUSION
3.1 Anaemia
3.1.1 Iron Deficiency Anaemia
A lack of iron in the body (mainly due to nutritional deficiency, chronic blood loss, malabsorption and
hookworm infestations and increased demand such as during pregnancy).

Clinical presentation: fatigue, palpitation, dizziness, glossitis, koilonychias (spoon shaped nails)
and pica

Investigations
• Full blood picture (FBP)
• Peripheral smear
• Iron studies- serum iron levels, total iron binding capacity, serum ferritin
• Stool analysis for hookworm ova and occult blood. If stool for occult blood is positive, do
Oesophagoduodenoscopy (OGD) to confirm upper gastrointestinal bleeding

Non-Pharmacological Treatment
• To prevent iron deficiency;
o Eat a variety of iron rich foods like meat, eggs, legumes (dried beans, lentils, peas),
spinach and dark green leafy vegetables, iron fortified breads and cereals, nuts and
seeds.
• To help in iron absorption from diet;
o Avoid drinking tea/coffee with meals
o Increase intake of vitamin C rich foods (e.g. citrus fruit, broccoli, cauliflower, guavas,
tomatoes, bell peppers and strawberries) with meals to maintain iron in its reduced
state

Pharmacological Treatment
Treat the undelying cause of iron deficiency anaemia.
Adults
A: ferrous sulfate (PO) 200mg 8hourly for 3months.
Children:
A: ferrous sulphate (PO) 5mg/kg 8hourly. Continue for 3months after the normal hemoglobin
has been achieved.
OR
B: Blood transfusion (is only indicated if anaemia is life threatening; e.g anaemia in failure,
hypoxia.)
OR
D: Iron sucrose (IV) 200mg in 100ml0.9% sodium chloride running for 15 minutes once a day
three times a week for 2 weeks.

Parenteral iron is indicated in patients who can not tolerate or are refractory to oral iron.
• Total cumulative dose = number of 100mg ampoules for Hb increase
• Divide the total cumulative dose in 200mg doses, given 24hourly

62

Table 3.1: Number of 100mg/ampoules of iron sucrose needed for Hb increase based on the
body weight.

• Duration of treatment may extend to 4 weeks based on the total cumulative dose required.
• Monitor blood counts and clinical assessment monthly.

Note
Formulations of iron combined with other nutritional supplements (vitamins, 0.4mg-5mg folic acid, zinc
and amino acids) are recommended to enhance absorption of iron and correct combined nutritional
deficiencies.

3.1.2 Megaloblastic Anemia


This is a condition whereby the bone marrow usually produces large, structurally abnormal,
immature red blood cells (megaloblasts) often due to inadequate intake or malabsorption of vitamin
B12 or folate.

Clinical presentation
Pallor, depression, hair loss, pins and needles, numbness in hands or feet, tremors and palsies,
mildly jaundiced (lemon yellow tint), beefy tongue, darkening of palms and ataxic gait.

Investigations
• FBC-Low Hb, sometime pancytopenia, raised mcv but maybe low or normal if coexisting
with iron deficiency (combined deficiency anaemia)
• Peripheral smear
• Serum vitamin B12,
• Serum folate level,
• TSH
• Reticulocyte count
• Bone marrow aspiration may be indicated

Pharmacological Treatment
Vitamin (B12 deficiency anaemia) and other macrocytic without neurological involvement.
C: hydroxycobalamine (IM) initially 1mg 3times a week for 2weeks then 1mg (IM) every
3months.
Review the patient’s blood counts and clinical assessment every 3months.

Pernicious Anaemia (B12 deficiency) with neurological symptoms and signs


C: hydroxycobalamine (IM) initially 1mg on alternate days until no further improvement
(maximum reversal or neuro-psychiatric signs and symptoms are achieved) then 1mg
every 2-3months
AND
A: folic acid (PO) 5mg 24hourly for at least 3months this must be started simultaneously
with injection vitamin B12
AND
A: ferrous sulphate (PO) 200mg 8hourly for at least 3months.

63

3.1.3 Haemolytic Anaemia
Haemolytic anaemia results from an increase in the rate of red cell destruction in the intravascular or
in the reticuloendothelial system in some pathological disorders

Clinical presentation:
• Pallor, jaundice, splenomegaly
• Anaemia, Reticulocytosis, indirect hyperbilirubinemia, and haemoglobinuria

Pharmacological Treatment
Immunosuppressants
A: prednisolone (PO) 1–1.5mg/kg/day for 1-3 weeks until Hb > 10g/dl
AND/OR
S: cyclosphophamide (IV) 50mg/kg/day for 4days

If no response;
A: folic acid (PO) 5mg 24hourly should be given for 1to 3months.
OR
B: blood transfusion if anaemia is severe
OR
S*: High dose human immunoglobulin G (IV) 400mg/kg/day for 5days

Surgical Management
Splenectomy may be considered in those who fail to respond to pharmacological treatment.

3.1.4 Sickle Cell Disease (SCD)


Clinical presentation
The clinical manifestations of SCA are variable;
• Symptoms usually occur after 6 months of life.
• acute onset of unexplained illness, including acute pain, anaemia, acute neurological
symptoms, loss of vision, respiratory infections, hepatosplenomegaly, jaundice, swollen
limbs and sepsis.
• Four types of crises occur in SCD; vaso-occlussive crisis, hemolytic crisis, sequestration
crisis, aplastic crisis.

Investigations
Screening test: sickling test, isoelectric focusing (electrophoretic separation)
Confirmatory Tests: Sickle Scan, haemoglobin electrophoresis, HPLC (High performance Liquid
Chromatography)

Other ancillary laboratory investigations useful in detection and monitoring of the disease include:
• FBP, Reticulocyte count, Peripheral
blood film,
• Blood culture and sensitivity,
• LDH, total and indirect bilirubin,
liver and renal profile,
• POC blood gases, ECG,
• mRDT, RBG,
• Blood grouping and cross match,
• Imaging eg CXR, ECHO,
Ultrasounds (abdominal and
transcranial doppler TCD USS),
and CT Scan head if suspicious of
stroke.

64
Note
Confirmatory test should be done to all patients with positive screening tests and those with
negative screening test results but have clinical presentation suggestive of SCD.

Screening
From the age of 10 years, screen for renal disease (proteinuria by urine dipstick) and retinopathy
annually
Annual screening for risk of stroke by transcranial Doppler from the age of 2years to 16years.

Pharmacological Treatment
A: folic acid (PO) 5mg 24hourly

Prophylaxis against Pneumococcal Infection


A: phenoxymethyl penicillin (PO) 125mg for children younger than 3years; phenoxymethyl
penicillin (PO) 250mg for children 3 years and older twelve hourly until 5years of age in all
children with SCA.

Immunisation against pneumococcal infection


A: pneumococcal conjugate vaccine (PCV-13) from two months of age, 3 doses 8 weeks
apart (i.e at age 2months, 4 months and 6 months) and a booster dose between 12-15
months. If the child has not previously received this vaccine, then at least one dose should
be given between 6-18 years. PCV-13 and vaccine against H. influenza is incorporated in
Tanzania EPI schedule.

S: pneumococcal polysaccharide vaccine (PPSV-23) - at 2 years then after every 5 years


for life.

Table 3.2: Analgesia for General Pain Relief


Severity Management
Mild Reassurance, hot packs, reposition, massage, distraction (stories, play)
Child: A: paracetamol (PO) 15mg/kg 6hourly
Adult: A: paracetamol (PO) 1g 6hourly
Moderate As for mild pain, PLUS
Child: A: ibuprofen (PO) 5mg/kg 8hourly
Adult: A: ibuprofen (PO) 400mg 8hourly
Severe As for moderate pain PLUS
Child:C: morphine (PO) 0.5mg/kg 3–4 hourly as needed
Adult: C: morphine (PO) 5–10mg, 3–4 hourly as needed
If unable to take orally, administer paracetamol (IV) 1g 6-8hourly and morphine
0.1mg/kg 8-12hourly
If morphine is not available, tramadol may be used.
B: tramadol (PO) 50-100mg 6hourly as needed

Hydration: Encourage oral fluids first; it should be used whenever possible. Give IV fluids,
preferably normal saline, if the patient is unable to drink well, has severe pain, or abdominal
symptoms.

Body weight (kg) Fluids (ml/kg/day)


<10 kg 150ml/kg/day
11 – 20kg 75ml/kg/day for every kilogram above 10kg
ADDED to 1500ml for the first 10kg of weight
> 20kg 30ml/kg for every kilogram above 20kg
ADDED to 225Oml for the first 20kg of weight
Divide the total daily volume by 24 hours to obtain hourly fluid rate

Indications for use of Hydroxyurea Include:


All children older than nine months with proven SCD; and
In adolescents and adults with the following;

65
• Recurrent vaso-occlussive crisis (3 or more severe episodes requiring admission in the
last 12 months),
• Severe and/or recurrent acute chest syndrome (ACS) (2 or more episodes in a lifetime),
• Severe symptomatic chronic anemia that interferes with daily activities or quality of life,
• Where chronic transfusion therapy is not feasible use it as an alternative to prevent new or
recurrent stroke,
• Silent infarcts, stroke and in patients with abnormal TCD (199cm/sec),
• Recurrent priapism,
• Chronic kidney disease on erythropoietin to improve anaemia.

Principle of Dosage Initiation and Monitoring:


S: hydroxyurea (PO) 15 mg/kg/day 24hourly; (5–10 mg/kg/day if patient has chronic kidney
disease).
S: hydroxyurea (PO) 20mg/kg/day, starting dosage for infants and children.

Increase the dose by 2.5–5 mg/kg/day every 3 months,Maximum tolerated dose (MTD) should not
exceed 30mg/kg/day.
Blood work monitoring
• Bi-monthly FBP, reticulocyte count for 1 month, then monthly for 3months, then once
every 3months if blood counts remain stable.
• HbF % analysis, liver function test, serum creatinine and urea every 6months.
• Weigh patient every three months and adjust the dosage accordingly.

Threshold for dose reduction


• Neutrophil ANC < 1.5 X109/L
• Reticulocyte count < 80 X1012/L
• Platelet count < 80 X109/L
• Hb < 6g/dl

If haematologic toxicity occurs;


• Discontinue hydroxyurea until counts recover, usually 1-2 weeks,
• Reinitiate hydroxyurea at a dose 2.5 mg/kg/day less than the dose given before onset of
cytopenias to achieve the maximum tolerable therapeautic dose,
• Do FBP according to the initiation schedule.

Note
• Clinical response to treatment with hydroxyurea may take 3-6months. A 6month trial on
MTD is required before considering discontinuation due to treatment failure.
• Hydroxyurea should be stopped at least three months prior to conception in both males
and females
• Hydroxyurea should be discontinued in all pregnant women
• Hydroxyurea should be discontinued in all breastfeeding women

Blood transfusion in SCA


Simple (Top-Up) Blood Transfusion:
Indicated in symptomatic anaemia, orhaemoglobin level has dropped by > 2g/dl below the steady-
state value.

Exchange Blood Transfusion:


Aim to reduce HbS to 30%.

Indications for Exchange Blood Transfusion


• Cerebrovascular Accidents (CVAs)
• Acute Chest Syndrome (ACS)
• Prior to major surgery
• Multi-organ failure, including Systemic Marrow Fat Embolism (SMFE)
• Multiple pregnancies
• Prevention of recurrent stroke.

66

Relative Indications for Exchange Blood Transfusion
• Intractable or very frequent severe crises
• Major priapism unresponsive to other therapy.

Note
• Because the cardiovascular system adjusts to the chronic anaemia, blood transfusion is not
routinely indicated in steady state SCD simply for the reason that haemoglobin level is below 8–
10g/dl.
• Packed red cells transfusion is preferred to minimize the risk of fluid overload

SCD in pregnancy
• Stop hydroxyurea 3 months before conception
• Educate the patient about the risks associated with pregnancy in SCD.
• Determine the haemoglobinopathy status of the partner.
• Document pre-pregnancy baseline results if any.
• Refer the patient to a high-risk antenatal clinic for proper follow up
• Prescribe routine prenatal vitamins, see under Obstetric and gynaecology chapter
• Prophylactic blood transfusion is not recommended.
• Vaginal delivery is preferred unless there is indication for caesarian section.
• Prescribe prophylaxis for venous thromboembolism (VTE) for patients with additional risk
factors for VTE e.g history of VTE. See details under coagulation disorders section 3.5
• Monitor hydration status, warmth and give analgesia as needed after delivery.
• Assess and manage neonatal opioid dependency and withdrawal all infants with history of
in utero opioid exposure.

Pharmacological Treatment.
A: acetylsalycylic acid (PO) 75mg 24hourly, starting from the second trimester to reduce
the risk of pre-eclampsia.

SCD emergency conditions


Acute chest syndrome
• Life threatening – admit the patient in a high dependency unit or ICU,
• Diagnostic criteria – respiratory distress (fast breathing, SPO2<95% on air) and/or pleuritic
pain, cough, fever, tachycardia, infiltrates on CXR,
• Investigations – arterial blood gases, creatinine, electrolytes, ALT, FBP, malaria test, blood
and urine culture and sensitivity, CRP, CXR, HPLC,
• Management – Give supplemental oxygen to maintain SPO2>95%, analgesia for pain
relief, fluids per hydration protocol, broad spectrum antibiotics while awaiting culture and
sensitivity results, top up blood transfusion or exchange transfusion if expertise available.
Acute anaemia
• Haemoglobin < 5g/dl or recent acute drop in Hb >2g/dl below steady state.
• Causes – infection, splenic sequestration, haemolytic crisis and aplastic crisis.
• Investigations – do FBP, reticulocyte count, creatinine, bilirubin, ALT, LDH, malaria test,
urine and blood culture and sensitivity, blood grouping and cross-matching,
• Management – immediately transfuse packed red cells 10mls/kg over 4hours, repeat
transfusion as needed as per transfusion protocol, treat the underlying cause, document
size of liver and spleen.
Stroke
• See management details under central nervous system chapter,
• Exchange transfusion or top up transfusion to prevent recurrent stroke.

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3.1.4 G6PD Deficiency
G6PD is an inherited X-linkded recessive genetic disorder, haemolysis results from oxidative
damage to RBCs due to loss of protective effect of the enzyme G6PD.

Clinical presentation
• Usually asymptomatic but liable to haemolysis (acute anaemia) if infection, incriminated
drugs (e.g. sulphonamides, chloroquine, primaquine or proguanil). or foods (e.g. fava
beans) are taken.
• Pallor,
• Jaundice and
• Dark urine (Coca-colored urine)

Investigations:
• FBP, peripheral smear, reticlocyte count,
• Methaemoglobin reduction (G6PD) test.

Pharmacological Treatment
A: folic acid (PO) 5mg 24hourly for 1 to 3 months.
AND
B: Transfusion of packed red blood cells in severe anaemia. Give 10ml/kg body weight.
Then assess the level of haemoglobin and clinical presentation.

3.1.5 Aplastic Anaemia (Bone Marrow Failure)


Aplastic anaemia is defined as pancytopenia resulting from aplasia of the bone marrow. it can be
inherited (Fanconi anaemia) or acquired (idiopathic, chemical or drug induced). It is one of
haematological emergency.

Clinical presentation
Vary with severity but include;
• Anaemia, easy bruising/bleeding, recurrent infection;
• splenomegaly is not a feature.

Diagnostic Criteria
• Pancytopenia,
• Bone marrow hypocellularity of < 30% hematopoietic cells.

Investigations
• FBP, peripheral smear, reticulocyte count,
• Viral screening (HIV, Hepatitis B and C),
• Bone marrow aspiration and trephine biopsy.

Pharmacological Treatment
Supportive treatment
B: blood transfusion (preferred irradiated, leucodepleted) when Hb<7g/dl
OR
S: platelet transfusion if bleeding or if platelet count is <10 X109/L. see dosage under
blood transfusion section 3.6
AND
Prophylactics antibiotics, hygiene, isolation of the patient, and use of masks to prevent neutropenic
sepsis in patients with ANC of less than 0.5 X 109/L.

Note
Culture and sensitivity in patients with neutropenic sepsis. Refer to management of neutropenic
sepsis under malignant diseases chapter.

Definitive treatment
Allogeneic haematopoietic stem cell transplantation is indicated in patients younger than 45yrs.
Immunosuppressive Therapy
S: anti-thymocyte globulin (ATG) (IV) 40mg/kg/daily 4-10days

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AND
S: cyclosporine (PO)2-10mg/kg/day 12hourly for 6-24months
AND
S: eltrombopag (PO): Children <5years; 2.5mg/kg 24hourly, 6-11years; 75mg 24hourly, >12
years; 150mg 24hourly for 6months

For patients who develop cyclosporine toxicity (nephrotoxicity, hypertension, gingival hypertrophy
and hirsutism), the following drugs may be used although the response rate is low.
D: methylprednisolone (PO) 5–10mg/kg for 3–14days
OR
S: cyclophosphamide (IV) 45mg/kg /day for 4days
OR
S: danazol (PO) 5mg/kg/day for 6months

Note
Give supportive therapy and refer patients to higher health facility with adequate expertise and
facilities.
Monitor blood counts bi-monthly for outpatients, and as needed for admitted patients.

3.1.6 Myelodysplastic syndrome (MDS)


Pre-malignant condition, primarily disease of the old people.

Investigations: similar to aplastic anaemia, plus analysis of 5q deletion.

Pharmacological treatment
B:blood transfusion for symptomatic treatment
AND
S: azacitidine (SC) 75mg/m2 24hourly for 7days, repeat after every 28days

3.2 Bleeding Disorders


3.2.1 Hereditary Bleeding Disorders
Hereditary bleeding disorders includes haemophilia A and B, Von Willebrand disease
3.2.1.1 Haemophilia
Haemophilia is an inherited, X-linked lifelong bleeding disorder which affects males almost
exclusively.

Clinical presentation
• Spontaneous muscle and joint bleeding without injury,
• Prolonged bleeding after injury,
• Epistaxis and easy bruising.
• Complication includes arthropathy and disability.

Haemophilia A (Factor VIII deficiency)


Is the most common of the hereditary clotting factor deficiencies and are caused by deficiency of
factor VIII.

Haemophilia B (Factor IX deficiency)


• It is caused by deficiency of clotting factor IX
• Presentation as in Haemophilia A, this is less common 20%.

Classification of Haemophilia
Haemophilia is classified as mild, moderate or severe according to the levels of circulating factor VIII
or IX and indicates the expected frequency of bleeding.

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Table 3.3: Classification of Haemophilia

Classificati Haemophilia A Haemophilia B Clinical features


on Factor VIII Factor IX level
level
Severe <1% of normal ≤ 1% of normal • Spontaneous haemorrhage
≤ 0.01 U/ml ≤ 0.01U/ml • Frequent spontaneous haemarthrosis
Moderate 2-5%of normal • Haemorrhage secondary to trauma or
0.01-0.05 U/ml surgery
• Occasional spontaneous
haemarthrosis
Mild 5-40%of 5-40% of normal • Haemorrhage post trauma or surgery
normal • Rare spontaneous

Investigations
• Prolonged aPTT but normal PT and Platelets counts
• Confirm by factor VIII or IX assay

Non-pharmacological Treatment
• Avoid I.M injections and use small gauge needles if necessary
• Inform the patient and parents thoroughly on the problem, and provide means of alerting
other medical/pharmaceutical personnel
• Genetic counselling
• For Acute Bleeding episodes (RICE): Rest, Ice/cold pack – 5 minutes on, 10 min off,
Compression and Elevate the joint.
For haemarthrosis – AVOID incising or aspiration of the affected joint. Treat by replacing the
specific factor e.g factor 8 or 9 concentrate if available or FFP (10 - 15ml/kg), joint support and tabs
Paracetamol for pain.

Pharmacological Treatment
Avoid use of NSAIDs, instead use paracetamol

Haemophilia A (Factor VIII Deficiency) no Inhibitor


Dose depends on bleeding severity
Minor bleed:
S: Factor VIII (IV) 20–40IU/kg.
Major bleed:
S: Factor VIII (IV) 50–100 IU/kg 12hourly for 3-5days or until bleeding stops

Expected response: 1IU/kg = 2% rise in factor VIII level


Half life Factor VIII: 8–24hours

Haemophilia B (Factor IX deficiency) no inhibitor


Dose depends on bleeding severity
Minor bleed:
S: Factor IX (IV) 20-50IU/kg
Major bleed:
S: Factor IX (IV) 100IU/kg

Expected response: 1IU/kg= 1.5 rise in the factor IX level


Half-life Factor IX: 16–24 hrs
D: Fresh frozen plasma (FFP) can be used where factor concentrate is unavailable.
Average dose 10-15mls/kg

Note
• If there is no response to appropriate replacement therapy tests for inhibitors (an inhibitor is
formed when one develops antibodies against factor concentrates)
• Detection of inhibitor is by aPTT mix study and confirmed by Bethesda assay (BU)

Factor VIII Inhibitor Management Options


• High dose factor concentrate infusion
• Use by-pass agent like FEIBA (Factor Eight Inhibitor By-passing Agent)

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• Immune tolerance induction therapy (ITI)
• In case of emergency surgery consider plasmapheresis
• Adjuvant antifibronolytic agents eg Tranexamic acid can used with either of the above

Note
• All patients suspected with haemophilia A or B refer to higher facility with adequate expertise
or consult haematology Unit.
• Children with severe haemophilia are recommended to be on low dose prophylaxis of factor
concentrate
• Male circumcision should be done at a hospital where factor concentrate is available.
Concentrate should be given before and after the procedure.

3.2.2 Von Willebrand Disease (VWD)


Von Willebrand Disease is inherited disease due to deficiency of vWF. It is the commonest bleeding
disorder in the population especially in women.

Clinical presentation
• History of easy bruising,
• Menorrhagia
• Gum bleeding
• Joint bleeding in severe cases

Investigations
• Confirmatory test: VWF level assay.
• PT, aPTT, and platelet count are normal except in severe cases.

Pharmacological Treatment
C: etamsylate (PO) 500mg 8hourly until the bleeding stop
OR
C: tranexamic acid (PO) 500mg 8hourly until bleeding is stopped.

If no response
S: Desmopresin (IV) 0.3µg/kg IV stat. Max. Dose20µg.

Note:
• Patient unresponsive to DDVAP may be treated with virus-inactivated vWF containing
FVIII concentrate.
• Never give Etamsylate or Tranexamic acid to patients bleeding per urethral

3.2.3 Acquired Bleeding Disorders/Platelet Disorders


3.2.3.1 Disseminated Intravascular Coagulation (DIC)
Clinical features
• Usually are related to the underlying disorder.
• Bleeding manifestation,
• Extensive organ dysfunction,
• Shock, renal cortical ischemia, coma, delirium and focal neurological symptoms.
Pharmacological Treatment
Rapid and appropriate treatment of the underlying disorder including;
• Antibiotics for infection,
• Surgical debridement of necrotic tissues,
• Chemotherapy for malignant causes,
• Evacuation of dead fetus;
• Platelets transfusion for thrombocytopenia,
• Fresh frozen plasma (FFP) for coagulation factor depletion.
• Monitor prothrombin time (PT), international normalized ratio (INR), activated partial
thromboplastin (aPTT), platelet count and fibrinogen.

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Note: If patient is not bleeding Platelets concentrate is contraindicated. If DIC is severe enough to
cause multiorgan dysfunction, management in an intensive care unit is required.
3.2.3.2 Idiopathic Thrombocytopenic Purpura (ITP)
Clinical features:
• long history of Purpura, menorrhagia, epistaxis and gingival haemorrhage.
• Intracerebral haemorrhage occurs infrequently but is the most cause of death
• overt bleeding is rare unless thrombocytopenia severe (less than 10 X109/L)
Note
A palpable spleen strongly suggests that ITP is NOT the cause for thrombocytopenia.

Non-pharmacological Treatment
• Patients with platelet counts over 50 X109/L usually do not have spontaneous bleeding and
may undergo invasive procedure.
• Emergency treatment of acute bleeding caused by severe thrombocytopenia need
immediate platelet transfusion

Pharmacological Treatment
A: prednisolone (PO) 1mg/kg/day for 3–6 weeks, then taper 10mg weekly (For all patients
with platelet counts below 30 X109/L)
OR
B: dexamethasone (IV) 40mg in 500ml Normal saline running for 4hours once a day for
4days.

If no response;
S:human Immunoglobulin G (IV) 0.4g/kg/day for 5days,
OR
S:human Immunoglobulin G (IV) 1g/kg/day for 2days followed by immediately platelets
transfusion
3.3 Coagulation Disorders
Venous thromboembolism (VTE) is a common disorder that comprises deep vein thrombosis (DVT)
and pulmonary embolism (PE). In most cases, pulmonary embolism arises from proximal deep vein
thrombosis i.e. popliteal, femoral or iliac veins in at least 90%.

3.3.1 Deep Vein Thrombosis (DVT)


Clinical presentation
• Leg pain, tenderness and swelling.
• A palpable cord representing thrombosed vessels.
• Discoloration, venous distention and prominence of superficial veins and cyanosis.
• The clinical diagnosis of DVT is highly nonspecific.

Investigations
• D-dimer,
• Doppler USS,
• PT, INR, Aptt

Pharmacological Treatment
Long term anticoagulation is required to prevent a frequency of symptomatic extension of
thrombosis and/or recurrent venous thromboembolic events. Warfarin is started with initial
unfractionated heparin or enoxaparine therapy and then overlapped for 5days.

C: warfarin (PO) 5mg 24hourly for 5days, then adjust the dose according to INR
levels for 3-6 months.
AND

72
S: Low Molecular weight heparin (SC)1mg/kg 24hourly for 5days
OR
S: Unfractionated heparin (IV) by 75units/kg followed by continuous infusion of
18units/kg/hrs.

Adolescents or children: loading dose 75units/kg then 15–25 Units /kg/hr by IV infusion or
250units/kg 12hourly by SC injection.

S: rivaroxaban (PO) 15mg 12hourly for 21days, then rivaroxaban (PO) 20mg 24hourly for
the remaining duration of treatment.

Pregnant women
Warfarin is teratogenic, therefore low molecular weight heparin is recommended during pregnancy.
D: Low Molecular weight heparin (SC) 1mg/kg 12hourly for the whole duration of treatment.

3.3.2 Pulmonary Embolism (PE)


It is a medical emergency.
Clinical presentation
• Transient dyspnea and tachypnea in the absence of other clinical features
• Pleuritic chest pain, cough, haemoptysis, pleural effusion, and pulmonary infiltrate
• Severe dyspnea and tachypnea and right-side heart failure
• Cardiovascular collapse with hypotension, syncope, and coma
• Several less common and nonspecific presentation including unexplained tachycardia or
arrhythmia, resistant cardiac failure, wheezing, cough, fever, apprehension and confusion.

Investigations
• PT, INR, aPTT, D-dimer, CXR and CT angiography

Pharmacological Treatment
Treat as Deep Vein Thrombosissection 3.3.1

Note
• Warfarin therapeutic INR ranges from 2 to 3 for VTE, and 2.5 -3.5 for patients with
mechanical heart valves
• Warfarin therapy should be monitored by INR after 5–7 days of treatment, then as needed
throughout the duration of treatment.
• If the cause of VTE is acquired thromboembolism, treatment lasts for 3-6 months, BUT if the
cause is inherited thrombophilia, treatment is lifelong.
• Warfarin interacts with many drugs therefore precaution should be taken when administered
with other drugs.
• If warfarin overdose/toxicity occurs, stop warfarin and give FFP 10-15mls/kg and vitamin K
5mg IV stat. Reinitiate warfarin after bleeding has stopped and INR is within therapeutic
range, using the lower dosage.
• For VTE prophylaxis in bedridden patients, give enoxaparin 40mg SC OR Rivaroxaban
10mg orally once a day until ambulation resume.
• Unfractionated heparin should be monitored by aPTT before and during treatment.

3.4 Blood Transfusion


Blood components
A single donation of blood can be separated into several blood components. Currently in Tanzania
the following blood components are available for transfusion: packed red blood cells, Fresh Frozen
Plasma, single unit platelet (plasma rich) and whole blood units.

I. Whole blood
One unit contains 450mls of blood. It is poor in platelets and clotting factors and can be stored
for 35days at 2-6°C.
Indications: Exchange transfusion, open heart surgery, and in the absence of PRBCs in
patients with acute blood loss and hypovolaemia.

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II. Packed red blood cells (PRBCs)
It can be stored for 35days at 2-6°C. One unit increases haemoglobin (Hb) level by approximately
1g/dl in adult, whereas in children, a dose of 10-15mls/kg will increase the Hb by about 3g/dl.

Indications: acute blood loss, exchange transfusion, cardiac patients with Hb level <8g/dl, chronic
symptomatic anaemia with Hb <5g/dl, preoperative patients with Hb level <8g/dl, pre-radiotherapy
patients with Hb level <10g/dl, pre and post chemotherapy patients with Hb <9g/dl, and patients
admitted to ICU with Hb <7g/dl.

III. Platelets
A single random donor platelet (RDP) from one whole blood unit and contains about 5.5X109/L
platelets in 50ml unit. It is stored at room temperature (20-24°C) and has a life span of 5days.
Dosage: 50mls per 10kg i.e 5-6 RDP units in adults. In infants < 10kg, the dose is 5mls/kg, one
adult therapeutic dose increases platelet counts by approximately 20-40 X109/L.

Indications
• Therapeautic: thrombocytopenia of platelet counts< 50X109/L with clinical evidence of
bleeding.
• Prophylactic in patients with platelet counts of: <10 X109/L, <20X109/L with additional risk
factor of bleeding, <50X109/L and planned for minor surgery, <100X109/L with multiple
injuries, or microvascular bleeding, or planned for major surgery. Also, in massive
transfusion to maintain a platelet count of >50X109/L.

Contraindications: Absolutely contraindicated in heparin induced thrombotic thrombocytopenia


(HITT) and thrombotic thrombocytopenic purpura (TTP). Relatively contraindicated in idiopathic
thrombocytopenia (ITP) unless a life-threatening bleeding is anticipated.

IV. Fresh frozen plasma (FFP)


FFP prepared from one unit of whole blood contains about 200-300mls of plasma. It is stored at -
18°C and contains all clotting factors in physiological levels except factors V and VIII which are
present in slightly reduced amount. It has a life span of 12 months. Thaw FFP in water bath at 30-
37°C and transfuse within 30 minutes after thawing. It expires 24 hours after thawing.

Dosage: 10-20ml/kg, approximately 4-6 units for adult, this will raise a minimum of 30% of plasma
clotting factors.

Indications: haemophilia if factor concentrates not available, patients with significant coagulopathy
eg DIC, Vitamin K deficiency and massive transfusion, thrombotic thrombocytopenic purpura (TTP)
or haemolytic uremic syndrome (HUS) as top up or exchange plasma transfusion, scoline apnoea,
haemorrhagic disease of the newborn.

Investigations
• Before transfusion:FBC, ABO and Rh-blood grouping and crossmatch (cross matching not
needed for platelets and FFP transfusion),
• If transfusion adverse reaction occurs: Assess for haemolysis (FBC, peripheral smear,
direct antiglobulin test, serum bilirubin, serum LDH), re-grouping and crossmatch, other
tests depending on the type of transfusion reaction.

Types of blood transfusion

I. Acute simple/episodic transfusion


Used in management of symptomatic patients with anaemia or bleeding tendencies

II. Chronic/top up transfusion


Used as prophylactic to prevent complications, eg. In patients with sickle cell anaemia (SCA)

III. Exchange blood transfusion


Used in management of severe neonatal jaundice, in patients with SCA with acute chest syndrome,
suspected acute stroke or transient ischaemic attack.

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IV. Massive blood transfusion
Transfusion of blood volumeto patient equivalent to his/her total blood volume in less than 24 hours,
or 10 units or more in 24 hours. Administer in parallel a 1:1:1 ratio of 6 Units of RBCs, 6 Units of FFP
and 6 Units of Platelets. The target is to achieve 1:1:1 ratio over 6 hours. Aim the PT, PTT <1.5x
control mean, fibrinogen >1 g/L, target platelet > 100x109/L if pts has CNS trauma, eye and >
50x109/L for other type of injuries.

Plasma Derived Medicinal Products (PDMPs) available from commercial outlets


• Haemosolvate factors VIII and IX used in management of haemophilia
• Immunoglobulins used in immune-mediated conditions
• Albumin used in management of hypovolaemia, hypoalbuminaemia and in therapeautic
plasma exchange.

Therapeautic phlebotomy
Indications: Polycythemia, and in hereditary iron overload.

Table: 3.4 Adverse effects of blood transfusion


Reaction Transfusion Management
Acute Acute haemolytic Stop transfusion, supportive care to maintain hemodynamics.
immunologic transfusion reaction Regroup and crossmatch donor and recipient’s samples.
reactions Assess for haemolysis.
Allergic reactions Stop transfusion, administer antihistamine eg
Chlorphenamine 4mg PO as needed +/- steroid eg
Hydrocortisone 100mg IV stat, resume transfusion if
symptoms subside. If anaphylactic reaction, add
vassopressors eg epinephrine and supportive care.
Febrile non-haemolytic Stop transfusion, administer antipyretics A: Paracetamol 1g
transfusion reaction PO as needed+/- steroid eg Hydrocortisone 100mg IV stat,
resume transfusion if symptoms subside
Transfusion-related Stop transfusion, oxygen supplementation and mechanical
acute lung injury ventilation if required.
(TRALI)
Transfusion associated Supportive care
graft-versus-host
disease (TA-GVHD)
Delayed Delayed hemolytic Symptomatic treatment, request extended cross match for
immunologic transfusion reaction additional transfusions.
reactions Post-transfusion Self limiting,
purpura S: IV immunoglobulin 0.4g/kg/day IV for 5days or plasma
exchange may be needed in severe cases.
Acute non- Transfusion-related Stop transfusion, administer diuretics, manage as cardiac
immunologic circulatory overload failure. See details under cardiovascular diseases chapter.
reactions (TACO)
Bacterial contamination Stop transfusion, antibiotics and supportive care

Delayed non- Infectious disease Manage the infection accordingly eg HIV, Hepatitis B & C.
immunologic transmission see details under respective chapters
reactions
Iron overload Iron chelation with deferroxamine

Blood transfusion in Jehovah’s witness


• Blood transfusion is a medical treatment, and therefore patients have the right to refuse
treatment.
• Inform the patient of the benefits and risks of transfusion.
• Enable the patients to understand the consequences of not receiving blood.
• Inform the patients of any alternatives to transfusion available eg autologous transfusion
and plasma derived medicinal products.
• Guarantee strict clinical confidentiality

75
Haematological malignancies
Include the following;
• Leukaemia – acute and chronic leukaemia
• Lymphomas – Hodgkin’s and Non-Hodgkin’s lymphoma
• Multiple myeloma
These are discussed in details under malignant disease chapter.

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CHAPTER FOUR
NOTIFIABLE DISEASES

Notifiable Diseases, conditions and events usually pose a great public health threat, with a potential
of international spread. They require immediate notification by health personnel (clinical, laboratory,
environmental, etc.), to health authorities, as required by the International Health Regulations (IHR
2005). Notification is mandatory, in order to ensure prompt and effective response, to avoid further
spread and to prevent deaths.

Note:
• Immediately notify the Public Health Authorities using the electronic reporting system for
priority diseases, i.e. the electronic Integrated Disease Surveillance and Response (e-
IDSR) System
• Ensure that the disease, condition or event is recorded in the Health Facility e-IDSR
reporting booklet
• Manage patients on site, in an isolation ward/room or an established isolation centre
• Use Personal Protective Equipment (PPE) before attending a suspected patient
• Strictly apply principles of IPC during patient management and waste disposal

4.1 Bacterial Infections


4. 1.1 Cholera
Cholera is an acute gastrointestinal infection caused by Vibrio cholerae. Infection occurs through
ingestion of contaminated water or food by Vibrio cholerae leading to severe diarrhoea and emesis
associated with body fluid and electrolyte depletion.

Note
Rational approaches to case management of cholera with oral and intravenous rehydration therapy
have reduced the case fatality of cholera from more than 50% to much less than 1%. When a case
of cholera is suspected at home, advise to rehydrate the patient using ORS if available while
preparing to take the patient to the nearest health facility or Cholera Treatment Centre

Clinical Presentation
• A sudden onset of painless watery diarrhoea that may quickly become severe with profuse
watery stool, vomiting, severe dehydration and muscular cramps, leading to hypovolemic
shock and death

Case Definition
• Suspected cholera case: In areas where a cholera outbreak has not been declared: Any
patient aged two years and older presenting with acute watery diarrhoea and severe
dehydration or dying from acute watery diarrhoea
• In areas where a cholera outbreak is declared: any person presenting with or dying from
acute watery diarrhoea
• Confirmed cholera case: A suspected case with Vibrio cholerae O1 or O139 confirmed by
culture or PCR (Polymerase Chain Reaction).

Laboratory Investigation
• Specimen: Liquid stool or rectal swab
• Diagnostic test: Isolate V. cholerae from stool culture and determine O1 serotype using
polyvalent antisera for V. cholerae O1. If desired, confirm identification with Inaba and
Ogawa antisera.
• If specimen is not serotypable, consider, V. cholerae O139
• Antibiotic Susceptibility Testing before provision of antibiotics; Follow up 48 -72 hours
after antibiotic initiation

Note
• For confirmation at the beginning of an outbreak, rectal swab or stool specimen should
be taken from first 5 to 10 suspected cases.
• If any are positive, every tenth case will be sampled for specimen throughout the

77
outbreak
• Manage a suspected cholera case in an isolation ward or in an established Cholera
Treatment Centre

Prevention
• Drink treated or boiled water from safe sources (taps, decontaminated deep wells, bottles)
• Boil water or treat to kill bacteria and make it safe for drinking and for other domestic uses
• Wash hands with liquid soap and running water after visiting the toilet, before preparing
foods, and before eating
• DO NOT eat uncooked food from the street and do not eat cooked food that is no longer
hot
• DO NOT eat street prepared fruits. Always eat home prepared fresh fruits

Management
Pharmacological Treatment
Cholera requires immediate treatment because the disease can cause death within hours. There are
three elements of treatment: Rehydration, Antibiotic Treatment, Zinc and Folic Acid Supplements.

i. Rehydration
• Assess the patient's level of dehydration as per National Guidelines for Prevention and
Control of Cholera. It is of paramount importance to make correct diagnosis and administer
the right treatment.
o plan A: No dehydration,
o plan B: Moderate dehydration and
o plan C: Severe dehydration.

For Severe dehydration:


• Administer intravenous (IV) fluid immediately to replace fluid deficit; Use Ringer Lactate
solution or, if that is not available, 0.9% sodium chloride solution. Give 100 ml/kg IV in 3
hours, 30 ml/kg as rapidly as possible (within 30 min) then 70 ml/kg in the next 2.5 hours.
• After the initial 30 ml/kg has been administered, the radial pulse should be strong and
blood pressure should be normal. If the pulse is not yet strong, continue to give IV fluid
rapidly. Administer ORS solution (about 5 ml/kg/hour) as soon as the patient can drink, in
addition to IV fluid.
• If the patient can drink, begin giving A: oral rehydration salt solution (ORS) by mouth while
the drip is being set up; ORS can provide the potassium, bicarbonate, and glucose that
saline solution lacks.

Note
When using 0.9% sodium chloride solution there is a possibility of hyper-metabolic Acidosis causing
kidney injury

ii. Antibiotic treatment

Antibiotic treatment to patients with severe dehydration is as follows:


Adults (Not for pregnant women)
A: doxycycline (PO) 300 mg or 5mg/kg stat then 200mg (PO) 12 hourly for 7 days
OR
A: ciprofloxacin (PO) 1g stat then 15mg/kg 12 hourly for 7 days or 500mg (PO) 12 hourly
for 7 days
OR
A: azithromycin (PO) 500mg once a day for 7 days

Expectant mothers:
A: erythromycin (PO) 500mg 8 hourly for 7 days

Children:
A: erythromycin syrup (PO) 12.5mg/kg 6 hourly for 5 days
OR
A: Azithromycin 250mg (PO) once a day for 7 days

78
For adolescents:
A: ciprofloxacin (PO) 12mg/kg2 times for 5 days
OR
A: doxycycline (PO) 300mg as stat or 5mg/kg (PO) stat
OR
A: azithromycin (PO) 500mg once a day for 7 days

Note
• Ciprofloxacin was previously contraindicated to children under 12 years. Recent studies
have shown it to be safe for use in children
• Start feeding 3-4 hours after oral rehydration begins. Preferably, give antibiotics with food
to minimize vomiting

For moderate Dehydration


• Give oral rehydration, approximately 75-100ml/kg in the first four hours
• Reassess after four hours; if improved, continue giving WHO based ORS, in quantity
corresponding to losses (e.g. after each stool) or 10 to 20ml/kg. If not improved, treat as
severe dehydration.

If no signs of dehydration
• Patients who have no signs of dehydration when first observed can be treated at home
• Give these patients ORS packets to take home, enough for 2 days
• Demonstrate how to prepare and give the solution
• Instruct the patient or the caretaker to return if any of the following signs develop;
increased number of watery stools repeated vomiting or any signs indicating other
problems (e.g. fever, blood in stool)
For each loose stool or vomiting give;
• 50-100 ml (¼ - ½ cup) of ORS solution for a child less than 2 years old.
• 100-200 ml for older children. Adults can take as much as they want

Note
Prophylactic treatment of cholera contacts with antibiotics is not recommended. Routine treatment of
a community with antibiotics, or mass chemoprophylaxis, has no effect on the spread of cholera, can
have adverse effects by increasing antimicrobial resistance and provides a false sense of security.

iii. Zinc and Folic Acid Supplements


• Zinc (PO) 20mg once daily decreases diarrhea and shortens the duration of illness in
children with cholera.
• Provide zinc supplementation, at a dosage of 20 milligrams per day for children older than
six months or 10 mg per day for those younger than six months, for 10–14 days.
• Folic acid (PO)2.5mg once daily for children < 6 months, or 5mg once daily for children >6
months for the duration of the treatment. For Pregnant women use Folic acid (PO) 5mg
once daily for the duration of the treatment.

Public Health Control Measures


• Establish treatment centre in locality where cases occur. Treat cases onsite rather than
referring them to treatment centers elsewhere.
• Initiate a line listing of suspected and confirmed cases and ensure laboratory results are
linked with cases
• Strengthen case management
• Mobilize community early to enable rapid case detection and treatment.
• Work with community leaders to limit the number of large gatherings, if seen mandatory,
establish by-laws
• Ensure availability and continuous access to clean and safe water.
• Promote safe preparation of food, including fruits, and vegetables
• Promote safe disposal of human waste.
• Ensure adequate collaboration with various sectors including water and sanitation to
ensure appropriate interventions are addressed.

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Note
Cholera Vaccine is available however its utilization must be accompanied with strategies to
improve water and sanitation

4.1.2 Anthrax
Anthrax is a bacterial disease caused by the spore forming Bacillus anthraces, a gram positive, rod-
shaped bacterium. It is a zoonotic disease whereby man is infected directly through contact with
infected hides or inhalation of spores in the lungs or ingestion of infected meat. It can be manifest on
the skin (Cutaneous Anthrax) in the lungs (Pulmonary / Inhalation Anthrax), and/or intestinal
(Gastrointestinal Anthrax and Oropharyngeal anthrax) or CNS (Meningeal Anthrax).
Clinical Presentation
Cutaneous Anthrax
• Itching
• Pruritic papule or vesicle
• Characteristic depressed black eschar surrounded by moderate to severe edema
• A malignant pustule,
• Pyrexia

Inhalation Anthrax
Mild inhalation Anthrax
• Cough, Fever, Fatigue, Myalgia, can resemble a viral respiratory illness, Pulmonary and
gastrointestinal signs may occur together

Severe inhalation Anthrax
• Diaphoresis, Stridor, Dyspnea, Hypotension, Acute respiratory distress
These patients may develop sepsis accompanied by cyanosis, shock, and hemorrhagic pneumonia.
Hemorrhagic pleural effusions often develop.

Gastrointestinal Anthrax
• Fever, Abdominal pain, Vomiting, Diarrhea Bloody stool.

Oropharyngeal anthrax
Signs of oropharyngeal anthrax may include Dysphagia with posterior oropharyngeal necrotic ulcers,
Unilateral neck swelling, Cervical adenopathy, Edema, Pharyngitis fever.

Meningeal Anthrax
Hemorrhagic meningoencephalitis that involves both
• Deep brain parenchymal hemorrhagic lesions
• Infection of the cerebrospinal fluid (CSF) in the subarachnoid space

Case Definition
Suspected Case: Any person with acute onset illness characterized by several clinical forms which
are:
• Cutaneous form: Any person with skin lesion evolving over 1 to 6 days from a papular
through a vesicular stage, to a depressed black eschar invariably accompanied by oedema
that may be mild to extensive.
• Gastro-intestinal:Any person with abdominal distress characterized by nausea, vomiting,
anorexia and followed by fever
• Pulmonary (inhalation): Any person with brief prodromal resembling acute viral
respiratory illness, followed by rapid onset of hypoxia, dyspnoea and high temperature,
with X-ray evidence of mediastinal widening
• Meningeal: Any person with acute onset of high fever possibly with convulsions, loss of
consciousness, meningeal signs and symptoms; commonly noted in all systemic
infections, but may present without any other clinical symptoms of anthrax.
AND
Has an epidemiological link to confirmed or suspected animal cases or contaminated animal
products?

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Confirmed case: A confirmed case of anthrax in a human can be defined as a clinically compatible
case of cutaneous, inhalational or gastrointestinal illness that is laboratory-confirmed by:
(a) Isolation of B. anthracis from an affected tissue or site; or
(d) Other laboratory evidence of B. anthracis infection based on at least two supportive
laboratory tests.

Laboratory Investigation
• Isolation of Bacillus anthracis from a clinical specimen (e.g. blood, lesions,
discharges)
• Demonstration of B. anthracis in a clinical specimen by microscopic
examination of stained smears (vesicular fluid, blood, cerebrospinal fluid,
pleural fluid, stools)
• Positive serology (ELISA, Western blot, toxin detection, chromatographic
assay, fluorescent antibody test).
• Detection of nucleic acid by PCR.

Other supporting tests


• Measurement of antibodies or toxin in blood
• Chest X-ray
• Computerized tomography (CT) scan
• Detection of B. anthracis by nucleic acid test (NAT) covering the genes coding for capsule
and virulence factors;

Prevention: Post Exposure Prophylaxis


• A: Initial 10-day exposure: ciprofloxacin (PO)500 mg 12hourly for5 daysor doxycycline100
mg(PO)
12 hourly (or, if pathogens are documented to be susceptible phenoxymethyl penicillin)
may be used
Adults: phenoxymethyl penicillin(PO) 250-500 mg 6 hourly.
Children 1-5 years: phenoxymethyl penicillin(PO)125 mg 6 hourly.
6-12 years: phenoxymethyl penicillin(PO)250 mg6 hourly
48 hours’ exposure:
OR
• S: clindamycin(PO) 150 to 300 mg 6 hourly for 5days
OR
• S: levofloxacin(PO)500 mg 12hourly for5 daysare alternative antimicrobial prophylaxis to
the local population within 48 hours of the initial exposure

Pharmacological Treatment
A: benzylpenicillin(IV)0.6 MU 6 hourly until local oedema subsides then continue with
A: phenoxymethy lpenicillin (IV)250 mg 6 hourly for 7 days

If not responding change to


A: doxycycline(PO)200mg initial dose then 100mg 12 hourly for 7 days
OR
A: ciprofloxacin(PO)500mg12 hourly for 7 days
AND
A: paracetamol(PO)15mg/kg 8 hourly for 5days
In severe forms ADD
Dexamethasone(PO) 0.6 mg/kg per day in divided doses every 8 hours for 4 days

Public Health Control Measures


• Standard infection control precautions (IPC) should be used when managing patients with
particular attention to body fluid spills, as organisms which remain on surfaces may form
spores which are infectious
• Personal protective equipment should be used in situations where there is potential for
splashes and inoculation injuries.
• Mobilize the community for early detection and care.
• Ensure proper burial or cremation (if practiced) of dead bodies (humans and animals)

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• Conduct community education on the disease symptoms and signs, early
reporting/seeking of medical care, disease transmission and prevention, application of
infection prevention and control for home care setting,
• Conduct active search for additional cases that may not come to the health care setting
(older women or small children patients, for example) and provide a door to door
information about prevention and when to seek care.
• Ensure adequate collaboration with other sectors such as livestock, agriculture,
environmental and sanitation, to ensure appropriate interventions are addressed.
• Request additional help from district/regional/national levels as needed

4.1.3 Plague
A zoonotic systemic bacterial infection caused by Yersinia pestis (plague bacillus) usually
transmitted to humans by rodent fleas or by handling an infected animal. There are 3 forms of
plague infection, depending on the route of infection:
• Bubonic plague is the most common, caused by the bite of an infected flea. Y. pestis,
which enters the body at the bite site and travels through the lymphatic system to the
nearest lymph node, replicates itself and causes the lymph node to be inflamed, tense
and painful, turning into open sores with pus.
• Septicaemic plague occurs when infection spreads through the bloodstream, following
untreated bubonic plague causing bleeding, tissue necrosis and shock.
• Pharyngeal and or Pneumonic plague is the most virulent form and is rare. It is
typically caused by spread to the lungs from advanced bubonic plague. Untreated
pneumonic plague can be fatal.

Human to human transmission only occurs with the pneumonic form of plague by infectious
droplets. Incubation period is 2 to 6 days and case fatality rate (CFR) may exceed 50-60% in
untreated bubonic plague and is nearly 100% in untreated pneumonic or septicaemic plague.
However, it is usually <1% with appropriate and timely treatment. Currently, plague is one of the
most important reemerging bacterial zoonoses in the world.

The main risk factor is exposure to infected populations of wild or domesticated rodents and
their fleas in plague endemic areas.

Case Definition
Bubonic Plague
Suspected case; Any person with a very painful swelling of lymph nodes – buboes And Fever (or
history of fever) or at least 3 of the following: headache or chills or generalized or severe asthenia
and consistent epidemiological features, such as exposure to infected animals and/or evidence of
flea bites and/or residence in or travel to a known endemic area within the previous 10 days.

Confirmed case: Any person with suspected case confirmed by isolation of Yersinia pestis from
blood or aspiration of buboes, or specific seroconversion or rapid diagnostic test detecting the Ag F1
in endemic areas

Pneumonic Plague
Suspected case: Anyone, of any age, with coughs of less than 5 days with one of the following
signs: Striated sputum from blood or dyspnea or chest pain and Fever (or history of fever) or at least
3 of the following: headache or chills or generalized or severe asthenia and Epidemiological context
(contact with suspect or confirm pneumonic plague case, etc).
Confirmed caseof pneumonic plague: Any suspected case of plague in which Yersinia pestis has
been isolated in culture
Or Suspect plague case with positive F1 rapid diagnostic test (RDT) and positive PCR or
Seroconversion or increase in IgG antibody titre by 4 to 15 days

Suspicious death of plague: Anyone who died suddenly without apparent cause but with an
epidemiological link to plague established and without biological sampling

Probable case of plague: Any suspected case of plague alive or deceased with F1 rapid diagnostic
test (RDT) Or

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Positive PCR alone

Note:
Human plague remains a public health concern in Tanzania despite its quiescence in most foci for
years, considering the recurrence nature of the disease. Plague hosts comprises about 50% of all
the animals trapped in West Usambara Mountains in north-eastern Tanzania.

Clinical Diagnostic Criteria


• Sudden onset of fever, chills, head and body aches
• Weakness, vomiting and nausea.
• Yersinia pestis is identified by laboratory testing from a sample of pus from a bubo,
blood or sputum.
A specific Y. pestis antigen can be detected by different techniques.

Note:
Differential diagnosis Bubonic plague may be confused with streptococcal or staphylococcal
lymphadenitis, infectious mononucleosis, cat-scratch fever, lymphatic filariasis, tick typhus, tularemia
and other causes of acute lymphadenopathy

Laboratory Investigation
• Aspiration after an injection of 1-2 ml of saline through an 18-22-gauge needle. Suitable
microbiological culture media (e.g. brainheart infusion, broth, sheep blood agar, or
MacConkey agar) should be inoculated with a portion of each specimen.
• Smears should be examined with Wayson or Giemsa stain and with Gram=s stain to show
Small gram-negative and/or bipolar-staining coccobacilli
• smears should also be submitted for direct fluorescent antibody testing (anti-F1 antibody)
• Serological testing - anti-F1 antigen titre by agglutination
• Molecular biological techniques based on PCR and DNA Hybridization

Note
Anti-F1 rapid diagnostic test (RDT) positive alone is not a confirmed case. Culture and PCR tests
need to done at the appropriate facility.

Prevention:
• Inform people of the presence of zoonotic plague and advised to take precautions
against flea bites
• Do not handle animal carcasses and avoid direct contact with infected body fluids and
tissues
• Apply standard precautions when handling potentially infected patients and while
collecting specimens

Vaccination: Not recommended except for high-risk groups (such as laboratory personnel who are
constantly exposed to the risk of contamination, and health care workers).

Pharmacological Treatment
A: streptomycin (IM)30 mg/kg/day (up to a total of 2 g/day) in divided doses, to be
continued for 10 days of therapy or until 3 days after the temperature has returned to
normal.
OR
A: erythromycin (PO) 500 mg (or 12.5 mg/kg) 8 hourly for 14 days
OR
A: doxycycline (PO) 200mg 12 hourly for 14 days

Public Health Control Measures


• Remove trash, food sources, and rat harborages to control rodent populations
• Protect against fleas with insect repellent on skin and clothing
• Conduct environmental flea control in houses, seaports and airports
• Isolate patients with pneumonic plague with precautions against airborne spread until at
least after 48 hours of appropriate antibiotic therapy.
• Always observe the standard infection prevention and control (IPC) measures.

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• Conduct community education on the disease symptoms and signs, early
reporting/seeking of medical care, disease transmission and prevention, application of
infection prevention and control for home care setting,
• Mobilize community to enable rapid case detection and treatment
• Provide chemoprophylaxis using tetracycline (PO) 15-30 mg/kg or chloramphenicol (PO)
30 mg/kg daily in 4 divided doses for 1 week after exposure ceases.
• Ensure adequate collaboration with other sectors such as livestock, agriculture,
environmental and sanitation sectors to ensure appropriate interventions are addressed.

4.1.4 Bacterial Cerebro-Spinal Meningitis


Bacterial epidemics for Cerebro-Spinal Meningitis are commonly caused by Neisseria meningitidis.
Other common bacteria are Haemophilus influenza, Staphylococcus aures and Streptococcus
pneumoniae. Human-to-human disease transmission is via large respiratory droplets from the nose
and throats of infected people. Incubation period is 2 to 10 days. Attack rates are highest among
children aged less than 15 years. Case fatality rates are usually 8-15% among treated patients, and
>70% among untreated cases. Many survivors suffer long-term sequelae including mental
retardation, hearing loss and loss of limb use. Further information on Meningitis for Nervous system
related management

Case Definition
Suspected meningitis case: Any person with a sudden onset of fever (>38.5 °C rectal or 38.0 °C
axillary), and neck stiffness or other meningeal signs and in case of infants, a bulging fontanelle.

Probable meningitis case: Any suspected case with macroscopic aspects of cerebrospinal fluid
(CSF) (turbid, cloudy or purulent); or with a CSF leukocyte count >10 cells/mm3 or with bacteria
identified by Gram stain in CSF; or positive antigen detection (for example, by latex agglutination
testing) in CSF

In infants: CSF leucocyte count >100 cells/mm3; or CSF leucocyte count 10–100
cells/mm3 and either an elevated protein (>100 mg/dl) or decreased glucose (<40
mg/dl) level.

Confirmed meningitis case: Any suspected or probable case that is laboratory confirmed by
culturing or identifying (i.e. polymerase chain reaction) a bacterial pathogen (Neisseria meningitidis,
Streptococcus pneumoniae, Haemophilus influenzae
type b) in the CSF or blood

Clinical Diagnostic Criteria


• Sudden fever
• Neck stiffness,
• Intense headache, nausea and vomiting,
• Altered consciousness and convulsions, Bulged anterior fontanelle (in infants)

Laboratory Investigation
• Lumbar puncture for Cerebrospinal Fluid Analysiswith a median opening pressure
• CSF leukocyte count in episodes with CSF leak–associated meningitis
• CSF Culture and Sensitivity
• Elevated white blood cell count (WBC) in CSF of over 1000 cells/mm3
• Glucose concentration, <1.9 mmol/L
• Ratio of CSF glucose concentration to blood glucose concentration, <0.23;
• Protein concentration
• WBC count, >2000 cells/mLCSF neutrophil count, >1180 cells/mL

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Table 4.1: Cerebrospinal Fluid Analysis Findings
CSF Normal Range Suggestive of Suggestive of Viral
Characteristic Bacterial Meningitis
Meningitis
Colour Clear Cloudy Cloudy
RBC Count None None None
Gram stain Usually Negative
Negative Usually Positive
(60%-90%)
Pressure* 20–30 cmH2O (16–24
mmHg or 2.1–3.2 kPa) Above > 42 cm H2O Normal
with the patient sitting up
Protein 15 to 20.2 milligrams per Above 20.2 Above 20.2 milligrams
deciliter (mg/dL) or 0.15 to milligrams per per deciliter (mg/dL)
0.6 milligrams per milliliter deciliter (mg/dL) ,>2.20 g/L
(mg/mL) ,>2.20 g/L
Glucose 50-75 mg/dL (around 1.9
mmol/L)
Below normal (<1.9 Usually normal or
50 to 75 mg/dL (or greater
mmol/L) below normal
than 2/3 of the blood
sugar level).
Lymphocytic None Positive with Positive with
pleocytosis neutrophilic lymphocytic
pleocytosis pleocytosis
*Measured by recording the height of CSF in the manometer tube with the patient's leg
gently and return the neck to a neutral position with the head supported with a pillow
Use intravenous tubing sets and a ruler to measure cm of pressure if manometer is not
available
Prevention
• Vaccines targeted against N. meningitidis serogroups A or C, or a tetravalent A, C, Y, and
W135 vaccine are useful for immunocompromized children.
• Hib conjugate vaccine is useful for immunocompromized children

Pharmacological Treatment
A: benzathine penicillin(IV/IM) 300,000U/kg/day with a maximum dose of 24MU/day for 10-
14 days, give 4 million units 4 hourly IV in adults and pediatric patients older than 1 month
for 10-14 days.
AND
A: chloramphenicol (IV) 50 to 100mg/kg/day with a maximum dose of 4 g/day give in
divided doses at 8 hourly intervals for 10-14 days.
o Serum concentrations requires monitoring due to chloramphenicol toxicity
o Recommended therapeutic levels include a trough of 5 to 10 mcg/mL and a peak of
10 to 20 mcg/mL

If no improvement in 3 days’ give


• C: ceftriaxone (IV) 2g (50 mg/kg in pediatric patients older than 1 month) 12 hourly for 10-
14 days OR cefotaxime (IV)2 g (50 mg/kg in pediatric patients older than 1 month) 6 hourly
for 10-14 days.
• C: ceftriaxone (IV or IM) 2g for Adults daily for 10-14 days is preferred for patients with
central nervous system involvement
AND
B: dexamethasone (IV/IM) 0.15mg/kg with a maximum dose of 10mg 8hourly for 3 days

Public Health Control Measures


• Mass vaccination within 4 weeks of crossing the epidemic threshold***
• Mobilize community to permit early case detection, treatment, and improve vaccine
coverage during mass vaccination campaigns for outbreak control.
• Conduct community education on the disease symptoms and signs, early
reporting/seeking of medical care, disease transmission and prevention.

85

• Maintain regular collection of 5-10 CSF specimens per week throughout the epidemic
season in all affected districts to detect possible serogroup shift. Distribute treatment to
health centres
• Treat all cases with appropriate antibiotics as recommended by National protocol.

***If a neighbouring area to a population targeted for vaccination is considered to be at risk


(cases early in the dry season, no recent relevant vaccination campaign, high population
density), it should be included in a vaccination programme.

4.1.5 Neonatal Tetanus


A neuromuscular toxin-mediated illness caused by the anaerobic spore-forming soil bacterium
Clostridium tetani. The disease is transmitted when spores enter open wounds (injections, cutting
the umbilical cord) or breaks in the skin. While tetanus may occur in adults, infection primarily affects
newborns. Neonatal tetanus has decreased dramatically in countries with improved maternal
tetanus immunization rates. Maternal and neonatal tetanus is targeted for elimination in the WHO
African Region, aiming to achieve neonatal tetanus incidence rates of less than 1 case per 1000 live
births. Incubation period is 3 to 21 days, with an average of approximately 6 days. Usually occurs
through introduction of tetanus spores via the umbilical cord during delivery through the use of an
unclean instrument to cut the cord, or after delivery by “dressing” the umbilical stump with
substances heavily contaminated with tetanus spores.

Clinical Diagnostic Criteria


• Sudden inability of a newborn to suck/feed between 2nd and 28th day after birth
• Generalized stiffness
• Convulsions

Laboratory Investigation
• Diagnosis is mainly clinical as there are no reliable laboratory tests for confirming tetanus
• Blood counts and blood chemical findings are unremarkable.
• Peripheral leukocytosis may be suggestive

Prevention
• Immunize women of reproductive age with TTCV, either during pregnancy or outside of
pregnancy. This protects the mother and also her baby through the transfer of tetanus
antibodies to the fetus.
• Good hygienic practices when the mother is delivering a child are also important to
prevent neonatal and maternal tetanus.

To be protected throughout life, WHO recommends that an individual receives 6 doses (3


primary plus 3 booster doses) of TTCV through routine immunization.

Non-pharmacological Treatment
• Rigorously cleanse the umbilical stump to stop the production of toxin at the site of
infection

Pharmacological Treatment
A: For children amoxycillin-clavulanate(PO) via Nasal Gastric Tube 20–30 mg/kg/day
divided 8 hourly for 7 days
For Adults amoxycillin-clavulanate (PO) via Nasal Gastric Tube 500mg 8 hourly for 7days
AND
A: metronidazole (PO) 7.5mg/kg for postnatal age ≤7days: Weighing 1200–2000g: 7.5
mg/kg/day(PO) given every 24 hours >2000 g: 15 mg/kg/day (PO) in divided doses every
12 hours. Postnatal age >7days: 1200-2000g: 15 mg/kg/day (PO) in divided doses every
12 hours >2000 g: 30 mg/kg/day(PO) in divided doses every 12 hours for 7 days

For Adults Metronidazole 400mg (PO) 8hourly for 7days


OR
C: ceftriaxone (IV) 2g (50 mg/kg in pediatric patients older than 1 month) 12hourly for
7days
For Adults ceftriaxone(IV) 2g once or in 2 divided doses for 7days

86
OR
C:cefotaxime) (IV) 2g (50 mg/kg) in pediatric patients older than 1 month 6hourly for 5days.
For Adults Cefotaxime 2g (IV) 24hourly or 1g 12hourly for 7days
OR
Immunotherapy to neutralise circulating toxin
B: Administer human antitetanus immunoglobulin TIG, (IM) 100–300IU/kg stat, with the
dose divided into two different muscle masses to the confirmed infected patients (Don’t
give vaccine to the confirmed infected patients)
AND
A: diazepam (PO) 0.5mg/Kg 8hourly as the effective management of muscle spasm,
give a sedative cocktail of ALL the following via NGT:

AND
A: chlorpromazine (PO) 2mg/kg 8 hourly
AND
B: phenobarbitone (PO) 6mg/kg 12 hourly

Table 4.2: Guidelines for Dosage Administration**


Time (hours) 0 3 6 9 12 15 18 21 24
Diazepam * * * * * *
Chlorpromazine * * *
Phenobarbitone * * *
** These are general guidelines. Frequency of drug administration should be titrated vs clinical
condition

• Airway / respiratory control


Provide mechanical ventilation.
• Provide adequate fluids and nutrition, as tetanus spasms result in high metabolic
demands and a catabolic state.

Public Health Control Mesures


The WHO global target for neonatal tetanus elimination is to reduce the incidence of neonatal
tetanus to less than 1 case of neonatal tetanus (NT) per 1000 live births in every district of every
country. To meet the target
• Immunize the mother and other pregnant women in the same locality as the case with at
least 2 doses of tetanus toxoid.
• Conduct a supplemental immunization activity for women of childbearing age in the
locality.
• Improve routine vaccine coverage through IVD and maternal immunization program
activities.
• Educate birth attendants and women of childbearing age on the need for clean cord cutting
and care. Increase the number of trained birth attendants.

4.1.6 Tick-Borne Relapsing Fever (TBRF)


A bacterial infection caused by bacteriaBorrelia duttonii, are known zoonoses transmitted to humans
through the bite of infected “soft ticks” Ornithodoros spp that live within rodent burrows feeding on
the rodent. Humans typically come into contact with soft ticks when they sleep in rodent-infested
cabins.

Common Symptoms
• Recurring episodes of fever, Non-specific headache, Non-specific Muscle pain, Non-
specific Joint pain, Non-specific Chills, Non-specific Vomiting, and Abdominal pain.

Bacteremia tends to be greater among pregnant women, and may sometimes result in more severe
infection. Symptoms tend to develop within 7days after the tick bite. Long-term sequelae of TBRF
are rare but include iritis, uveitis, cranial nerve and other neuropathies.

Clinical Diagnostic Criteria


• Recurring episodes of high fever, headache, muscle and joint aches, and nausea

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• Recurring symptoms, producing a telltale pattern of fever lasting roughly 3 days, followed
by 7 days without fever, followed by another 3 days of fever. Without antibiotic treatment,
this process can repeat several times.

Laboratory Investigation
• Microscopy from the peripheral blood smear will reveal a long and spiral-shaped
bacteriumSpirochetemia (spirochetes in blood) in TBRF patients often reaches high
concentrations (>106 spirochetes/ml). Direct microscopic observation of relapsing fever
spirochetes using dark field microscopy or stained peripheral blood smears

Prevention
• Avoid sleeping in rodent-infested buildings whenever possible. Although rodent nests may
not be visible, other evidence of rodent activity (e.g., droppings) are a sign that a building
may be infested.
• Prevent tick bites. Use insect repellent (on skin or clothing) or permethrin (applied to
clothing or equipment).

Pharmacological Treatment
A: erythromycin(PO) 500mg (or 12.5 mg/kg) 8 hourly for 14days
A: tetracycline(PO)500mg 6hourly for 14days
C: ceftriaxone (IV or IM) 2 grams daily for 10-14days is preferred for patients with central
nervous system involvement

Public Health Control


• Provide public education, awareness, preventive control measures, and avoidance of
areas where infected ticks are most abundant.
• Assessing evidence of rodent activity in and around structures of infected people
• Removal of rodents and their nests
• Reduce tick exposures by removing tick infested structures with an appropriate pesticide
applied by a professional pest control operator who is familiar with the types of “crack and
crevice” treatments used to control cockroaches or other wall-dwelling pests

4.2 Viral Infections


4.2.1 Viral Haemorrhaghic Fevers (VHF)
Viral Haemorrhagic Fever (VHF) is a general term for a severe illness caused by viruses and
sometimes associated with bleeding. Their distribution is dependent on the ecology of reservoir
hosts with a potential to cause life-threatening illness in humans. Diagnosis and management is
challenging due to the non-specificity of early symptoms, limited laboratory facilities in endemic
areas, severity of disease, lack of effective therapy, strict infection control requirements and
propensity to cause epidemics with secondary cases in healthcare workers.

Primary transmission is from animal to human, through contact with an infected animal or its
product. Secondary transmission is from person to person through:
• Contact with a sick person or direct contact with the blood and/or secretions or with
objects, such as needles that have been contaminated with infected secretions of an
infected person.
• Breast feeding
• Sexual contact

Public Health Control measures


• Maintain strict viral haemorrhagic disease (VHD) infection prevention and control (IPC)
practicesthroughout the outbreak.
• Mobilize the community for early detection and care and conduct community education
about how the disease is transmitted and how to implement IPC in the home care setting
and during funerals and burials. Consider social distancing strategies.
• Conduct contact follow-up and active searches for additional cases that may not come to
the health care setting.
• Establish an isolation ward or treatment centre to handle additional cases that may come
to the health centre and ensure strict IPC measures to avoid transmission in health care
settings.

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• Suspected cases should be isolated and treated for more common conditions with similar
symptoms, which might include malaria, typhoid, louse borne typhus, relapsing fever or
leptospirosis. Ensure a barrier is instituted between suspected and confirmed cases.
• Provide psychosocial support for the family, community and staff.
• Consider quarantine for high risk contacts with home support during the incubation period
and ensure daily follow up of their movements.
• There are promising vaccine candidates under development for some VHDs that might be
useful to be used in the event of outbreak in a ring vaccination approach and for health
care workers.
• Treat conservatively the symptoms which might be presented; severe cases require
intensive support care; if dehydrated ensure fluid replacement with fluids that contain
electrolytes.

4.2.1.1 Ebola
Ebola Virus Disease (EVD) is a deadly disease in people and non-human primates. The viruses that
cause EVD are located mainly in sub-Saharan Africa. People can get EVD through direct contact
with an infected animal (bat or nonhuman primate) or a sick or dead person infected with Ebola
virus. Symptoms appear from 2 to 21 days after contact with the virus, with an average of 8 to 10
days.

Case Definition:
Suspected case: Illness with onset of fever and no response to treatment of usual causes of fever in
the area, and at least one of the following signs: bloody diarrhoea, bleeding from gums, bleeding
into skin (purpura), bleeding into eyes and urine.

Confirmed case: A suspected case with laboratory confirmation (positive IgM antibody, positive
PCR
or viral isolation), or epidemiologic link to confirmed cases or outbreak.

Note
During an outbreak, case definitions are likely to be adapted to new clinical presentation(s) or
different modes of transmission related to the local event. In outbreak setting, the following standard
case definitions apply;

Suspected case: Any person, alive or dead, suffering or having suffered from a sudden onset of
high fever and having had contact with: - a suspected, probable or confirmed Ebola case; - a dead
or sick animal
OR
• Any person with sudden onset of high fever and at least three of the following symptoms: -
headaches - lethargy - anorexia / loss of appetite - aching muscles or joints - stomach pain -
difficulty swallowing - vomiting - difficulty breathing - diarrhoea - hiccups;
• OR
• Any person with inexplicable bleeding; OR
• Any sudden, inexplicable death; OR
• A person (alive or dead) suffering or having suffered from a sudden onset of high fever and
having had contact with: a dead or sick animal.

Clinical Diagnostic Criteria


A combination of symptoms suggestive of EVD AND a possible exposure to EVD within 21 days
before the onset of symptoms is suggestive of Ebola.

Symptoms
• Fever
• Aches and pains, such as severe headache, muscle and joint pain, and abdominal
(stomach) pain
• Weakness and fatigue
• Gastrointestinal symptoms including diarrhea and vomiting
• Abdominal (stomach) pain
• Unexplained hemorrhaging, bleeding or bruising
Other symptoms may include red eyes, skin rash, and hiccups (late stage)

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An exposure may include contact with:
• Blood or body fluids from a person sick with or who died from EVD,
• Objects contaminated with blood or body fluids of a person sick with or who died from
EVD,
• Infected fruit bats and non-human primates (apes or monkeys), or
Semen from a man who has recovered from EVD.

Laboratory Investigations
Ebola virus can be detected in blood after onset of symptoms. It may take up to three days after
symptoms start for the virus to reach detectable levels. Investigations includes:
• Blood for RT-PCR
• Antigen detection or IgM (ELISA)

Note
Do not take specimen before wearing appropriate PPE and ensuring the patient is in an Isolation
Ward/ Centre

Pharmacological Treatment
A: paracetamol (PO/IV) 15mg/kg 8 hourly for 3 days
B: Give oxygen and manage hypoglycaemia if present

Fluid and electrolyte balance


A: compoundsodium lactate OR NS intravenously if cannot take fluids orally
B: Give Oxygen therapy to maintain oxygen status.
A: compoundsodium lactate (Ringers Lactate), NS intravenously if cannot take fluids orally.
Provide IV fluids and electrolytes (body salts) through infusion into the vein (intravenously)
A: Manage hypoglycaemia with 5% DNS or 25% Dextrose Solution if hypoglycaemia is
shown by RBG testing
A: Using medication to support blood pressure, reduce vomiting and diarrhea and to manage fever
and pain.
A: Treating other infections or any complicating infection and co-morbid condition
A: Psychological support is given to patient and family
C: Refer for Provision of Mechanical ventilation, renal dialysis, and anti-seizure therapy may be
required.

Prevention
• Isolate person with signs of EVD and has had a possible exposure from other people
• Notify the public health authorities
• Blood samples from the patient should be collected and tested to confirm infection
• Prompt identification of cases, contact tracing, and monitoring of high-risk individuals are
essential to stopping Ebola virus from spreading
• Early recognition of EVD is critical for infection control. However, because early symptoms
are not specific to EVD, it can be hard to distinguish it from other illnesses,
including malaria, leptospirosis, influenza (flu), yellow fever, dengue and other viruses
spread by insects, or viral or bacterial infections of the intestines, like typhoid fever.
• EVD should be considered when clinical illness is combined with an epidemiologic risk
factor, like direct contact with a suspected or confirmed case or travel to an Ebola-affected
area.
• Once a case of EVD is identified, everyone who has come in direct contact with the sick
patient is traced
• Contacts are watched for signs of illness for 21 days from the last day they came in
contact with the Ebola patient. If the contact develops a fever or other EVD symptoms,
they are immediately isolated, tested, and provided care.

4.2.1.2 Marburg Haemorrhagic Fevers


Marburg virus belongs to the family Filoviridae, divided into three genera: ebolaviruses,
marburgviruses, and cuevaviruses. The reservoir host of Marburg virus is the African fruit

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bat, Rousettus aegyptiacus. Fruit bats infected with Marburg virus do not to show obvious signs of
illness. Primates (including humans) can become infected with Marburg virus, and may develop
serious disease with high mortality. The disease can spread rapidly within the health care setting.
The virus enters through broken skin, mucous membrane or exchange of bodily fluids or ingestion,
inhalation and injection of infectious material

Case Definition
Suspected case: Illness with onset of fever and no response to treatment of usual causes of fever
in the area, and at least one of the following signs: bloody diarrhea, bleeding from gums, bleeding
into skin (purpura), bleeding into eyes and urine.

Confirmed case: A suspected case with laboratory confirmation (positive IgM antibody, positive
PCR
or viral isolation), or epidemiologic link to confirmed cases or outbreak.

In an outbreak setting, the following standard case definitions apply;

Suspected case: Any person, alive or dead, suffering or having suffered from a sudden onset of
high fever and having had contact with: - a suspected, probable or confirmed Marburg case; - a
dead or sick animal
OR
Any person with sudden onset of high fever and at least three of the following symptoms: -
headaches - lethargy - anorexia / loss of appetite - aching muscles or joints - stomach pain -
difficulty swallowing - vomiting - difficulty breathing - diarrhoea - hiccups; OR
• Any person with inexplicable bleeding OR
• Any sudden, inexplicable death; OR
• A person (alive or dead) suffering or having suffered from a sudden onset of high fever and
having had contact with a dead or sick animal

Non-Pharmacological Treatment:
Supportive therapy includes:
• Mechanical ventilation, renal dialysis, and anti-seizure therapy may be required.
• Management of complications symptomatically
• Maintaining Oxygen status and Blood Pressure

Pharmacological Treatment
There is no specific treatment for Marburg Haemorrhagic Fever.
A: paracetamol (PO/IV) 15mg/kg 8hourly for 3days
B: Give oxygen and manage hypoglycaemia if present
If there is Fluid and electrolyte imbalance:
A: compound sodium lactate (Ringers Lactate), NS intravenously if cannot take fluids orally
B: Give Oxygen therapy to maintain oxygen status.
A: sodium lactate compound (Ringers Lactate), NS intravenously if cannot take fluids orally. Provide
IV fluids and electrolytes (body salts) through infusion into the vein (intravenously)
A: Manage hypoglycaemia with 5% DNS or 25% Dextrose Solution if hypoglycaemia is shown by
RBG testing
A: Using medication to support blood pressure, reduce vomiting and diarrhea and to manage fever
and pain.
A: Treating other infections or any complicating infection and co-morbid condition
A: Psychological support is given to patient and family
D: Refer for Provision of Mechanical ventilation, renal dialysis, and anti-seizure therapy may be
required.

4.2.1.3 Rift Valley Fever


Rift Valley Fever (RVF) is a viral disease that affects mainly animals and occasionally humans. The
virus is a member of the Phlebovirus genus, one of the five genera in the family Bunyaviridae. The
disease is frequently reported following heavy rainfall and floods. RVF is mainly transmitted from
animals (sheep, cattle, goats, camels) to humans through close contact with infected animals (such
as handling meat and body fluids and consumption of raw milk). During established RVF outbreaks
in animals, humans can also get infected through bites of infected mosquitoes and other biting
insects.

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The incubation period of RVF varies from 2 to 6 days. These symptoms usually last from 4 to 7
days. Most of the infected people recover on their own. However, a small proportion gets
complications such as vomiting blood, nose bleeding and passing bloody stool. Rift Valley fever is
difficult to distinguish from other viral haemorrhagic fevers as well as many other diseases that
cause fever, including malaria, shigellosis, typhoid fever, and yellow fever.

Case Definitions
Suspected case: Early Disease: Acute febrile illness (axillary temperature >37.5 ºC or oral
temperature of >38.0ºC) of more than 48 hours’ duration that does not respond to antibiotic or
antimalarial therapy, and is associated with:
• Direct contact with sick or dead animal or its products AND / OR
• Recent travel (during last week) to, or living in an area where, after heavy rains, livestock
die or abort, and where RVF virus activity is suspected/confirmed AND / OR
• Abrupt onset of any 1 or more of the following: exhaustion, backache, muscle pains,
headache (often severe), discomfort when exposed to light, and nausea/vomiting AND /
OR:
• Nausea/vomiting, diarrhoea OR abdominal pain with 1 or more of the following:
• Severe pallor (or Hb < 8 gm/dL)
• Low platelets (thrombocytopenia) as evidence by presence of small skin and
mucous membrane haemorrhages (petechiae) (or platelet count < 100x109 /
d
• Evidence of kidney failure (edema, reduced urine output) (or creatinine > 150
mol/L) AND / OR
• Evidence of bleeding into skin, bleeding from puncture wounds, from mucous
membranes or nosefrom gastrointestinal tract and unnatural bleeding from
vagina AND / OR
• Clinical jaundice (3-fold increase above normal of transaminases)

Late stages of diseases or complications


(2-3 weeks after onset)
• Patients who have experienced, in the preceding month a flu-like illness,
with clinical criteria, who additionally develop the following:
o CNS manifestations which resemble meningo-encephalitis AND/OR:
o Unexplained visual loss OR
o Unexplained death following sudden onset of acute flu-like
illness with haemorrhage, meningo-ecephalitis, or visual loss
during the preceding month.
Confirmed case:
Any patient who, after clinical screening, is positive for anti-RVF IgM ELISA
antibodies (typically appear from fourth to sixth day after onset of symptoms) or
tests positive on reverse transcriptase polymerase chainreaction (RT-PCR).

Transmission to human is mainly through direct or indirect contact with blood or organs of infected
animals. The virus can be transmitted to human through;
• Handling of animal tissue during slaughtering or butchering, assisting with animal births,
conducting veterinary procedures.
• Inoculation e.g via wound from infected knife or through contact with broken skin or
through inhalation of aerosols produced during the slaughter of an infected animals.
• Infected mosquito.
Human become viraemic; capable of infecting mosquitoes shortly before onset of fever and for the
first 3–5 days of illness. Once infected, mosquitoes remain so for life.

Clinical Diagnostic Criteria


• Acute febrile illness that does notrespond to antibiotic or antimalarial therapy,
• Exhaustion, backache, muscle pains, headache (often severe),
• Photophobia
• Nausea/vomiting
• Evidence of bleeding into skin, bleeding from puncture wounds, from mucous membranes
or nose, from gastrointestinal tract and unnatural bleeding from vagina

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• Clinical jaundice (3-fold increase above normal of transaminases)
Clinical diagnosis is difficult, because RVF symptoms can be mild and non-specific, especially early
in the course of the disease.

Laboratory Investigations
Definitive diagnosis of RVF involves laboratory testing of blood (during illness) or other tissue
samples (postmortem tissue).
• The virus detection in the blood then virus isolation in cell culture
• Molecular techniques (reverse transcriptase polymerase chain reaction or RT-PCR).
• Antibody testing using Enzyme-Linked ImmunoAssay (ELISA) confirms infection with
RVFV
• IgM antibodies reflect a recent infection and IgG antibodies persist for several years
(Detection of anti-RVF IgM suggests an ongoing transmission of RVFV in humans during
inter-epidemic periods.).
• FBC
o Low Hb [Hb<8gm/dL - Severe pallor
o Low platelet < 100 x109 /Dl (Thrombocytopenia) – small skin and mucous
membrane hemorrhages (Petechiae))
• Serum Creatinine

Note
Acute RVF can be diagnosed using several different methods
1. Serological tests such as ELISA may confirm the presence of specific IgM antibodies
to the virus. The virus itself may be detected in blood during the early phase of illness
or in post-mortem tissue using a variety of techniques including, antigen detection
tests by ELISA, RT-PCR, virus propagation (in cell cultures), Immunohistochemistry in
formalin-fixed tissues
2. ELISA IgG can be used for retrospective diagnostic.

Management
Management of RVF in humans is mainly supportive as there is no definitive treatment for RVF.
Early detection and management of the disease is important. Human control of RVF is through
control of the disease in animals through a sustained vaccination program and limiting human-
animal contact. Use of insecticide treated nets and mosquito repellents can also reduce infections in
human. In addition to human suffering and death, RVF has far reaching economic implications to the
Livestock industry. In outbreak settings, the disease manifestation includes non-haemorrhagic
febrile syndromes, and laboratory testing should be considered among persons with milder
symptoms suggestive of viral illness.

Prevention
People living in or visiting areas with RVF shall be protected from the RVF infection with these
steps:
• Protect people from contact with blood, body fluids, or tissues of infected animals. (Use
PPEs like gloves, boots, long sleeves, and a face shield)
• Protect people from unsafe animal products. All animal products (including meat, milk, and
blood) should be thoroughly cooked before eating or drinking.
• Protect people from mosquitoes and other bloodsucking insects. Use insect repellents and
bed nets, and wear long sleeved shirts and long pants to cover exposed skin.

No vaccines are currently available for vaccination in people at risk of RVF infection.

Public Health Control Measures


• Mobilize the community for early detection and care.
• Conduct community education about the confirmed case, how the disease is
transmitted, and how to prevent contact with tissues of infected animals and avoid
mosquito bites.
• Provide information about prevention in the home and when to seek care.
• Provide supportive treatment to all cases identified
• Collaborate with the animal health specialists to search and document cases
among animals as well.

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4.2.1.4 Yellow Fever
Yellow fever virus is an RNA that belongs to the genus Flavivirus and is related to West Nile, St.
Louis encephalitis, and Japanese encephalitis viruses. It is transmitted human-to-human via the
domestic species of Aedes mosquitoes (Urban epidemics) or to humans from primate reservoir via a
forest mosquito species (Sylvatic cycle). About 15% of infections progress to fever and jaundice.
While only the minority of cases are severe, case fatality rate may be 25% to 50% among patients
with syndrome of haemorrhage, jaundice, and renal disease. A small proportion of patients develop
“toxic phase” with jaundice (yellowing of the skin and eyes, hence the name ‘yellow fever’), dark urine
and abdominal pain with vomiting. Bleeding can occur from the mouth, nose, eyes or stomach and
half of those die within 7 to 10 days.

Risk factor: Sporadic cases often linked to occupation or village location near woods or where
monkeys are numerous, also non-vaccinated persons. Infection and disease can be prevented
by vaccination. With a vaccine efficacy > 95% and duration of immunity is life time

Case definition
Suspected case: Any person with acute onset of fever, with jaundice appearing within 14 days of
onset of the first symptoms.

Probable case: A suspected case with one of the following;


• Epidemiological link to a confirmed case or an outbreak
• Positive post-mortem liver histopathology

Confirmed case: A probable case with one of the following;


• Detection of YF-specific* IgM
• Detection of four-fold increase in YF IgM and/or IgG antibody titres between
acute and convalescent serum samples
• Detection of YFV-specific* neutralizing antibodies

*YF-specific means that antibody tests (such as IgM or neutralizing antibody) for other
prevalent flavivirus are negative. This testing should include at least IgM for Dengue and
West Nile and may include other flavivirus depending on local epidemiology.
OR
One of the following
• Detection of YF virus genome in blood or other organs by PCR
Detection of yellow fever antigen in blood, liver or other organs by immunoassays Isolation of the
yellow fever virus

Laboratory Investigations
• ELISA for the presence of yellow fever Specific IgM and IgG antibodies.
• Exclusion of Dengue, West Nile virus and other locally prevalent flavivirus will be
necessary for the confirmation of yellow fever.
• PCR, YF specific seroneutralization, virus isolation or histopathology

Management
Non-Pharmacological Treatment
No specific anti-viral treatment, supportive therapies are recommended. Good and early supportive
treatment for dehydration, liver and kidney failure, and fever improves outcomes. Associated
bacterial infections can be treated with antibiotics

Prevention
Prevention and Control involve mosquito control and provision of Yellow Fever vaccine. The yellow
fever vaccine is safe, affordable and a single dose provides life-long protection against yellow fever
disease.

Indication of Yellow Fever Vaccination


• Persons ≥ 9 months of age
• Planning travel to or residence in an endemic area
• Planning travel to a country with an entry requirement
Needs to be given ≥ 10 days prior to arrival in endemic area

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Contraindications of Yellow Fever Vaccination
• Infants aged less than 9 months;
• Pregnant women – except during a yellow fever outbreak when the risk of infection is high;
• People with severe allergies to egg protein; and
People with severe immunodeficiency due to symptomatic HIV/AIDS or other causes, or
who have a thymus disorder

Public Health Control Measures


• Identify all cases and provide clinical, epidemiological and laboratory evidences
• Identify contacts, screen and test for confirmation
• Educate the communities affected on mosquito control
• Destroy known sources of standing water and any newly discovered sites for the presence
of mosquito larvae.
• Surveillance of Mosquito by Mosquito control professionals

4.2.1.5 Dengue Fever


Dengue virus is an arbovirus transmitted by aedes mosquitoes (both Ae. aegypti and Ae.
albopiticus). Dengue fever is caused by four serologically distinct, but closely related Dengue
viruses: dengue virus (DENV) 1, 2, 3, and 4 of the Flaviviridae family. Dengue fever is an emerging
pandemic that has spread globally during the past 30 years as a result of changes in human
ecology. Dengue haemorrhagic fever (DHF) is a potentially deadly complication that has become a
leading cause of hospitalization and death among children in Asia and Africa. There is good
evidence that sequential infection with the different serotypes of dengue virus increases the risk of
more severe disease that can result in dengue shock syndrome (DSS) and death.

Infected humans are the main carriers and multipliers of the virus, serving a source of the virus for
uninfected Aedes aegypti mosquitoes which maintain the urban dengue transmission cycle. The
virus circulates in the blood of infected human for 2-7 days, at approximately the same time that they
have a fever. A sylvatic transmission cycle has been documented in West Africa where DENV-2 has
been found in monkeys. There is no evidence of person-to-person transmission.

DENV is frequently transported from one place to another by infected travelers; when susceptible
vectors are present in these new areas, there is the potential for local transmission to be
established.

Case Definition
Dengue Fever Suspected case: Any person with acute febrile illness of 2-7 days duration with 2 or
more of the following: headache, retro-orbital pain, myalgia, arthralgia, rash, haemorrhagic
manifestations, leucopenia.

Dengue Fever Confirmed case: A suspected case with laboratory confirmation (positive IgM
antibody, four-fold or greater rise in IgG antibody titres, positive PCR or viral isolation).

Dengue Haemorrhagic Fever: A probable or confirmed case of dengue with bleeding tendencies
as evidenced by one or more of the following: positive tourniquet test; petechieae, ecchymoses or
purpura; bleeding: mucosa, gastrointestinal tract, injection sites or other; haematemesis or melaena;
and thrombocytopenia (100,000 cells or less per mm3) and evidence of plasma leakage due to
increased vascular permeability, manifested by one or more of the following: 20% rise in average
haematocrit for age and sex, 20% drop in haematocrit following volume replacement therapy
compared to baseline, signs of plasma leakage (pleural
effusion, ascites, hypo-proteinaemia).

Dengue Shock Syndrome: All the above criteria, plus evidence of circulatory failure manifested by
rapid and weak pulse, and narrow pulse pressure (≤ 20 mm Hg) or hypotension for age, cold,
clammy skin and altered mental status.

Laboratory Investigations
• Reverse Transcriptase–Polymerase Chain Reaction (RT–PCR)
• Rapid Tests for Dengue NSI antigen
Serological methods, such as Enzyme-Linked Immunosorbent Assays (ELISA) for IgM and IgG
anti-dengue antibodiesFBP

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Management
There is no specific treatment for dengue, but appropriate medical care frequently saves the lives of
patients with dengue haemorrhagic fever.

Non-Pharmacological Treatment
No specific treatment is available for Dengue fever.

Pharmacological Treatment:
A: paracetamol (PO/IV) 15mg/kg 8hourly for 3days
A: Maintainance fluid (Ringers lactate, NS) intravenously if one cannot take enough fluid orally
B: Blood transfusion and clotting factors.
B: Oxygen and manage hypoglycaemia if present

Note
• No antibiotics are of proven value.
• Children below 12 years require close monitoring for dangerous form.
• Steroids should not be used.
Non-Steroidal Anti-Inflammatory Drugs (NSAIDs) such as ibuprofen and aspirin should
be avoided. These anti-inflammatory drugs act by thinning the blood, and in a disease
with risk of hemorrhage, blood thinners may exacerbate the prognosis

Prevention
At present, the only method of controlling or preventing dengue virus transmission is to
combat the vector mosquitoes using environmental management and chemical methods.
• Prevent dengue by avoiding mosquito bites by Aedes. aegypti and Aedes.
albopictus bite during the day and night (Using mosquito repellant, bed nets and
removing reservoirs).
• All four dengue viruses are spread primarily through the bite of an
infected Aedes mosquito.
• A dengue vaccine is available for use in some parts of the world
Public Health Control Measures
• Wear full sleeve clothes and long dresses to cover the limbs
• Use mosquito repellents
• Use mosquito nets – to protect babies, old people and others, who may rest during the
day. Effectiveness of such nets can be improved by treating them with permethrin
(pyrethroid insecticide). Curtains (cloth or bamboo) can also be treated with insecticide and
hung at windows or doorways, to repel or kill mosquitoes

4.2.1.6 Chikungunya Fever


Chikungunya Virus Disease is the arthropod-borne virus caused by Chikungunya Virus (CHIKV),
transmitted by the Aedes aegyptiand Aedes albopictus mosquitos the same which transmit Dengue
virus, West Nile and Yellow Fever viruses. Chikungunya disease (Seroprevalance 7.7% to 26.9% in
Tanzania) does not often result in death, but the symptoms can be severe and disabling. People at
risk for more severe disease include newborns, older adults (≥65 years), and people with medical
conditions such as high blood pressure, diabetes, or heart disease. The word "Chikungunya" is
Makonde for "that which bends up," in reference to the stooped posture of patients afflicted with the
severe joint pain associated with the disease. Epidemics of fever, rash and arthritis, resembling
Chikungunya fever were recorded as early as 1779. However, the virus was first isolated between
1952-1953 from both man and mosquitoes during an epidemic in Tanzania.

Case Definition
Acute clinical case
• Clinical criterion: Fever >38.50 C (101.30F) and joint paina (usually incapacitatingb) with
acute onseta AND
• Epidemiological criterion: resident or visitor in areas with local transmission of
Chikungunya on the last 15 days (suspected case for epidemiological surveillance) b OR
• Laboratory criterion: confirmation by laboratory: PCR, serology or viral culture (confirmed
case for epidemiological surveillance)

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• Usually accompanied by exanthema, myalgia, back pain, headache and, occasionally,
vomiting and diarrhoea (pediatric age group).
• In children aged <3 years, joint pain is expressed as inconsolable crying, irritability,
rejection to mobilization and/or walking

Atypical case
Clinical case of laboratory confirmed Chikungunya accompanied by other manifestations:
neurological, cardiological, dermatological, ophthalmological, hepatic, renal, respiratory, or
haematological, among others.

Severe acute case


Clinical case of laboratory-confirmed Chikungunyapresenting dysfunction of at least one organ or
system that threatens life and requires hospitalization

Suspected and confirmed chronic cases


Suspect chronic case: Person with previous clinical diagnosis of chikungunya after 12 weeks of the
onset of the symptoms presenting with at least one of the following articular manifestations: pain,
rigidity, or edema, continuously or recurrently.
Confirmed chronic case: Every chronic case with a positive chikungunya laboratory test

Laboratory Investigations
Chikungunya is a biosafety level-3 (BSL-3)
• Detection of Chikungunya virus (CHIKV) viral culture of blood in the first 3 days
• RT-PCR for Viral RNA from the serum collected <6 days after onset of illness.
Serological tests show a four-fold rise in antibody titer to Chikungunya virus;
Non-Pharmacological Treatment:
The mainstay treatment for Chikungunya is the supportive symptomatic treatment.
A: Assure plenty of rest to patients

Pharmacological Treatment
A: Maintain body fluids Sodium Lactate Compound (Ringers Lactate) intravenously.
A: Control Fever and Pain by giving paracetamol (PO/IV]15mg/kg 8hourly for 3days

Note
• No antibiotics are of proven value.
• Steroids should not be used.
• Non-Steroidal Anti-Inflammatory Drugs (NSAIDs) such as ibuprofen and aspirin should
be avoided. These anti-inflammatory drugs act by thinning the blood, and in a disease
with risk of hemorrhage, blood thinners may exacerbate the prognosis
• Do not use products containing oil of lemon eucalyptus (OLE) or para-menthane-diol
(PMD) on children under 3 years old.
• Do not apply insect repellent to a child’s hands, eyes, mouth, cuts, or irritated skin

Prevention
The most effective way to prevent infection from Chikungunya virus is to prevent mosquito bites
during the day and night.
• Use insect repellent (DEET, Picaridin (known as KBR 3023 and icaridin IR3535, Oil of
lemon eucalyptus (OLE), Para-menthane-diol (PMD), 2-undecanone)
• Modification of the mosquito bleeding sites
• Wear long-sleeved shirts and pants,
• Treat clothing and gears with permethrin
• Take steps to control mosquitoes indoors and outdoors

Public Health Control Measures


• Symptomatic treatment for mitigating pain and fever using non-steroidal anti-inflammatory
drugs along with rest usually suffices. Persistent joint pain may require analgesic and long-
term anti-inflammatory therapy.
• Prevention is entirely dependent upon taking steps to avoid mosquito bites and elimination
of mosquito breeding sites.

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• To avoid mosquito bites:
o Wear full sleeve clothes and long dresses to cover the limbs
o Use mosquito repellents
o Use mosquito nets – to protect babies, old people and others, who may rest
during the day.
o The effectiveness of such nets can be improved by treating them with permethrin
(pyrethroid insecticide). Curtains (cloth or bamboo) can also be treated with
insecticide and hung at windows or doorways, to repel or kill mosquitoes

4.2.2 Measles (Rubeola)


Measles is an acute, highly communicable (contagious) infectious viral disease caused by Measles
virus (MeV) which is the member of the family Paramyxoviridae, genus Morbillivirus. The mode of
transmission is airborne, by droplet spread through coughing or sneezing, or by direct contact with
nasal or throat secretions of infected persons. It is the fourth leading cause of death in children
less than 5 years of age in many African countries.

Case Definition
Suspected case:
Any person with fever and maculopapular (non-vesicular) generalized rash and cough, coryza or
conjunctivitis (red eyes) or any person in whom a clinician suspects measles.
Confirmed case:
A suspected case with laboratory confirmation (positive IgM antibody) or epidemiological link to
confirmed cases in an outbreak.

Clinical Diagnostic Criteria


• Generalized, reddish (erythematous), blotchy (maculopapular) rash;
• History of fever usually above 38˚C (if not measured, then "hot" to touch);
• Dry cough; Sore throat; Runny nose (coryza);
• Inflamed eyes (conjunctivitis), tiny white spots with bluish-white centers on a red
background found inside the mouth on the inner lining of the cheek- also called Koplik's
spots.
• In addition, children with measles frequently exhibit a dislike of bright light (photophobia),
and often have a sore red mouth (stomatitis).
Symptoms usually develop 10–12 days after exposure to an infected person and last 7–10 days

Laboratory Investigation
With coordination from the WHO, the Global Measles and Rubella Laboratory Network (GMRLN)
performs case-based laboratory surveillance standardized methods to confirm Measles Infection by
• Detection of viral RNA by RT-PCR (increasing role in case confirmation),
• Enzyme Immunoassay (EIA) for immunoglobulin M (IgM)

Pharmacological Treatment
Note
No specific antiviral treatment exists for measles virus

Adults: A: paracetamol(PO) 1g 8hourly for 5days


AND
A: vitamin A (PO) 200000 IU stat

In case of ocular involvement, add


A: oxytetracycline eye ointment 1% apply once daily for 7 days

Children:
A: paracetamol (PO) 10–15mg/kg 8hourly for 5days
A: vitamin A if less than 1 year give 100,000IU (PO) start and if over 1 year give 200,000IU

Prevention
Routine measles vaccination for children combined with mass immunization campaigns
• Administration of the first dose of measles-containing vaccine (MCV) at 9 months and 18
months in measles-endemic regions (Tanzania) and at 12–15 months in non-endemic
regions.

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• Accelerated immunization activities have had a major impact on reducing measles deaths.
• The World Health Organization (WHO) defines measles elimination as “the absence of
endemic measles virus transmission in a defined geographical area (e.g. region or country)
for at least 12 months in the presence of a surveillance system that has been verified to be
performing well.

Public Health Control Measures


Efforts to reduce the secondary spread of measles include;
• Improve routine vaccine coverage through the IVD, and lead supplemental vaccination
activities in areas of low vaccine coverage.
• Mobilize the community early to enable rapid case detection and treatment.
• Provide Vitamin A: Dose 1: immediately, Dose 2: next day

4.2.3 Rabies
Rabies is a zoonotic disease (a disease that is transmitted to humans from animals) that is caused
by a virus. Rabies infects domestic and wild animals, and is spread to people through close contact
with infected saliva (via bites or scratches) The rabies virus infects the central nervous system,
causing disease in the brain and, eventually, death. Early symptoms in people include: fever,
headache, and general weakness or discomfort. As the disease progresses, symptoms include;
insomnia, anxiety, confusion, slight or partialparalysis, excitable behaviour, hallucinations, increase
in saliva, difficulty swallowing, and fear of water (hydrophobia).

In unvaccinated humans, rabies is almost always fatal if post-exposure prophylaxis is not


administered before the onset of severe symptoms. Death usually occurs within days of the onset
of neurological symptoms. Dogs are the main carrier of rabies in Africa and are responsible for
most (approximately 97%) of the human rabies deaths worldwide WHO estimates approximately
55,000 human deaths worldwide due to rabies each year; in Africa the annual death toll is 24,000.

Case Definition
Suspected: A person with one or more of the following: headache, neck pain, nausea, fever, fear of
water, anxiety, agitation, abnormal tingling sensations or pain at the wound site, when contact with
a rabid animal is suspected.
Confirmed: A suspected case that is laboratory confirmed

Laboratory Investigation
Human rabies is confirmed by intra-vitam and post mortem diagnostic techniques that detect whole
viruses, viral antigens, or nucleic acids in infected tissues (brain, skin or saliva). E.g. Direct
fluorescent antibody (DFA) test, which targets rabies virus antigens in brain tissue, Identification of
viral nucleic acid by reverse transcriptase PCR on fixed tissue collected post mortem or in a clinical
specimen (brain tissue or skin, cornea or saliva) or Detectable rabies-neutralizing antibody titre in
the CSF of an unvaccinated person.

Pharmacological Treatment
Post-exposure prophylaxis (PEP) is the immediate treatment of a bite victim after rabies exposure by
• Extensive washing and local treatment of the bite wound or scratch as soon as possible
after a suspected exposure;
• Providing effective rabies vaccine that meets WHO standards
• Administration of rabies immunoglobulin (RIG), if indicated.

Local wound therapy: -wash wound thoroughly with running water and soap for 10 minutes, and
repeat process with:
A: 10% Povidone iodine; to prevent secondary bacterial infection.
If patient present with Anxiety, Agitation, Seizures,
A: diazepam Adults 10mg IV slowly in 3–5minutes (0.1–0.3 mg/kg in 3–5 min) 10mg in 3–
5minutes, repeated 1–4 hourly Paediatrics 0.1–0.3 mg/kg in 3–5min, repeated 1–4 hourly
to provide (total 2.4–12 mg/kg IV for 24 h)
OR
A:diazepam (IV) slowly in 3–5minutes, repeated 1–4hourly for 24hours

99

OR
A: diazepam (IM) 20mg 2hourly for 24hours
OR
A: diazepam (Intrarectally) 10mg 1–4 hourly for 24 hours
OR
A: lorazepam 25–50mcg/kg 6 hourly for 24 hours
OR
C: midazolam 0.08 – 0.2mg/kg (IV) repeated 1–4 hourly for 24 to 48 hours
OR
C: midazolam (intrarectally)10–30mg over 24 hours by pump for 24 to 48 hours

If patient present with Anxiety


A: Haloperidol 5mg (IM or SC) hourly until calm, then 4 or 6 hourly and when necessary
OR
A: haloperidol 5 mg (IV) 5–15mg/24 hours
OR
A: chlorpromazine (IM) 25–50mg/6–8 hourly for 48hours

Table 4.3: Support for Patient with Fever, Hypersecretion and Pain
Route of
Indication Drug Dose: adult Dose: paediatric
administration
1 g every 8 h,
iv infusion over
maximum 3-4
15 minutes
g/24 h
A: paracetamol
1g every 4–6h, 10–15mg/kg (PO)
intrarectal maximum 3-4 every 8 hours for
g/24 h 5 days
Fever
300–400 mg 8
A: ibuprofen intrarectal
hourly
450–900mg
4hourly,
A: aspirin intrarectal
maximum 3.6
g/day

A: Hyoscine 400 mcg 4 10 mcg/kg 4–


sc or iv injection
Hypersecretion (scopolamine) hourly 8hourly
hydrobromide sc infusion 1.2–2 mg/24 h 40–60 mcg/kg/24h
slow iv, sc or im 10 mg 4hourly
C: morphine 15–30 mg
intrarectal 100 mcg/kg
Pain 4hourly
transdermal 12–25 mcg/h 12 mcg/h every
S: fentanyl
patch every 72 h 72h

Prevention
• Rabies can be prevented by
• Vaccinating pets
• Staying away from wildlife
• Seeking medical care after potential exposures before symptoms start
• Immunization

Immunization
Active Immunization
Pre-exposure immunization is recommended for people in certain high-risk occupations such as
laboratory workers handling live rabies and rabies-related (lyssavirus) viruses; and people (such as
animal disease control staff and wildlife rangers)
Active immunization: Human Diploid Cell Vaccine (HDCV) –either ID or IM
A: anti-rabies Vaccines (2- 3 IU/dose)
o IM: 1ml on days 0, 3, 7, 14, 28 (5 doses)

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o ID: 0.2ml by dividing 0.1 ml on left shoulder and 0.1ml on right shoulder, on days 0, 3,
7 and 28 (4 doses). Intradermal (ID) is mostly advised.
In addition, patients should receive rabies immune globulin with the 1st dose (day 0)

Passive Immunization
B: anti-rabies human immunoglobulin 20 IU/kg half the dose given parenterally and the other
half injected into and around the wound for victims suspected to be infected
AND
A: tetanus toxoid vaccine, please refer to the section on Tetanus

Note
Treat the person immediately after the animal bite, before onset of symptoms
Corticosteroid therapy generally is not considered for the management of brain edema in rabies.

Public Health Control Measures


• Post exposure prophylaxis to prevent rabies
• Isolate patient and immunize contacts to prevent infection of others
• Vaccinate local dogs and cats to prevent outbreaks
• Promote public awareness of rabies
• Target immunization campaign for domestic or wild animals in high-risk areas
• Maintain active surveillance of rabies in animals

4.2.4 Zika Virus Disease


Zika virus is a flavivirus that is transmitted primarily through the bite of an infected mosquito,
primarily Aedes aegypti, and also Aedes albopictus, the same mosquitoes that transmit dengue,
chikungunya, and yellow fever. Zika virus can also be transmitted in-utero from mother to fetus, and
through sexual contact, blood transfusion, and organ transplantation. Zika virus infections are
usually asymptomatic. When symptoms occur, they tend to be mild and include mild fever, rash,
conjunctivitis, and muscle and joint pain that last for 2 to 7 days. There is no specific treatment but
symptoms can be treated with common fever medicines, rest and drinking fluids.

Zika virus infection during pregnancy can result in preterm birth, fetal loss, stillbirth, and congenital
malformations including microcephaly, limb contractures, eye abnormalities, brain calcifications, and
other manifestations of Congenital Zika Syndrome.
Zika virus is also associated with an increased risk of Guillain-Barré syndrome, and other
neurological complications requiring close medical management and possibly intensive care and
mechanical ventilation.

Case Definition
Suspected Case: Any person presenting with rash and/or fever and at least one of the following
signs or symptoms:
• arthralgia; or
• arthritis; or
• conjunctivitis (non-purulent/hyperaemic).

Probable case: A suspected case with presence of IgM antibody against Zika virus and an
epidemiological link (with no evidence of infection with other flaviviruses).

Confirmed case: Any person with laboratory confirmation of recent Zika virus infection presence of
Zika virus RNA or antigen in serum or other samples (e.g. saliva, urine, tissue, whole blood); or IgM
antibody against Zika virus positive and Plague Reduction Neutralizing Test (PRNT90) for Zika virus
with titre ≥20 and Zika virus PRNT90 titre ratio ≥ 4 compared to other flaviviruses; and exclusion of
other flaviviruses.

Clinical Diagnostic Criteria:


• Fever, skin rashes, conjunctivitis,
• Joint pain, malaise, Headache - usually mild and last for 2–7 days.
• Neurological and auto-immune complications of Zika virus disease, babies born with
microcephaly (Observed in northeast Brazil).

101

Laboratory Investigations
• Reverse transcriptase-polymerase chain reaction (RT-PCR) for viral RNA
• Serology for IgM detection
• Plaque reduction neutralization test (PRNT)

Non-Pharmacological Treatment:
The mainstay treatment for Zika Virus is the supportive symptomatic treatment.
• A: Assure plenty of rest to patients
Pharmacological Treatment
• A: Maintain body fluids Sodium Lactate Compound (Ringers Lactate) intravenously.
• A: Control Fever and Pain by giving Acetaminophen or Paracetamol 15mg/kg (PO/IV) 8
hourly for 3 days

Note
• No antibiotics are of proven value.
• Steroids should not be used.
• Non-Steroidal Anti-Inflammatory Drugs (NSAIDs) such as ibuprofen and aspirin should be
avoided. These anti-inflammatory drugs act by thinning the blood, and in a disease with
risk of hemorrhage, blood thinners may exacerbate the prognosis
• Do not use products containing oil of lemon eucalyptus (OLE) or para-menthane-diol
(PMD) on children under 3 years old.
• Do not apply insect repellent to a child’s hands, eyes, mouth, cuts, or irritated skin

Prevention
• Vector control: - removal and modification of breeding sites and reducing contact between
mosquitoes and people
• Wearing clothing (preferably light-coloured) that covers as much of the body as possible;
• Using physical barriers such as window screens and closed doors and windows;
• Applying insect repellent to skin or clothing that contains DEET, IR3535 or icaridin

Public Health Control Measures


• Strengthen event-based surveillance to detect the emergence of clusters of cases
presenting with rash and febrile syndrome of unknown aetiology.
• Actively engage other sectors (e.g., environment, agriculture, tourism) to respond to Zika
virus through a multi-sectoral approach (One Health approach).
• Enhance surveillance of Zika virus disease and of the conditions that may be associated
with it, including microcephaly and congenital Zika syndrome and Guillain-Barré syndrome
(GBS).
• Enhance surveillance at prenatal and postnatal clinics to monitor possible congenital
infections and complications.
• Conduct community-based assessments to determine the abundance of vector
mosquitoes, identify the most productive larval habitats, promote and implement plans for
appropriate vector control.
• Report any identified unusual increase in the incidence of congenital neurological
malformations including microcephaly in neonates and adverse pregnancy outcomes not
explained through alternate causes, to the relevant public health authorities using IDSR
framework.
• Intensify of efforts to reduce mosquito populations including elimination of potential
breeding sites (e.g., removal of trash and standing water sites around homes, covering
home water storage containers, and use of larvicides) and adult mosquito control methods.
• Promotion of personal protection measures such as use of light-coloured protective
clothing (long sleeves and pants), insect repellent, and physical barriers such as screens,
closed doors and windows, and sleeping under mosquito nets including during the day
when Aedes mosquitoes are most active.
• Develop risk communication messages to address population concerns, enhance
community engagement, improve reporting, and ensure application of vector control and
personal protective measures targeting reduction of contact with the vector.

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• Provide women of childbearing age and particularly pregnant women with the necessary
information and materials on family planning and to reducing risk of exposure.
• Provide clinical and psychosocial support services for affected children and families.
• Zika can be transmitted through blood and blood products. Precautions already in place for
ensuring safe blood donations, transfusions, and prevention of bloodborne pathogens
should be followed.
• Zika can be transmitted sexually. Men and women need to get counselling on safer sexual
practices, and be offered condoms and full range of contraceptive methods.
• Ensure that pregnant women who have been exposed to Zika virus be counselled and
followed for birth outcomes based on the best available information and national practice
and policies.
• Refer most severe cases with complication to hospitalized cares.

4.2.5 COVID-19
Coronavirus Disease 2019 (COVID-19) is a recently discovered disease, caused by a Coronavirus,
named SARS-CoV-2, which is genetically related to the virus causing Severe Acute Respiratory
Syndrome (SARS) of 2003 and Middle East Respiratory Syndrome (MERS). This virus belongs to
the family Coronaviridae, of the order Nidoviralessuspected to originate from an animal host
(zoonotic origin) followed by human-to-human transmission. The disease was first detected in
Wuhan, the capital city of Hubei, China, in December of 2019 and declared by the WHO to be a
Public Health Emergency of International Concern, in 11 March 2020 due to its evident rapid
disease spread worldwide in less than 6 months. Most estimates of the incubation period for COVID-
19 range from 1-14 days, most commonly around five days.

Current evidence suggests that COVID-19 spreads between people through direct, indirect (through
contaminated objects or surfaces), or close contact with infected people via mouth and nose
secretions (saliva, respiratory secretions or secretion droplets).

People with the virus in their noses and throats may leave infected droplets on objects and surfaces
(called fomites) when they sneeze, cough on, or touch surfaces, such as tables, doorknobs and
handrails. Other people may become infected by touching these objects or surfaces, then touching
their eyes, noses or mouths before cleaning their hands.

Case definition
The case definitions are based on the current information available and might be revised as new
information accumulates.

Suspect case: A patient with acute respiratory illness (fever and at least one sign/symptom of
respiratory disease, e.g., cough, shortness of breath), AND a history of travel to or residence in a
location reporting community transmission of COVID-19 disease during the 14 days prior to
symptom onset.
OR
A patient with any acute respiratory illness AND having been in contact with a confirmed or probable
COVID-19 case (see definition of contact) in the last 14 days prior to symptom onset;
OR
A patient with severe acute respiratory illness (fever and at least one sign/symptom of respiratory
disease, e.g., cough, shortness of breath; AND requiring hospitalization) AND in the absence of an
alternative diagnosis that fully explains the clinical presentation.
Probable case: Any suspect case for whom testing for COVID-19 is inconclusive or is tested positive
using a pancoronavirus assay and without laboratory evidence of other respiratory pathogens.
OR
A suspect case for whom testing could not be performed for any reason
OR
Any suspect case or death with epidemiologic link to confirmed cases or outbreak
OR
Any suspect case with typical appearance of COVID-19 in Chest Computed Tomography (CT) or
chest x-rays.

Confirmed case: An individual (contact or suspect case) with a laboratory-confirmed COVID-19 by


real-time reverse-transcription polymerase chain reaction (rRT-PCR).

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OR
A suspect case with a strong epidemiological link to COVID-19 patient and detection of antigen
using validated/adequate direct SARS-CoV-2 antigen detection tests.
OR
A suspect case with a strong epidemiological link to COVID-19 patient and detection of exposure to
virus (Antibodies – IgM and/or IgG, IgA) using validated/adequate serology tests (indirect antibody
detection tests).

Clinical Diagnosis
Most common symptoms:
• Fever, Dry Cough and Tiredness

Less common symptoms:


Headache, Sore throat, Loss of taste or smell,Chills, Runny nose, Headache, Chest pain ,
Muscle aches, Diarrhea,, Conjunctivitis, Skin rash , or Discoloration of fingers or toes

Serious symptoms- Severe Acute Respiratory Infection (SARI):


• Difficulty breathing or shortness of breath
• Chest pain or pressure
• Loss of speech or movement

The risk of serious illness from COVID-19 includes serious heart diseases, such as heart failure,
coronary artery disease or cardiomyopathy, Cancer, Chronic obstructive pulmonary disease
(COPD), Type 2 diabetes, Type 1 diabetes, Asthma, Liver Disease, Cystic Fibrosis, Severe obesity,
Chronic kidney disease, Sickle cell disease, Immunocompromized patients by solid organ
transplants, bone marrow transplant, HIV or cancer medications.

Laboratory Investigation
Rule out Community-Acquired Pneumonia (Streptococcus pneumonia, Haemophilus influenza type
b, Staphylococcus aureaus, Klebsiella pneumoniae, Legionella pneumophila, Influenza viruses, and
Respiratory Syncytial virus).

Specimen collection, processing, and laboratory testing shall follow biosafety procedures.
• Collect blood cultures for bacteria that cause pneumonia and sepsis, ideally beforeantimicrobial
therapy.
• DO NOT delay antimicrobial therapy while waiting for blood culture results.
• Collect specimens from BOTH the upper respiratory tract (URT; nasopharyngealand
oropharyngeal) AND lower respiratory tract (LRT; expectorated sputum, endotracheal aspirate, or
Broncho alveolar lavage) for SARS-CoV-2testing by RT-PCR.
Clinicians may elect to collect only LRT samples when these are readily available (for example, in
mechanically ventilated patients).
• Use appropriate PPE for specimen collection (droplet and contact precautions forURT specimens;
airborne precautions for LRT specimens).
• When collecting URT samples, use viral swabs (sterile Dacron or Rayon, not cotton) and viral
transport media.

Note
Do not take sample from the nostrils or tonsils

Where feasible both URT and LRT specimens can be tested for other respiratory viruses
like Influenza A and B (including zoonotic influenza A), Respiratory syncytial virus,
Parainfluenzaviruses, Rhinoviruses, Adenoviruses, Enteroviruses (e.g. EVD68), Human meta
pneumovirus, and Endemic human coronaviruses (i.e. HKU1, OC43, NL63, and 229E).

104
Testing
• Routine confirmation of cases of COVID-19 is based on detection of unique sequences of
virus RNA by Nucleic acid amplification tests (NAAT) such as real-time reverse-
transcription polymerase chain reaction (rRT-PCR).
• Serological testing (indirect antibody detection tests) can aid investigation of an ongoing
outbreak and retrospective assessment of the attack rate or extent of an outbreak.
• Viral sequencing to providing confirmation of the presence of the virus, regular
sequencing of a percentage of specimens from clinical cases can be useful to monitor for
viral genome mutations
• Viral culture is not recommended as a routine diagnostic procedure.

Severity of Illness Categories


• Asymptomatic or Pre-Symptomatic Infection: Individuals who test positive for SARS-CoV-2 using a
virologic test (i.e., a nucleic acid amplification test or an antigen test), but who have no symptoms
that are consistent with COVID-19.
• Mild Illness: Individuals who have any of the various signs and symptoms of COVID-19 (e.g., fever,
cough, sore throat, malaise, headache, muscle pain, nausea, vomiting, diarrhea, loss of taste and
smell) but who do not have shortness of breath, dyspnea, or abnormal chest imaging.
• Moderate Illness: Individuals who show evidence of lower respiratory disease during clinical
assessment or imaging and who have saturation of oxygen (SpO2) ≥94% on room air at sea level.
• Severe Illness: Individuals who have SpO2 <94% on room air at sea level, a ratio of arterial partial
pressure of oxygen to fraction of inspired oxygen (PaO2 /FiO2) <300 mmHg, respiratory frequency
>30 breaths per minute, or lung infiltrates >50%.
• Critical Illness: Individuals who have respiratory failure, septic shock, and/or multiple organ
dysfunction.

Management
• All patients with suspected COVID-19 who have severe acute respiratory infection should
be triaged and isolated at the first point of contact with the health care system.
• Emergency treatment should be started based on disease severity.
• For those presenting with mild illness, hospitalization may not be required unless there is
concern about rapid deterioration. If there is only mild illness, providing care at home may
be considered if available.
• Moderate to severe and critical cases must be admitted for management.
• Admitted cases must be monitored for early identification of deterioration and appropriate
treatment offered as per national treatment protocol for moderate to severe COVID-19
patients.
• Oxygen is the mainstay of therapy for those whose SpO2 drops according the guideline.
• Recovered patients may be discharged if 2 RT-PCR taken at least 24 hours apart are
negative with clinical recovery (temperature resolved for more than 48 hours and no need
for oxygen therapy).

Note
• All areas for treatment of COVID-19 patients should be equipped with pulse oximeters, functioning
oxygen systems and disposable, single-use, oxygen-delivering interfaces (nasal cannula, simple
face mask, and mask with reservoir
bag).
• Use contact precautions when handling contaminated oxygen interfaces of patients with SARS-
CoV-2 infection.

Early General Supportive Therapy and Monitoring


Patients with SARI shall be managed in isolated critical care units
• Give supplemental oxygen therapy immediately to patients with SARI and respiratory
distress, hypoxemia, or shock.
o Initiate oxygen therapy at 5 L/min and titrate flow rates to reach target SpO2≥90%
in non-pregnant adults and SpO2≥92-95 % in pregnant patients.
o Children with emergency signs (obstructed or absent breathing, severe
respiratory distress, central cyanosis, shock, coma or convulsions) should
receive oxygentherapy during resuscitation to target SpO 2 ≥94%; otherwise, the
target SpO2is≥90%.

105
• Use conservative fluid management in patients with SARI when there is no evidence of
shock.
• Treat cautiously with intravenous fluids, becauseaggressive fluid resuscitation may worsen
oxygenation, especially in settings limited availability of mechanical ventilation.

• Give empiric antimicrobials to treat all likely pathogens causing SARI.


o Azithromycin 500mg (PO) day 1 following initial assessment, then followed by
500mg (PO) 8hourly on Days 2-5 when sepsis or superimposed pneumonia is
suspected (based on the clinical diagnosis). Give Steroids
• Prednisolone 10mg to 20mg (PO) once a day for 7 days OR Dexamethasone 6mg (PO/ IV)
once a day for up to 7days or until hospital discharge) based on patents conditions in ICU /
Critical Care Units

Give Supplements
• Magnesium 300mg or 400mg (PO) once a day for 7days
• Zinc 7mg (PO) for children aged 1– years of age, increasing up to 25mg (PO) for adults
and females of any age who are pregnant or lactating
• Vitamin C dose of 70-150mg 24hourly for 7 days

Closely monitor the patient’s clinical condition 12 hourly


• Monitor signs of SARI, clinical deterioration, like rapidly Progressive respiratory failure and
sepsis, and apply supportive care interventions immediately.

Note
• Application of timely, effective, and safe supportive therapies is the cornerstone of therapy
for patients that develop severe manifestations ofSARS-CoV-2 infection
• Do not routinely give systemic corticosteroids for treatment of viral pneumonia.
(No survival benefit and possible harms (avascular necrosis, psychosis, diabetes, and
delayed viral clearance).
• corticosteroid should be used with caution in the treatment of COVID-19 patients < 7 days:
corticosteroids are not recommended for patients with mild conditions

Focused Supportive Management


Infection Control:
• For health care workers who are performing aerosol-generating procedures on patients
with COVID-19, Using an N95 respirator (or equivalent or higher-level respirator) rather
than surgical masks, in addition to other personal protective equipment (i.e., gloves, gown,
and eye protection such as a face shield or safety goggles)
• Endotracheal intubation in patients with COVID-19 to be performed by health care
providers with extensive airway management experience, if possible
• Intubation be performed using video laryngoscopy, if possible

Hemodynamic Support:
• Norepinephrine as the first-choice vasopressor
• For adults with COVID-19 and refractory septic shock who are not receiving corticosteroids
to treat their COVID-19,
Low-dose corticosteroid therapy (“shock-reversal”) over no corticosteroid therapy

Ventilatory Support:
• For adults with COVID-19 and acute hypoxemic respiratory failure despite conventional
oxygen therapy, high-flow nasal cannula (HFNC) oxygen over noninvasive positive
pressure ventilation (NIPPV) (BI).
• For patients with persistent hypoxemia despite increasing supplemental oxygen
requirements in whom endotracheal
intubation is not otherwise indicated, considering a trial of awake prone positioning to
improve oxygenation
• For mechanically ventilated adults with COVID-19 and acute respiratory distress syndrome
(ARDS), use low tidal volume (VT) ventilation (VT 4–8 mL/kg of predicted body weight)
over higher tidal volumes (VT >8 mL/kg)
• For mechanically ventilated adults with COVID-19 and refractory hypoxemia despite
optimized ventilation, prone ventilation for 12 to 16 hours per day over no prone ventilation

106
Acute Kidney Injury and Renal Replacement Therapy:
• For critically ill patients with COVID-19 who have acute kidney injury and who develop
indications for renal replacement therapy, provide continuous renal replacement therapy
(CRRT), if available. If CRRT is not available or not possible due to limited resources,
provide prolonged intermittent renal replacement therapy rather than intermittent
hemodialysis

Pharmacologic Interventions:
• For the therapeutic Management of Patients with COVID-19 use of Dexamethasone and
Remdesivir, either alone or in combination.
• In patients with COVID-19 and severe or critical illness, there are insufficient data to
recommend empiric broad-
spectrum antimicrobial therapy in the absence of another indication.

Implementation of additional Precautions for suspected SARS-CoV-2infections


Contact and Droplet precautions for suspected SARS-CoV-2 infection:
- Place patients in adequately ventilated single rooms. For naturally ventilated general ward rooms
this is considered to be 160 L/second/patient;
- Apply Infection prevention and control measures when providing health care where novel
coronavirus (SARS-CoV-2) infection is suspected, the Interim Guidance is to:
• Place patient beds at least 1m apart;
• Where possible, cohort HCWs to exclusively care for cases to reduce the risk of spreading
transmission due to inadvertent infection control breaches;
• Use of PPE (medical mask, Use eye/facial protection (i.e. goggles or a face shield); Use a
clean, non-sterile, long-sleeved fluid resistant gown; Use gloves)
• Use either single use disposable equipment or dedicated equipment (e.g. stethoscopes,
blood pressure cuffs and thermometers). If equipment needs to be shared among patients,
clean and disinfect between each patient use (e.g. ethyl alcohol 70%);
• Refrain from touching eyes, nose or mouth with potentially contaminated hands;
• Avoid the movement and transport of patients out of the room or area unless medically
necessary.
• Use designated portable X-ray equipment and/or other important diagnostic equipment.
• If transport is required, use pre-determined transport routes to minimize exposures to staff,
other patients and visitors and apply medical mask to patient;
• Maintain a record of all persons entering the patient’s room including all staff and visitors.

Prevention
Application of Standard Precautions for all patients and people at risks in the public include hand
and respiratory hygiene; use of Personal protective equipment (PPE) depending on risk; in hospitals
use safe waste management; environmental cleaning and sterilization of patient-care equipment and
linen. Ensure the following respiratory hygiene measures.

- Offer a medical mask (N95) or double cloth mask in health care settings
- Cover nose and mouth during coughing or sneezing with tissue or flexed elbow for others
- Perform hand hygiene after contact with respiratory secretions.

Personal Protective Equipment (PPE)


Rational, correct, and consistent use of available PPE and appropriate hand hygiene helps to
reduce the spread of the pathogens. PPE effectiveness depends on adequate and regular supplies,
adequate staff training, proper hand hygiene and specifically appropriate human behavior.

Health care workers and Administrators should ensure that environmental cleaning and disinfection
procedures are followed consistently and correctly. Thorough cleaning of environmental
surfaces with water and detergent and applying commonly used hospital level disinfectants (such
as sodium hypochlorite) is an effective and sufficient procedure. Laundry, food service utensils
and medical waste should be managed in accordance with safe routine procedures.

107
Public Health Control Measures
• Establish an alert management system e.g call center with hotlines
• Verify the alerts to determine if they meet the standard case definition for COVID-19
• Respond as for suspected case if they meet the standard case definition
• Record all alerts in an alert/rumor log sheet.
• Provide epidemiological information to conduct risk assessment at the national, regional
and global level.
• Conduct epidemiological investigation to identify risk factors for infection and populations
at risk for severe disease.
• Maintain strict acute respiratory disease infection control practices throughout the
epidemic.
• Mobilize the community for early detection and care and conduct community education
about how the disease is transmitted and how to implement IPC at the home care setting
and during funerals and burials. Consider social distancing strategies.
• Conduct contact follow-up and active searches for additional community cases or deaths
that may not come to the health care setting.
• Distribute laboratory specimen collection kits to health care facilities
• Establish treatment unit to handle additional cases that may come to the health center in
line with the national protocols.
• Maintain strict acute respiratory disease infection control precautions and establish an
isolation ward to manage additional cases who may present for care.
.

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CHAPTER FIVE
MALARIA
Malaria case definition
A malaria case is a person with malaria infection, confirmed by microscopy or mRDT, regardless of
whether fever and other clinical symptoms are present.

5.1 Asymptomatic Malaria Case


Asymptomatic malaria case can be found during Active Case Detection (ACD) by health workers in
the community and in households. Therefore, all patients with parasitemia are considered “malaria
cases”, regardless of whether clinical symptoms are present or not.
5.2 Symptomatic Malaria Case
5.2.1 Uncomplicated Malaria
Uncomplicated malaria is defined as symptomatic malaria without signs of severity or evidence
(clinical or laboratory) of vital organ dysfunction.

Clinical presentation
• Fever • Diarrhoea
• Headache • Body ache, body weakness
• Joint pains • Poor appetite
• Malaise • Pallor, enlarged spleen
• Vomiting

Investigations
The recommended investigations are:
• Quality malaria microscopy or quality malaria Rapid Diagnostic Tests (mRDTs)

Note
• It is compulsory to test and confirm all suspected malaria patients. Give antimalarial only to
those who test positive.
• In cases where non-response to malaria treatment (treatment failure) is suspected in
patients who initially tested positive, microscopy is the recommended laboratory procedure
as mRDTs are not recommended because parasite antigens persist up to 4 weeks after
parasitaemia has cleared.

Non-Pharmacological Treatment
• Continue with feeding and fluid intake
• Followed up immediately if the condition worsens or on the fourth day if symptoms persist.

Pharmacological Treatment
Drug of choice for treatment of uncomplicated malaria is:
A: Artemether+Lumefantrine (FDC) (PO) 20mg+120mg
Common formulations:
• Fixed formulation Artemether 20mg, Lumefantrine120mg; 6, 12, 18 and 24 tablets blister
• Fixed formulation Artemether 80mg, Lumefantrine 480mg; 6 tablets blister

Dispersible tablets: Fixed formulation for children


A: Artemether 20mg + Lumefantrine120mg; 6 tablets blister (5–14kg): 1 tablet; 15–24 kg: 2
tablets)

Table 5.1: Dosage regimen forALu (artemether 20mg/lumefantrine 120mg)

Day 1 Day 2 Day 3


Dose 1st 2nd 3rd 4th 5th 6th
Kg Hours 0 (*) 8 24 36 48 60
Age (years) Tablets Tablets tablets tablets tablets Tablets
up to 15 0 to 3 1 1 1 1 1 1

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15 up to 25 3 up to 8 2 2 2 2 2 2
25 up to 35 8 up to 12 3 3 3 3 3 3
35 and 12 and 4 4 4 4 4 4
above above
(*) 0 hours means the time of starting medication

Table 5.2: The recommended dosing schedule for ALu strength 80/480 mg

Day 1 Day 2 Day 3


st nd rd th
Kg Dose 1 2 3 4 5th 6th
Hours 0 (*) 8 24 36 48 60
Age tablets Tablets Tablets Tablet tablets Tablets
(years) s
35 and 12 and 1 1 1 1 1 1
above above
(*) 0 hours means the time of starting medication

For practical purposes, a simpler dosage regimen is recommended in order to


improve compliance: the first dose should be given as DOT; the second dose
should strictly be given after 8 hours; subsequent doses could be given 12hourly
in the second and third day of treatment until completion of 6 doses

The alternative medicines for the treatment of uncomplicated malaria, where there is no response to
Artemether-Lumefantrine or it is contraindicated, is Dihydroartemisinin-Piperaquine.
C: dihydroartemisinin+piperaquine (FDC) (PO).
Adult formulation containing 40 mg Dihydroartemisinin + 320 mg Piperaquine. Paediatrics formulation
contains a fixed combination of 20 mg of Dihydroartemisinin +160 mg Piperaquine.

Table 5.3: Dose Schedule for Dihydroartemisinin + Piperaquine

Daily dose (mg) Number


Body of
Dihydro Tablet strength
Weight (kg) Piperaquine tablets
artemisinin per dose
1 tablet
5 to <8 20 160 20mg / 160mg
x 3 days


8 to <11 30 240 20mg / 160mg tablet x
3 days

1 tablet
11 to <17 40 320 40mg / 320mg
x 3 days


17 to <25 60 480 40mg / 320mg tablet x
3 days

2 tablets
25 to <36 80 640 40mg / 320mg
x 3 days

3 tablets
36 - <60 120 960 40mg / 320mg
x 3 days

110
Daily dose (mg) Number
Body of
Dihydro Tablet strength
Weight (kg) Piperaquine tablets
artemisinin per dose
4 tablets
60 to <80 160 1,280 40mg / 320mg
x 3 days

5 tablets
>80 200 1,600 40mg / 320mg
x 3 days

Management of fever
Patients with high fever (38.50C and above) should be given an anti-pyretic medicine like
paracetamol (Error! Reference source not found.) or acetylsalicylic acid every 4 to 6 hours
(maximum 4 doses in 24 hours) until symptoms resolve, usually after two days.

Note
Children below 12 years should not be given acetylsalicylic acid because of the risk of developing
Reye's syndrome.

Table 5.4: Treatment Schedule for Paracetamol (500mg) Tablets Children


10mg/kg body weight

Age (years) Weight (Kg) Dose

2 months up to 3 yrs 4 up to 14 ¼

3 up to 5 14 up to 19 ½

5 up to12 19 up to 35 1

12 up to 14 35 up to 45 1 1 /2

14 and above 45 and above 2

5.2.2 Severe Malaria


In a patient with P. falciparum asexual parasitaemia and no other obvious cause of symptoms the
presence of one or more of features listed below classify the patient as suffering from severe
malaria.

Clinical presentation
• Prostration/extreme weakness • Jaundice
• Impaired consciousness • Circulatory collapse/shock
• Change of behaviour • Vomiting everything
• Convulsions • Inability to drink or breast feed
• Respiratory distress (due to lactic • Bleeding tendency/DIC
acidosis and/or pulmonary
oedema)

Investigations
In severe malaria, blood slide (BS) is a recommended malaria test as it quantifies parasitemia. In
severe ill patients receiving injectable antimalarial, serial BS investigations monitors level of
parasitemia to verify malaria recovery, or if clinical condition is not improving to rule out another
serious condition.
• Blood film for malaria parasites
• Blood glucose estimation in patients with altered consciousness
• Haematocrit and/or haemoglobin estimation
• Lumbar puncture to exclude meningitis (if facilities for LP assessment are available)
• Serum creatinine or urea– to assess Kidney function

111

• Electrolytes– for early detection of acute renal failure
• Full blood cell count and differential white cell count for additional diagnosis of other
infectious diseases
• Blood gases, pH and anion gap– to diagnose acidosis
• Radiological investigation: Chest X–ray; look for pulmonary oedema or lobar consolidation
• Blood culture and sensitivity where feasible

Non-Pharmacological Treatment
A rapid assessment must be conducted including airway, breathing, circulation, coma, convulsion,
and dehydration status.

Referral: If effective management of severe malaria and supportive care for complications is not
possible, patients should be given pre-referral treatment and referred immediately to an appropriate
facility for continued treatment.

Pharmacological Treatment
A: Parenteral artesunate
Dosage:
• 2.4 mg/kg in body weight. (IV) or (IM) given on admission (time = 0 hour), then at 12 hours
and 24 hours for a minimum of 3 injections in 24 hours regardless of patient’s recovery.
• Children weighing less than 20 kg Dosage: 3 mg/kg/dose (or higher). Same schedule as
indicated above (0, 12, 24 hours)
• Complete artesunate injection treatment by giving a complete course (3days) of
artemether-lumefantrine (ALu) or other ACT.
Consider broad spectrum antibiotic as treatment of septicemia.

Administration and dosage (30 mg, 60mg and 120mg strength): Injectable artesunate has 2-steps
dilutions.
• Step 1: The powder for injection should be diluted with 1ml of 5% sodium bicarbonate
solution (provided in each box) and shaken vigorously 2–3 minutes for better dissolving
until the solution becomes clear.
• Step 2: For slow intravenous infusion (3–4 minutes), add 5 ml of 5% dextrose or normal
saline, to obtain artesunate concentration of 10 mg/ml. For deep intra–muscular injection,
add 2 ml of 5% dextrose or normal saline to obtain artesunate concentration of 20 mg/ml.

Table 5.5: Dilution of Artesunate for Injection


Route IV injection IM injection
Strength 30 mg 60 mg 120 mg 30 mg 60 mg 120 mg
Sodium bicarbonate 5% 0.5 1 2 0.5 1 2
Normal saline or 5% of glucose 2.5 5 10 1 2 4
Total (ml) 3 6 12 1.5 3 6
Artesunate concentration (mg/ml) 10 10 10 20 20 20

Table 5.6: Dosage Schedule for Artesunate Injection


Vials of Artesunate 60mg
Weight Dose ml per dose strength 60mg
needed**
Kg mg/kg IV IM*
10 mg/ml 20 mg/ml
<5 3.0 1.5 1 1
5–8 3.0 2 1 1
9–12 3.0 4 2 1
13–16 3.0 5 3 1
17–20 3.0 6 3 1
21–25 2.4 6 3 1
26–29 2.4 7 4 2
30–33 2.4 8 4 2
34–37 2.4 9 5 2
38–41 2.4 10 5 2
42–45 2.4 11 6 2

112

46–50 2.4 12 6 2
51–54 2.4 13 7 3
55–58 2.4 14 7 3
59–62 2.4 15 8 3
63–66 2.4 16 8 3
67–70 2.4 17 9 3
71–75 2.4 18 9 3
76–79 2.4 19 10 4
80–83 2.4 20 10 4
84–87 2.4 21 11 4
88–91 2.4 22 11 4
92–95 2.4 23 12 4
96–100 2.4 24 12 4

*Half the dose is rounded up to 1ml; **Full vial (s) might not be required for a given weight band. The
left–over solution must be discarded within 1hr of preparation and must not be reused

If the patient can tolerate oral medication after 24 hours provide a full treatment course of AL. Initiate
the first dose of AL 8 hours after the last injection.

Alternative
C: Injectable Artemether
Injectable Artemether is to be used when Artesunate is contraindicated (in case of allergy, medicine
interaction or non- response) and when not available. Artemether should be administered in a dose
of 3.2mg/kg loading dose IM stat (0hour) then 1.6mg/kg (24hours and 48hours).

Table 5.7: Artemether Injectable Dosage by Weight

Loading dose Second and subsequent doses


0 hour 24, 48, hours
Dose Strength Dose Strength
Weight 3.2 mg/Kg 80 mg/ml 1.6 mg/kg 80 mg/ml
Kg Mg ml mg ml
<5 16 0.2 8 0.1
5-8 26 0.3 13 0.2
9-12 38 0.5 19 0.2
13-16 51 0.6 26 0.3
17-20 64 0.8 32 0.4
21-25 80 1.0 40 0.5
26-29 93 1.2 46 0.6
30-33 106 1.3 53 0.7
34-37 118 1.5 59 0.7
38-41 131 1.6 66 0.8
42-45 144 1.8 72 0.9
>45 160 2.0 80 1.0

If the patient can tolerate oral medication after 24 hours provide a full treatment course of ALu.
Initiate the first dose of ALu 8hours after the last injection.

Management of complications
To reduce the unacceptably high mortality of severe malaria, patients require intensive care. Clinical
observations should be made as frequently as possible. Airway maintenance, nurse on side, fanning
if hyperpyrexia is present, fluid balance review:

113
Coma (cerebral malaria): maintain airway, nurse on side, and exclude other causes of coma (e.g.
hypoglycemia, bacterial meningitis); avoid giving corticosteroids.

Dehydration: Correct dehydration

Hyperpyrexia: fanning, paracetamol if patient can swallow

Convulsions: maintain airways; treat with


Adult
A: diazepam (IV) 0.15 mg/ kg (maximum 10 mg) slow bolus IV injection.
Children
A: diazepam (rectal) 0.5–1.0 mg/ kg1.
If convulsions persist after 10 minutes repeat rectal diazepam treatment as above. Should
convulsions continue despite a second dose, give a further dose of rectal diazepam
OR
A: phenobarbitone (IM/IV) 20 mg/ kg after another 10 minutes.

Hypoglycemia: remains a major problem in the management of severe malaria especially in young
children and pregnant women. It should be deliberately looked for and treated accordingly. Urgent
and repeated blood glucose screening.
In children:
B: dextrose 10% (IV) 5 ml/kg
OR
C: dextrose 25% (IV) 2.5ml/kg as bolus;
If 50%dextrose solution is available, it should be diluted to make 25% by adding an equal volume of
water for injection or normal saline.
In adults:
B: dextrose 10% (IV) 125ml
OR
C: dextrose 25% (IV) 50ml as bolus.
Where dextrose is not available, sugar water should be prepared by mixing 20g of sugar (4–level
teaspoons) with 200ml of clean water. 50ml of this solution is given ORALLY or by nasogastric tube
if unconscious.

Severe anaemia: Refer to haematologychapter

Acute pulmonary oedema: Refer to respiratory conditions chapter

Acute renal failure: Refer to cardiovascular disease condition chapter

Shock: Refer to emergency and critical care chapter

5.3 Management of Malaria in Special Groups


5.3.1 Malaria in Pregnancy (MIP)

The effects of malaria in pregnancy are related to the malaria endemicity, with abortion more
common in areas of low endemicity and intrauterine growth retardation more common in areas of
high endemicity.

5.3.1.1 Uncomplicated Malaria in Pregnancy


In high-transmission areas (moderate to high immunity); malaria is usually asymptomatic in
pregnancy or is associated with only mild, non-specific symptoms. (See section 5.1 above)

Pharmacological Treatment
Artemether/Lumefantrine (ALu) is the recommended treatment of choice of a confirmed
uncomplicated malaria to pregnant women in all trimesters.

1
Draw the IV preparation into a small syringe and remove the needle. Insert 5 cm of a nasogastric tube into the rectum. Inject
the diazepam into the nasogastric tube and flush it with 5 ml of water. If a nasogastric tube is not available, use a syringe
without a needle. Hold buttocks together for few minutes to ensure retention and absorption of the medicine

114
5.3.1.2 Severe Malaria in Pregnancy
In low-transmission areas (low malaria immunity); women in the second and third trimesters of
pregnancy are more likely to develop severe malaria than other adults, often complicated by
pulmonary oedema and hypoglycaemia.
The following are common features of severe malaria during pregnancy:
• High fever • vere haemolytic anaemia
• Hyperparasitemia • Cerebral malaria
• Low blood sugar • Pulmonary oedema
Pharmacological Treatment Intramuscular/ intravenous Artesunate is the drug of
choice for treatment of severe malaria in all trimesters.

5.3.1.3 Intermittent Preventive Treatment in Pregnancy (IPTp)


Malaria parasites can easily accumulate and multiply in the placenta leading to placenta malaria
infections, resulting to complications such as maternal anaemia, low birth weight, premature
delivery, congenital infection and/or perinatal death.

Note
IPTp is an administration of antimalarial in full therapeutic doses at predetermined intervals during
pregnancy
individuals with no signs/symptoms of malaria. The aim is to prevent above mentioned
complications with adverse
effects to both mother and fetus3

The medicine of choice for IPTp


A: sulphadoxine+pyrimethamine (FDC) (PO) 500mg +25mg
• The dose is 3 tablets once
• A minimum of 3 doses in entire pregnancy period
• The first dose should be administered from 14 weeks of pregnancy onwards
• Each dose should be given at least 4 weeks apart
• The last dose can be administered up to the time of delivery, without safety concerns

Note:
• SP should not be administered to women receiving cotrimoxazole prophylaxis or pregnant
women who are taking folic acid at a daily dose equal or above 5 mg, as it counteracts its
efficacy
• SP can be administered safely with combined ferrous sulphate 200mg + folic acid 0.25mg
• If malaria is diagnosed to a scheduled pregnant woman for IPT with SP; SP should not be
given, instead a full treatment with antimalarial should be given

5.3.2 Management of Malaria in Neonates


Neonatal malaria is defined as symptoms attributable to malaria with evidence of ring forms of
malaria parasite in the blood of an infant within the first twenty-eight days (4 weeks) of life.
Congenital malaria is defined as symptoms attributable to malaria with evidence of ring forms of
malaria parasite in the blood of an infant within the first seven days (1 week) of life. The signs and
symptoms resemble those seen in the new-born with septicemia

Clinical presentation

• Fever • Laboratory findings will include the


• Lethargy presence of malaria parasites.
• Unable to breastfeed
• Vomiting
• Irritability
• Respiratory distress
• Seizures
• Jaundice
• Pallor
• Hepatosplenomegaly

115
Investigations
• Full blood picture
• blood sugar
• blood culture and sensitivity, blood smear for malaria parasite, serum electrolytes
• CSF for analysis

Management of neonatal malaria


• Neonatal malaria should always be considered as severe malaria
• Neonates with suspected malaria should be admitted to hospital immediately as they can
deteriorate quickly and die at home
• Parental Artesunate is recommended treatment of choice for neonates. Injectable Artemether
can be used as an alternative if Artesunate is not available
• Broad spectrum antibiotic as majority of severe malaria accompanied with septicemia. Refer
septicemia treatment section.

Nursing care and monitoring


• Monitor vital signs (PR, RR & Temperature)
• Monitor input/output
• Check BS for malaria parasite daily
• Ensure feeding
• Advise on use of LLINs

5.3.3 Management of Malaria in HIV and AIDS Patients


If malaria is diagnosed, depending on classification of the malaria diagnosis, a full treatment with
antimalarial should be given according to the malaria classification.

However, it should be noted that, clearance of parasitaemia may not necessarily be accompanied by
clearance of symptoms (fever) due to the presence of other underlying opportunistic infections. HIV
and AIDS infected adults with low CD4 cell counts may be more susceptible to treatment failure of
anti-malaria drugs.

Note
• In suspected cerebral malaria in a HIV and AIDS patient, cerebrospinal fluid (CSF)
examination to rule out other life-threatening conditions such as bacterial and cryptococcal
meningitis

116
CHAPTER SIX
HIVA ND AIDS
AIDS is defined as Acquired Immuno- Deficiency Syndrome caused by Human Immunodeficiency
Virus (HIV). Clinical features are usually due to immune system suppression.

Clinical presentation
• Fever, diarrhoea, weight loss, skin rashes, sores, generalized pruritis, altered mental
status, persistent severe headache, oral thrush or Kaposi’s sarcoma may be found in
patients with advanced disease
• Opportunistic infections e.g. tuberculosis, candidiasis or pyogenic infections, Advanced
HIV Disease
6.1 Treatment of HIV and AIDS in Adults and Adolescents
• All HIV infected individuals are eligible for ART. Early initiation of combination treatment
(ART) is associated with health benefits in terms of reduced morbidity and mortality in all
age groups.
• Antiretroviral therapy (ART) has dramatically reduced HIV-associated morbidity and
mortality and has transformed the HIV disease into a chronic, manageable condition. In
addition, treatment of HIV infected individuals with ART is highly efficient at preventing
transmission to sexual partners and mother to child transmission (MTCT).

Evaluation to be done before Initiating ART


From the moment a patient tests HIV positive, he/she should be linked to the Care and Treatment
Clinic (CTC). In health facilities where ART is being initiated at RCH and TB clinics, patients can be
managed at those clinics. Mobile outreach clinics can also be used for key and vulnerable
population and hard to reach areas.

6.1.1 First-Line Regimens for Adults and Adolescents

Table 6.1Recommended First-Line Regimens for Adults and Adolescents


Patient group Preferred (Default) Regimen Alternative Regimen

Adults and adolescents (>15 A: TDF +3TC +DTG (TLD) A: ABC + 3TC+ DTG
years), Pregnant/lactating A: TDF + 3TC +EFV (TLE 600 or TLE
mothers 400)

Special situations:
A:AZT + 3TC + DTG

HIV and TB co-infections A: TDF + 3TC +DTG (Double A: TDF + 3TC +EFV (TLE600)
dosage of DTG)
A: ABC + 3TC+ DTG (Double dosage of
DTG)

Special situations:
A:AZT + 3TC + DTG (Double dosage of
DTG)

People who Inject Drugs A: TDF + 3TC +DTG A: ABC + 3TC+ DTG
(PWID)
A: TDF + FTC +ATV/r

6.1.2 ART in Women of Childbearing Potential or Pregnant Women


Mother-to-child transmission (MTCT) of HIV refers to the transmission of HIV infections from HIV-
infected mothers to their infants. MTCT can occur during pregnancy, labour and delivery, and
breast-feeding. Without intervention, the overall risk of MTCT is approximately 20%–45%. However,
with interventions, this risk can be reduced to less than 5%. Transmission of HIV from mother to her
child accounts for over 90% of all HIV infections in children aged below 15 years.

117
Figure 6.1 Estimated HIV Outcomes for Infants Born to Mothers Living with HIV

55–80 infants will


100 infants born to HIV-infected mothers
NOT be HIV-
who breastfeed
infected

10-15 infants 5-20 infants


infected
10-15 infant infected
during
infected labour and during breast-
delivery feeding
during
pregnancy

25-50 infants will be HIV-infected

6.1.3 Prevention of Mother to Child Transmission

All HIV infected pregnant women and lactating mothers are eligible for ART regardless of CD4 cell
count and clinical stage. The pregnant or breast-feeding women with HIV should be started on
lifelong ART at the time of diagnosis.

The recommended first line regimen is once a day fixed dose regimen of TDF + 3TC + DTG.
Although TDF+ 3TC + EFV may be an option for use during the pre-conception period through the
first eight weeks of pregnancy to avoid potential risk of neural tube defects.Then TLD should be
continued postpartum
• A women-centered approach is adopted. Women of childbearing potential including those
who are using long term effective contraception should be given adequate information to
enable making informed decision and choice.
• Women should receive on-going counselling support to continue with HIV care and
treatment in order to maintain good health and to reduce the risk of HIV transmission to
others.

Available alternative first-line ART regimen includes


A:TDF+FTC+EFV600mg (FDC)
OR
A: ABC+3TC+EFV600 or DTG
OR
A: AZT+3TC+EFV600 or DTG

Prophylaxis for HIV Exposed Infants


• Administer NVP syrup immediately after birth to all HIV exposed infants and continue until
six weeks of age
• In case a high risk HIV exposed infant is identified, administer duo prophylaxis containing
NVP syrup (once daily) and AZT syrup (twice daily) for the first 6 weeks of life, then
continue with daily NVP alone up to 12 weeks of life
High-risk infants are those who are:

o Born to women diagnosed to be living with HIV during current pregnancy or breast-
feeding period.
o women known to be HIV positive but not yet on ART or
o already on ART but with high viral load (≥50/UL of blood)

• Infant prophylaxis is most effective when given as soon as possible after birth, preferably
within 6–12 hours
• HIV exposed infants identified beyond the age of 4 weeks should not be given ARV
prophylaxis

118
Table 6.2: NVP Dosing Recommendation
Infant age NVP daily dosing
Birth to 6 weeks
§ Birth weight 2000–2499g 10mg (1 ml) once daily
§ Birth weight ≥2500g 15mg(1.5ml) once daily

Based on the dosing required to sustain exposure in the infant of >100 ng/mL with the fewest dose
changes
Low birth weight infants <2000g should receive mg/kg dosing; suggested starting dose is 2mg/kg
once daily.

6.1.4 Second-line ART in Adults and Adolescents


Before treatment failure is confirmed every effort should be made to rule out causes other than drug
resistance.

Table 6.3: Recommended Second-Line Regimens for Adults and Adolescents

Patient group Preferred (Default) Alternative Regimen


Regimen

Adults, adolescents A: AZT+3TC+ATV/r: if TDF A: ABC+3TC+ATV/r


(>15 years) and was used in first line A: ABC+TC+LPV/r
Pregnant women / A: TDF+FTC+LPV/r
breastfeeding mothers A: TDF+FTC+ATV/r: if AZT
was used in first line A: AZT + 3TC + DTG (For patients who did
not use DTG in the first line)
a
HIV and TB co- A: AZT+3TC+LPV/r A: ABC+3TC+LPV/r
a
infection A: TDF+FTC+LPV/r

Note: double dosage of LPV/r to 800/200mg


for Rifampicin based TB treatment

People Who Inject A: AZT+3TC + DTG A: AZT+3TC+ ATV/r


Drugs (PWID) A: ABC+3TC +ATV/r

The second line NRTI choice for adults and adolescents depends on the first line regimen. For
patients on TDF based regimens in first line, the preferred second line option is AZT plus 3TC
combined with a ritonavir-boosted PI, preferably ATV/r because it is dosed once daily and has fewer
metabolic complications and side effects. The same NRTIs, with exception of 3TC and FTC used in
previous regimen should not be used in subsequent regimens during switching due to treatment
failure. LPV/r can be used as an alternative to ATV/r in patients using anti-TB drugs (with ritonavir
super boosting) and children below six years. Also, ATV/r (300/100mg) cannot be used in children
below 30kg.

For patients who were on AZT and had never used TDF regimen, the default second line option will
be TDF or ABC based regimen combined with a boosted PI (TDF+FTC+ATV/r).

For patients who were introduced to TDF in first line due to AZT toxicity, the default second line
option is to use ABC plus 3TC combined with a ritonavir-boosted PI ATV/r or LPV/r. (ABC+3TC +
LPV/r or ATV/r). However, ABC may be rendered ineffective due to cross resistance with TDF
associated resistance mutations.

6.1.5 Third-line Antiretroviral Therapy


Patients failing 2nd line regimens may have extensive NRTI and NNRTIs associated resistance
mutations (RAMS) which preclude/minimise their use in third-line regimens. Therefore, 3rd line

119

regimens, in order to have at least two or preferably three effective drugs, need to be constructed
using other new classes of drugs or second-generation formulations of previous drugs. These
second-generation drugs usually have a higher genetic barrier to resistance and their efficacy is not
compromised by RAMs associated with the first-generation formulations.
Therefore, this guideline recommends the use of:
• Integrase Strand Transfer Inhibitors (INSTIs) or Integrase Inhibitors Dolutegravir 50mg
(DTG) and Raltegravir 400mg (RAL),
• Second generation PIs Darunavir 800mg /Ritonavir 100mg (DRV/r),

Table 6.4: Recommended Third-Line Regimens for Adults and Adolescents


Patient group Preferred (Default) Alternative Regimen
Regimen

Adults, adolescents (>15 S: DTG + DRV/r + AZT/3TC RAL + DRV/r + AZT/3TC


years)

Pregnant S: (DTG or RAL) + DRV/r + DTG + DRV/r (AZT/3TC)


women/breastfeeding AZT/3TC
mothers

HIV and TB co-infection S: DTG (BD) + LPV/r + RAL+(AZT/3TC or


(AZT/3TC or TDF/FTC) TDF/FTC) +LPV/r

People Who Inject Drugs S: DTG+DRV/r+ AZT/3TC DTG+ATV/r+ AZT/3TC


(PWID)

Note
• DTG in third line regimen should be given twice daily for clients who were previously exposed to
INSTIs.
• For TB and HIV co-infected patients on LPV/r should be switched to DRV/r after completion of TB
treatment
• For second- and third-line regimens which are non TDF based, in case of new Hepatitis B co - infection
TDF with FTC should be added to the new regimen as treatment of Hepatitis B.

6.2 Changing Antiretroviral Therapy


6.2.1 Drug Specific Adverse Events-Toxicities
• Intolerable side effects
• Drug interactions
Treatment failure
• Clinical failure-occurrence or persistence of HIV related OIs
• Immunological failure
• Virological failure

Changing ART due to toxicity


From a clinical perspective, it is generally recommended that when changing a client’s regimen due
to toxicity, only the toxic drug(s) should be replaced, wherever possible, by a drug without
overlapping toxicities. Table 6.5 provides guidance on ARV drug combinations with some common
toxicity substitution within first-line regimens.

120
Table 6.5: Types of toxicities associated with first and second-line ARV drugs (Refer to
National Guidelines for Management of HIV and AIDS 7th Edition 2019)

ARV Major types of toxicity Risk factors Suggested management


and substitution
TDF Tubular renal dysfunction, Underlying renal disease
Fanconi syndrome Older age If TDF is being used in first-
BMI <18.5 (or body weight line ART, substitute it with
<50kg) AZT or ABC
Untreated diabetes mellitus
Untreated hypertension If TDF is being used in
Concomitant use of second-line ART (AZT use in
nephrotoxic drugs or a first line ART), substitute it
boosted PI with ABC
Decreases in bone mineral History of osteomalacia and
density pathological fracture
Risk factors for osteoporosis
or bone loss
Lactic acidosis or severe Prolonged exposure to
hepatomegaly with steatosis nucleoside analogues
Obesity

Exacerbation of hepatitis B Discontinuation of TDF due to No available alternative drug


(hepatic flares) toxicity in the country for treatment
of hepatitis B e.g. Entecavir
ABC Hypersensitivity reaction Genetic predisposition (HLA-B If ABC is being used in first-
5701 gene) line ART, substitute with TDF
or AZT
AZT Anaemia, neutropaenia, Baseline anaemia or If AZT is being used in first-
myopathy, lipoatrophy or Neutropaenia line ART, substitute it with
3
lipodystrophy CD4 cell count ≤200 cells/mm TDF or ABC
Lactic acidosis or severe BMI >25 (or body weight >75
hepatomegaly with steatosis kg) If AZT is being used in
Prolonged exposure to second-line ART, substitute it
nucleoside analogues with ABC
Hepatotoxicity Underlying hepatic disease
HBV and HCV co-infection
Concomitant use of
hepatotoxic drugs
LPV/r Pancreatitis Advanced HIV disease Replace it with ATV/r

Lipoatrophy or metabolic Risk factors unknown


syndrome dyslipidaemia,
severe diarrhea and risk of
prematurity
ATV/r Indirect hyperbilirubinaemia Underlying hepatic disease Indirect hyperbilirunemia is
(clinical jaundice) HBV and HCV co infection usually transient and ATV/r
Concomitant use of can be continued, however, if
hepatotoxic drugs severe jaundice develops
and is associated with
significantly raised
transaminases, then ATV/r
should be replaced with
LPV/r

Nephrolithiasis and risk of Risk factors unknown Replace it with LPV/r


prematurity
Persistent central nervous Depression or other mental
system toxicity (such as disorder (previous or at
Replace it with DTG or NVP.
dizziness, abnormal dreams, baseline)
If the person cannot tolerate
depression or mental Taking with high fat meal
either INSTI or NNRTI, use
confusion)
boosted PIs
EFV Hepatotoxicity Underlying hepatic disease –
HBV and HCV co infection

121

Concomitant use of
hepatotoxic drug
Convulsions History of seizure
Hypersensitivity reaction,
Stevens-Johnson syndrome
Male gynaecomastia Risk factors unknown
NVP Hepatotoxicity Underlying hepatic disease
HBV and HCV co-infection
Concomitant use of
hepatotoxic drugs
CD4 >250 cells/mm3 in
EFV. If the person cannot
women
tolerate either NNRTI, use
CD4 >400 cells/mm3 for men
DTG or a boosted PI
First month of therapy (if lead-
in dose is not used)
Severe skin rash and Risk factors unknown
hypersensitivity reaction
(Stevens-Johnson syndrome)
DTG Increase in cholesterol levels; History of dyslipidemia, Monitor cholesterol levels;
mild elevated liver enzymes; diabetes, hypertension monitor Liver function
significant rises in creatinine especially in HBV and HCV.
levels; Insomnia and Provide symptomatic
headache may also be treatment
experienced.
RAL Increased Cholesterol levels, History of dyslipidemia, In case of severe adverse
Glucose, Aspartate Amino diabetes, hypertension effects, switch to DTG if
Transferase (AST), and patient is >12 years old
Bilirubin. Rash, Cough,
Fatigue, dizziness and
insomnia
DRV/r Increased Cholesterol levels, History of dyslipidemia Monitor severity and
triglycerides; Diarrhea, occurrence of fever and
Headache, Rash, Abdominal other symptoms. Provide
pain and Nausea symptomatic treatment

Figure 6.2: Substitution within first-line Antiretroviral Regimens

Note
For TB co-infected patients, the dose for DTG should be given twice daily i.e. 50mg

122

6.2.2 Changing ART due to Treatment Failure

Table 6.6: WHO definitions of treatment failure in chronological order of occurrence:


virological, immunological and clinical failure for the decision to switch ART regimens

Failure Definition Comments


Virological Plasma viral load above An individual must be taking ART for at least six
1000 copies/ ml based on months before it can be determined that a regimen has
two consecutive viral load failed.
measurements after 3
months, with adherence
support
Immunological CD4 cell count falls to the Without concomitant or recent infection or steroid use
baseline (or below) to cause a transient decline in the CD4 cell count
or Persistent CD4 levels Immunological and clinical characteristics of treatment
3
below 100 cells/mm failure develop much later after virological failure.
Immunological and clinical criteria of treatment failure
may also misclassify treatment failure and lead to
unnecessary ARV switch to subsequent (line of
treatment) regimen
Clinical New or recurrent clinical The condition must be differentiated from IRIS
event indicating severe
immunodeficiency (WHO
clinical stage 4 conditions)
after six months of effective
treatment.

Switching to Third-line ARV regimens


It is crucial that before a regimen is declared to have failed, a multidisplinary switch team is
convened to rule out non-adherence which is the commonest cause of reduced CD4 cell count and
a VL rise but is often not associated with HIV drug resistance. This team will also plan for enhanced
adherence and support, for a period of 3 months before a second VL test. In case of non-adherence,
these measures will lower the VL, increase CD4 cell count and avert a switch to a subsequent
regimen

Before switching to third-line ARV regimens, genotypic HIV drug resistance is recommended to rule
cross resistance between 1st and 2nd generation drugs and assist in the determination of whether
treatment failure is from non-adherence. Genotyping will also inform possibility of recycling drugs
used in previous regimens i.e. some drugs used in 1st or 2nd regimens may still be effective in third-
line.

6.3 Monitoring Patients on Antiretroviral Therapy


Monitoring of patients on ART is based on clinical and laboratory parameters. Refer table 6.7

Table 6.7 Clinical and laboratory monitoring of patients on first line drug regimen

Regimens Monitoring Tests Frequency Rationale

TDF+3TC+DTG HVL (All Clients) For HVL monitoring, ART monitoring


refer to HVL algorithm
ABC+3TC+DTG
AZT+3TC+ (EFV or NVP) CD4 (All clients) Baseline (All) ART monitoring
TDF+FTC+ (EFV or NVP) After every six months if
CD4 is <350 cells/ml

FBP/Hb (All clients) Baseline, week 4, Anaemia monitoring


thereafter six monthlies
If a client has Hb

123

<8.5g/dl avoid AZT

Serum Creatinine Baseline, and after Screening for early renal


(For patients on every six months and toxicity
TDF) whenever symptomatic

ALT (For patients Baseline, one month, Liver toxicity


on DTG or NVP) after every six months
and whenever
symptomatic

AZT+3TC+ATV/r Bilirubin (For all Baseline, 6 months or Indirect hyper-


clients on ATV/r) whenever symptomatic bilirubinaemia
TDF+FTC+ATV/r
ABC+3TC+LPV/r or DTG

Note
Clinical evaluation will determine more frequent laboratory tests if required.

Laboratory monitoring of patients on second line drugs


The following laboratory tests are recommended for Monitoring of patients on second line drugs:
• FBC, baseline, then monthly for 3 months, then after every 6 months (with CD4 and viral
load)
• Fasting cholesterol and triglyceride, baseline, 6 months and thereafter every 12 months
• Liver function tests, (ALT) 6 monthly
• Fasting glucose, every 12 months
• Urinalysis at baseline and after every 3 months
• Serum creatinine at baseline and once a year.

When changing treatment, the following should be observed:


• Never change a single drug in the combination if the reason for changing is treatment
failure. Change at least two drugs, preferably change all three drugs
• If changing due to toxicity, change only the drug suspected to be causing the problem.
• Never change to monotherapy (i.e. single drug)
• When selecting drugs, choose drugs that have not been used before, drugs which do not
have cross-resistance/or no overlapping toxicities or drug-drug interactions.
• Lamivudine has advantage of decreasing viral fitness therefore it may be retained when
changing the failing regimen
6.4 Immune Reconstitution Inflammatory Syndrome (IRIS)
IRIS is a phenomenon associated with the occurrence or worsening of opportunistic
infections/malignancies which can occur early after initiation of ART or at later (several months)
during ART. There is an increased risk for occurrence of IRIS in the following situations:
• Treatment naïve patients
• Patients with advanced HIV disease with CD4 cell count < 50 cells/mm3
• Patients with undiagnosed and untreated opportunistic conditions
• Patients who have been introduced on ART before or shortly after initiation of treatment of
opportunistic infection/malignancy
• In the advent of DTG use, there is increased likelihood for IRIS because of rapid HIV viral
load suppression.

Note
Any OI, malignancy and autoimmune diseases may present as IRIS

Diagnostic Criteria:
The criteria for making a diagnosis of IRIS are delineated below

124

Diagnosis of IRIS would require:
Both major (A plus B) criteria or criterion A plus 2 minor criteria
Major criteria
A. A typical presentation of “opportunistic infections or tumours” in patients responding to anti-
retroviral therapy (ART) includes:
• Localized disease e.g. lymph nodes, liver, spleen
• Exaggerated inflammatory reaction e.g. severe fever, with exclusion of other causes of
painful lesions
• Atypical inflammatory response in affected tissues e.g. granulomas, suppuration, necrosis,
perivascular lymphocytic inflammatory cell infiltrate
• Progression of organ dysfunction or enlargement of pre-existing lesions after definite,
clinical improvement with pathogen specific therapy prior to commencement of ART and
exclusion of treatment toxicity and new diagnoses
• Development or enlargement of cerebral space occupying lesions after treatment for
cerebral cryptococcus or toxoplasmosis
• Progressive pneumonitis or the development of organizing pneumonia after treatment of
pulmonary-TB or PCP
• New onset or worsening of uveitis/vitritis after resolution of CMV retinitis
• Fever and cytopenia after treatment for disseminated Mycobacterium avium complex
(MAC) disease
• Enlargement of Kaposi’s sarcoma lesions and subsequent resolution or partial regression
without
• Commencement of radiotherapy, systemic chemotherapy or intralesional therapy
B. Decrease in plasma HIV-RNA level by > 1 log base ten copies/ml (1 log drop = 9/10 of Baseline
VL copies). This applies in settings where baseline VL is performed.

Minor criteria
• Increased blood CD4+ cell count after initiation of ART
• Increase in immune response specific to the relevant pathogen e.g. delayed type
hypersensitivity to mycobacterial antigens (PPD conversion)
• Spontaneous resolution of disease without specific antimicrobial therapy or tumour
chemotherapy with continuation of anti-retroviral therapy.

Treatment of IRIS
Mild to moderate forms:
• Reassure the patient and do not stop ART
• Provide specific treatment for the opportunistic infections/malignancies or other diseases

Severe life-threatening IRIS


• Reassure the patient and Stop ART temporarily
• Provide high doses of prednisolone 1mg/kg for 4 weeks then taper down the dose.
• Provide other appropriate supportive measures such as management of fever, oxygen
therapy, i.e. fluids
• Restart ART when the patient stabilizes.

Note
When using high dose steroids, it is important to rule out Strogyloides stecolaris infection to avoid
disseminated strongylodiasis.

6.5 Antiretroviral Therapy in Children and Adolescents Living with HIV


ART in children has been proven to increase survival and decrease HIV-related morbidity and
mortality. Children should be started on ART as soon they are diagnosed including those who are
presumably diagnosed.

125

Table 6.9: When to start ART in Children Under 15 Years

Age When you start


Children 0-15 years Treat all of them regardless of WHO clinical stage or CD4
cell count
Children below 18 months old who qualify for Start ART while awaiting for DNA-PCR confirmation test
presumptive diagnosis results.

Children <18 months of age with a positive Start ART while waiting for the second DNA/RNAPCR test
DNA/RNA PCR test result

Table 6.10: First-Line ARV Regimens in Infants and Children under 15 years
st
Patient Preferred 1 Line Justification Alternatives Comments
group Regimen

Infants and ABC+3TC+LPV/r Higher genetic AZT+3TC+LPV/r LPV/r is available in


Children resistance barrier three formulations
weighing (syrup, granules and
Avoids NNRTI
<20kg AZT/3TC+DTG tablets)
transmitted resistance
(25mg or 10mg
from mother during - LPV/r oral solutions
DTG if available)
PMTCT for younger infants
until they can take
Potential for malaria
granules
prevention
- LPV/r granules for
Spares AZT for
infants and younger
second line
children

-LPV/r 100mg/25mg
heat stable tablets for
children 10kg and
above and able to
swallow whole tablets

Children and ABC+3TC + -Lowers HIV viral ABC+3TC+LPV/r


adolescents DTG load very fast
ABC+3TC
weighing
-Has high genetic Dispensable Tablet
≥20kg
barriers to resistance 120/60mg plus DTG
compared to both PIs 50mg
and NNRTIs

-Spares AZT for


second line

Children and TDF+3TC+DTG Higher genetic ABC+3TC+DTG TLD Fixed Dose


Adolescents resistance barrier Combination
TDF+3TC+EFV600
weighing
Avoids NNRTI or EFV400
≥30 kg
transmitted
resistance from
mother during
PMTCT
Possibility of malaria
prevention
Spares AZT for
second line

126

For TB and ABC+3TC+LPV/r Continue with ABC+3TC+LPV/r in
HIV co- ABC+3TC+LPV/r but the morning and only
infected the dose of LPV/r LPV/r in the evening
children should be doubled
already on due to the interaction
LPV/r-based between ritonavir and
regimen rifampicin

For TB and ABC+3TC+DTG For children 20-25 ABC+3TC+DTG in


HIV co- kg who get TB/HIV the morning and only
infected co-infection it is DTG in the evening
children advisable to give
already on them ABC+3TC+EFV
DTG based for the time of the TB
regimen treatment then revert
to ABC+3TC+DTG
after completion of
TB Treatment

For children > 25 kg


Continue with
ABC+3TC+DTG but
the dose of DTG
should be doubled
due to the interaction
between ritonavir and
rifampicin

For TB and TDF+3TC+DTG For children 20-25 TLD in the morning


HIV co- kg who get TB/HIV and only DTG
infected on co-infection it is (50mg) in the
TLD advisable to give evening
them TDF+3TC+EFV
for the time of the TB
treatment then revert
to TDF+3TC+DTG
after completion of
TB Treatment

For children > 25 kg

Continue with the


same regimen,
Double dose of DTG

For dosing of ARV regimens see Annex 6, Paediatric Antiretroviral Dosing

Note
Children with weight above 30kg can use TDF as a fixed dose combination with 3TC.

Special Considerations for LPV/r syrup, granules and tablets


• The LPV/r liquid requires a cold chain only during storage at the facility
• After dispensing, the liquid is stable at room temperature for 1 month so patients should be
given a maximum of 1-month supply
• Patients do not have to refrigerate the LPV/r liquid
• LPV/r granules for infants who can safely swallow LPV/r granules but who are unable to
swallow LPV/r tablets whole.

127

• LPV/r tablet is heat stable but must be swallowed whole and should not be split or crushed
as it loses effectiveness

6.6. Changing ART in Children Under 15 Years

I. Drug toxicity
The principles for changing ARVs and the managing drug toxicity in children are like those applied to
adults.

II. Treatment failure


Virological treatment failure: Viral load is the most reliable method to detect early treatment
failure. Virological treatment failure is recognized if the child is adherent to the current ART regimen,
for 6 months or more and has two consecutive viral load measurements over 1000 copies/ml at 3
months apart.
Immunological treatment failure: If adherence is good, immunological criteria indicating that
a change to second-line therapy is warranted where/when HVL test is not available includes
the following:

Table 6.11: CD4 Criteria Suggesting Immunological Failure a


Immunological failure is recognized as developing or returning to the following age-related
immunological thresholds after at least 6 months on ART, in a treatment-adherent child:
<5 years of age CD4 count of <200 cells/mm3 or CD4 <10%
≥5 years of age CD4 count of <100 cells/mm3
a
Preferably, at least two CD4 measurements should be available
Use of CD4 in children <5 years and absolute CD4 cell counts in those ≥5 years of age is
preferred.
If serial CD4 values are available, the rate of CD4 cell count declines from the peak, CD4 cell
count reached should be taken into consideration.

Note
CD4 cell percent should not be measured during an inter-current infection but can be determined
when the child has
recovered.

If there is a modest decline in CD4 cell count or percent (< 5%); and if there is no failure to thrive do
not change medication, instead maintain close monitoring.

Clinical Treatment Failure: Clinical conditions indicating that a change to second-line therapy is
warranted include:
• Poor growth (failure to gain weight, declining or stagnant weight) over a 6-month period,
after excluding other causes, such as TB, feeding problems and food insecurity
• No improvement of neuro-developmental milestones
• Development of HIV encephalopathy
• Recurrent infections, such as oral candidiasis, persistent diarrhoea, recurrent severe
bacterial pneumonia
• Advancement from one clinical stage to another or new evidence of new WHO stage 3 or 4
disease

Note
• Short inter-current episodes of pneumonia, LRTI and gastroenteritis should not be
regarded as clinical failure
• Pulmonary or lymph node TB, which are clinical stage 3 conditions, are not indications of
treatment failure, and thus may not require consideration of second-line therapy
• The response to TB therapy should be used to evaluate the need for switching therapy
• Before an ARV regimen is thought to be failing based on clinical criteria, the child should
have received the regimen for at least 6 months.
• The condition must be differentiated from immune reconstitution inflammatory syndrome.

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Table 6.12: Laboratory parameters for monitoring infants and children under 15 years at
baseline, before and during ART
Laboratory tests for diagnosis and Baseline At initiation of Every six As required or
monitoring (at entry first-line or months symptom-
into care) second-line directed
ART regimen

HIV diagnostic testing √

Haemoglobin √ √ √

WBC and differential count √ √

%CD4+ or absolute CD4 cell √ √b √


count

Pregnancy testing in adolescent √ √


girls

Full chemistry (including, but not √ √e √


restricted to, liver enzymes, renal
function, glucose, lipids, amylase,
lipase and serum electrolytes) e

HIV VL measurement √d √

OI screening (where possible) √ √ √ √

a. HIV re-testing for verification before ART initiation, re-testing is not indicated when
switching to 2nd or 3rd line
b. For children of <5years continue CD4 monitoring every six months
c. CD4 cell count should be taken on emergence of WHO stage 3 or 4 disease
d. Viral load monitoring is done annually if the first two VL results 6th month apart are
<1000 copies/mL
e. Regular monitoring (every six months) of full chemistry, particularly lipid levels, liver
enzymes and renal functions, should be considered for infants and children on ART.

Assessment of Infants and Children receiving ARV Therapy


Important clinical signs of response to ARV therapy in children include improvement in growth and
development and decreased frequency of infections (bacterial infections, oral thrush, and/or other
opportunistic infections).

Clinical monitoring of ARV treatment in children should include:


• Feeding practice and nutritional status
• Growth monitoring: weight, height, MUAC (mid-upper arm circumference)
• Head circumference should be monitored in children under 3 years old
• Neurologic symptoms and developmental milestones
• Cotrimoxazole prophylaxis taken daily
• Adjustment of ARV dose based on weight
• WHO disease clinical staging
• Immunization status
• Other medical conditions
• Screening for malaria and TB.

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Table 6.13: Recommended Second-line ARV regimens for children under 15 years
Patient group If is on the Preferred 2L Comments
following first line

Children and adolescents ABC/3TC+LPV/r Maintain PI -Higher genetic


<20kg whose 1st regimen resistance barrier
was EFV or NVP based, then
-Spare INSTI for third-
transitioned to LPV/r based AZT/3TC+LPV/r AZT/3TC+LPV/r
line
regimen

Children and adolescents ABC/3TC+DTG AZT/3TC+ATV/r Maintain DTG in the


≥20kg whose 1st regimen was 2nd line due to higher
AZT/3TC+DTG
EFV or NVP based, then genetic barrier than
transitioned to DTG based AZT/3TC+DTG ABC/3TC+DTG PIs.
regimen (for those who
cannot tolerate
AZT)

Children and adolescents TDF/3TC/DTG AZT+3TC+ATV/r


weighing ≥30kg
ABC+3TC+ATV/r

Note
• Infant and children take longer time to attain adequate viral suppression. Before confirming
treatment failure, calculate drop in VL (using 0.5 log two years and above, 0.7log below 2
years- for further details on how to convert VL into numbers.
• ATV/r can be used as an alternative to LPV/r in children above 6 years old if paediatric
formulation is available but adolescents >30kg can take adult formulation.

Third-Line ARV regimens in children under 15 years and adolescents


Clients failing 2nd line regimen have extensive NRTI and NNRTIs associated resistance mutations
which minimise their use in third-line regimens. Third-line regimen is constructed using new classes
of drugs or second-generation formulations, in order to have at least two or three effective drugs. For
examples, Darunavir (DRV) is a second-generation PI without cross resistance to Lopinavir/r used in
the previous regimens.

Criteria for Change to Third line


Failing any 2nd line regimen
• Referral to specialist care is recommended where third line regimen can be chosen
according to genotype resistance testing and managed by an expert panel at tertiary care
facilities.
• The criteria for diagnosing second-line failure are the same as those used for diagnosing
first-line failure.

Eligibility for Third Line Evaluation:


All clients should have undergone an Enhanced Adherence Counselling
• Failing 2nd line regimens
• Documented virologic failure (VL > 1000) on a PI regimen; except children below 3 years

Third-line Regimens for Children and Adolescents


Selection of third-line regimen should consider genotype resistance test results as well as treatment
history.

130

Table 6.14: Third-line Regimens for Children and Adolescents
Patient group 3L Options Justification

Children <20kg RAL + DRV/r + DRV/r -High genetic barrier, Effective for patients
AZT+3TC with resistance to LPVr and ATVr, cannot be used in
children <3 years of age
Children >20kg DTG + DRV/r +
and above AZT+3TC RAL-Can be used for children <20 kg
DTG-Can be used for children >20 kg

Adverse reactions in childrenand adolescents


Drug-related adverse reactions while on ART can occur immediately (soon after a drug has been
administered), early (within the first days or weeks of treatment) or later (after months of treatment).
Adverse reactions can vary in severity from mild to severe to life-threatening and may be specific to
the drug or general to the class of drugs in use.

Table 6.15: Major Types of ARV Toxicity in Children and adolescents


ABC ABC is associated with hypersensitivity reactions. Patients may have severe skin rashes or
other non-specific symptoms such as fever, arthralgias and lymph node enlargement.

AZT AZT is associated with risk of haematological toxicity which can include anaemia neutropenia
and thrombocytopenia. Measuring haemoglobin is recommended before initiating ART among
children with low body weight, low CD4 cell counts and advanced HIV disease. Patients with
severe anaemia at baseline (haemoglobin < 7.5 g/dL) should avoid AZT as first line therapy.

TDF TDF is associated with nephrotoxicity. Nephrotoxicity is more common in elderly patients, but it
also occurs in children, especially if co-administered with PI based therapy. Monitoring of
creatinine clearance is recommended.
EFV EFV’s main type of toxicity is central nervous system side effects, which typically resolve after
few weeks. However, in some cases, they can persist for months or never resolve at all.

NVP NVP’s major toxicities include severe skin rash and hypersensitivity reaction (Steven’s Johnson
syndrome) and hepatotoxicity. Because of the risk of potentially life-threatening hepatotoxicity
associated with NVP, hepatic dysfunction of any aetiology in a child on NVP requires careful
consideration of whether NVP should be continued.
LPV/r LPV/r’s major toxicity includes hepatotoxicity, pancreatitis, diarrhoea and lipoatrophy. The risk
of hepatotoxicity is increased in patients with underlying hepatic disease and the risk of
pancreatitis is increased in patients with advanced HIV disease. Electro-cardiac abnormalities
are also possible; patients with pre-existing conduction system disease are at increased risk

ATV/r Toxicities of ATV/r are like those of LPV/r. ATV/r can cause jaundice (indirect
hyperbilirubinemia). Jaundice (indirect hyperbilirubinemia) is usually transient and ATV/r can be
continued. If severe jaundice develops and there are significantly raised transaminases, then
ATV/r should be replaced with LPV/r
DRV/r DRV/r’s major toxicity is hepatotoxicity. Patients with underlying hepatic disease, hepatitis B or
C co-infection or who are taking other hepatotoxic drugs are at higher risk. The other side effect
is severe skin and hypersensitivity reactions. Patients with sulphonamide allergy are at higher
risk
RAL RAL’s potential toxicity includes rhabdomyolysis, myopathy and myalgia as well as hepatitis
and hepatic failure and severe skin rash and hypersensitivity reactions.

DTG DTG major toxicity is hepatotoxicity and hypersensitivity reactions. Patients with underlying liver
disease or hepatitis B or C co-infection are at higher risk.

Principles in the management of ARV drug toxicity


Severe life-threatening reactions:Immediately discontinue all ARV drugs, manage the medical
event (i.e. provide symptomatic and supportive therapy) and reintroduce ARV drugs using a
modified regimen (i.e. with an ARV substitution for the offending drug) when the patient is stabilized

131

Severe reactions: Substitute the offending drug without stopping ART

Moderate reactions: Consider continuation of ART if it is feasible. If the patient does not improve on
symptomatic therapy, consider single-drug substitution

Mild reactions: Reassure a child and caregiver that while the reaction may be bothersome, it does
not require a change in therapy; provide counselling and support to mitigate adverse reactions.
Emphasize on the maintenance of adherence despite mild and moderate reactions.

Table 6.16: Suggested ARV Substitutions

Toxicity events Responsible Suggested first-line ARV drug substitution


ARV
Acute symptomatic NVP EFV
hepatitis If the patient cannot tolerate either NNRTI, use
boosted PI
Severe or life-threatening boosted PI
rash (Stevens-Johnson
syndrome)
Hypersensitivity reaction ABC AZT

Lipoatrophy/metabolic LPV/r If LPV/r is used in first line ART for children, use an
syndrome age appropriate NNRTI (NVP for children below 3
years and EFV for children with 3 years and above)

ATV/r can be used for children above 6 years


Severe anaemia or AZT Substitute with ABC if < 35 kg
neutropenia
Severe gastrointestinal Substitute with TDF if > 35 kg
intolerance
Persistent and severe EFV NVP
central nervous system
toxicity
Tubular renal dysfunction TDF If TDF is being used in first line ART, substitute with
AZT or ABC
If TDF is being used in second line ART, substitute
with ABC

Note
Patients on third line ARV regimen who develop toxicities should be referred to next level facility with
adequate expertise and facilities

6.7 HIV Prevention


6.7.1 Post Exposure Prophylaxis (PEP)
Post Exposure Prophylaxis (PEP) is the immediate provision of preventive measures and medication
following exposure to potentially infected blood or other bodily fluids in order to minimize the risk of
acquiring infection. Several clinical studies have demonstrated that HIV transmission can be
reduced by 81% following immediate administration of antiretroviral agents.

Effective post-exposure management entails the following elements:


• Management of exposure site
• Exposure reporting
• Assessment of infection risk
• Appropriate treatment
• Follow-up and counselling.

When an exposure occurs, the circumstances and post exposure management procedure applied
should be recorded in the exposed person’s confidential form for easy follow up and care.
Evaluation of the Exposed Individuals

132
Evaluation of the Exposed Individuals
Individuals exposed to HIV should be evaluated within two hours and no later than 72 hours. A
starter pack should be initiated within 2 hours after exposure and before testing the exposed person.
Exposed healthcare workers should be counselled and tested for HIV at baseline in order to
establish infection status at the time of exposure. PEP should be discontinued if an exposed
healthcare worker refuses to test. Vaccination against Hepatitis B should be considered.
In addition, rape survivors should be:
• Offered counselling, crisis prevention and provision of an on-going psychosocial support to
reduce/minimize immediate rape trauma disorder and long-term post-traumatic stress
disorder should be offered.
• Referred to mental care, police and legal services, according to the law and regulations.

Evaluation of the Source Person


Evaluation of the source person should be performed when the exposed individual agrees to take
PEP.
• If the HIV, HBV and HCV status of the source person is unknown perform these tests after
obtaining consent. The exposed healthcare worker should not be involved in obtaining
consent from the source person.
• If the source person is unknown, evaluation will depend on other risk criteria.
• Do not test discarded needles or syringes for viral contamination.

ARVs used for HIV PEP


Adults
A: TDF 300mg+3TC 300mg+DTG 50mg (FDC) (PO) 24hourly for 4weeks

Children (based on body weight)


A: AZT+3TC+LPV/r 12hourly for 4weeks
Children whose weight is more than 20kg DTG can be used instead of LPV/r and maintain AZT+3TC
as backbone.

Note
If the source is using PI based regimen, then the PEP regimen should be PI based. (Similar to the
source’s regimen)

Follow-up of HIV Exposed individuals


HIV antibody tests should be performed at least after 4–6 weeks’ post-exposure (i.e. at 6 & 12
weeks). HIV testing should also be performed for any exposed person who has an illness that is
compatible with an acute retroviral syndrome, irrespective of the interval since exposure.

If PEP is administered, the exposed person should be monitored for drug toxicity at baseline and 2
weeks after starting PEP. Minimally, it should include a Full Blood Count (FBC), renal function test
(RFT-Serum creatinine and urinalysis) and hepatic function tests (LFT- ALT).

Exposed persons should be re-evaluated within 72 hours, after additional information about the
source of exposure including serologic status, viral load, current treatment, any resistance test
results (if available) or information about factors that would modify recommendations, is obtained.

PEP should be administered for 4 weeks if tolerated. If not tolerated manage symptoms accordingly
and if intolerance persists, change to more tolerable PI based regimen. If the patient seroconverts
and the exposed person becomes HIV infected, he/she should be referred to a CTC for proper care
and treatment service.

6.7.2 Pre-Exposure Prophylaxis (PrEP)


Pre-Exposure Prophylaxis (PrEP) is the use of ARV drugs daily by HIV uninfected persons to
prevent acquisition of HIV before the person becomes exposed to HIV. PrEP is used by people who
are at substantial risk for HIV acquisition to lower their chances of getting HIV infection.

133
Pre • Before

Exposure • Activity that can lead to HIV infection

Prophylaxis
• Prevention

Eligible clients for PrEP

• Aged 15 years and older • Creatinine clearance >60ml/min**


• HIV sero negative • Willingness to consent for and use
• At substantial risk* of HIV infection PrEP as prescribed
• No suspicion of acute HIV infection

*Substantial risk of HIV infection means:

• Vaginal or anal sex without a condom with more than one partner
• History of a new sexually transmitted infection
• Use of post exposure prophylaxis for sexual exposure
• Has a known HIV positive sexual partner(s) who is not on ART/ on ART less than six
months or refuses to report a risk category but still requests PrEP

Clients who are not eligible for PrEP include:

• Acute HIV Infection (AHI)


• Client with eGFR* <60ml/min
• Significantly mobile persons that will not be able to attend visits as prescribed. For
example:
o clients who will not be in a region where PrEP can be provided at the next visit
o clients who do not have contact information
• Unwilling/unable to take daily medication
• Allergy or contraindication to any medication within PrEP regimen.

ARVs used for PrEP


The recommended PrEP regimen in Tanzania is:
A:Emtricitabine200mg+Tenofovir Disoproxil Fumarate300mg(PO) 24hourly.

Indications for PrEP discontinuation


Individuals taking PrEP require ongoing risk assessment and PrEP can be discontinued if individuals
acquire HIV infection, are no longer at substantial risk for HIV infection or decide to use other
effective prevention methods and poor adherence.
Before discontinuation of PrEP, clients should be provided for at least 28 days after the last possible
exposure to HIV. The client should return after completing the final prescription for an HIV test to
confirm status. Refer the client to other relevant prevention services.

134
CHAPTER SEVEN
TUBERCULOSIS AND LEPROSY

7.1General Management of Tuberculosis


Tuberculosis is chronic airborne infectious disease caused by Mycobacterium tuberculosis. It is
transmitted from one person to another when a patient is cough, sneezing or singing.

Clinical presentation
• Cough of more than two weeks or of any duration in among PLHIV
• Fever
• Excessive night sweats
• Haemoptysis (sputum mixed with blood stains)
• Loss of weight
• Others includes swelling of lymph nodes, ascites, difficulty in breathing, chest pain,
swelling of joints etc., depending on the site of the disease

Investigations
• Sputum- smears microscopy or sputum for rapid molecular tests like Gene –Expert
• Culture and sensitivity; this is done for diagnosis of drug resistance and surveillance
• Chest X-rays: done to assist clinical diagnosis of TB or in case of triaging presumptive

Note.
• Conduct HIV provider-initiated testing and counseling (PITC)for all TB patients
• Conduct Provider Initiated TB screening (PITS) for all health facility outpatients and
inpatients

For detailed diagnosis and investigation of TB refer to ‘Manual for the Management of Tuberculosis
and Leprosy in Tanzania’.

Pharmacological Treatment
TB treatment is divided into two phases:
• Initial /intensive phase, which consists of:
• RHZE for 2 months - new and re-treatment cases
• Continuation phase, which consists of:
• RH for 4 months - new and re-treatment cases
• RH for 10 months for severe forms TB such TB meningitis, Miliary TB and TB of the spine
Table 7.1 Recommended daily doses – regimens of first-line anti-TB drugs for adults and
children
New/Retreatments Initial Phase Continuation Phase
New/Retreatments Rifampicin + Isoniazid + Pyrazinamide and Rifampicin + Isoniazid in fixed
Ethambutol in fixed dose (RHZE) for 2 dose (RH) for 4 months
months

Table 7.2 Daily dosage of anti-TB drugs (FDCs) in new and retreatment adult patients

Body weight Number of tablets in initial phase: 2 Number of tablets in continuation


months (R150/H75/Z400/E275) mg phase: 4 months (R150/H75) mg
21–30 kg 2 2
31–50 kg 3 3
51–74 kg 4 4
≥75 kg 5 5

135

Table 7.3 Daily dosages of anti-TB Drugs (FDCs) in new and retreatment paediatric patients

Intensive phase * (2 months) Continuation phase (4 months)


Weight (kg) RHZ (paediatric) 75/50/150 Ethambutol RH (paediatric) 75/50 mg
mg 100mg
For infants below 2 kg, consult a paediatric specialist, DTLC, and RTLC for treatment advice

2-2.9kg

3-3.9kg 1 1
4-7.9kg 1 1 1
8-11.9kg 2 2 2

12-15.9kg 3 3 3
16-24.9 kg 4 4 4
25 kg+ Go to adult FDCs dosages

Note
• The oral drugs must be swallowed under observation from health facility staff or treatment
supporter of his/her choice at home
• The oral drugs should preferably be given on an empty stomach in a fixed dose combination

7.1.1 Drug Resistance Tuberculosis (DR-TB)


It is a laboratory diagnosis confirmed after testing Mycobacterium tuberculosis strains for resistance
using WHO recommended rapid genotypic tests like gene-expert or conventional phenotypic culture
and DST.

Clinical presentation
The features are the same as susceptible tuberculosis but patient’s shows resistance to the first line
treatments. Signs and symptoms of DR-TB are like those of drug-susceptible TB (cough, bloody
stained sputum, fever, night sweats and weight loss). Patients with the following features have high
DR-TB risk (presumptive DR-TB patients)
• History of previous TB treatment
o Treatment failure after using first-line anti-TB medicines
o Relapse and return after loss to follow-up, without recent treatment failure
o Patients who remain sputum smear-positive at month two or later during
treatment of TB using first-line anti TB medicines
• Close contact of a known DR-TB case
• Healthcare workers presenting with TB symptoms.
• Vulnerable groups in congregate settings (prisoners, urban poor, miners, PWIDs)

All presumptive DR-TB cases adults and children must receive the Xpert MTB/RIF test as the initial
diagnostic test to ensure universal coverage of DST

Pharmacological Treatment
When you diagnose RR/MDR TB communicate with DTLC for initiation of treatment.

136
Table 7.4 Proposed MDR TB treatment regimens
Proposed regimens
If any of the medicines cannot be used,
consult the DR-TB consillium to
Age Intensive phase
Patient condition consider replacement if needed using
group --------------------------------
one or more of the following based on
Continuation phase*
DST, prior use and likelihood of efficacy
(in order of priority)
6 Lfx - Bdq - Lzd - Cfz –
MDR/RR-TB susceptible
Cs E, Z, Pto, PAS
to fluoroquinolone
12 Lfx - Cfz - Cs
MDR/RR-TB with
resistance to 6 Bdq - Lzd - Cfz - Cs –
fluoroquinolone (pre- Dlm E, Z, Pto, PAS
Adults and XDR) or extensive drug 14 Lzd - Cfz - Cs
children resistance (XDR-TB)
>12 yrs 6 Lfx - Lzd - Cs – Pto – HD
Central nervous system INH (if low-level H resistance - inhA
Z 1
disease mutation)
14 Lfx - Lzd – Cs - Z
Consult consillium on all pregnant
cases. Consider strengthening the
Pregnant RR/MDR-TB 20 Lfx - Cs - E -Cfz- Z regimen post-partum with the addition of
Bdq and Lzd (for 6 months; to replace
Class C medicines if possible).

Table 7.5: Paediatric treatment regimens for children <12 years with non-severe disease

Proposed regimens
If any of the medicines cannot be used,
consult the DR-TB consillium to consider
Age Intensive phase
Patient condition replacement if needed using one or more
group -------------------------------
of the following based on DST, prior use
Continuation phase*
and likelihood of efficacy (in order of
priority)
1
RR/MDR TB Cfz, Dlm (E if documented sensitivity), Z
6 Lfx – Bdq – Lzd – Cs
susceptible to (Cfz preferred over Cs if 50mg capsule
3 Lfx – Lzd – Cs
fluoroquinolone available)
Children RR/MDR-TB with
6 – 12 resistance to 1
Cfz, Dlm (E if documented sensitivity), Z
yrs fluoroquinolone (pre- 6 Bdq - Lzd - Cs - PAS
(Cfz preferred over PAS if 50mg capsule
XDR) or extensive 3 Lzd - Cs - PAS
available)
drug resistance (XDR-
TB)
1
Cfz, Dlm , PAS (E if documented
sensitivity), Z; Eto should not be used if
RR/MDR TB
9 Lfx/Mfx - Lzd - Cs - inhA mutation
susceptible to
Eto (Cfz preferred over Eto if 50mg capsule
fluoroquinolone
available)
3 – 6 yrs
Cfz, PAS (E if documented sensitivity), Z;
RR/MDR-TB with 1
6Lzd - Cs – Dlm - Eto Eto should not be used if inhA mutation
resistance to
3 Lzd – Cs - Eto (Cfz preferred over Eto if 50mg capsule
fluoroquinolone
available)
Cfz, PAS (E if documented sensitivity), Z;
RR/MDR-TB
9 Lfx/Mfx - Lzd - Cs - Eto should not be used if inhA mutation
susceptible to
Eto (Cfz preferred over Eto if 50mg capsule
fluoroquinolone
< 3 yrs available)
1
RR/MDR-TB with Cfz, Dlm (E or Z if documented sensitivity)
6 Lzd - Cs – PAS – Eto
resistance to (Cfz preferred over Eto if 50mg capsule
3 Lzd- Cs - PAS
fluoroquinolone available)

137
Table 7.6: Modified Short Treatment Regimen

Age Patient condition Proposed regimens


group
Intensive phase Continuation
phase

15 yrs Patient eligible for short treatment 6 Bdq – Lzd – Lfx – Cfz – Cs 3-5 Lfx – Cfz –
and regimen –Z Cs – Z
above
Patient eligible for short treatment
regimen but cannot tolerate
linezolid (Haemoglobin (Hb) < 8
6 Bdq – Dlm– Lfx – Cfz – Cs 3-5 Lfx – Cfz –
g/dL, neutrophils <0.75 x109/L or
–Z Cs – Z
platelets <50 x109/L or severe
peripheral neuropathy grade ≥2 or
optic neuritis grade ≥2 at baseline)

7.1.2 Treatment of Tuberculosis in Special Cases


Treatment of TB/HIV co-infected patients
Consideration is needed when handling a patient with TB/HIV co-infection.

Table 7.7 Special considerations for ART in TB/HIV co-infected patients


Start ART for all TB patients living with HIV Treat TB first and start ART as soon as possible,
irrespective of CD4 counts preferably within two weeks of initiating treatment
Already on ART at TB diagnosis Refer to HIV and AIDS chapter

Also, the following shall be considered in treatment of TB patients:

Pregnancy
Anti-TB is safe during pregnancy and breast feeding.

TB Prevention;
TPT is offered to:
• Under 5 household contacts of bacteriologically confirmed PTB cases who have no
active TB.
• All PLHIV who have no active TB.

Dosage
In adult and adolescent
A: isoniazid (PO) 300mg 24hourly for 6months to complete one cycle of TPT
In children
A: isoniazid (PO) 10mg/kg (10-15 mg/kg) 24hourly for 6months.

Note
• TPT should only be given in one cycle in lifetime and no repeat cycle is needed.
• People living with HIV who successfully completed their TB treatment should immediately
receive TPT for six months.
• In case of neuropathy due to INH, Pyridoxine should be used for treatment of neuropathy.
• TB Preventive Therapy is not contraindicated in pregnancy and it can be given during any
trimester.

Breast feeding: In the mothers with pulmonary tuberculosis, the baby should receive INH
preventive (5mg/kg) for 6 months followed by BCG vaccination.

Oral contraceptives: Rifampicin interacts with oral contraceptives and reduces the efficacy of this
contraception.

138

Liver disease: Most of anti-TB medicines can cause liver damage. In case a patient develops
jaundice, treatment should be stopped and restarted as soon as the jaundice resolves. In severely ill
patients, start moxifloxacin and ethambutol only.

Renal failure: Ethambutol is excreted by the kidneys and should either be avoided or given in a
reduced dose.

7.2 General Treatment of Leprosy


Leprosy is a chronic granulomatous disease caused by Mycobacterium leprae. It mainly affects the
skin, the peripheral nerves and the mucous membranes. Leprosy is the commonest cause of
peripheral neuritis in the world.

Clinical presentation
Presence of any one among the three cardinal signs of leprosy below:
• Skin patch with loss of sensation
• One or more enlarged peripheral nerves
• Presence of leprosy bacilli–positive smear

Classification of Leprosy
Multibacillary (MB) Leprosy
• Patients with six or more leprosy skin lesions
• Positive skin smear

Paucibacillary (PB) Leprosy


• Patients with one to five leprosy skin lesions
• Negative skin smear

Note
• If there is any doubt regarding the classification, the patient should be classified and
treated as a multi-bacillary case.

Pharmacological Treatment
Patients should be treated by multidrug combination therapy; dosage may depend with classification
and whether patient is adult or children

Table 7.8 Treatment of Leprosy


Classification Medicine dosage Duration of treatment
Adult MB: Day 1: Rifampicin 600mg (2x 300mg) +Clofazimine 12 blister packs to be taken
15years and 300mg (3 x 100mg) + Dapsone 100mg. Daily within a period of between
above Treatment: Day 2–28, Clofazimine 50mg + Dapsone 12–18 months
100mg
Child MB: Day 1: Rifampicin 450mg (3 x 150mg) + Clofazimine 12 blister packs to be taken
below 15years 150mg (3 x 50mg) + Dapsone 50mg. Daily Treatment: within a period of between
Day 2–28 Clofazimine 50mg every other day + 12–18 months
Dapsone 50mg daily.
Adult PB: Day 1: Rifampicin 600mg (2x 300mg) +Clofazimine 6 blister packs to be taken
15years and 300mg (3 x 100mg) + Dapsone 100mg. Daily within a period of between
above Treatment: Day 2–28, Clofazimine 50mg + Dapsone 6–9 months
100mg
Child PB: Day 1: Rifampicin 450mg (3 x 150mg) + Clofazimine 6 blister packs to be taken
below 15years 150mg (3 x 50mg) + Dapsone 50mg. Daily Treatment: within a period of between
Day 2–28 Clofazimine 50mg every other day + 6–9 months
Dapsone 50mg daily.

7.2.1 Treatment of Leprosy in Special Cases


Tuberculosis: Patients suffering from both tuberculosis and leprosy require appropriate anti-
Tuberculosis therapy in addition to the MDT. Rifampicin must be given in the dose required for the
treatment of tuberculosis. Once the intensive phase of anti TB treatment is completed, the patient
should continue with his/her monthly rifampicin for leprosy treatment.

139

There are two types of reactions
• Reverse Reaction or type I reaction
• Erythema Nodosum Leprous (ENL) or type II reaction (For detail refer Manual for the
Management of Tuberculosis and Leprosy in Tanzania)

Treatment of Reaction: Depending on severity, treatment of reverse reaction is by giving anti-


inflammatory drugs or corticosteroids usually prednisolone for a prolonged period.

Note
Health care worker should communicate with DTLC and RTLC when suspect leprosy reaction

140

CHAPTER EIGHT
NERVOUS SYSTEM DISEASE CONDITIONS

8.1 Infections of the Nervous System


Infections of the nervous system can arise secondary to bacteria, fungi, protozoa, helminthes or
viruses. Clinical features will depend on the site of the nervous system involved.

8.1.1 Bacterial infections


8.1.1.1 Bacterial Meningitis
Bacterial meningitis is a serious infection involving layers (meninges) covering the brain and spinal
cord. Causative bacteria differ among different age groups.

Clinical presentation
• Headache, high grade fever
• Altered mental status, convulsions, coma.
• Photophobia
• Nausea and vomiting
• Signs of meningeal irritation

Investigations
CBC, Blood C/S, Lumbar puncture for CSF analysis

Pharmacological Treatment
I. Where the organism is not known:
A: benzyl penicillin (IV) 5MU 6hourly for 14days.
AND
B: chloramphenicol (IV) 1000mg 6hourly for 14days
Alternatively
D: ceftriaxone+Sulbactam (FDC) (IV) 1.5g 12hourly for 14days
Alternatively
A: ampicillin (IV) 2g 6hourly for 10–14days
AND
S: cefepime (IV) 2g 8hourly for 10–14days
Alternatively, and based on C/S results give
S: meropenem (IV) 2g 8hourly for 10days

II. Where the organism is known:


Meningococcal meningitis (Refer to notifiable diseases section)

Haemophilus influenza meningitis


B: chloramphenicol (IV) 1g 6hourly for 7–10days.
OR
D: ceftriaxone+Sulbactam (FDC) (IV) 1.5g 12hourly for 14days

Pneumococcal meningitis
A: benzyl penicillin (IV) 5MU 6hourly for 14days
OR
D: ceftriaxone + Salbactam (FDC) (IV) 1.5mg 12hourly for 14days

8.1.1.2 Tuberculous Meningitis


Tuberculous meningitis (TBM) is the most common form of central nervous system tuberculosis,
associated with high mortality and morbidity from neurological sequelae.

Clinical presentation
• Headache • Seizures
• Low grade fever • Nausea and vomiting
• Altered mental status, coma. • cranial nerve palsies

141
Laboratory investigations
• CBC
• Blood C/S
• LP for CSF analysis
o lymphocytic-predominant pleiocytosis usually between 100-500 cells/µL
o elevated protein levels typically between 100 and 500 mg/dL
o low glucose-usually less than 45 mg/dL or CSF:Plasma ratio <0.5.
• CSF GeneXpert
• CSF for AFB
• HIV testing

Imaging Investigations
• Contrast head CT scan-can demonstrate multiple ring-enhancing lesions, meningeal and
basal cisterns enhancement
• Contrast brain MRI with diffusion weighted sequences (DWI)

Pharmacological management
Refer to TB and leprosy chapter

Non-pharmacological management
• Screen for postinfectious hydrocephalus as it is a common complication of all meningitis
cases and can occur early during treatment—monitor for persistent headache, vomiting,
papilledema on fundoscopy and parinauds syndrome.
• Refer all patients presenting with clinical or radiological features of increased ICP from
hydrocephalus for neurosurgical evaluation directed at treatment of the associated
hydrocephalus by external ventricular drainage (EVD) or VP shunt once CSF is sterile.
• Monitor urine output and serum sodium levels as syndrome of inappropriate antidiuretic
hormone secretion (SIADH) is a common complication

8.1.1.3 Tetanus
It is an acute, often fatal disease caused by an exotoxin produced by the anaerobic bacterium
Clostridium tetani. It is acquired through wounds contaminated with spores of the bacteria and in the
case of neonates, through the umbilical stump, resulting in neonatal tetanus.

Clinical presentation
• Generalized spasms and rigidity of • Dysphagia
skeletal muscles • Diaphoresis
• Locked jaws • Local spasms may also occur
• Patients are usually fully conscious
and aware.

Non-pharmacological Treatment
• Admit in intensive care unit (ICU)
• Nurse in dark, quiet room to avoid unnecessary external stimuli which can trigger spasms
• Protect the airway (evaluation for early tracheostomy is required)
• Thorough cleaning of the site of entry site (e.g., wound), leaving it exposed without
dressing
• Maintenance of fluid balance and nutrition (via NGT)
• Avoid giving medications via IV/IM route as injections can trigger spasms
• Sedation (see below) and care as for unconscious patient

Pharmacological Treatment
Treatment is generally aimed at the following:
Pain management as the spasms can be very painful
A: paracetamol (PO/NGT) 1gm 8 hourly for 5 days

For prevention of further absorption of toxin from the wound


A: human tetanus immunoglobulin (IM) Adults give 3000IU stat
AND
A: amoxicillin (PO/NGT) 500mg 8hourly for 5days

142
AND
A: metronidazole (PO/NGT) 400mg 8hourly for 5days

Control of spasms: Give a sedative cocktail of the following medications preferably via NGT:
A: diazepam (PO/NGT) 10-30mg 4-6hourly for 7-14days
AND
A: chlorpromazine (PO/NGT)100–200mg 8hourly for 7-14days
AND
A: phenobarbitone (PO/NGT) 50–100mg 12hourly for 7-14days

Table 8.1:Guidelines for Dosage Administration**


Time (Hours) 0 3 4 6 9 12 15 18 21 24
diazepam * * * * *
chlorpromazine * * *
phenobarbitone * *

Prevention: tetanus (toxoid) vaccine (IM) 0.5ML; repeat after 4 weeks and after 6-12months, then
boost every 10years thereafter.

8.1.1.4 Brain Abscess


Brain abscess is a focal collection of purulent material within the brain parenchyma, which can arise
as a complication of a variety of local cranial or remote systemic infections, trauma, or surgery. The
manifestations of brain abscess depend on the site, size, and the immune status of the patient.

Clinical presentation
• Headache • Focal neurological deficit
• Fevers • Altered mental status that may
• Seizures progress to coma

Imaging Investigations
• Contrast head CT scan--can demonstrate a ring enhancing lesion and possible source of
infection e.g., from paranasal sinuses, ear infections
• Contrast brain MRI with diffusion weighted sequences (DWI)
• MR spectroscopy to distinguish from brain tumors where diagnosis is unclear
• CXR
• ECHO in suspected valvular heart disease

Lab Investigations
• Gram stain, C/S of pus from possible sources
• Purulent aspirate from the abscess for C/S
• Ziehl Neelsen stain

Non-pharmacological Treatment
• Follow the ABCD protocol
• If unconscious insert NGT for feeding
• insert urethral catheter

Pharmacological Treatment:
• Control fever and pain with IV Paracetamol
• Manage seizures with antiepileptic drugs
• Prompt initiation of intravenous antibiotics
• Steroids in selected case

143
Table 8.2: Pharmacological management of Brain abscess
Condition Treatment Duration
Brain abscess A: benzyl penicillin (I.V) 5MU 6hourly 4-6weeks
(unspecific bacterial) OR
C: amoxicillin +clavulanate (FDC) (IV) 1.2g 12hourly
OR 4-6 weeks
D: ceftriaxone+sulbactam (FDC) (IV) 1.5g 12hourly
AND
A: metronidazole (IV) 500mg 8 hourly

alternative regimen based on C/S results


S: piperacillin+tazobactam (FDC) (IV) 4.5g 8hourly
OR
S: meropenem (IV) 2g every 8hourly 2weeks

2weeks
Brain abscess (Staph. S: vancomycin (IV) 1g 12hourly (used 4-6weeks
aureus) with cefotaxime or ceftriaxone+Sulbactam)
Seizures control C: phenytoin (IV) 15mg/kg loading dose infused at Until seizure
50mg/min followed by 100mg (IV/PO) 8hourly free for at least
OR 6 months
A: carbamazepine (PO/NGT) 200mg 12hourly
OR
C: sodium valproate (PO) 250mg 12hourly (escalate
dose as required based on response)

ICP control in selected B: dexamethasone (IV) 0.15mg/kg 6hourly 3-5days


cases

Note:
If allergic to penicillin, chloramphenicol 500mg IV every 6hours can be used instead.In case
antiepileptic drugs are used for prolonged durations 5mg daily Folic acid supplement should be
added for the entire duration of anticonvulsants treatment especially in women of childbearing
age.

Surgical management
• Refer all patients diagnosed with a brain abscess for neurosurgical evaluation.
• Surgical options include stereotactic abscess aspiration and craniotomy for abscess
excision. In cases where the source of
infection is paranasal sinuses or ear infection, involve concomitant ENT surgeon
evaluation for primary source control interventions.

8.1.2 Fungal Infections


Cryptococcus Meningitis (CM)
CM is the most common form of fungal meningitis worldwide. It often develops in patients who are
immune compromised e.g., HIV-positive patients with low CD4 cell count, diabetic mellitus and
iatrogenic immunosuppression, as in post organ transplant patients.

Clinical features
• Headache, fever, intolerance to light • In advanced stages it may present
and sound, with confusion,
• Neck stiffness, vomiting, seizures, • Altered mental status that may
deafness, impaired vision progress to coma.

Investigations
• CSF gram stain
• CSF India Ink stain test
• Serum or CSF Cryptococcus antigen (CrAg) test
• CSF cultures
• Contrast brain MRI

144
o may demonstrate cryptococcomas
o assist to rule out differential diagnoses

Pharmacological Treatment
The treatment should be done in 3 phases:
Phase 1: Induction phase
S: amphotericin B (IV) 0.7-1mg/kg/day
AND
S: 5 flucytosine (PO)100mg/kg/day for 7days followed by 1 week of
AND
A: fluconazole (PO): Adult 1200mg/day,
Children/adolescents 2mg/kg/day, up to a maximum dose of 800mg daily

In the absence of flucytosine, alternative therapy should be:


S: amphotericin B (IV) if available give 3-6mg/kg for 10days
AND
A: fluconazole (PO) 1200mg once daily for 14days
OR
C: fluconazole (IV) 1200mg once daily for 14days

Phase 2: Consolidation phase


A: fluconazole (PO) 800mg/day for 8weeks or until CSF is sterile.

Phase 3: Maintenance phase


A: fluconazole (PO) 200mg 24hourly for 1year
Discontinue maintenance treatment if CD4 ≥100 with undetectable (<50 copies), viral load or CD4 ≥
200 if viral load monitoring not available.

Note
• It is recommended to initiate ART 5 weeks after initiation of Cryptococcal meningitis
treatment in ART naïve patient to prevent IRIS and reduce mortality.
• Monitor creatinine, BUN, serum Potassium and magnesium in all patients on Amphotericin
B every 24hours.

Non-pharmacological Treatment
• Refer to section on bacterial meningitis in unconscious patients.
• Perform serial Lumbar puncture for management of increased ICP in cryptococcal
meningitis. Opening pressure should be measured during LP and therapeutic CSF
drainage done (20-30ml per session) for pressures >25cm H2O.
• Failure to control ICP after several LPs (recommended 3 attempts) should prompt
neurosurgical evaluation for ventriculoperitoneal shunt insertion to divert CSF.

Note
The usage of Mannitol, Hypertonic saline, acetazolamide, or corticosteroids to manage increased
ICP in Cryptococcal meningitis is ineffective and NOT recommended.

8.1.3 Protozoa infections


Toxoplasmosis
Immunocompetent persons with primary infection are usually asymptomatic, but latent infection can
persist for the life of the host. In immunosuppressed patients, especially patients with AIDS, the
parasite can reactivate and cause disease, usually when the CD4 lymphocyte count falls below 100
cells/mm3.

Clinical presentation
• Altered mental status • Seizures
• Focal neurological deficits • Neuropsychiatric manifestations

145
Imaging Investigations
• Contrast head CT scan-demonstrates ring-enhancing lesions
• Contrast brain MRI with diffusion weighted sequences (DWI)
• CXR

Laboratory Investigations
Toxoplasma serology (IgM)

Non-pharmacological Treatment
Similar to bacterial meningitis

Pharmacological Treatment For


acute infection give:
D:sulfadiazine (PO) 1g 6hourly for 6weeks
AND
D: pyrimethamine (PO) 100mg loading dose then 50mg /day for 6weeks
AND
S: folinic acid (PO) 10mg /day for 6weeks.

After six weeks of treatment give maintenance treatment with


D: sulfadiazine (PO) 500mg 6hourly
AND
D: pyrimethamine (PO) 25-50mg /day
AND
S: folinic acid (PO) 10mg /day until CD4 counts is above 200cells/microlitre and/or
undetectable viral load for 3-6months

For those allergic to sulphur replace Sulfadiazine with


S: clindamycin (PO) 450mg 6hourly for for 6weeks.

8.1.4 Helminthic infections


Neurocysticercosis (NCC)
NCC is a neurologic infection caused by the larval stage of the tapeworm Taenia solium. In the
developing world NCC is the most common cause of new onset acquired epilepsy among the adult
population. Humans are the definitive hosts for this parasite, and swine are the intermediate hosts.
The mature tapeworm develops in humans after they ingest live cysticercus in undercooked pork.
NCC develops when humans accidentally ingest eggs from fecal contaminated food.

Clinical presentation
• Headache • Features of increased intracranial
• Seizures pressure
• Focal neurological deficit

Imaging Investigations
• Contrast head CT scan-can demonstrate ring enhancing lesions, calcified lesions
• Contrast brain MRI can demonstrate viable cystic lesions with scolices

Laboratory Investigations
• FBP, serum electrolytes
• Enzyme-linked immunotransfer blot (EITB)
• Liver function tests

Non-pharmacological Treatment
• If unconscious, airway and breathing management
• Insert NGT for feeding
• Insert urethral catheter

146
Pharmacological Treatment
Table 8.3: Pharmacological Management of NCC
Condition Treatment Duration
Antihelminthic A: albendazole (PO) 15mg/kg/day divided into two daily 2-4weeks
treatment for single doses (maximum of 1200mg/day)
viable lesion
Anthelminthic treatment A: albendazole (PO) 15mg/kg/day divided in two daily 2-4weeks
for multiple viable doses (maximum of 1200mg/day)
lesions AND
A: praziquantel (PO) (50mg/kg/day) 2weeks
Seizures control C: phenytoin (IV) 15mg/kg loading dose infused at Until seizure free
50mg/min followed by 100mg (IV/PO) 8hourly for at least 6
OR months
A: carbamazepine (PO) 200mg 12hourly (can be adjusted
based on individual response)
OR
C: sodium valproate (PO) 250mg 12hourly
(escalate dose as required based on response)
Control of increased D: dexamethasone (PO) 0.15mg/kg 6 hourly for 3-5days 2weeks
ICP then taper down.
OR
B: dexamethasone (IV) 0.15mg/kg 6 hourly for 3-5days
then taper down

Note
Fundoscopic examination is mandatory for all patients before initiation of anthelminthic therapy.

Surgical management
• Refer all patients diagnosed with CNS cysticercosis associated with clinical or radiological
features of increased intracranial pressure from hydrocephalus for neurosurgical
evaluation directed at management of the associated hydrocephalus.
• In patients with untreated hydrocephalus or diffuse cerebral edema, management of
elevated intracranial pressure should proceed anthelminthic treatment.

8.1.5 Viral infections


Viral infections of the nervous system are mainly caused by Herpes simplex virus (HSV) and Human
immunodeficiency virus (HIV). (Refer to section on viral infections and HIV)

Herpes simplex encephalitis


Most of cases in adults are caused by HSV-1, a small number are caused by HSV-2 usually in
immunosuppressed states or in neonates. It should be suspected in all patients not responding to
antibiotics/other treatments.

Clinical presentation
• Early features are fever, headache & altered consciousness which may develop gradually
over days or rapidly over hours
• The most common manifestations are personality change, dysphasia, behavioural
disturbance, and occasional psychotic features
• Focal or generalized seizures

Investigations
• Lumbar puncture--CSF is under increased pressure and may appear normal or show a
mild-moderate lymphocytosis, a mild-moderate elevated protein levels and normal or
decreased glucose.
• CSF PCR
• HSV1+HSV2 CSF Rapid test
• MRI—demonstrate predominant involvement of the limbic system structures, medial
temporal lobes, and insular cortex

147
Pharmacological Treatment
B: acyclovir (IV/PO) 10–15mg/kg 8hourly for 14–21days

Non pharmacological treatment


Provide supportive therapy as for unconscious patients

8.2 Initial Management of Stroke


8.2.1 Management of Acute Hemorrhagic Stroke
Spontaneous, nontraumatic intracerebral hemorrhage (ICH) remains a significant cause of morbidity
and mortality throughout the world. However, population-based studies indicate that most ICHs in
most patients are survivable with good medical care thus emphasizing the importance of improved
clinical care. in determining ICH outcome.

Clinical presentation
• Severe headache, vomiting, • decreased level of consciousness
• Focal neurological deficits that may progress to coma
• symptom progression over minutes
or hour

Investigations
• Rapid neuroimaging: plain CT to distinguish ischemic stroke from ICH
• MRI with angiography-useful to evaluate for underlying structural lesions e.g., vascular
malformations and tumors in suspicious cases

Admit all patients with ICH in an ICUor dedicated stroke unit for initial management and
monitoring.

Pharmacological Treatment
For elevated SBP (150-220mmHg), initiate BP lowering treatment, target at 140mmHg. Consider
more aggressive reduction if SBP>220mmHg.
C: labetalol (IV) at 1mg/min until target SBP is attained.

Anticoagulation-related ICH: withhold anticoagulants and correct INR, if elevated, start on vitamin K
and consider FFP transfusion
B: phytomenadione (vitamin K) (IV) 1mg slow infusion over 60 minutes

If increased ICP based on clinic radiological features, give


C: mannitol (IV bolus) 0.25-1gm/kg 4-6hourly for 24-72hours
OR
C: hypertonic saline 3% (IV bolus) at 3-5ml/kg 4-6hourly for 24-72hours

Monitor serum osmolarity and renal function when giving Mannitol or Hypertonic saline, stop if
osmolarity goes >320mOsm/L
Treat fever with antipyretic medications and/or external cooling methods
D: paracetamol (IV) 1g 8hourly for 3-5days then when required

Perform regular monitoring and control of blood glucose to prevent both hyperglycemia and
hypoglycemia.
Treat clinical or electrographic seizures associated with decreased loss of consciousness
S: levetiracetam (PO/IV) 500mg 12hourly for 2weeks
C: phenytoin (IV) 15mg/kg loading dose over 30min, then maintenance at 100mg 8hourly
for 2weeks.

Non-pharmacological Treatment
• Apply compressive stockings or intermittent pneumatic compression at admission to
prevent VTE
• LMWH can be started later after cessation of bleeding in immobile patients.
• Consider systemic anticoagulation or IVC filter only in patients with symptomatic deep
vein thrombosis or Pulmonary embolism.

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Surgical management
• Consider neurosurgical evaluation for External Ventricular drainage (EVD) in patients
with decreased level of consciousness from resultant hydrocephalus in the setting of
intraventricular hemorrhage.
• Refer for surgical evacuation of hematoma as soon as possible in patients with
cerebellar hemorrhage who are deteriorating neurologically or who have brainstem
compression and/or hydrocephalus from ventricular obstruction
• For supratentorial hematomas, consider evacuation in deteriorating patients with or
without decompressive craniectomy as a life-saving measure in selected cases, based on
expert neurosurgical clinical judgement.
• Consider minimally invasive clot evacuation via stereotactic or endoscopic aspiration with
or without thrombolytic usage, based on expert clinical judgement and available resources.

8.2.2 Initial Management of Acute Subarachnoid Hemorrhage from Ruptured


Cerebral Aneurysm
Subarachnoid haemorrhage (SAH) refers to presence of blood in the fluid-filled subarachnoid
spaces around the brain and spinal cord. The most common presentation is sudden onset of severe
novel headache. SAH from ruptured cerebral aneurysms is associated with high mortality and
morbidity hence clinician’s high index of suspicion and proper initial management is crucial for
patient’s survival and improved functional outcome.

Clinical presentation
• Severe headache (worst headache • Focal neurological deficits
of life) • Seizures
• Altered mental status that may
progress to coma

Laboratory Investigations
• CBC, PT/PTT/INR
• Serial ABGs, electrolytes
• serum and urine osmolality

Imaging investigations
• CT angiography
• Four vessel catheter angiography/digital subtraction angiography (DSA)
o Perform 4-vessel catheter angiography to determine source of bleeding
o The timing of study takes into consideration the patient’s condition (unstable or
premorbid patients are not candidates), the feasibility of early treatment, the
likelihood of endovascular therapy (based on patient’s age and predicted
aneurysm location as well as availability of required resources and expertise)
• CXR—monitor for pulmonary edema if in hyperdynamic therapy

Principles of initial management of aneurysmal SAH are focused on


• Initial hemodynamic stabilization and life support of the patient
• Prevention of rebleeding through timely coiling or surgical clipping
• Prevention, identification, and early management of hydrocephalus
• Prevention and management of delayed ischemic neurologic deficit (DIND) from
vasospasm

Admitting orders
• Admit all aneurysmal SAH patients to ICU regardless of their initial GCS score
• Document initial Hunt & Hess, WFNS clinical scores, and Fisher CT scan score
• Bedrest with head of bed elevation at 30°.
• Initiate SAH precautions (low level of external stimulation, restricted visitation, dim light, no
loud noises)
• Check neurological status every 1 hour.
• Bed pan, indwelling Foley catheter if patient is lethargic, incontinent with strict Inputs &
outputs measurements.
• Keep Nil per Oral (if in preparation for surgery or endovascular intervention)

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• Maintain SBP 120–160mmHg in unsecured (unclipped/uncoiled) aneurysm to minimise
rebleeding risk, consider

D: labetalol (IV) 1mg/min until target SBP is attained.

• IV fluids: 0.9% NS + 20 mEq KCl/L at 2 ml/kg/hour maintenance fluid

Prophylactic anticonvulsants:
S: levetiracetam (PO/IV) 500mg 12 hourly while aneurysm is unsecured, continue for
1week post clipping/endovascular intervention
OR
C: phenytoin (IV) 15mg/kg loading dose at 50mg/min rate then 100mg 8hourly for 2-4
weeks

Sedation (not over sedation):


D: propofol (IV) (for intubated patients) at 25-75mcg/kg/minute

Give
B: dexamethasone (IV) 4mg 6 hourly for 3-5days to reduce neck pain
AND
S: fentanyl (IV) 25–100mcg (0.5–2 ml) every 1–2hours when required in ICU.

Stool softener: Initiate


C: lactulose (PO) 30mls 8hourly until aneurysm is secured.

Anti-emetics:
D: ondansetron (IV) 4mg over 2–5minutes, may repeat 8hourly for 1–2days.

Prevention of vasospasm: Initiate


S: nimodipine (PO/NGT) 60mg 4hourly, continue for 21days

Stress ulcer prophylaxis:


C: pantoprazole (IV) 40mg 24hourly for 1-2weeks

Oxygenation goals (for intubated ventilated patients)


o pO2 > 100mm Hg, O2 saturation 100% in patients at risk for vasospasm, aim for 92%
saturation in all others.
o To achieve above goals, increase FiO2 and mean airway pressure (PEEP) in
ventilated patients
o in non-intubated patient: Give O2 2L per nasal cannula PRN (based on ABG)
• Strive for normocarbia, avoid prophylactic hyperventilation
• Avoid arterial hyperoxia (paO2 > 300mm Hg)- to avoid risk of vasoconstriction
• maintain normothermia and encourage other cooling measures to reduce and prevent fever.
D: paracetamol (IV) 1g 8hourly for 3-5days then when required
• Hemoglobin and hematocrit: Transfuse whole or PRBC when Hct drops < 40%)
• Monitor serum glucose and maintain normoglycemia

Surgical management
Refer to a centre that can handle neurovascular cases for prompt neurosurgical evaluation and
subsequent surgical clipping or endovascular intervention (coiling or embolization) to secure the
ruptured cerebral aneurysm.

8.2.3 Initial management of Acute Ischemic Stroke


Acute ischemic stroke (AIS) is a leading cause of adult disability in the developed world.In AIS, a
thrombus impairs cerebral blood flow, resulting in brain tissue infarction. Collateral blood flow gives
rise to an area of hypoperfused tissue (ischemic penumbra) that is at risk of infarction if
hypoperfusion persists. Prompt reopening of an occluded blood vessel to re-establish blood flow to
the ischemic area (reperfusion) in eligible patients, can rescue the ischemic penumbra from death
and spare the patient from serious long term disabilities.

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Clinical presentation
• Severe headache • seizures
• Focal neurological deficits • symptom progression over minutes
• decreased level of consciousness or hours
that may progress to coma

Investigations
• FBP, PT/PTT/INR, • CT angiogram in potential
• Random blood glucose candidates for reperfusion
• serial ABGs, serum electrolytes • CT/MR perfusion studies
• Non contrast CT scan to distinguish • MR angiography (MRA) with
AIS from ICH
• DWI for selected patients. (contraindicated with cardiac pacemakers, metal implants)
• Four-vessel catheter angiography
• Baseline ECG and ECHO

Prehospital and lower level health facilities


• Provide initial airway management and hemodynamic stabilization
• Exclude stroke mimics like hypoglycemia
• International stroke guidelines recommend rapid identification of all fibrinolytic-eligible and
mechanical thrombectomy-eligible patients to facilitate initiation of treatment in the fastest
achievable onset-to-treatment time
• Consider prompt referral to a centre that can handle stroke patients including rapid
neuroimaging and administration of reperfusion therapy.

Referral hospital and specialized centres


• Provide initial stabilization of the patient as per ABCDE protocol
• Perform rapid careful neurological examination.
• Order emergency brain imaging evaluation before initiating any stroke specific treatments.
• Screen for reperfusion eligible patients and initiate appropriate treatment protocol.
• In patients with AIS who awake with stroke symptoms or have unclear time of onset > 4.5
hours from last-known-well (LKW) state, perform brain MRI to identify diffusion-positive,
FLAIR-negative lesions to aid selecting those who can benefit from IV alteplase
administration.
• In potential candidates for mechanical thrombectomy, consider imaging of the extracranial
carotid and vertebral arteries, in addition to the intracranial circulation, to provide useful
information on patient eligibility and endovascular procedural planning.

Reperfusion criteria: all must be met


• Onset of stroke or Last known well (LKW) state <4.5hours
• No increased bleeding risk contraindications
• Blood pressure controlled to <185/105mmHg target.
• Non contrast brain CT has excluded intracranial hemorrhage and/or
• established a hypodense zone or hyperdense vessel sign.

Non-pharmacological Treatment
• Oxygenation—support airway, maintain O2 saturation >94%
• Monitor BP, if elevated, initiate BP lowering treatment to target BP<185/110 mmHg
• For patients who are non-eligible for fibrinolysis aim to lower BP by 15% in the first 24
hours
• Monitor body temperature and initiate treatment when >38°C
• In immobile stroke patients without contraindications, offer compressive stockings, or
pneumatic compression devices for DVT prophylaxis.
• Start on enteral diet (PO/NGT) within 7days of admission after AIS.

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Pharmacological treatment

A: acetylsalicylic acid (PO) 325mg 24hourly for 4weeks


AND
C: labetalol (IV) 10-20mg infusion 1-2min, repeated until target BP is attained.
AND
D: paracetamol (IV) 1g 8hourly for 3-5days then when required.

Note
For those treated with alteplase, acetylsalicylic acid administration should be delayed until 24 hours
later

For seizure control


C: phenytoin (IV) 15mg/kg loading dose over 30min, then 100mg 8hourly for 4weeks.
OR
S: levetiracetam (PO/IV) 500mg 12hourly for 2-4 weeks

• Initiate statins in eligible patients and continue statins in patients already taking statins at
the time of onset of AIS.

Reperfusion treatment:
In patients qualified for intravenous thrombolysis, benefit of therapy is time dependent, and
treatment should be initiated as quickly as possible.

Admit the patient to an ICU or designated stroke unit for monitoring and initiate,
S: alteplase (IV) 0.9mg/kg maximum dose 90mg (given over 60minutes with initial 10% of dose
given as bolus over 1 minute)

Important precautions:
• Be prepared to treat potential emergent adverse effects, including bleeding complications
and angioedema in patients undergoing fibrinolytic therapy.
• Maintain BP at <180/105mmHg for at least 24 hours following Alteplase infusion.
• Obtain a follow-up CT or MRI scan at 24 h after IV alteplase before starting anticoagulants
or antiplatelet agents.
• For management of intracranial hemorrhage complication within 24 hours following
thrombolysis:
o Stop alteplase, obtain an emergent non contrast head CT.
o Obtain hematology and neurosurgery consultations
o Provide supportive care and initiate

C: tranexamic acid (IV) 1g infused over 10 minutes.


AND
D: cryoprecipitate (includes factor VIII): 10 U infused over 10–30 min
• In case of angioedema following Alteplase infusion, stop alteplase and provide
airway support as required. Give

D: methylprednisolone (IV) 125mg


AND
A: chlorpheniramine (IV) 10mg stat
If there is further increase in angioedema, administer
A: adrenaline (S/C) (0.1%) 0.3 mL or by nebulizer 0.5 mL stat

Non-pharmacological Treatment
Mechanical thrombectomy
• Consider for selected patients who present between 6 and 16 hours of LKW with an
anterior-circulation large-vessel occlusion (ICA or proximal MCA) and meet other
specified eligibility criteria based on expert assessment, clinical judgement, and availability
of required resources.

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Surgical management of AIS
• Consider decompressive craniectomy in patients ≤60 years of age who deteriorate
neurologically within 48 hours from brain swelling associated with unilateral MCA
infarctions despite appropriate medical therapy.
• Consider external ventricular drainage (EVD) in the treatment of obstructive
hydrocephalus following cerebellar infarction.
• Emergency carotid end arterectomy (CEA) in the acute stage is not well established hence
not recommended in initial management of AIS.
8.3 Management of Epilepsy
Epilepsy is a common neurological disorder characterised by recurring seizures. About two-thirds of
people with active epilepsy have their epilepsy controlled satisfactorily with anti-epileptic drugs
(AEDs). Other treatment approaches may include surgery and neuromodulation. Optimal
management is required to improve patient’s health outcomes and minimise detrimental impacts on
social, educational, and occupational activities.
Clinical presentation
Recurrent seizures

Investigations
• Serum electrolytes
• Serum antiepileptic drug levels
• Electroencephalogram (EEG)
• Brain CT scan
• Brain MRI with epilepsy protocol

Classification of epileptic syndromes


Classify epileptic seizures and epilepsy syndromes in all patients using a multi-axial diagnostic
scheme (refer to ILAE classification) as failure to classify the epilepsy syndrome correctly can lead
to inappropriate treatment and persistence of seizures.

Pharmacological management
• Utilize a single AED (monotherapy) and increase dose until seizures are controlled or side
effects cannot be tolerated.
• If the initial treatment is unsuccessful, initiate alternative monotherapy with different drugs
before resorting to drug combinations.
• Combination therapy (adjunctive or 'add-on' therapy) should only be considered when
attempts at monotherapy with AEDs have not resulted in seizure freedom.
• If trials of combination therapy do not bring about worthwhile benefits, revert treatment to
the initial monotherapy regimen that has proved most acceptable to the patient and
consider referral for expert evaluation.
For management of status epilepticus—refer to emergency and critical care chapter
I. Focal seizures
First Line:
A: carbamazepine (PO) 10-20mg/kg 12hourly for 4weeks
OR
S: lamotrigine (PO) 1-5mg/kg 12hourly for 4weeks

Second line:
S: levetiracetam (PO) 10mg/kg 12hourly for 4weeks

Add-on treatment: gabapentin or sodium valproate as adjunctive treatment if first-line treatments are
ineffective or not tolerated.

II. Generalised tonic–clonic (GTC) seizures


C: sodium valproate (PO) 10-15mg/kg 12hourly for 4weeks
OR
S: lamotrigine (PO) 1-5mg/kg 12hourly for 4weeks

Add on treatment: offer levetiracetam as adjunctive treatment if first-line treatments are ineffective or
not tolerated.

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III. Absence seizures
First Line:
C: sodium valproate (PO) 10-15mg/kg 12hourly for 4weeks

Second line: consider levetiracetam

Note
DO NOT offer carbamazepine, phenytoin or pregabalin for absence seizures.

IV. Myoclonic seizures


First Line:
C: sodium valproate (PO) 10-15mg/kg 12hourly for 4weeks

Second line:
S: levetiracetam (PO) 10mg/kg 12hourly for 4weeks

V. Lenox Gastaut syndrome (LGS)


First Line:
C: sodium valproate(PO) 10-15mg/kg 12hourly for 4weeks

Second line:
S: lamotrigine (PO) 1-5mg/kg 12hourly as adjunctive treatment
Note
DO NOT offer carbamazepine or pregabalin.

VI. Idiopathic generalised epilepsy (IGE)


First Line:
C: sodium valproate (PO) 10-15mg/kg 12hourly for 4weeks

Second line:
S: lamotrigine (PO) 1-5mg/kg 12hourly for 4weeks

VII. Juvenile Myoclonic epilepsy (JME)


First line:
C: sodium valproate (PO) 10-15mg/kg 12hourly for 4weeks
Second line:
S: lamotrigine (PO) 1-5mg/kg 12hourly for 4weeks
OR
S: levetiracetam (PO) 10mg/kg 12hourly for 4weeks

VIII. Childhood absence epilepsy


First Line:
C: sodium valproate (PO) 10-15mg/kg 12hourly for 4weeks
Second line:
S: lamotrigine (PO) 1-5mg/kg 12hourly for 4weeks
Add-on treatment: consider clonazepam, levetiracetam if first-line treatments are ineffective or not
tolerated.

Management of epilepsy in pregnancy


The use of antiepileptic drugs (AEDs) is associated with increased baseline risk of fetal
malformations during pregnancy. Prescribe Folic acid to all women of childbearing age and girls on
AEDs preconception. Attempt to decrease pharmacological treatment to monotherapy and utilize
the lowest possible effective dose of drugs that have shown minimal risk of maternal and fetal neural
tube defects
S: lamotrigine (PO) 1-5mg/kg 12hourly for 4weeks
OR
S: levetiracetam (PO) 10mg/kg 12hourly for 4weeks
AND
A: folic acid (PO) 5mg 24hourly for 3-6months

In women who have not had a seizure for at least 2years, attempt complete withdrawal of AEDs.

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Non-pharmacological Treatment
• Consider ketogenic diet—based on specialist assessment and expert opinion
• Refer all medically refractory seizures for expert neurosurgical evaluation for epilepsy
surgeries
• Consider evaluation for Vagus Nerve Stimulation (VNS) as an adjunctive treatment in
reducing the frequency of seizures in adults who are refractory to AEDs but who are not
suitable for resective surgery
8.4. Parkinson’s Disease
Parkinson’s disease (PD) is a common chronic, progressive, neurodegenerative disorder in geriatric
population, characterized by the loss of dopaminergic neurons from the substantia nigra that
subsequently results in the loss of control of voluntary movement over time.
Clinical presentation
Motor symptoms: Tremors, rigidity, akinesia or bradykinesia, postural instability
Non motor symptoms: drooling, dementia, depression, orthostatic hypotension
Diagnosis is clinical based on United Kingdom Parkinson’s Disease Society Brain Bank (UKPDSBB)
criteria
Pharmacological management of motor symptoms
First line:
D: levodopa+carbidopa (FDC) (PO) 100/25mg 8 hourly (escalate dose based on individual
response) for 4weeks

Give adjunctive treatment for motor symptoms: MAO-B or COMT inhibitors in persistent motor
symptoms despite adequate tolerable doses of Levodopa+carbidopa FDC treatment.

S: selegiline (PO) 2.5-5mg 24hourly (maximum dose 10mg/day)

Pharmacological management of non-motor symptoms

Drooling:
S: glycopyrrolate (PO) 0.5-1mg 8hourly for 2weeks

Orthostatic hypotension: consider Levodopa dose reduction and give


S: fludrocortisone (PO) 0.1mg 24hourly for 2 weeks

Depression: Individualize therapy, consider


S: fluoexetine (PO) 20mg 24hourly (maximum 60mg/day) for 4weeks
OR
A: amitriptyline (PO) 50mg 24hourly for 4-12 weeks

Impulse control disorders: Consider modification of dopaminergic drug dosages.

Non-pharmacological management
• Provide physiotherapy, occupational, speech and language therapies
• Refer for expert neurosurgical evaluation for Deep Brain Stimulation (DBS) in patients
with advanced Parkinson's disease whose symptoms are not adequately controlled by best
medical therapy.

8.5 Congenital Pediatric Nervous System Diseases


8.5.1 Pediatric Hydrocephalus
Pediatric hydrocephalus (HDC) is a common surgically correctable neurological problem in children
with estimated incidence of 1 in every 500 children. HDC can result from various congenital and
acquired causes including aqueductal stenosis, Chiari malformations, intraventricular hemorrhage,
trauma, tumors, and infection. There are effective surgical interventions that can preserve and
improve quality of life in patients with HDC.

Clinical presentation
• Abnormal increase in head size

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• Delayed/regressed developmental • Seizure
milestones
• Headache and impaired vision

Investigations
• Cranial Ultrasound
• Non contrast head CT scan
• MRI brain scan

Pharmacological management
Management of associated seizures:
A: phenobarbital (PO) 5mg/kg 12hourly for 4weeks
OR
C: sodium valproate (PO) 10-15mg/kg 12hourly for 4weeks

Non pharmacological management


• Both CSF shunts and endoscopic third ventriculostomy (ETV) are options in the treatment
of pediatric hydrocephalus. Refer for expert neurosurgical evaluation.
• Consider Endoscopic third ventriculostomy with choroid plexus coagulation (ETV+CPC)
as first line option in cases with clear obstruction to CSF flow.
• Consider insertion of ventriculoperitoneal shunt (VP shunt) where ETV+CPC is not
available, has failed or is contraindicated. Other alternative CSF shunts include
ventriculoatrial (VA) or ventriculopleural shunts.
• Prescribe preoperative antibiotics to prevent shunt infection in patients undergoing shunt
surgery.

Pharmacological management
D: ceftriaxone+sulbactam (FDC) (IV) 100mg/kg stat during anesthesia induction

8.5.2 Management of Pediatric CSF Shunt Infections


Clinical presentation
• CSF leak, purulence, skin erosion,
• Fever, meningismus, erythema,
• exposed or protruding hardware

Lab investigations
• FBP, CRP
• CSF analysis, C/S
• Blood C/S

Pharmacological management
Initiate empirical antibiotic treatment
C: amoxicillin +clavulanate (FDC) (IV) 12hourly for 2weeks
OR
D: ceftriaxone+sulbactam (FDC) (IV) 100mg/kg 12hourly for 2weeks
AND
B: metronidazole (IV) 7.5mg/kg/day 8hourly for 2weeks

Alternative regimen based on C/S results


S: piperacillin+tazobactam (FDC) (IV) 300mg/kg/day (of piperacillin component) divided in
4doses per day
OR
S: meropenem (IV )10mg/kg 8 hourly, (may increase up to 40mg/kg) for 10-14days
Shift to organism’s specific regimen after CSF/hardware culture results
For confirmed Staph spp. infections add
S: vancomycin (IV) 10mg/kg 6hourly for 2weeks or more.

Non-pharmacological management
• Consider partial (externalization) or complete infected shunt hardware removal.

156
• Insert External ventricular drain (EVD) as interim measure for intracranial pressure
monitoring and therapeutic diversion of CSF in the setting where an infected internal shunt
device has been removed.

8.5.3 Congenital Spina Bifida


Spina Bifida (SB) is one of the commonest complex congenital birth defects in developing countries.
Children with SB are faced with multiple medical and psychosocial issues that require a
comprehensive multidisciplinary care plan.

Clinical presentation
• Swelling on the back • Lower limb weakness
• CSF leak • Lower limb deformities

Investigations
Prenatal diagnosis
• Ultrasound in second trimester of pregnancy
• Amniotic fluid analysis

Postnatal diagnosis
• Cranial Ultrasound—evaluate for associated hydrocephalus
• Neuraxial MRI-is indicated in complex cases to plan surgical management and evaluate for
associated defects—Hydrocephalus, chiari malformations, tethered cord
• Preoperative screening echocardiogram (ECHO)

Pharmacological Treatment
Initiate antibiotics in children with open infected spinal bifida lesions
B: ceftriaxone (IV) 100mg/kg 12hourly for 2 weeks
OR
B: amoxicillin +clavulanate (FDC) (PO) 15mg/kg 8hourly for 2weeks
OR
C: amoxicillin +clavulanate (FDC) (IV)15mg/kg 8hourly for 2weeks
AND
A: metronidazole (PO) 7.5mg/kg/day 8hourly for 2weeks
OR
B: metronidazole (IV) 7.5mg/kg/day 8hourly for 2weeks

Non-pharmacological Treatment
Surgical management of SB
• Refer for expert neurosurgical evaluation for surgical closure of the spinal defect and
subsequent evaluation for the need to treat associated hydrocephalus with CSF shunts or
ETV+CPC.

Supportive and preventive and measures


• Provide routine screenings and testing for specific secondary conditions (HDC, skeletal
limb deformities, UTIs) to minimize medical complication rates and help control cost of
care.
o Provide lower limb orthoses (splints, calipers)
o Provide wheelchair for ambulation
• Track and counsel women about recurrence risk and prescribe 5mg of folic acid beginning
at least one month (preferably 3 months) before another conception and continue through
the first 3 months of pregnancy.

8.6 Cranial Nerve Disorders


8.6.1 Trigeminal Neuralgia
Trigeminal neuralgia (TN) is a syndrome characterized by chronic paroxysmal brief episodes of
unilateral electric shock-like pains, in one or more divisions of the trigeminal nerve. TN is often
mistaken as a dental problem leading to delayed correct diagnosis and appropriate treatment.
The diagnosis is based on the characteristic clinical picture.

157
Clinical presentation
Unilateral jaw pain exacerbated by cutaneous stimuli,
e.g., chewing, brushing

Investigations
• CT scan to exclude structural brain pathologies
• MRI to assess the trigeminal nerve root entry zone (REZ)

Pharmacological Treatment
First line treatment:
A: carbamazepine (PO) 200mg 12hourly for 4-12weeks

Non-pharmacological management
Refer to neurosurgeon for procedures that involve controlled trigeminal ganglion ablation to alleviate
pain
• Radiofrequency ablation
• Gasserian ganglion baloon compression rhizotomy
• Glycerol rhizolysis
• Stereotactic radiosurgery rhizotomy

Surgical management
Refer all patient with poor response to conservative management for expert neurosurgical
evaluation for microvascular decompression (MVD), a surgical procedure undertaken to identify,
isolate and separate a vascular loop abutting the trigeminal nerve at the root entry zone (REZ).

8.6.2 Bell’s Palsy


Bell's palsy, also referred to as idiopathic facial nerve palsy is unilateral paralysis of all the muscles
of facial expression of suspected viral etiology. Inflammation and edema of the facial nerve likely
play a role in pathogenesis. Reactivation of herpes simplex virus (HSV) is also thought to play an
etiologic role. Most patients recover within a few weeks or months.
Clinical presentation
• Unilateral facial paralysis (sudden • Drooping at the affected corner of
onset) the mouth
• Inability to close the eye • Decreased tearing
• Hyperacusis
Investigations
• HIV testing
• RBG
• otoscopic exam

Pharmacological management
A: prednisolone (PO) 60mg 24hourly for 5 days, then taper down to 50mg 24hourly for
next 5days.
AND
B: acyclovir (PO/IV)800mg 4-8hourly for 7-14days.
Non-pharmacological management
• Provide facial muscle massage and exercises
• Provide eye patch for ocular protection during sleep.
• Refer for ophthalmological evaluation in severe cases

8.7 Spinal Cord and Peripheral Nerve Disorders


8.7.1 Acute Transverse Myelitis (TM)
Acute onset, usually postinfectious, rapidly progressive neurologic syndrome caused by focal
inflammation of the spinal cord. Thoracic spinal cord level is the most commonly involved.

Clinical presentation
• Rapid progressive bilateral lower • Numbness and paresthesis
limb weakness • Bladder and bowel incontinence
• Backache and neuropathic pain

158
Investigations
• FBP, serum electrolytes
• CSF analysis
• Emergency MRI or CT/myelogram to rule out a compressive lesion.
• Brain MRI—may be required to exclude multiple sclerosis

Perform baseline severity score such as American Spinal Injury Association (ASIA) impairment
score to assist in clinical management decisions and monitor improvement.

Pharmacological management
Give high-dose steroids
D: methylprednisolone (IV) 500-1000mg/day for 3–5days

Consider cyclophosphamide in refractory cases (under the direction of an oncologist)


S: cyclophosphamide (IV) 800-1000mg/m2 pulse dose.

Long term management


Manage generalized pain with
A: diclofenac (IM) 75mg 12hourly for 3-5days
OR
B: tramadol (PO) 50mg 8hourly for 7-14days.

Manage neuropathic pain with


D: pregabalin (PO) 75mg 12hourly (maximum dose 300mg) for 2-4weeks

Manage spasticity with


S: baclofen (PO) 10mg 8hourly, (maximum dose 120mg/day) for 2weeks
OR
S: tizanidine (PO) 2mg 8hourly, (maximum dose 36mg/day) for 2weeks

Non-pharmacological management
• Monitor respiratory function, support ventilation where required
• Catheterize bladder and offer stool softeners to aid bowel emptying
• Provide manual position changes 2hourly to avoid pressure sores
• Provide rehabilitation--exercises to assist ambulation
• Offer assisted ambulation devices—e.g., high back wheelchairs

8.7.2 Guillan Barre Syndrome


Guillain–Barré syndrome (GBS) is potentially fatal, immune-mediated acute-onset ascending
sensorimotor neuropathy usually triggered by infections. Timely recognition, diagnosis, and prompt
referral to a centre equipped to provide ventilatory support is essential to improve mortality and
minimize long term morbidity.

Clinical presentation
• Rapid ascending bilateral lower • Cardiac arrhythmias
limb weakness • Facial or bulbar palsy
• Little or no sensory deficits
• Evolving respiratory distress

Investigations
• FBP, serum electrolytes
• CSF analysis-albuminocytologic dissociation (↑ protein without pleocytosis)
• Emergency MRI to exclude acute spina cord inflammation or compression

Pharmacological management
Admit to ICU and provide ventilatory support to all patients with evolving respiratory distress or
severe autonomic cardiovascular dysfunction
S: human immunoglobulin G (IV) 0.4g/kg 24hourly for 5days (started within 2weeks of
disease onset)

159
For severe cases, consider
S: plasma exchange 200-250ml plasma/kg body weight for 5sessions (started within
4weeks of disease onset)

Monitor respiratory function-patient is deemed at risk of respiratory failure if the vital capacity is
<20ml/kg, the maximum inspiratory pressure is <30cmH2O or the maximum expiratory pressure is
<40cmH2O

Non-pharmacological management
• Provide rehabilitation-exercises to assist ambulation
• Assisted ambulation devices—e.g., high back wheelchairs

8.7.3 Peripheral Neuropathy


Peripheral neuropathies encompass disorders of peripheral nerve cells and fibers which manifest
secondary to a wide range of pathologies that can affect motor, sensory, and autonomic fibers.
Peripheral neuropathies can be classified as mononeuropathies, multifocal neuropathies, and poly-
neuropathies. Further sub classifications categorize peripheral neuropathies as axonal,
demyelinating, or mixed types, which is essential for treatment and management purposes.
Clinical presentation
• Numbness and paresthesis, • Loss of coordination
• Neuropathic pain • Orthostatic hypotension
• Extremities weakness, • Cold, pale feet

Investigations
• FBP • Nerve conduction studies (NCS)
• Renal function tests and needle
• RBG and HbA1c (Diabetes is a electromyography (EMG) to
common cause of neuropathy) differentiate axonal from
• Testing for vitamin and mineral demyelinating neuropathies
deficiencies such as copper, • MRI or CT scans in suspected
thiamine, pyridoxine, folate, B12. nerve compression
• Infectious workup for HIV, and • Urine Test for Bence-Jones
• Thyroid function testing proteins
• Anti-body testing for specific • Genetic testing (for inherited
autoimmune diseases known to neuropathies)
cause peripheral neuropathies such • Nerve biopsy in selected cases
SLE and rheumatoid arthritis where expertise and resources are
available

Table 8.5 Guide to clinical diagnosis of peripheral neuropathies


Type Clinical features Common causes
Distal -Length-dependent: diffuse Most common cause: diabetes, Chronic
Symmetric involvement Idiopathic axonal polyneuropathy, Alcohol,
Polyneuropathy -affects distal segments first chemotherapy induced.
-Symptoms occur below the knees
prior to affecting fingertips
Mononeuropath -Symptoms restricted to distribution of Entrapment neuropathies e.g., carpal tunnel,
y single nerve, myotome, or dermatome peroneal nerve entrapment. Post traumatic
-Asymmetric reflexes neuropathies, diabetes
Mononeuropath -Occurrence of several concurrent Autoimmune vasculitic etiologies
y multiplex mononeuropathies
Hereditary -Distal calf atrophy, hammertoes, pes Genetic diseases
neuropathies cavus
-Motor deficits ≥ sensory deficits
-Diffuse areflexia

Pharmacological management
• Focus on the management of the underlying disease process if identified.

160
• Ensure glucose control in diabetic neuropathy, alcohol cessation in alcoholic neuropathy
and correction of vitamin or mineral deficiencies in nutrition related peripheral
neuropathies.
• For drug related neuropathies, stop the offending medicine and give a suitable substitute.
e.g., substitute stavudine or didanosine with tenofovir or lamivudine.
• Initial management of symmetric polyneuropathies and postherpertic neuralgia

D: pregabalin (PO) 150mg 12hourly for 4-12weeks


OR
A: amitriptyline (PO) 50-100mg 12hourly for 4-12weeks
AND
B: vitamin B1, B6, and B12 (FDC) (PO) 12hourly for 4-12weeks

• If the initial treatment is not effective, consider one of the combination therapies.

(1) Gabapentanoid+Tricyclic Antidepressant

D: pregabalin (PO) 150mg 12hourly for 4-12weeks


AND
A: amitriptyline (PO) 25-50mg 12hourly for 4-12weeks
AND
B: vitamin B1, B6, and B12 (FDC) (PO) 12hourly for 4-12weeks

(2) Gabapentanoid +Selective Serotonin Reuptake Inhibitors

D: pregabalin (PO) 150mg 12hourly for 4-12weeks


AND
S: fluoxetine (PO) 20mg 24hourly for 7days then titrate 12hourly for 4-12weeks
AND
B: vitamin B1, B6, and B12 (FDC) (PO) 12hourly for 4-12weeks

In chronic demyelinating polyneuropathies add steroids


A: prednisolone (PO) 20-60mg 24hourly for 6weeks (taper down based on response)

Offer rescue therapy if required, to patients undergoing long term treatment.


B: tramadol (PO) 50mg 8hourly for 7-14 days

For localized symptoms, consider topical agents as adjunctive treatment.


D: lidocaine 5% patches apply for 60minutes.

For patients on isoniazid related neuropathies, start on


B: pyridoxine (PO) 25–50 mg 8hourly for 3weeks, then 25mg 24hourly until completion of
TB dose.

Non-pharmacological management
• Transcutaneous electrical nerve stimulation (TENS) for pain relief.
• Educate patients on increased risk of injury and infection due to loss of sensation
• Recommend wearing socks with closed-toed shoes to decrease the risk of infection.
• Offer support on cessation to patients with alcohol-induced neuropathy

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CHAPTER NINE
RESPIRATORY DISEASE CONDITIONS
9.1 Acute Respiratory Infections (ARI)
It is an infection affecting upper or lower respiratory tract. Commonly caused by bacteria or viruses,
other microbes including rickettsia or fungi may be present.

9.1.1 Pneumonia
Pneumonia is the inflammation of the lung tissue. Pneumonia can either be primary (to the causing
organism) or secondary to pathological damage in the respiratory system.

Clinical presentation
• Fever (typically>380C) • Respiratory distress
• Dry or productive cough • Chest pain and tachypnoea
• Central cyanosis

Table 9.1: Tool used for assessing Adult Patient with Pneumonia
CURB 65 Clinical Feature Points
C Confusion 1
U Urea>7mmol/L 1
R RR>30 1
B SBP<90mmHg or DBP,60mmHg 1
65 Age >65 1
CURB-65 Score Risk group 30-day mortality Management
0-1 1 1.5% Low risk, consider home
treatment
2 2 9.2% Probable admission vs close
outpatient management
3-5 3 22% Admission, manage as severe
DBP = diastolic blood pressure; SBP = systolic blood pressure. a Defined as a Mental Test Score of
≤8, or new disorientation in person, place or time. Predicted 30-day mortality

Note
• For patients with pneumonia treatment should be instituted when they have FEVER, COUGH
AND CXR with findings suggestive of pneumonia.
• Consider alternative diagnosis when a patient is not responding.
• Pulmonary embolism should be investigated carefully for patient with shortness of breath and
not responding to treatment of pneumonia

9.1.1.1 Pneumonia in Children


(For more details, refer to Integrated Management of Childhood Illness (IMCI) guidelines)

Table 9.2: Important clinical presentation of pneumonia in under-fives


Age Signs Classification
Infants less than Severe chest in-drawing or Severe pneumonia (all young infants with
2 months 60 breaths per minute or more pneumonia are classified as severe)
No severe chest in-drawing No pneumonia:
Less than 60 breaths per-minute Cough or cold
Children from 2 Chest in-drawing Severe pneumonia
months to 1 No chest in-drawing Pneumonia
year 50 breaths per minute or more
No chest in-drawing No pneumonia
Less than 50 breaths per minute Cough or cold
Children from 1 Chest in-drawing Severe pneumonia
year to 5 year No chest in-drawing Pneumonia
40 breaths per minute or more
No chest in-drawing No pneumonia
Less than 40 breaths per minute Cough or cold

162
Investigations
• Measure oxygen saturation
• FBC (look for increased WBC, neutrophilia) CRP/ESR (increased), ABG (look for pH,
bicarbonate), Blood culture, Sputum culture and sensitivity, Serology for HIV test (if
Unknown)
• CHEST X-ray-PA/LATERAL (look for consideration, tap effusion>5cm), Bronchoscopy
(Consider if immunosuppression, critically ill, fail to respond, suspected TB or PCP or
inadequate
• CT Scan: if patient is not improving, suspicion of fungal, ILD

Non-pharmacological Treatment:
• Oxygen therapy if available
• Supportive care
o Remove clothes
o If wheezing giving rapid-acting bronchodilator: Nebulized Salbutamol
o Ensure that the child receives daily maintenance fluid appropriate for the child’s age
but avoid over-hydration refer to IMCI/ STG & Essential Medicines List for Children

Pharmacological Treatment
Non-severe pneumonia
A: amoxicillin (PO) 25mg/kg 8hourly for 5days
AND
A: paracetamol (PO) 15mg/kg 8hourly for 5days(if fever present)
OR
A: paracetamol (supp) 10–15mg/kg (if there is fever)
OR
A: ibuprofen (PO) 15mg/kg 12hourly for 5days

Give the first dose at the clinic and teach the mother how to give the other doses at home.
Encourage breasting and feeding.

Severe Pneumonia
A: benzyl penicillin (IV/IM) 50000 units/kg every 6hours for at least 3days
THEN
A: amoxicillin (PO) 40 mg/kg 8hourly for 7days.
Alternatively
A: ampicillin (IV/IM) 50 mg/kg every 6hourly for 5days
AND
A: gentamicin (IV/IM) 7.5 mg/kg 24hourly for 5days
THEN
A: amoxicillin (PO) 40 mg/kg 8hourly for 7days.

Note
• For children above 5 years, atypical pneumonia should be considered e.g. mycoplasma
• Consider alternative diagnosis after three visit /not responding, refer patient to a
pediatrician

9.1.1.2 Pneumonia in Adults


Community Acquired Pneumonia
CAP refers to a pneumonia that is acquired outside hospital commonly caused by Streptococcus
pneumoniae, Haemophilus influenzae, Moraxella catarrhalis, atypical bacteria (ie, Chlamydia
pneumoniae, Mycoplasma pneumoniae, Legionella species) and viral respiratory pathogens (i.e
rhinovirus and influenza)

Clinical presentation
• Fever, • Tachypnea
• Cough dry or productive • Crepitation/Rales heard over the
with/without purulent sputum, involved lobe or segment
• Dyspnea, • Increased tactile fremitus, bronchial
• Pleuritic chest pain breath sounds may be present if
consolidation has occurred.

163
• Decreased tactile fremitus and dullness on chest percussion

Investigations
• Measure oxygen saturation use pulse oximetry or Monitor
• FBC (look for increased WBC, neutrophilia),
• CRP/ESR (increased in bacterial infection)
• ABG (look for pH, bicarbonate),
• Serology for HIV test (if Unknown)
• Sputum culture and sensitivity (are indicated for inpatients and those with severe disease
(ICU admission),
• Blood culture (are not recommended for ambulatory patients
• CHEST X-ray-PA/LATERAL (look for one or more focal pulmonary infiltrates,
consolidation, tap effusion>5cm),
• Bronchoscopy (Consider if immunosuppression, critically ill, fail to respond, suspected
TB or PCP or inadequate
• CT-CHEST Scan Or HRCT: if patient is not improving, suspicion of fungal, ILD etc.

Note
Do not use CT chest to diagnose pneumonia

Non-pharmacological Treatment
• Stop smoking if previously smoking
• Vaccination when indicated, in specialized centre for patient >65yrs and below 5years

Pharmacological Treatment
First line treatment

Table 9.3: First Line Treatment of Typical Community Acquired Pneumonia


Condition Treatment Duration
Mild CAP (treated on out-patient A: erythromycin (PO) 500mg 8hourly 5-7days
basis) OR
(common organism S pneumonia B: ampicillin + cloxacillin (FDC)(PO) 500–1000mg
and these patients have no 8hourly
comorbidities)
Mild to Moderate CAP (failed to A: doxycycline (PO) 100 mg 12hourly (culture guided) 5-7days
respond to Initial treatment) OR
B: azithromycin (PO) 500mg stat and then 250mg
24hourly
OR
C: clarithromycin (PO) 500mg 12hourly
MILD CAP in patients with B: amoxicillin + clavulanic acid (FDC) (PO) 5-7 days
comorbidities (i.e. chronic heart, 500mg/125mg 8-12hourly or 875mg/125mg 12hourly
lung, liver, or renal disease; OR
diabetes mellitus; alcoholism; D: cefuroxime (PO) 500mg 12hourly
malignancy; asplenia; AND
immunosuppression; prior antibiotics A: doxycycline (PO) 100mg 24hourly
within 90 days OR
C: clarithromycin (PO) 500mg 12hourly
Severe pneumonia/Aspiration D: ceftriaxone + sulbactam (FDC) (IV) 1.5g 12hourly 7–
pneumonia (in-patient) If suspicion of anaerobes or Aspiration pneumonia 10days
Add:
B: metronidazole (IV) 500mg 8hourly
Do culture and imaging if nonresponse consider
second line
Second line treatment
If no response to first line further investigation is required. If patient is in respiratory distress, or no
response after 3 days of first line treatment, or patient’s condition deteriorates, then investigate, start
empiric treatment while wait for culture and sensitivity

S: piperacillin + tazobactam (FDC) (IV) 4.5g 6hourly for 7days

164
Table 9.4: Treatment of Typical and Atypical Community Acquired Pneumonias Organism
Specific
Condition Treatment Duratio
n
Atypical pneumonias A: erythromycin (PO) 500mg 6hourly 7-
(Bordetella pertussis, Mycoplasma pneumonia, OR 10days
Chlamydophila pneumonia) C: clarithromycin (PO) 500mg 12hourly

Pseudomonas pneumonia A:ciprofloxacin (PO) 500mg 12hourly 7-


(Risk factors structural lung disease, COPD, If culture sputum-positive or HRCT 10days
and bronchiectasis) suggestive
S: piperacillin + tazobactam (FDC) (IV) 4.5g e
6-8hourly
OR
S: cefepime (IV) 2g 8hourly
OR
D: ceftazidime (IV) 2g 8hourly
OR
S: meropenem (IV) 1g 8hourly
H. influenza A: amoxicillin (PO) 500mg 8hourly 7-
OR 10days
D: cefuroxime (PO) 250-500mg 8hourly
(culture & sensitivity should be done in order to
choose alternativeantibiotics)
Pneumocystis jirovecii Pneumonia (PJP) A: co-trimoxazole (PO) 1920mg 8hourly 21days
(Refer to Tanzania HIV Guideline for more AND
details) A: folic acid (PO) 5mg 24hourly (if cytopenic)
In sulphur allergy:
S: clindamycin (PO) 450–600mg 6hourly
Staphylococcus aureus Pneumonia B: ampicillin + cloxacillin (FDC) (IV) 1g 6hourly 14days
OR
S: clindamycin (IV/PO) 600mg 6-8 hourly
Klebsiella B: chloramphenicol (IV) 500mg 6hourly 10-
Pneumonia AND/OR 14days
(due to high mortality observe the duration of A: gentamicin (IV) 4-5mg/kg 24hourly in 2
antibiotic given not < 10days) divided doses
For critical ill patient and those with risk factors S: vancomycin (IV) 15mg/kg 12hourly 5-7days
for MRSA include hemoptysis, recent,
influenza, neutropenia, hemodialysis, and
congestive heart failure)

Note
• In severe Pneumocystis jirovecii pneumonia (PCP), add 30 – 40mg prednisolone for 14days
consider tapering down after recovery
• Patients with pneumonia should be afebrile for 48-72hours and have improved clinically
before antibiotic therapy is stopped. The duration of therapy may need to be increased if the
initial empirical therapy has no activity against the specific pathogen or if the pneumonia is
complicated by extra pulmonary infection.

Alternative in Staphylococcal and Klebsiella Pneumonia:


D: ceftazidime (IV/IM) 2g 8hourly for 7–14days

9.1.1.3 Hospital Acquired Pneumonia/Nosocomial Pneumonia


This is defined as pneumonia that occurs two days (48hrs) or more after hospitalization but that was
not incubating at the time of hospital admission.

Clinical Presentation
• Fever • Shortness of breath
• Increase in respiratory rate

165
Pharmacological Treatment
Empirical treatment until bacteriology available
C: ciprofloxacin (IV) 400mg 12hourly for 7days
OR
D: ceftriaxone + sulbactam (FDC) (IV) 1.5g 12hourly for 7days
Note
In specialized unit management of CAP/HAP can be changed with supportive culture and sensitivity
done, this may necessitate use of other broader spectrum antibiotics 48-72hours until the results are
obtained

9.2 Obstructive Lung Diseases


It’s a chronic airway disease which result in airway flow limitation can be either reversible or
irreversible

Clinical presentation
• Wheezing • Cough (dry or productive cough)
• Difficulty in breathing or shortness • Finger clubbing
of breath
• Chest tightness

9.2.1 Asthma
It is a chronic reversible obstructive inflammatory airways disease in which many cells and cellular
element play a role by constriction of bronchial smooth muscle causing bronchospasm, oedema of
bronchial mucous membrane and blockage of the smaller bronchi with plug of mucous.

Clinical presentation
• wheeze, • Tachycardia,
• shortness of breath, • Diffuse musical wheezes,
• chest tightness • Prolonged phase of exhalation,
• cough This presentation particularly • Chest hyperinflation.
at night or in the early morning • Use of Accessory muscle.
• Tachypnea,

Investigations
• FBP (Look for eosinophilia) with reversibility test, PEFR
• Serum IgEa measurement with a peak flow
• ESR meter), Exhaled NO should be
• ABG done to asses evidence of variable
• CXR if highly suspicion of expiratory airflow limitation
pneumonia
• Sputum for cytology a (look for
eosinophilia),
a • Lung function Test (e.g.: spirometry
Very important test to establish diagnosis of asthma

Non-pharmacological Treatment
• Avoid polluted environment (both • Stop smoking
indoors and outdoors) • Avoid both overweight and
• Avoid non-selective β-blockers, underweight
which can trigger asthmatic attack
• Avoid heavy exercise

Note
• The management of asthma in children is like that in adult. Infants under 18 months, may not
respond well in bronchodilator
• Uncertain in diagnosis should prompt early referral, because asthma-COPD overlap has worse
outcome.
• Patient intolerant of NSAIDs or who exhibit any of the high-risk clinical features for intolerance to
these drugs (severe asthma, nasal polyps or chronic rhino sinusitis) should use NSAIDs only
under close medical supervision.

166
Table 9.5: Assessment and Treatment of Asthma attack in Children ≥2years & Adults
Attack Clinical Treatment (Children & Adults)
Presentation
MILD- Able to talk in I. Salbutamol inhalation (can be given by pMDI or spacer or
2
MODER sentences or Nebulization)
st
ATE phrases Give: 4-10 puffs by pMDI/ spacer/ every 20minutes for 1 hour
ATTAC Not agitated A: salbutamol(nebulization) Adult: Salbutamol respules 5mg 6hrly
K Pulse rate 100- (2-3cycles and reassess); Pediatric: 2.5mg 6hrly (2-3cycles and
120bpm reassess).
Sat 02(on air)-90- If symptoms completely subside observe for 1–4hours, give Salbutamol
95% for 24–48hours (2-4 puffs every 4–6hours) for 3 days. If attack is only
PEF>50% partially resolved give 2–4 puffs of Salbutamol every 3–4 hours if attack
predicted is mild; 6 puffs every 1–2 hours if the attack is moderate, until symptoms
subside. When attack completely resolved proceed as above.

II. Prednisolone
A: prednisolone (PO): Adult 40mg am 7/7; Pediatrics 1-2mg/kg max
40mg
Do tapering if exceed seven days.

III: Controlled oxygen (if available): target saturation 93-95% (children:


94-98%)

Note: If symptoms worsen or do not improve, treat as SEVERE


ATTACK
SEVER • Talks in words I. Admit the patient, place in semi-sitting position
E i.e. cannot
ATTAC complete a II. Oxygen continuously 5L/min (maintain O2 saturation for adult 93-95%
K sentence in 1 (children 94-98%)
breath or too
breathless to III. Inhalation
talk/ feed A: salbutamol (nebulization) 4-10puffs every 20-30min in children
• Sits hunched <5years, up to 20 puffs in children >5years and adults
forwards Add
• Agitated S: ipratropium bromide (inhalation)0.25-0.5mg 6-8hourly
• Respiratory rate AND
>30/min. A: hydrocortisone (IV) 5mg/kg in children, 100mg in adults 6hourly
• Accessory then switch to oral
muscles being A: prednisolone (PO)1-2mg/kg 24hourly to complete 7days of treatment
used If attack is completely resolved continue with salbutamol inhalation 2–
• Pulse rate > 120 4puffs every 4hours for 24-48hours and oral prednisolone 1-2mg/kg
bpm 24hourly to complete 3–5days of treatment.
• O2 saturation (on
air): < 90% If not improving or condition worsens, treat as LIFE-THREATENING
ATTACK
• PEF ≤ 50%
predicted or best

Use a spacer to increase effectiveness. If conventional spacer not available, take a 500ml plastic bottle, insert the mouthpiece of the
inhaler into a hole on the bottom of the bottle (the seal should be as tight as possible). The child breathes from the mouth of the
bottle in the same way as he would with a spacer

167
LIFE- Altered level of I. Admit the patient, place in semi-sitting position
THREA consciousness
TENIN (drowsiness, II. Oxygen continuously 5L/min (maintain O2 saturation between 94-98%)
G confusion, coma)
ATTAC Exhaustion III. A: salbutamol (nebulization) 2.5mg for children <5years and in
K Silent chest children >5years & adults 2.5-5mg every 20–30min then switches to
Paradoxical salbutamol aerosol when clinical improvement is achieved.
thoracoabdominal Add:
movement S: ipratropium bromide (inhalation) 0.25-0.5mg 6-8hourly.
Cyanosis AND
Collapse A: hydrocortisone (IV) 5mg/kg in children, 100mg (IV) in adults every
Bradycardia in 6hours then switch to
children or A: prednisolone (PO) 1-2mg/kg 24hourly to complete 7days of
arrhythmia/ treatment
hypotension in In adult administer a single dose of
adults A: magnesium sulphate (Infusion of 1-2g in 0.9% Sodium Chloride
O2 saturation<92% over 20 minutes)

In children use continuous nebulization rather than intermittent


nebulisation.
Patient with life threatening asthma should be managed in HDU/ICU.

Note
Patients who get night attacks should be advised to take their medication on going to bed

9.2.2 Chronic Asthma in Adults


The assessment of the frequency of daytime and nighttime symptoms and limitation of physical
activity determines whether asthma is intermittent or persistent. There are 4 categories (see table
9.5)
Therapy is stepwise (Step 1–4) based on the category of asthma and consists of:
• Preventing the inflammation leading to bronchospasm (controllers)
• Relieving bronchospasm (relievers)

Controller medicines in asthma


• Inhaled corticosteroids (ICS) e.g. Beclomethasone, Budesonide, Fluticasone
• Leukotriene modifiers: e.g. Montelukast can added from step 2 patient (should be
administer when low ICS or ICS-LABA has failed to achieve desired outcome.
• long acting muscarinic antagonist (LAMA) e.g tiotropium
• Long acting β2 agonists (LABA) e.g. formoterol, salmeterol

Reliever medicines in asthma


• Short acting β2 agonists (SABA) e.g. Salbutamol
• short acting muscarinic antagonist (SAMA) e.g. ipratropium bromide (should be used in
acute asthma attack)

Note
• In specialized centre when low dose ICS alone fails to achieve good control for difficult to
treat and severe asthma, the addition of LABA + ICS should be instituted.
• The most common side effects of inhaled steroids are a sore throat, hoarseness of
voice, and infections/fungal infections in the throat and mouth.
Things you can do to avoid or reduce these side effects include:
• Rinsing your mouth and gargling after taking an inhaled steroid
• Using a spacer/holding chamber to reduce the amount of steroid landing in your mouth
and throat (For children and elderly patient)

168

Table 9.6: Long-Term Treatment of Asthma According to Severity
Categories Treatment
STEP 1 A: As needed low dose ICS
Intermittent asthma OR
• Intermittent S: ICS AND LABA
symptoms < B: budesonide (inhalation) 100-200µg 12hourly
once/week OR
• Nighttime symptoms < B: budesonide (inhalation) 100-200µg 12hourly
twice/ month AND
• Normal physical activity C: salmeterol 100- 200mcg 2puff 12hourly
OR
Low dose ICS taken whenever SABA is taken
STEP 2 Daily low dose ICS plus as needed SABA
Mild persistent asthma OR
• Symptoms > once/ week As needed low dose ICS+ salmeterol
but < once/ day OR
• Nighttime symptoms > Low dose ICS taken whenever SABA is taken
twice/ month ICS
• Symptoms may affect Add: -
activity LTRA;
D: montelukast (PO) 4mg nocte (6month to 6years) or > 6years to
15years (PO) 5mg nocte or >15years (PO) 10mg nocte
(for period not less than 3/12)
STEP 3 Refer these patients to physician/ respiratory physician/ pulmonologist
Moderate persistent asthma low dose ICS+LABA
• Daily symptoms OR
• Symptoms affect activity Medium dose ICS
• Nighttime symptoms OR
>once/ week Low dose ICS +LTRA
• Daily use of Salbutamol
LTRA;
D: montelukast (PO) 4mg nocte (6month to 6years) or (PO) 5mg nocte >
6-15years or (PO) 10mg nocte >15years
(for period not less than 3/12)
STEP 4 Refer this patient to Respiratory physician/Pulmonologist
Severe persistent asthma Medium dose ICS+LABA
• Daily symptoms OR
• Frequent nighttime High dose ICS
symptoms Add
• Physical activity limited S**: tiotropium Mist (inhalation) 6mcg 2puff 24hourly
by symptoms OR
Add on
LTRA
D: montelukast (PO) 4mg nocte (6month to 6years) or (PO) 5mg nocte
>6years to 15years or (PO) 10mg nocte>15years
(for period not less than 3/12)
Add:
S: tiotropium mist inhaler 6mcg 2puff 24hourly
OR
S: ipratropium Bromide (Inhalation) 40 mcg 2puff 12hourly
For patient with rhinitis and asthma add sublingual immunotherapy (SLIT)
provided FEV1>70% predicted
STEP 5 Refer to expert opinion (respiratory physician/pulmonologist for
Severe asthma phenotypic investigation+/- add on treatment
• Symptoms throughout
the day High dose ICS-LABA
• Night symptoms seven Low dose OCS but consider side effects
times per weeks S: tiotropium (inhalation) as step 4
• Physical activity extreme Biologics as indicated
limited by symptoms S: omalizumab (SC) 75-600mg every 2-4weeks;

169

Table 9.7 Low, Medium and High Dose Inhaled Corticosteroids Adults and Adolescents (≥12
Years)
Inhaled corticosteroid Total daily dose (mcg)
Low Medium High
Budesonide (DPI) 200-400 >400-800 >800
Fluticasone propionate (DPI OR 100-250 >250-500 >500
HFA)
Mometasone furoate 110-220 >220-440 >440
Triamcinolone acetonide 400-1000 >1000-2000 >2000

DPI: Dry powder inhaler, HFA: hydrofluoroalkane, CFC: Chlorofluorocarbon propellant (included for
comparison),

Table 9.8 Low, Medium and High Dose Inhaled Corticosteroids Children 6–11 Years
Inhaled corticosteroid Total daily dose (mcg)
Low Medium High
Budesonide (DPI) 100-200 >200-400 >400
Budesonide (nebules) 250-500 >500-1000 >1000
Fluticasone propionate (DPI) 100-200 >200-400 >400
Fluticasone propionate (HFA) 100-200 >200-500 >500
Momentansone furoate 110 >220-≤440 ≥440
Triamcinolone acetonide 400-800 >800-1200 >1200

9.3 Bronchitis
9.3.1 Acute Bronchitis
Acute bronchitis was defined as an acute self-limited lower respiratory tract infection manifested
predominantly by cough with or without sputum production, lasting no more than 3 weeks with no
clinical or any recent radiographic evidence to suggest an alternative explanation.In acute bronchitis
some isolated virus (influenza A and B viruses, parainfluenza virus, respiratory syncytial virus,
coronavirus, adenovirus, and rhinovirus) and bacteria (Bordetella pertussis, Chlamydophila
(Chlamydia) pneumoniae, and Mycoplasma pneumonia)
Clinical presentation
• Patients with acute bronchitis present with a cough lasting more than five days (typically
one to three weeks), which may be associated with sputum production.
• Cough in the absence of fever, tachycardia, and tachypnoea suggests bronchitis,
• Acute bronchitis should be distinguished from chronic bronchitis (see below), it is not a
form of COPD

Note
When the acute bronchitis persists or worsens, we suggest that the patient is advised to seek
reassessment and do below targeted investigation(s).

Investigation in COPD (bronchitis and Emphysema)


• FBP
• ESR /CRP OR Procalcitonin
• Serum alpha-1 antitrypsin levels
• Chest radiography (if the patient is elderly or physical findings suggest pneumonia)
• Sputum cytology (if the cough is persistent)
• Blood culture and microbial sensitivity (if bacterial super-infection is suspected)
• Bronchoscopy (to exclude foreign body aspiration, tuberculosis, tumours, and other
chronic diseases and patient with worsening symptoms)
• Lung function Test (Spirometry and Peak expiratory flow rate)

Note
An exception, however, is cough in elderly patients; pneumonia in elderly patients is often
characterized by an absence of distinctive signs and symptoms.

170

Symptomatic Treatment
• With non-steroidal anti-inflammatory drugs: paracetamol, acetyl salicylic acid
• Cough management refer section 9.1.1
• There is NO benefit from antibiotic use in acute bronchitis.
• Discourage smoking and other irritating factors.

9.3.2 Chronic Bronchitis


It defined by a chronic productive cough for three months in each of two successive years in a
patient in whom other causes of chronic cough have been excluded. Patients may get secondary
bacterial infection with development of fever and production of thick smelly sputum.

Table 9.9: Risk Factor for Chronic Bronchitis


Risk factor
1. Cigarette smoking
2. Indoor air pollution
>Exposure from burning wood >Exposure to biofuel mass exposure
>Heating in poorly vented dwellings
3. Occupational exposure
Coal miners >Tunnel Workers >Hard-rock miners >Concrete manufacture
>Livestock farming (i.e. to pesticides)
4. Exposure to agricultural
5. Use of domestic solid fuel

Investigation
As in acute bronchitis
Non-pharmacological Treatment
• Stop smoking (Reducing loss of lung function) and/or remove from hazardous environment
• Prompt treatment of infective exacerbations
• Controlled oxygen therapy
• Physiotherapy
• Pulmonary Rehabilitation (consist of education, lifestyle modification, regular physical
activities, physiotherapy and avoid indoor and outdoor pollutants)
• Nutrition support
• BIPAP in specialized center
• Influenza vaccine in specialized center

Pharmacological Treatment
• Pharmacologic therapy for Chronic Bronchitis is directed towards 3 major goals
• Relieving symptoms during stable disease

Mucoactive Agents-Reduced overproduction and hypersecretion, increases elimination


For pharmaceutical management; refer to emergency and critical care chapter
Hypertonic saline-stimulate productive cough and decreases sputum viscoelasticity, increases
mucociliary clearance.
7% hypertonic saline or 0.9% saline bd for PRN

Bronchodilators (Beta-agonists)-Promotes mucus clearance by increasing airway luminal


diameter and ciliary beat frequency, reduces hyperinflation, improve PEF
A: SABA: Salbutamol (Inhalation) 100µg 2puff 6hourly
OR
LABA: salmeterol+fluticasone or in combination with steroids
(salmeterol+fluticasone or budenoside fluticasone)
OR
Muscarinic antagonists -Decrease contractility of smooth muscle in the lung, inhibits
bronchoconstriction and mucus secretion
SAMA: S: ipratropium bromide (aerosol) 20–80mcg, 6–8 hourly
LAMA: S: tiotropium (mist inhaler) 6mcg 2puff 24hourly Preventing
exacerbations

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Mucoactive Agents-Refer cough section
Macrolides- (As indicated) antibacterial effects; Immune-modulatory and anti-inflammatory effects
(Azithromycin/clarithromycin)

Note
• In specialized center they may use N-acetyl cysteine and carbocysteine as mucolytic agents
• Macrolide should be given in consultation with respiratory physician/Pulmonologist to avoid
antimicrobial resistance (Azithromycin and clarithromycin may be used).
Avoid use of systemic glucocorticoids due to numerous adverse side effects

9.4 Emphysema
It is a destructive process in the gas-exchanging air spaces of the lung that results in perforations,
obliteration of airspace walls, and coalescence of small distinct airspaces into much larger ones,
leading to enlargement of the gas exchanging units of the lungs These changes cause loss of elastic
recoil of the lungs and abnormal gas exchange.

Clinical presentation
• Shortness of breath • Coarse early inspiratory crackles.
• Cough, sometimes caused by the • Use of accessory muscles
production of mucus • Pursed-lip breathing
• Wheezing • Signs of cor pulmonale. (Raised
• Slow and prolonged expiration JVP, peripheral oedema,
• Chest wall hyperinflation, hepatomegaly etc)
• Limited diaphragmatic motion on • Cyanosis
auscultation, • Asterixis
• Distant breath sounds, and heart
sounds
Investigations
• Haematocrit(men>52% and • Sputum culture and Microbial
>47men) Or FBP (look at sensitivity
haematocrit) • Pulmonary function tests
• ABG(look for bicarbonate-metabolic • Six minutes’ walk test
alkalosis) • CT SCAN OF THE CHEST/HRCT
• CXR (for evaluation for Lung Volume
Reduction Surgery)

Non-pharmacological Treatment:
• Stop smoking
• Give oxygen after evaluation

Pharmacological Treatment
Inhaled bronchodilators relax and open the airways. They may be short-acting (albuterol,
ipratropium) or long-acting (salmeterol, tiotropium,). These medicines may be available as inhalers
("puffers") or as a solution. A nebulizer machine aerosolizes the bronchodilator solution, which is
then breathed through a tube. For more detail refer Treatment in section 9.2 above

Table 9.10: COPD Staging and recommended Therapies


GOLD Exacerbation Mild symptoms Mod/Severe Symptoms
FEV1Stage Per Year
I: ≥80% ≤2 GROUP A GROUP B
II: 50-79% Bronchodilator (SABA- LAMA OR LABA
PRN)

III: 30-49% ≥2 GROUP C GROUP D


LAMA+ LABA LAMA or LAMA + LABA or ICS+
LABA
IV: 30%

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9.5 COPD Exacerbation
Chronic Obstructive Pulmonary Disease (COPD) exacerbation is a worsening or “flares up” of your
COPD symptoms, commonly caused by infection in the lungs but in some cases the cause is
unknown.

Clinical presentation
• Worsening of cough, • Change in phlegm quality, and
• Increase in phlegm production, increase in dyspnea
Table 9.11: COPD Exacerbation Management

AGENT DOSE
SAMA
S: ipratropium bromide (aeresol) MDI 4-8 puffs every 1-2 hours
Nebulizer 0.5mg every 1-2hours
SABA
A: salbutamol (inhalation) MDI 4-8 puffs every 1-2hours
Nebulizer 2.5-5mg every 1-2hours
Corticosteroids
A: prednisone (PO) 40mg AM for 5days
If severe
A: hydrocortisone (IV) 1-2mg/kg 6hourly
D: methylprednisolone (IV) 125mg 6hourly for 72hours
(Then switch oral)
Antibiotic (If infection Presents) (Penicillin/Macrolide/Fluoroquinolone)
A: amoxicillin (PO) 500mg 8hourly for 7days

OR
A: ciprofloxacin (PO) 500mg 12hourly for 7days
OR
A: doxycycline (PO) 100mg every 12hrs 7days

OR

C: clarithromycin (PO) 500mg 12hourly for 7days


If possible, do culture and sensitivity

Noninvasive positive pressure ventilation


Oxygenation if indicated

9.6 Other Respiratory Infections


9.6.1 Acute Laryngo-Tracheobronchitis
Laryngo-tracheobronchitis (croup) is acute inflammation of the larynx, trachea and bronchi which
occurs in young children (usually between 6 months to 3 years of age). It arises as a result of
narrowing of the airway in the region of the larynx. The most common cause is viral infection
(particularly parainfluenza viruses) but may also be due to bacterial infection. The obstruction is due
to inflammation and oedema.

Clinical presentation
• The symptoms include paroxysmal “barking” cough, inspiratory stridor, fever, wheezing,
hoarseness of voice and tachypnoea
• Such symptoms usually occur at night
• Respiratory failure and pneumonia are potentially fatal complications.

Non-pharmacological Treatment
• Prevent asphyxiation
• Treat inflammatory oedema
• Humidification of inhaled air
• Hospitalization may be necessary

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Note
• No stridor at rest, give no antibiotics
• Stridor at rest or chest in-drawing or fast breathing REFER IMMEDIATELY to hospital

Mild Croup
• Only stridor when upset, no • Home care – steam inhalation
moderate/severe ARI • Antibiotics NOT required
• Likely of viral origin
Severe Croup
• Likely bacterial origin • Antibiotics are NOT effective and
• Stridor in a calm child at rest should not be given
• Chest in drawing

Pharmacological Treatment
Admit to hospital, give Oxygen therapy to all patients with chest in-drawing (using nasal prongs only,
DO NOT use nasopharyngeal or nasal catheter) until the lower chest wall in-drawing is no longer
present
D: dexamethasone (PO) 0.6mg/kg 24hourly in 1–2 divided doses
AND
A: adrenaline (inhalation) 400mcg/kg 2hourly if effective; repeat after 30min if necessary.

9.6.2 Laryngeal Diphtheria


Is an infection caused by Corynebacterium diphtheria; it is directly transmitted from person to person
by droplets. Children between 1–5 years of age are most susceptible although non-immune adults
are also at risk. Diphtheria is characterized by grayish-white membrane, composed of dead cells,
fibrin, leucocytes and red blood cells as a result of inflammation due to multiplying bacteria.

Non-pharmacological Treatment
• Isolate the child
• Gently examine the child’s throat – can cause airway obstruction if not carefully done.
• NGT for feeding if unable to swallow
• Avoid oxygen unless there is incipient airway obstruction
• May need tracheostomy if there is incipient airway obstruction

Pharmacological Treatment:
Drug of choice
A: phenoxymethylpenicillin (PO) 250mg 6hourly for 14days
OR
A: erythromycin (PO) 125–250mg 6hourly for 14days
OR
B: azithromycin (PO) 500mg 24hourly for 3days
OR
A: benzyl penicillin (IV) 25,000–50,000units/kg to a max. of 1.2MU 12hourly until the
patient can take oral medicine
AND
A: diphtheria antitoxin (IM or slow IV) dose depends upon the site and severity of infection:
• First give a test dose of 0.1ml of 1 in 10 dilution of antitoxin in 0.9% Sodium Chloride
intradermal to detect hypersensitivity
• It should be given immediately because delay can lead to increased mortality
• The dose should be administered intravenously over 60minutes in order to inactivate toxin
rapidly
• 20,000–40,000 units for pharyngeal/laryngeal disease of <48 hours’ duration,
• 40,000–60,000 units for nasopharyngeal disease
• 80,000–120,000 units for >3days of illness or diffuse neck swelling "bull-neck"

Note
Tracheostomy may be required for airway obstruction

9.6.3 Whooping Cough


It is a highly infectious childhood disease caused by Bordetella pertussis. It is most severe in young
infants who have not yet been immunized.

174
Clinical presentation
• Paroxysmal cough associated with a whoop
• Fever
• Nasal discharge

Non-pharmacological Treatment
• Place the child head down and prone, or on the side, to prevent any inhaling of vomitus
and to aid expectoration of secretions.
• Care for the airway but avoid, as far as possible, any procedure that could trigger
coughing, such as application of suction, throat examination
• Do not give cough suppressants, sedatives, mucolytic agents or anti-histamines.
• If the child has fever (>38.50C) give paracetamol.
• Encourage breastfeeding or oral fluids
• Whooping cough is preventable by immunization with pertussis vaccine contained in DPT-
HepB-Hib vaccine at week 6, 10 and 14.
Oxygen
• Give oxygen to children who have spells of apnoea or cyanosis, or severe paroxysms of
coughing.
• Use nasal prongs, not a nasopharyngeal catheter or nasal catheter which can provoke
coughing.

Pharmacological Treatment
A: erythromycin (PO) 12.5 mg/kg 6hourly for 10days.
This does not shorten the illness but reduces the period of infectiousness
• If there is fever
In Children older than age 2 months:
A: trimethoprim + sulfamethoxazole (FDC) (PO) 8mg+40mg/kg 12hourly

9.6.4 Bronchiectasis
Bronchiectasis is a progressive respiratory disease characterized by permanent dilatation of the
bronchi and associated with a clinical syndrome of cough, sputum production and recurrent
respiratory infections.

Investigations
FBP, ESR, Serum IgE and IgE to aspergillus, serum immunoglobulin (IgG, IgA, IgM) CXR, Sputum
culture and sensitivity, CT-Chest (CT contrast if suspicion of PE/HRCT, bronchoscopy.

Non-pharmacological Treatment
• Physiotherapy and postural drainage
• Avoid smoking
• Airways clearance technique
• Pulmonary rehabilitation
• Respiratory care during childhood measles helps prevent the development of
bronchiectasis in children

Pharmacological Treatment
Consider antibiotics in patients with bronchiectasis with >3 exacerbations per year. (empirical
treatment while wait for culture and sensitivity)
Adults:
A: ciprofloxacin (PO) 500mg 12hourly for 10days
AND
A: metronidazole (PO) 400mg 8hourly for 10days
Children:
A: amoxicillin (PO) 40mg/kg in 2 divided doses for 7days
AND
A: metronidazole (PO) 7.5 mg/kg 8hourly for 5–7days

If pseudomonas aeruginosa suspicion (should be culture guided)


D: ceftazidime (IV) 2g 8hourly for 14days
OR

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S: piperacillin+tazobactam (FDC) (IV) 4.5mg 8hourly for 14days
AND
D: itraconazole (PO) 100mg-200mg 12hourly

Prevention of infection
A: ciprofloxacin 500mg (PO) 24hourly for 7–14days
OR
A: erythromycin (PO) 250–500mg 24hourly for 7–14days

9.6.5 Lung Abscess


Lung abscess is a cavity within the lung parenchyma filled with necrotic tissues, which occurs as a
result of tissue-destroying infection.

Clinical presentation
It is characterized by high fever, breathlessness, cough productive of large amounts of foul-smelling
sputum and haemoptysis.

Investigation
FBP, ESR, CXR, Sputum Analysis (Gram Stain, Cytology, Gene Xpert, Culture), Blood Culture, CT
Chest, Bronchoscopy, Sputum for ova and parasite (if Parasitic cause is suspected).

Non-pharmacological Treatment
Postural drainage

Pharmacological Treatment
B: ampicillin + cloxacillin (FDC)(IV) 500–1000mg for 7days then (PO) 8hourly for 3–
6weeks (children 50mg/kg/dose)
AND
B: metronidazole (IV) 500mg 8hourly for 7days then (PO) 400mg 8hourly for 4–6weeks
(children 7.5mg/kg)

Note
The duration of antibiotics therapy depends on the clinical and radiographic response of the
patient, but completely healing, with radiographic normalization can be seen after two months.
Refer patient to specialized unit ifLarge cavity size (ie, >6cm in diameter), persistent fever.

D: ceftriaxone + sulbactam (FDC) (IV) 1.5-3g 6hourly 4-6weeks


OR
S: clindamycin (IV) 600mg 8hourly for 7days and then (PO) 300mg 8hourly 4-6weeks
OR
S: piperacillin + tazobactam (FDC) (IV) 4.5g 6hourly 4-6weeks
OR
S: meropenem (IV) 1g 8hourly for 4-6 weeks

9.6.6 Aspergilosis
Clinical presentation
• Cough • Wheezing may be noted on
• Fever auscultation.
• Chest pain. • Mucous plugs upon coughing.
• Difficulty breathing • Tachypneic and have rapidly
• Hemoptysis ranging from mild to progressive worsening
severe. • Hypoxemia.

Investigations
• Chest X-ray and CT, pulmonary aspergillosis classically manifests as a halo sign and later
an air crescent sign
• Sputum Culture.
• Bronchoscopy (BAL)

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Non-pharmacological Treatment
• Surgical treatment
• Bronchial artery embolization (for life threatening hemoptysis)

Pharmacological Treatment
D: itraconazole (PO) 100-200mg 24hourly 6-12weeks

9.6.7 Pneumocystis Pneumonia (PCP)


Clinical presentation
• Cough dry/productive • Scattered crackles and wheeze
• Exertional dyspnoea may be present, or rarely signs of
• Fever focal consolidation
• Tachypnoea • Pulse oximetry may show low
• Chest pain SaO2 at rest
• There may be signs of AIDS such • Extra-pulmonary disease may
as thrush, oral hairy leucoplakia or manifest as hepatosplenomegaly,
Kaposi's sarcoma lymphadenopathy or ocular disease

Investigations
• Elevated lactate dehydrogenase
• ABG may show hypoxia.
• The alveolar-arterial oxygen tension gradient may be increased.
• Serum (1-->3) Beta-D-glucan levels (high in PCP) is currently being investigated as a
diagnostic test.
• Chest X-ray
• CT-CHEST (ground glass infiltrates but has low sensitivity and specificity.)
• Gallium scanning is highly sensitive but with low and variable specificity.
• PFT (Reduction in Vital capacity (VC) and the total lung capacity (TLC).

Management
Refer table 9.4

9.6.8 Silicosis
Clinical presentation
• Asymptomatic • Fine/coarse crackles
• Chronic cough • Rhonchi and/or wheezes
• Dyspnea on exertion • Tachypnea

Investigations
• Cor pulmonale • PFT
• Chest X-ray • Lung function tests
• CT Scan (if indicated) • Lung biopsy (if indicated)

Non-pharmacological
• Avoid further exposure to respirable • Vaccination against influenza and
silica pneumococcus
• Smoking cessation • Oxygen therapy (if indicated)
• Bronchodilators (if indicated) • Lung transplantation

9.6.9 Coal worker’s pneumoconiosis

Clinical presentation
• Asymptomatic • Dyspnea on exertion
• Chronic cough • Fine/coarse crackles

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• Rhonchi and/or wheezes • Cor pulmonale
• Tachypnea

Investigations
• Chest X-ray • Lung function tests
• CT Scan (if indicated) • Lung biopsy (if indicated)

Non-pharmacological
• Avoid further exposure to coal dust • Vaccination against influenza and
• Smoking cessation pneumococcus
• Bronchodilators (if indicated) • Oxygen therapy (if indicated)
• Lung transplantation

9.6.10 Sarcoidosis

Clinical presentation
• The common symptoms/signs • Nerve palsies, headache, ataxia,
depend on which organ or system cognitive dysfunction, weakness,
is affected. and seizures.
• Rales/crepitations • Anterior uveitis
• Jaundice is rare • Tachyarrhythmias and
• Macules, papules, and plaques bradyarrhythmias
may arise as single isolated lesions • Polyarthritis, chronic arthritis
• Skin lesions frequently leave Scars,
pits, and pale, depigmented areas

Investigations
• FBP • Auto immune profile
• ESR • Biopsy
• LFT • Images:
• RFT • CXR,
• RF, • CT SCAN,
• CPR, S/Electrolytes, LP, • PETSCAN, FUNDOSCOPY.

Pharmacological Treatment
A: prednisolone (PO) 1mg/kg/day

Referral: Refer to Specialized center (specialist- physician /dermatologist /rheumatologist


/pulmonologist)

9.6.11 Obstructive Sleep Apnea Syndrome (OSA)


Obstructive sleep apnea (OSA) is characterized by episodes of complete or partial collapse of the
airway with an associated decrease in oxygen saturation or arousal from sleep. OSA is a sleep
disorder that involves cessation or significant decrease in airflow in the presence of breathing effort.

Clinical Presentation
• Daytime sleepiness • Heartburn or gastro esophageal
• Restless sleep reflux disease; and heavy night
• Loud snoring sweats
• Morning headaches; • Trouble concentrating; mood
• Insomnia; changes such as irritability, anxiety
• Decreased sex drive; and depression; Forgetfulness;
• Unexplained weight gain; Increased heart rate and/or blood
• Increased urination and/or nocturia. pressure;

178
Investigations
• Nocturnal polysomnography • Multiple Sleep Latency and
• Thyrotropin test Maintenance of Wakefulness Tests
• Cysteine levels

Non-pharmacological Treatment
• Lifestyle modification (avoid alcohol, sleeping pills, and other sedatives)
• Continuous positive airway pressure (CPAP)
• The oral appliance (e.g. a mandibular advancement splint)

Pharmacological Treatment
C: acetazolamide (PO) 500mg-1g 24hourly for 3-5days

Surgical intervention
(Maxillomandibular advancement, Tonsillectomy) Uvulopalatopharyngoplasty)

9.6.12 Cor Pulmonale


Cor pulmonale is defined as an alteration in the structure (hypertrophy or dilation) and function of the
right ventricle (RV) of the heart caused by a primary disorder of the respiratory system resulting in
pulmonary hypertension.

Clinical Presentation
• Fatigue • Systolic murmur of tricuspid
• Tachypnea regurgitation.
• Exertional dyspnea • Shortness of breath
• Cough • Wheezing
• Anginal chest pain • Chronic wet cough
• Syncope with exertion • Swelling of the abdomen with fluid
• lower limb edema • Swelling of the ankles and feet
• Raised JVP • Enlargement of the liver
• Wheezes and crackles • Bluish discoloration of face

Investigations
• Electrocardiography (ECG) • Other test to rule out etiology
• Echocardiography • FBP/Hematocrit level
• ABG • Serum alpha1-antitrypsin
• BNP • Antinuclear antibody (ANA)
• CXR • Anti-SCL-70 antibodies
• Chest computed tomography • Coagulations studies (serum levels
(CT)+/-CTPA of proteins S and C, antithrombin
• Ventilation/perfusion (V/Q) III, factor V Leyden, anticardiolipin
scanning antibodies, homocysteine)
• Cardiac magnetic resonance
(CMR) (as indicated)

Non-pharmacological Management
• Oxygen therapy when PaO2 is less • Surgical embolectomy
55mmHg • Lung transplant
• Pulmonary embolectomy • Pulmonary rehabilitation
• Uvulopalatopharyngoplasty (UPPP)

179
Pharmacological Treatment
Treat Heart Failure (right sided heart failure)
B: nifedipine ER (PO) 30mg 12hourly
Pulmonary Hypertension management
S: sildenafil (PO) 5mg -20mg 8hourly
OR
warfarin or rivaroxaban for indicated patient (For dosage refer to Pulmonary embolism management)

9.6.13 Pleural Effusion


Pleural effusion, is excessive collection of fluid in the pleural space, is rarely a primary disease
process but is usually secondary to other diseases.
Clinical presentation
• Progressive dyspnea
• Cough
• Pleuritic chest pain
When pleural fluid >300ml you will get these symptoms
• Dullness to percussion
• Decreased tactile fremitus
• Asymmetrical chest expansion
• Pleural friction rub
• Displacement of the trachea and mediastinum toward the side of the effusion

Investigations
• CXR
• Full blood picture
• Erythrocyte Sedimentation Rate (ESR)
• Serum ADA
• Point care bed side USS
• Pleural fluid analysis: - (The pleural fluid analysis above will be requested as per indication
of suspected diagnosis.)
o pleural fluid cytology
o pleural fluid culture
o pleural fluid Gene x pert, ADA, LDH, glucose, pH
o pleural fluid cell count.
o pleural fluid amylase
o pleural fluid triglycerides and cholesterol
o pleural fluid bilirubin

• Tumour markers as indicated (e.g. • ECHO


CA-15, CEA, CA-125etc). • ECG
• Rheumatoid Factor (if indicated) • CT-Scan Chest with contrast
• Autoimmune profile or single • Thoracoscopy
marker (ANA, ACE etc) • Pleural Biopsy (when suggestive of
• Renal function (creatinine and malignancy)
BUN) • Bronchoscopy
• Liver function and liver enzymes
(Albumin, bilirubin total, direct, PT,
PTT, INR ALT, AST, GGT, ALP)

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Table 9.12 Staging Pleural Infections and Recommending Drainage

Effusion Stage Pleural Space Features Bacteriology Pleural Fluid Thoracentesis/


Chemistry Drainage
I (uncomplicated Minimal, free-flowing Culture and pH unknown No/No
parapneumonic) effusion (< 10 mm on Gram stain
lateral decubitus) results unknown
II (uncomplicated Small-to-moderate free- Negative culture pH ≥ 7.20 or Yes/No
parapneumonic) flowing effusion (> 10 mm and Gram stain glucose ≥ 60
and less than one-half mg/dL
hemithorax)
III (complicated Large, free-flowing Positive culture pH < 7.20 or Yes/Yes
parapneumonic) effusion (one-half or Gram stain glucose < 60
hemithorax or greater); mg/dL
loculated effusion; effusion
with thickened parietal
pleura
IV (empyema) Pus Tests not Yes/Yes
indicated

Non-pharmacological Treatment
• Serial Thoracentesis-This approach may require an average of eight thoracenteses in 2 -
4weeks, this is for non-complicated pleural effusion.
• Chest Tube Drainage-Chest tubes vary in size but can be classified as large-bore (24F to
34F) or smallbore (8F to 24F) viscous pleural pus, the surgical tradition recommends the
use of large-bore chest tubes (28F to 32F)
• Fibrinolytic Therapy-use of streptokinase, urokinase, and rtPA, indicated for patients with
empyema and complicated parapneumonic pleural effusions.
• Thoracoscopy-medical thoracoscopy and video-assisted thoracoscopic surgery
(VATS), indicated for patient with fibrinopurulent pleural infections and loculated effusion.
• Thoracotomy, Decortication, and Open Drainage-Thoracotomy remains the main
salvage procedure after unsuccessful thoracoscopy, as defined by the failure of lung
expansion to the chest wall

Indication for thoracostomy/decortication


• Indicated for Patients with organized empyemas who cannot tolerate thoracotomy or have
trapped lungs can undergo rib resection with open drainage
• Chronic empyemas with bronchopleural fistulas or chronic empyemas that are not
amenable to surgery
• Critical ill and toxic patients with associated mediastinitis or bronchopleural fistulas who
require mediastinal drainage or fistula closure.
For Malignant Effusions
Chest tube drainage, radiation, chemotherapy, surgical pleurectomy, pleuroperitoneal shunt,
pleurodesis or decortication.

Note
• Emergent thoracentesis and/or chest tube placement is necessary in patients with pleural
effusion with significant respiratory or cardiac decompensation
• Do consultation with a pulmonologist, interventional radiologist, or thoracic surgeon,
depending on the location of the effusion and the clinical situation for patients not
responding to treatment.

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9.6.14 Respiratory Failure
Respiratory failure is a clinical condition that happens when the respiratory system fails to maintain
its main function, which is gas exchange, in which PaO2 lower than 60 mmHg and/or PaCO2 higher
than 50 mmHg. Respiratory failure is classified according to blood gases abnormalities into type 1
and type 2.
Hypoxemic respiratory failure (type I): has a PaO2 < 60 mmHg with normal or subnormal PaCO2.
In this type, the gas exchange is impaired at the level of alveoli-capillary membrane. Examples of
type I respiratory failures are carcinogenic or non-cardiogenic pulmonary edema and severe
pneumonia.

Hypercapnic respiratory failure (type II): has a PaCO2 > 50 mmHg. Hypoxemia is common, and it
is due to respiratory pump failure

Investigations
• ABG • CXR
• FBP • Electrolytes
• Creatine kinase • Creatinine and BUN
• ECHO • AST/ALT/ALP/GGT, albumin and
• ECG bilirubin total, direct
• Troponin-I • PFT-if patient able to perform
• TSH

Non-pharmacological Treatment
Noninvasive Ventilatory Support: Patients with mild-to-moderate acute respiratory failure.

Mechanical Ventilation
Refer to management of cardiogenic pulmonary edema and acute exacerbations of chronic
obstructive pulmonary disease (COPD) in obstructive lung disease

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CHAPTER TEN
GASTROINTESTINAL DISEASE CONDITIONS

10.1 Infections of Gastrointestinal Tract


10.1.1 Amoebiasis
Amoebiasis is an infection caused by the protozoa organism Entamoeba histolytica, which can
cause colitis and other extra-intestinal manifestations. The infection is primarily acquired through
ingestion of contaminated food and water and occasionally can be acquired through oral-anal sexual
practices.

Clinical presentation
• Bloody diarrhea • Peritonitis in severe forms
• Crampy abdominal pain • Evidence of motile trophozoites or
• Fever cysts on saline wet mount from a
• Weight loss stool specimen
Pharmacological Treatment
A: metronidazole (PO) 400–800mg 8hourly for 5days
OR
B: tinidazole (PO) 2g 24 hourly for 3days

10.1.2 Amoebic Liver Abscess


It is the most frequent extra-intestinal manifestation of Entamoeba histolytica infection which results
from the invasion of the portal venous system from the colon leading to inflammation and
subsequently abscess formation particularly involving the right lobe of the liver.

Clinical presentation
• High grade fever, 39°C • Positive imaging evidence of liver
• Right upper quadrant pain, abscess
• Tender and enlarged liver • Serological evidence of E.
histolytica antibodies or antigens.

Pharmacological Treatment
B: metronidazole (IV) 800mg 8hourly for 10days.
OR
B: tinidazole (PO) Adults: 2g once daily for 3days

Note
• Metronidazole and Tinidazole should not be given in the first trimester of pregnancy due to
potential teratogenic effects.
• Should not be taken with alcohol due to disulfiram like effects

Surgery:
Abscess cavity (size >5 cm in diameter) not regressing despite 7days treatment should be aspirated.

10.1.3. Giardiasis
It is the infestation of the upper small intestine caused by the flagellate protozoan Giardia lamblia (or
G. intestinalis), cytopathic effects of which leads to malabsorption and diarrhea. It is more common
in immune compromised individuals and is acquired through ingestion of contaminated water

Clinical presentation
• Crampy abdominal pain • Steatorrhea
• Chronic diarrhoea • Weight loss

183

Investigations
• Evidence of Giardiaintestinalis trophozoites or cysts on serial 3 samples of stool
examination
• Serological evidence of G. Intestinalis trophozoites antigen or antibody
• Evidence of G. Intestinalis in duodenal aspirates or biopsy specimen.
Pharmacological Treatment
A: metronidazole (PO) 400–800mg 8hourly for 5days
OR
B: tinidazole (PO) 2g once daily for 3days

10.1.4 Ascariasis
It is a small intestinal infestation caused by Ascaris lumbricoides which leads to malnutrition, iron
deficiency anaemia, impaired growth and cognition in susceptible hosts. It is most common
infestation in children, and it is acquired through ingestion of contaminated food and water.

Clinical presentation
• Chronic Diarrhea • Chronic Cough (Loffler’s syndrome)
• Steatorrhea • Intestinal obstruction
• Malnutrition • Obstructive jaundice

Investigations
• Stool examination: evidence of ova or worms on wet mount

Pharmacological Treatment
A: mebendazole (PO) 500mg stat or 100mg 12hourly for 3days.
OR
A: albendazole (PO) 400mg stat

10.1.5 Ancylostomiasis
It is a hookworm disease caused by infestation of the small intestine with Ancylostoma duodenale or
Necator americanus leading to anaemia and malnutrition.

Clinical presentation
• Abdominal pains
• Chronic diarrhea
• Melena stool
• Weight loss
• Chronic cough (Loffler’s syndrome) PLUS
• Evidence of ova or worms on wet mount stool examination
• Anaemia

Pharmacological Treatment
A: mebendazole (PO) 500mg stat or 100mg 12hourly for 3days.
OR
A: albendazole (PO) 400mg stat

Note
If persistent, give second course after 4 weeks. Iron replacement and nutritional supplementation
(protein and vitamins) should be part of the management strategy. Albendazole is
contraindicated in the first trimester of pregnancy

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10.1.6 Strongyloidiasis
Small intestinal infestation caused by Strongyloides stercoralis usually asymptomatic in immune
competent adult but can lead to life-threatening infestation and disseminated strongyloidiasis in an
immune-compromised host associated with high mortality rates
Clinical presentation
• Pruritic papulo–vesicular rash at • Colicky abdominal pains
the site of penetration or urticarial • Chronic diarrhea and passage of
rash involving the perennial region mucus
extending to the buttocks, thighs • Weight loss
and abdomen • Hyper-infection syndrome
• Chronic cough

Investigations
• Evidence of rhabditiform larva in wet mount stool examination with Serological evidence
(ELISA) for anti-strongyloides antibody

Pharmacological Treatment
A: albendazole (PO) 400mg 12hourly for 3days (Repeat after 4 weeks if still positive stool
findings)
OR
A: ivermectin (PO) 200 µg /kg 24hourly for 2days

Note
Give treatment for 10 days in case of disseminated/super infestation

10.1.7 Taeniasis
Is a tapeworm disease acquired from eating raw or not-well cooked food? Can be due to Taenia
saginata (beef tapeworm), Taenia solium (pork tapeworm), Diphyllobothrium latum (fish tapeworm)
and Hymenolepsis nana (faecal oral contamination from human and dogs) leading to chronic
malnutrition (Taeniasis) or multi-organ dissemination and dysfunction (Cysticercosis)

Clinical presentation
• Taeniasis • Constipation or diarrhea
• Colicky abdominal pain • Pruritus ani
• Body Weakness • Hyperexcitability
• Loss of or increased appetite

Investigations
• Evidence of characteristic ova, proglottids or scolex in the wet mount stool examination

Cysticercosis - The cysticerci are most often located in subcutaneous and intermuscular tissues,
followed by the eye and then the brain. The CNS is involved in 60-90% of patients i.e.
Neurocystercosis which may manifest as

Convulsions and/or seizures:


• Intracranial hypertension: headache, nausea, vomiting, vertigo, and papilledema.
• Personality and mental status changes (Neuropsychiatric changes)
• Behavioral changes and learning disabilities more marked in children and
immunocompromised adults. PLUS
• Head CT scan OR Brain MRI

Note
Refer the patient to high centers for further investigation and expertise.

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Pharmacological Treatment
Taeniasis
A: praziquantel (PO) 5–10mg/kg stat
AND
A: magnesium sulphate (PO) 5–10 g in a glass of water after 2hours

Cysticercosis (NCC)
A: praziquantel (PO) 50mg/kg 24hourly for 21days
OR
A: albendazole (PO) 15mg/kg 24hourly for 30days.
AND
B: dexamethasone (IV) 4mg 12hourly can be given up to 7days.
AND
A: carbamazepine (PO) initially 200 mg 12-24hourly, increased slowly to 0.8–1.2 g
24hourly in divided doses

Note
Hydrocephalus should be treated with surgical shutting. Ocular manifestation cysticercosis, should
be referred to eye specialist

10.1.8 Echinococcosis
It is a canine tape worm Echinococcus Granulosus which is transmitted by dogs, sheep and horses.
Human infestation is through contamination of food or water causing visceral cysts (Hydatid Cyst
Disease) particularly in the liver and lungs and is usually asymptomatic in susceptible host.

Clinical presentation
• Upper abdominal discomfort and pain, poor appetite,
• Upper abdominal mass swelling with enlarged liver.
• Cough with features of acute hypersensitivity reaction. (for ruptured cysts)
• Portal hypertension, biliary obstruction or Budd-Chiari syndrome (for complicated cases)

Pharmacological Treatment
A: albendazole (PO) 400mg 12hourly for 3months
OR
A: mebendazole (PO) 500mg 12hourly for 3months

Referral: For symptomatic/ complicated cases refer to higher centres with management and
expertise.

10.1.9 Schistosomiasis
Parasitic disease caused by blood flukes (trematodes) of the genus Schistosoma. Common species
found in Tanzania are S. haematobium responsible for urogenital schistosomisis and S. mansoni
responsible for intestinal schistosomiasis as a result of immune mediated reaction which leads to
progressive inflammation and fibrosis of the urinary bladder or portal venous system respectively.

Clinical presentation
Schistosoma mansoni • Anemia
• Swimmer’s itch or katayama fevers • Hepatomegaly
in acute infection phase. • Portal hypertension with bleeding
• Colicky abdominal pains esophageal varices
• Diarrhoea and dysentery • Decompensated liver disease

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Schistosoma hematobium
• Dysuria and terminal hematuria • Glomerulonephritis and amyloidosis
• Hematospermia • Bladder carcinoma
• Obstructive uropathy • Chronic kidney failure
(hydronephrosis, hydroureters)

Investigations

• Laboratory evidence characteristic eggs in urine, (S. Hematobium) or in stool (S. manson,
S. japonicum) examined by kato katz thick smear procedure or PCR assays of both urine
and stool samples.

Pharmacological Treatment
A: praziquantel (PO) 40mg/kg stat or in 2 divided doses

10.1.10 Typhoid and Paratyphoid


It is an acute systemic disease resulting from infection by Salmonella typhi and S. paratyphi, serovar
group A and B respectively. Infection is acquired through ingestion of contaminated food and water.

Clinical presentation
• Fever, severe headache, abdominal and muscle pains (myalgia)
• Delirium, obtundation, intestinal hemorrhage, bowel perforation,
• Sequela neuropsychiatric complications
Investigations
• Laboratory evidence of positive cultures from bone marrow aspirates; blood or stool done
within 1 week of acute infection OR
• Salmonella stool antigen test
• Indirect fluorescent Vi antibody, ELISA for immunoglobulin M (IgM) and IgG antibodies to
S. Typhi polysaccharide.

Pharmacological Treatment
Uncomplicated typhoid fever
A: ciprofloxacin (PO) 500mg 12 hourly for 10-14days
OR
B: azithromycin (PO) Adult 500mg 24hourly for 7days
OR
S: cefixime 400mg (PO) 24hourly for 7-14days

For complicated typhoid fever


C: ciprofloxacin (IV) 200-400 mg 12hourly daily 7days
OR
B: ceftriaxone (IV) 1-2gm 24hourly 4-7days

Note
Definitive treatment of typhoid (enteric fever) is based on susceptibility. For patients with severe or
complicated disease (e.g. systemic toxicity, depressed consciousness, prolonged fever, organ
system dysfunction or other features that prompt hospitalization), initial therapy with a parenteral
agent is appropriate.

10.1.11 Shigellosis
Shigella organisms are a group of gram-negative, facultative intracellular bacteria pathogens. They
are grouped into 4 species: Shigella dysenteriae, Shigella flexneri, Shigella boydii, and Shigella
sonnei, also known as groups A, B, C, and D respectively. Shigellosis is spread by means of fecal-
oral, by ingestion by ingestion of contaminated food or water and leads to bacillary dysentery.

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Clinical presentation
• Acute abdominal cramping, high-grade fever, emesis and large-volume watery diarrhea
• Tenesmus, urgency, fecal incontinence, mucoid bloody diarrhea
• Severe headache, lethargy, meningismus, delirium, and convulsions
• Hemolytic uremic syndrome (HUS), microangiopathic hemolytic anemia,
thrombocytopenia, and renal failure
• Profound dehydration and hypoglycemia

Investigations
• Laboratory evidence of microscopic isolation of the bacteria from stool or rectal swabs
specimens
• Stool culture for suspected cases in early course of infection
• An enzyme immunoassay (ELISA) for shiga toxin detection in stool for S. dysenteriae type
I.

Pharmacological Treatment
A: ciprofloxacin (PO) 500mg 12hourly for 5days
OR
A: erythromycin (PO) 500mg 6hourly for 5days.

10.1.12 Cholera
For diagnostic criteria, investigations, prevention and treatment refer to under notifiable diseases.

10.2. Disorders of Gastrointestinal Tract


10.2.1 Peptic Ulcer Disease
Refers to acid related peptic ulceration involving the lower esophagus; stomach and duodenum as a
result of active inflammation induced by acid –pepsin leading to disruption of the mucosal integrity
causing local defect or excavation

10.2.1.1 Gastroesophageal Reflux Disease (GERD)


It is a disorder resulting from gastric acid-pepsin activity and other gastric contents reflux into the
esophagus due to incompetent barriers at the gastroesophageal junction leading to active
inflammation of the distal third of the esophagus (prolonged contact with acid can evolve to stricture)

Clinical presentation
• Heartburn and regurgitation are cardinal symptoms.
• Odynophagia, dysphagia, weight loss and bleeding
• Chronic cough, laryngitis, pharyngitis
• Chronic bronchitis, asthma, COPD, pneumonia, chronic sinusitis and dental decay

Investigations
• Endoscopic evidence mucosal ulceration
• Histological evidence of chronic active inflammation
• Positive finding with a gold standard 24-hours esophageal pH testing.

Pharmacological Treatment
Non-erosive, symptomatic
A: omeprazole (PO) 20mg 24hourly for 8weeks
OR
S: esomeprazole (PO) 20mg-40mg 24hourly for 8weeks.

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Erosive esophagitis
C: pantoprazole (PO) 40mg 24hourly for 8-16weeks
For refractory cases acid suppression therapy may require continuation up to 6 months. Lifestyle
modification and avoidance of triggers is important including avoidance of smoking, alcohol and
NSAID use.

Referral: Refer to next level center with adequate expertise and facility for refractory cases or cases
with alarming symptoms (red flags) such as bleeding, anemia, early satiety, progressive dysphagia
or odynophagia, unexplained weight loss, recurrent vomiting or family history of gastrointestinal (GI)
cancers, age ≥ 40 years.

10.2.1.2 Gastroduodenal Ulcers (PUD)


This is a disorder resulting from breakdown of mucosal defense mechanisms against hydrochloric
acid and proteolytic enzymes, most commonly secondary to H. Pylori infection or NSAID use.

Clinical presentation
• Burning epigastric abdominal pains, • Hematemesis or melena stools
usually relived by antacids. • Weight loss
• Anorexia, early satiety, bloating,

Investigations
• Endoscopic evidence of gastric or duodenal mucosal ulceration

Pharmacological Treatment
A: omeprazole (PO) 20mg 24hourly for 8weeks
OR
C: pantoprazole (PO) 40mg 24hourly for 8weeks
OR
S: esomeprazole (PO) 20mg 24hourly for 8weeks
AND
A: antiacid liquid (PO) 10-15ml 12hourly to 8hourly for 7-14days

For bleeding PUD: refer to higher centers


C: pantoprazole (IV) 80mg stat then 40mg 12hourly for 2-3days, then (PO) as above if
bleeding stops
OR
S: esomeprazole (IV) 40mg 12hourly for 2-3days, then (PO) as above if bleeding stops

10.2.1.3 Helicobacter Pylori Related Peptic Ulcer Disease


Helicobacter pylori is a ubiquitous organism that is present in about 50% of the global population.
Chronic infection with H pylori causes atrophic and even metaplastic changes in the stomach, and it
has a known association with peptic ulcer disease. The most common route of H pylori infection is
either oral-to-oral or fecal-to-oral contact.

Clinical presentation
• As above in cap 10.2.1.1

Investigations
• Positive stool antigen test (Stop • Positive urease test on endoscopic
PPI 2 weeks before testing) biopsy sample
• Positive urease breath test • Identification of the pathogen by
histopathology examination

Pharmacological Treatment
Triple therapy is indicated for complete eradication of the organism

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A: omeprazole (PO) 20mg 12hourly for 10-14days
AND
A: amoxycillin (PO) 1000mg 12hourly 10-14days
AND
A: metronidazole (PO) 400mg 12hourly for 10–14days
Alternatively
C: lansoprazole (PO) 30mg 12hourly for 10-14days
AND
C: clarithromycin (PO) 500mg 12hourly 10-14days
AND
B: tinidazole (PO) 500mg 12hourly for 14days
OR
Concomitant Therapy (all for 7 days)
A: omeprazole (PO) 20mg 12hourly
AND
A: amoxicillin (PO) 1000mg 12hourly
AND
A: metronidazole (PO) 400mg 12hourly
AND
C: clarithromycin (PO) 500mg 12hourly

Treat with Bismuth-based therapy for H. pylori treatment failure


C: pantoprazole (PO) 40mg 12 hourly 10-14days
OR
S: esomeprazole (PO) 40mg 12hourly 10-14days
AND
S: bismuth subsalicylate (PO) 525 mg 6hourly 10-14days
AND
A: metronidazole (PO) 250 mg 6 hourly or 500 mg 8hourly 10-14days
AND
S: tetracycline (PO) 500 mg 6hourly for 10-14days.
Note
H.pylori diagnostic tests should be repeated 5 weeks after the last dose of eradication therapy, and
the PPI should be stopped 2weeks before testing the H.pylori stool antigen test to confirm
eradication.

10.2.2 Ulcer Related Conditions


10.2.2.1 Non-ulcer Dyspepsia (Functional Dyspepsia, Indigestion)
It is a chronic recurrent dyspeptic disorder characterized by upper abdominal symptoms, discomfort,
pain, fullness, early satiety, bloating, burning epigastric pain syndrome and post prandial distress
syndrome without any organic, systemic or metabolic disease to explain its presence.

Clinical presentation
• Dyspeptic symptoms present for • Early satiety
last 3 months and onset at least • Epigastric pains
months prior to diagnosis • Epigastric burning
• Bothersome abdominal discomfort
post prandial fullness.

Investigations
• Lack of evidence of structural disease by upper endoscopic examination.

Pharmacological Treatment
H. pylori eradication (see under H. pylori)
A: omeprazole (PO) 20mg 24hourly for 4-8weeks
OR

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C: pantoprazole (PO) 40mg 24hourly for 4-8weeks
OR
S: esomeprazole (PO) 40mg 24hourly for 4-8weeks
AND
C: metoclopramide (PO) 10mg 8hourly when required (bloating and nausea symptoms,
delayed gastric emptying)
OR
D: domperidone (PO) 10mg 8hourly when required to alleviate bloating and nausea
symptoms, delayed gastric emptying.
AND
A: amitriptyline (PO) 25mg at bedtime when required for refractory cases

Note
Presence of alarm features (see list above under GERD) warrant OGD.

10.2.2.2 Gastritis
This is an inflammatory mucosal response to injury from variety of agents and mechanisms including
infections, drugs, alcohol, acute stress, radiation, allergy, acid and bile, ischemia or direct trauma.
The inflammation may involve the entire stomach (pangastritis) or a region of the stomach (antral
gastritis) while the severity of inflammation may be erosive or non-erosive.

Clinical presentation
• Nausea, vomiting, loss of appetite, belching, and bloating
• Acute abdominal pain or abdominal discomfort
• Fever, chills, and hiccups also may be present

Investigations
• Endoscopic evidence of gastric mucosal inflammation
• Histologic evidence of chronic active inflammation of biopsy specimen.

Non-pharmacological Treatment
• Reduce the use of drugs known to cause gastritis (e.g., NSAIDs, alcohol)
• Stop smoking
• Reduce fatty, spicy and deep-fried foods

Pharmacological Treatment
Triple therapy for H. pylori eradication if confirmed present.
Administer fluids and electrolytes as required, particularly if the patient is vomiting.

C: pantoprazole (IV) 40mg 6hourly 2-3days


OR
S: esomeprazole (IV) 40mg 12hourly 2-3days
AND
C: metoclopramide (IM) 10mg 12hourly when required (for cases presenting with
intractable vomiting) in order to relieve symptoms.
Switch to oral PPI once patient can tolerate oral intake.
Referral
Refer to next level service with adequate expertise and facilities for complicated case with alarm
features (anemia, vomiting blood and weight loss, see complete list under GERD above).

10.2.3 Gastrointestinal (GI) Bleeding


Intraluminal blood loss anywhere from the oropharynx to the anus. Classification: upper = above the
ligament of Treitz; lower = below the ligament of Treitz “Severe” GIB: defined as having associated
shock, orthostatic hypotension, fall in hematocrit by 6% (or decrease in Hb by 2 g/dL), or requiring
transfusion ≥2U PRBCs. Requires hospitalization.

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10.2.3.1 Upper GI Bleeding (UGIB)
PUD caused by Helicobacter pyloriinfection or NSAID use is the most common cause of nonvariceal
UGI bleeding. Characteristic findings are hematemesis, melena, or (infrequently) bright-red blood
per rectum or a high serum BUN/creatinine ratio. Slow and/or chronic bleeding is suggested by iron
deficiency and is typical of erosive disease, tumor, esophageal ulcer, portal hypertensive
gastropathy, Cameron lesion (erosions found within large hiatal hernias), and angiodysplasia.

Table 10.1: Differential Diagnosis of Upper GI Bleeding


Presentation Diagnosis
Dyspepsia, H. pylori infection, NSAID use, Peptic ulcer disease
anticoagulation, severe medical illness
Stigmata of chronic liver disease, evidence of portal Variceal bleeding
hypertension or risk factors for cirrhosis (alcohol
use, viral hepatitis)
History of heavy alcohol use and retching before Mallory-Weiss tear
hematemesis, hematemesis following weightlifting,
or young woman with bulimia
Heartburn, regurgitation, and dysphagia; usually Esophagitis
small-volume or occult bleeding
Progressive dysphagia, weight loss, early satiety, Esophageal or gastric cancer
or abdominal pain; usually small-volume or occult
bleeding
NSAID use, heavy alcohol intake, severe medical Gastroduodenal erosions
illness; usually small-volume or occult bleeding

Initial management
Assess severity: vital signs including orthostatic changes, JVP. Tachycardia (can be masked by βB
use) suggests 10% volume loss, orthostatic hypotension 20% loss, shock >30% loss. After the
patient is stabilized, upper endoscopy is required to document the source of bleeding. If upper
endoscopy shows an ulcer, test for H. pylori infection.
Resuscitation: placement of 2 large-bore (18-gauge or larger) intravenous lines, volume
replacement: NS or LR to achieve normal vital signs, urine output, and mental status.

Pharmacological Treatment
For variceal bleeding refer to (10.4.2.3 Bleeding Esophageal Varices)
For bleeding peptic ulcer disease
C: pantoprazole (IV) 40mg 12hourly for 2-3days
OR
S: esomeprazole (IV) 40mg 12hourly for 2-3days

Note
• Treat high-risk ulcers endoscopically (haemoclips, thermal therapy, or injection therapy)
and continuous IV PPI infusion for 72 hours. Blood transfusion to target haemoglobin level
of 7 g/dl Repeat endoscopic therapy for continued bleeding
• Surgery or interventional radiology if endoscopic therapy unsuccessful

Laboratory Investigations
• FBP, LFT, RFT. • Viral hepatitis screening
• Abdominal ultrasound • H. pylori stool antigen

10.2.3.2 Lower gastrointestinal (GI) Bleeding


Acute, painless LGI bleeding in older adult patients is usually due to colonic diverticula or
angiodysplasia. Ten percent of rapid rectal bleeding has an UGI source.
Consider outpatient follow-up or early discharge when:

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• patient age <60 years
• no hemodynamic instability
• no evidence of gross rectal bleeding
• identification of an obvious anorectal source of bleeding

Table 10.2: Differential Diagnosis of Lower GI Bleeding


Presentation Diagnosis
Painless, self-limited, massive hematochezia Diverticular bleeding (most common overall cause)
Chronic blood loss or acute painless hematochezia Angiodysplasia
in an older adult patient
Stool positive for occult blood in an asymptomatic Colonic polyp or cancer
patient
Risk factors for atherosclerosis and evidence of Ischemic colitis
vascular disease in an older adult patient; typically,
with LLQ abdominal pain
Aortic stenosis Angiodysplasia (Heyde Syndrome)
History of bloody diarrhea, tenesmus, abdominal IBD
pain, fever
Rapid UGI bleeding Dieulafoy lesion (large, tortuous, submucosal
arteriole)
Large hiatal hernia Cameron lesion (mucosal erosions)
Recent liver or biliary procedure Hemobilia
Necrotizing pancreatitis Hemosuccus pancreaticus (bleeding from
pancreas)
Aortic aneurysm repair Aortoenteric fistula
Painless hematochezia in a young patient and Meckel diverticulum
normal upper endoscopy and colonoscopy
Mucocutaneous telangiectasias Hereditary hemorrhagic telangiectasia

Note
• According to expert opinion, the blood transfusion threshold for patients with colonic bleeding is a
haemoglobin value <9 g/dL (note this is different for the evidence-based threshold for UGI bleeding).
• If the patient is hemodynamically unstable, resuscitate the patient before diagnostic studies are
performed. Most episodes of LGI bleeding resolve spontaneously.
• Colonoscopy is recommended early, usually within the first 48 hours of admission, and endoscopic
therapy is used to control continued bleeding.
• If colonoscopy does not identify a discrete lesion or endoscopic therapy does not control the bleeding,
interventional angiography or surgery may be indicated.
• Patients with angiodysplasia in the setting of AS (Heyde Syndrome) may benefit from valve
replacement surgery.

10.2.3.3 Bleeding of Obscure Origin


Obscure GI bleeding is recurrent blood loss without an identified source of bleeding despite upper
endoscopy and colonoscopy.Patients aged ≤50 years are more likely to have tumors (leiomyomas,
carcinoid, adenocarcinoma, or lymphoma), Dieulafoylesion, or Crohn’s disease. Older patients are
more likely to have vascular lesions, such as angiodysplasia. Angiodysplasia is the most common
cause of obscure GI bleeding overall (40% of all cases). Patients may present with either melena or
hematochezia or positive fecal occult blood test (FOBT). The first step is to repeat upper endoscopy
and/or colonoscopy, which is diagnostic in approximately 40% of cases.

For patients with obscure activeGI bleeding


• nuclear studies (technetium 99m-labeled erythrocyte or sulfur colloid nuclear scan) first,
followed by angiography
• if unrevealing, consider push enteroscopy or balloon-assisted enteroscopy (deep
enteroscopy)

193
• surgery and intraoperative enteroscopy is a last diagnostic option

For patients with occult GI bleeding


• capsule endoscopy (first choice GIE 2015; 81:889) or deep enteroscopy
• if unrevealing, repeat endoscopic examinations (upper endoscopy, colonoscopy, capsule
endoscopy), or deep enteroscopy
10.3 Diseases of the Intestine
10.3.1 Inflammatory Bowel Diseases
Inflammatory bowel disease (IBD) is an idiopathic disease involving an immune reaction of the body
to its own intestinal tract. The 2 major types of IBD are ulcerative colitis (UC) and Crohn’s disease
(CD). Pathologically, ulcerative colitis is limited to the colon while Crohn’s disease can involve any
segment of the gastrointestinal (GI) tract from the mouth to the anus.

10.3.1.1 Ulcerative Colitis (UC)


Inflammatory condition that involves the rectum and extends proximally to affect a variable extent of
the colon up to the caecum

Clinical presentation
• Diarrhoea • Crampy abdominal pain
• Rectal bleeding • Fevers and chills
• Tenesmus, passage of mucus

Investigations
• Endoscopic evidence of diffuse and continuous colonic mucosal inflammation with friability
and loss of mucosal vascularity characteristic cobble stone appearance.
• Histologic evidence of abnormal crypt architecture and superficial inflammation typical of
UC.

Pharmacological Treatment
D: sulfasalazine (PO) 1000mg 6hourly a day for acute disease, reducing to 1000mg once
daily for maintenance
OR
S: mesalazine (PO) 1.5g–4g/day in divided doses reduced to 0.75–2g g/day in divided
doses for maintenance
AND
A: prednisolone (PO) 30–60mg 24hourly for severe, acute and extensive disease; tapering
gradually after induction of remission within 8 weeks.

For severe disease flares give IV corticosteroids,


D: methylprednisolone (IV) 16-20mg 8hourly 5- 7days

If irresponsive (i.e. fewer stools, less bleeding) to IV corticosteroids for 5-7days, or acute
complications give the following;
S: cyclosporine (IV) 2-4mg/kg 12hourly for 7days
THEN change to
S: azathioprine (PO) 1.5-2.5 mg/kg 24hourly for maintenance.
OR
S: infliximab (IV) 5 mg/kg at 0, 2, and 6weeks, then every 8weeks

Note
Complication of UC may present with massive haemorrhage, toxic mega colon, AND perforation with
features of peritonitis necessitates hospitalization. Colonoscopy with random biopsy 8 years after
diagnosis to evaluate for dysplasia, every 1-3 years thereafter based on risk factors. Use steroids only
when the disease is confirmed and for induction of remission only.

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10.3.1.2 Crohn’s Disease
Crohn’s disease is an idiopathic, chronic, transmural inflammatory process of the bowel that often
leads to fibrosis and obstructive symptoms and can affect any part of the gastrointestinal tract from
the mouth to the anus.

Clinical presentation
• Abdominal pain, diarrhea, weight • Small bowel obstruction, due to
loss, anorexia and fever structuring
• Gross rectal bleeding or acute • Perianal disease associated with
hemorrhage is uncommon fistulization
• Anemia due to illeal disease • Gastroduodenal ulceration
involvement

Investigations
• Endoscopic evidence of rectal sparing skip lesions, cobble stoning with linear ulceration
appearance with,
• Histological evidence of transmural disease, aphthous ulcers, and non-caseating
granulomas

Pharmacological Treatment
S: methotrexate (PO) 7.5–15mg weekly
OR
S: azathioprine (PO) 50mg 24hourly for maintenance of remission.
AND
A: prednisolone (PO) 1–2mg/kg for induction of remission only (Taper in 8 weeks)
AND
A: metronidazole (PO) 400mg 8hourly for 7–10days
OR
A: ciprofloxacin (PO) 500mg 12hourly for 7–10days – can be added in presence of
perianal disease or evident septic complications.

For severe disease flare or acute complications


Patients who have had inadequate response to conventional therapy, also for reducing the number
of draining enterocutaneous and rectovaginal fistulas and maintaining fistula closure in adult patients
with fistulizing Crohn disease.

S: infliximab (IV) 5 mg/kg at 0, 2, and 6 weeks, THEN every 8weeks thereafter


AND
S: azathioprine (PO) 1.5-2.5 mg/kg 24hourly

Note
Resuscitative and supportive management should be instituted as for UC section note above.

10.3.2 Pseudomembranous Colitis


This condition is caused by Clostridium difficile, a gram positive, anaerobic bacterium causing
antibiotic associated diarrhoea as a result of altered bacterial flora and release of enterotoxins.

Clinical presentation
• Bloody Diarrhea • Nausea, fever, dehydration
• Abdominal cramps and tenderness

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Investigations

• Lower endoscopic pathognomonic findings of pseudomembranous yellowish plaques


overlying the ulcerated and friable rectal sigmoid colon mucosa
• Laboratory evidence of C. difficile toxin A-B isolation from cultured stool samples (Toxin B)
OR ELISA assay (Toxin A)

Pharmacological Treatment
Stop the causative antibiotics
A: metronidazole (PO) 400mg 8hourly for 10-14days
OR
S: vancomycin (PO) Adults, 125mg–500mg 6hourly for 10-14days

Note
Resuscitative and supportive management should be instituted as for UC above. Refer to next level
of care with adequate expertise and facilities for all suspected cases for initial evaluation and
management and cases presenting with acute complications such as Toxic mega colon

10.3.3 Radiation Proctitis


Radiation proctopathy is defined as epithelial damage to the rectum due to radiation that is
associated with minimal or no inflammation. Acute radiation proctitis occurs during or within six
weeks of radiation therapy. Chronic radiation proctitis has a more delayed onset. The first symptoms
often occur 9 to 14 months following radiation exposure but can occur any time post-irradiation up to
30 years after exposure.

Clinical presentation
• Symptoms of acute radiation proctitis include diarrhea, mucus discharge, urgency,
tenesmus, and, uncommonly, bleeding.
• Patients with chronic radiation proctitis have similar symptoms as patients with acute
radiation proctitis, but bleeding is usually more severe. In addition, patients may have
symptoms of obstructed defecation due to strictures with constipation, rectal pain, urgency,
and, rarely, fecal incontinence due to overflow.
• Concomitant injury to the genitourinary tract or small bowel may lead to fistulas, small
bowel obstruction, small intestinal bacterial overgrowth, urethral stenosis, and cystitis
• Acute radiation proctitis should be suspected in patients with diarrhea, mucus discharge,
urgency, tenesmus, or bleeding during or within six weeks of radiation therapy. Chronic
radiation proctitis should be suspected in patients who develop these symptoms nine
months or more after pelvic radiation exposure.

Investigations
• Stool studies for C. difficile toxin, routine stool cultures (Salmonella, Shigella,
Campylobacter, and Yersinia), Escherichiacoli O157:H7. Microscopy for ova and parasites
(three samples)
• Testing for STI, including C. trachomatis, N. gonorrhoeae, HSV, and Treponema pallidum,
• Endoscopy (colonoscopy and biopsy)
• Magnetic resonance imaging

Pharmacological Treatment
D: sulfasalazine (PO) 3g 24hourly for 4weeks
AND
S: sucralfate enemas (rectal preparation) 2g 12hourly for 4weeks

Note
Refer to higher level facility with expertise and experience in the management complications such as
bleeding. Endoscopic therapy — Argon plasma coagulation (APC) for bleeding. Surgery — Surgery
should be reserved for patients who have. intractable symptoms such as a stricture, pain, bleeding,
perforation, or a fistula

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10.3.4 Irritable Bowel Syndrome
Irritable bowel syndrome (IBS) is a functional GI disorder characterized by abdominal pain and
altered bowel habits in the absence of specific and unique organic pathology.
Four bowel patterns may be seen with IBS;
I. IBS-D (diarrhea predominant)
II. IBS-C (constipation predominant)
III. IBS-M (mixed diarrhea and constipation)
IV. IBS-U (unclassified; the symptoms cannot be categorized into one of the above three
subtypes)

Clinical presentation
• Recurrent abdominal pains or discomfort at least 3 days per month in the last 3 months
associated with two or more of the following
• Improvement with defecation
• Onset associated with a change in frequency of stools
• Onset associated with a change in form of stool
• Bloating or feeling of abdominal fullness

Non-pharmacological Treatment
• Counseling on compelling psycho –social factors, lifestyle modification, avoidance of
trigger factors, and reassurance are corner stone of long-term management strategy. Plus,
supportive therapies such as:
• High fiber diet and eating a healthy diet.

Pharmacological Treatment
A: hyoscine butyl bromide (PO) 10mg 6hourly when required
OR
D: mebeverine (PO) 135mg 8hourly when required
AND
A: amitriptyline (PO) 25mg nocte for one week then 50mg nocte week 2-4.
AND
C: lactulose (PO) 20mls 12hourly (when required for constipation)
OR
A: bisacodyl (PO) 5-15mg when required for constipation

For diarrheal predominant IBS


B: loperamide (PO) 4mg stat, for diarrhoea followed by 2mg 8hourly or after each
unformed stool until diarrhoea is controlled.

10.3.5 Diverticulosis
Acquired herniations of colonic mucosa and submucosa in areas where vasa recta penetrate,
thought to occur in setting of abnormal motility and increased intraluminal pressure.

Clinical presentation
Asymptomatic but 5–15% develop diverticular hemorrhage (see “GIB” above) and <5% diverticulitis

10.3.6 Diverticulitis
Retention of undigested food and bacteria in diverticulum leads to fecalith formation with obstruction
which compromise diverticulum’s blood supply, infection, perforation
Uncomplicated: microperforation leading to localized infection
Complicated: macroperforation leading to abscess, peritonitis, fistula, obstruction

Clinical presentation
• LLQ abdominal pain, fever, nausea, vomiting, constipation or diarrhea

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• Physical findings range from LLQ tenderness and/or palpable mass to peritoneal signs and
septic shock
• Differential diagnosis includes IBD, infectious colitis, PID, tubal pregnancy, cystitis,
colorectal cancer

Investigations
• Plain abdominal radiographs to rule out free air, ileus or obstruction
• Abdominal CT scan with contrast, to assess complicated disease (abscess, fistula)
• Colonoscopy contraindicated acutely as increases the risk of perforation; do 6–8 weeks
after to rule out neoplasm

Pharmacological Treatment
Mild: outpatient indicated if patient has little comorbidity and can tolerate oral intake

A: amoxicillin + clavulanate FDC (PO) 625mg 12hourly daily for 7–10days


AND
A: metronidazole (PO) 400mg 8hourly for 7–10days
AND
Liquid diet until clinical improvement
Alternatively
A: ciprofloxacin (PO) 500mg 12hourly daily for 7–10days
OR
A: metronidazole 400mg (PO) 8hourly for 7–10days
AND
Liquid diet until clinical improvement
For severe cases
B: ceftriaxone (IV) 1-2g 24hourly for 7-10days
OR
S: piperacillin + tazobactam (IV) 4.5gm 6-8hourly 7-10days (for severe/complicated cases)
OR
S: meropenem (IV) 1gm 8hourly 7-10days
AND
B: metronidazole (IV) 500mg 8hourly for 7-10days

Note
• Abscesses >4 cm should be drained percutaneously or surgically.
• Surgery: if progressions despite medical treatment, undrainable abscess, free perforation.
• After source control, 4days antibiotics may be enough.
• Resection for recurrent bouts of diverticulitis on a case-by-case basis.

10.3.7 Polyps and Adenomas


Accumulation of mutations in colonic epithelial cell DNA affecting oncogenes and tumor suppressor
genes which leads to tumor initiation (formation of adenoma) tumor progression (adenoma to
carcinoma).
Neoplastic polyps: adenomas (tubular, villous, tubulovillous dysplasia), sessile serrated
adenomas/polyps (concern for interval CRC), carcinomas.
Non-neoplastic polyps: hyperplastic, juvenile, Peutz-Jeghers, inflammatory.

Investigations
Colonoscopy is gold standard

Note
• Colonoscopy in all patients starting at age 50 years, then typically every 10years unless
pathology found.
• If positive family history, start age 40, or 10 years before age of diagnosis in youngest
family member, repeat every 5 years.

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10.3.8 Hemorrhoids
Hemorrhoid disease is due to enlargement or thrombosis of the veins in the external or internal
hemorrhoidal plexus.

Clinical presentation
• Painless anal rectal piles • Pruritus
• Painless bleeding –post defecation • Prolapse
• Pain

Investigations
• Endoscopy (Anoscopy, or proctosigmoidoscopy) for evidence of characteristic anal recta
piles.

Treatment
• Depends on severity of the disease
• Grade I hemorrhoids are treated with conservative medical therapy and avoidance of
nonsteroidal anti-inflammatory drugs (NSAIDs) and spicy or fatty foods
• Grade II or III hemorrhoids are initially treated with nonsurgical procedures
(sclerotherapy, band ligation
• Very symptomatic grade III and grade IV hemorrhoids are best treated with surgical
hemorrhoidectomy

Pharmacological Treatment
A: benzyl benzoate 1.25%, bismuth oxide 0.875%, bismuth subgallate 2.25%,
hydrocortisone acetate 0.25%, Peru balsam 1.875%, zinc oxide 10.75% (PR) suppository
one or twice a day
OR
S: (Euphobia prostrate extract 100mg + Calcium dobesilate 500mg) (PO) 24hourly
(chewable do not swallow)
AND
S: (Prednisolone hexanoate 1.3mg +Cinchocaine hydrochloride 1mg) Suppository
24hourly 5-7days

10.3.9 Anal Fissures


These are painful linear ulcers in the anal canal. Young and middle-aged adults most affected.
Primary fissure occurs in the posterior midline. It can also be secondary to Crohn’s disease, anal
cancer, or infection such as syphilis, TB in which case they occur more lateral. Passage of hard
stools is a common predisposition to primary fissures.

Clinical presentation
• Severe sharp pain during and after defecation with/out bright red bleeding.

Investigations
• Evidence of linear anal rectal ulceration on proctoscopy examination
Non-Pharmacological Treatment
• Ensure high fluid intake

Pharmacological Treatment
• Topical anesthetics and frequent seat baths can reduce sphincter spasm (should be
offered before surgery)
• Use non stimulant osmotic laxatives

Surgery: Surgical sphincterotomy is definitive treatment.

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10.3.10 Fistula in Ano
Is a chronic abnormal communication lined by degree of granulation tissues which runs outward
from mucosal lumen.

Risk factors
• Previous perianal abscess formation
• Chhorn’s disease
• Diabetes mellitus
• Tuberculosis
• Trauma
• Radiotherapy
• Immunosuppression-HIV, malignancy

Classifications of fistula in ano


I. Intersphincteric III. Transphincteric
II. Suprasphincteric IV. Extra sphincteric

Clinical presentation
• Purulent or bloody discharges
• Pruritis ani
• History of anorectal abscess

Investigations
• Fistulography • Fistulotomy, Fistulectomy, Seton,
• Endoanal USS Fibrin glue, anal fistula plug,
• Pelvic MRI-gold standard Advancement flap
• Surgical Treatment options

10.3.11 Appendicitis
This is characterised by inflammation of the appendix, and usually requires urgent surgical
intervention.

Clinical presentation
• Sudden peri-umbilical pain often • Bloated abdomen.
migrating to the right iliac fossa. • Rebound tenderness
• Nausea and vomiting • guarding and rigidity.
• Loss of appetite • Right iliac fossa tenderness.
• Fever • Right iliac fossa rebound pain.
• Constipation or occasionally • Severe persistent abdominal pain.
diarrhea.

Investigations
• FBP • Lipase/amylase excludes
• Urinalysis pancreatitis
• Pregnancy test in females • Abdominal USS
• LFT • CT scan

Complications
• Perforation/peritonitis • Appendicular mass
• Appendicular abscess

Pharmacological management
B: ceftriaxone (IV) 1g 12hourly for 5-7days
AND
B: metronidazole (IV) 500mg 8hourly for 5-7days
AND
A: diclofenac (IM) 75mg 8hourly for 3days

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10.4 Pancreatitis
Pancreatitis is an inflammatory process in which pancreatic enzymes auto digest the pancreatic
gland leading to functional and morphologic loss of the gland.

10.4.1 Acute Pancreatitis


It is due to sudden inflammation of the pancreas due to pancreatic enzymes auto digestion.
Common risk factors which trigger the acute episode are presence of gallstones and alcohol intake.

Clinical presentation
• Severe, unremitting epigastric pain, • Local complications: inflammatory
radiating to the back mass, obstructive jaundice, gastric
• Nausea and vomiting outlet obstruction
• Signs of shock may be present • Systemic complication: sepsis,
• Ileus is also common acute respiratory distress
syndrome, acute renal failure

Investigations
• Raised Serum levels for lipase and amylase greater than 3 times the upper limit of normal
ULN (Lipase is more specific and sensitive than amylase). And,
• Radiological (ultrasound, CT, MRI) evidence of inflamed and/or necrotizing pancreatitis.

Treatment
• Principles of management include supportive therapies.
• Intravascular volume expansion (colloids/crystalloid)
• Opiates analgesia usually required (follow WHO analgesic ladder)
• Enteral feeding, (only in absence of illeus) start within 72 hours
• Correction of electrolytes and metabolic deficit accordingly

Pharmacological Treatment
B: ceftriaxone (IV) 1g 12hourly for 7days
OR
C: ciprofloxacin (IV) 200-400mg 12hourly for 7days
AND
B: metronidazole (IV) 500mg 8hourly for 7days
OR
S: meropenem (IV) 1g 8hourly for 7days

Note
• Fever can be because of pancreatitis itself; antibiotics should be avoided before 7 days.
Pancreatic necrosis: Nonviable pancreatic tissue. CT-guided FNA if infection suspected.
Sterile necrosis: if asymptomatic, can be managed expectantly, no role for prophylactic
antibiotics.
Infected necrosis: high mortality. Treat with carbapenem or metronidazole plus
fluoroquinolone
• If stable, defer drainage to >4 weeks. If symptomatic or unstable, percutaneous drainage
and minimally invasive surgical debridement or endoscopic necrosectomy superior to open
necrosectomy. ERCP + Sphincterotomy may be needed.

10.4.2 Chronic Pancreatitis


Chronic pancreatitis is long-term (chronic) inflammation of the pancreas that leads to permanent loss
of function and morphology of the gland.

Clinical presentation
• Chronic upper abdominal pain associated with nausea, vomiting and loss of appetite.
• Malabsorption diarrhoea (exocrine pancreatic insufficiency (steatorrhea))

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• Recurrent attacks of pancreatitis weight loss
• Diabetes

Investigations
• Radiological (Abdominal Ultrasonography/CT scan) evidence pancreatic calcification and
atrophy.

Pharmacological Treatment
Supportive therapies with analgesics in the following order;

A: paracetamol (PO) 1g 8hourly daily when required


OR
B: tramadol (PO) 50mg 12hourly when required for chronic pain relief.
OR
C: morphine (PO) 5-10mls 6hourly when required

If pain unresponsive to above medications


ADD
A: amitriptyline (PO) 25mg nocte when required for pain control
OR
D: pregabalin (PO) 75mg once daily when required for pain relief

Manage complications
Pancreatic enzymes deficiency and steatorrhea
S: pancreatic (PO) 1–3tablet 24hourly to supplement digestive enzyme and improve food
absorption.

Diabetes mellitus
Refer to metabolic and endocrine disease conditions chapter

Note
• In patients with persistent or refractory pain look for a dilated pancreatic duct and
intraductal calcifications. These patients may benefit from endoscopic stenting, lithotripsy,
or surgical drainage (pancreatojejunostomy).

10.4 Disorders of The Liver and Biliary Tract


10.4.1 Hepatitis
This is the term referring to inflammation of the liver, which may result from various causes, both
infectious (i.e. viral, bacterial, fungal, and parasitic organisms) and non-infectious e.g. alcohol,
drugs, autoimmune and metabolic diseases; this section focuses on viral hepatitis and its sequels.

10.4.1.1 Viral Hepatitis


It is a systemic infection predominantly affecting the liver caused hepatotropic viral agents namely
Hepatitis A virus (HAV), Hepatitis B virus (HBV), Hepatitis C virus (HCV), HBV – associated delta
agent or Hepatitis D virus (HDV), and Hepatitis E virus (HEV); in most cases leads to a self-limiting
disease but can take a fulminant course and lead to hepatic failure or progress to chronic liver
disease (HBV, HBV-HDV and HCV)

Note
For comprehensive management of viral hepatitis refer to the National Guidelines for Prevention and
Management of Viral Hepatitis 2020.

Hepatitis A Virus (HAV)


HAV is the RNA virus from piconaviridae family under genus hepatovirus. It primarily infects the
liver. The disease occurs sporadically or in epidemics and has an incubation period of 14- 28 days.
The group most affected is aged between 5-14 years and adults are often infected by spread from
children.

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Clinical presentation
Mild flulike symptoms of anorexia, nausea and vomiting, fatigue, malaise, low-grade fever (usually <
39.5°C), myalgia, and mild headache, dark urine appears first (bilirubinuria). Pale stool soon follows;
Jaundice occurs in most adults. Abdominal pain itching (pruritus), Arthralgias and skin rash, (less
frequent than the above symptoms).

Investigations
Specific diagnosis involves serological detection of Hepatitis A specific immunoglobulins IgM or IgG
antibodies in blood for acute and resolved infection respectively. Viral RNA detection through PCR
is definitive and confirmatory specialized laboratory test. Other tests include FBP, LFT, RFT and
tests for other viral hepatitis viruses (HBV±HDV, HCV, and HEV).

Treatment
• Supportive management such as hydration, adequate feeding and avoidance of
concomitant use of hepatotoxic medications including herbals is all that is required in mild
infections. The disease resolves spontaneously in several weeks or months.
• Hospitalization is necessary in settings of acute liver failure. Therapy is aimed at
maintaining fluid replacement, balanced nutritional feeding, relief of pains and fever
including specific management for liver failure.

Hepatitis B Virus (HBV)


New-onset hepatitis B infection that may or may not be icteric or symptomatic. Diagnosis is based
on detection of hepatitis B surface antigen (HBsAg) and IgM antibodies to hepatitis B core antigen
(anti-HBc). Recovery is accompanied by clearance of HBsAg with seroconversion to anti-HBs
(antibodies to hepatitis B surface antigen), usually within 3 months.

Clinical presentation
• Fever, anorexia, malaise, jaundice and abdominal pain
• Enlarged and tender liver
• Altered consciousness, coma (hepatic encephalopathy), and bleeding stigmata (in
fulminant cases).

Investigations
• Serological evidence of specific viral antigen/ core antibody tests (HBc IgM or HBc IgG);
and biochemical alteration of liver transaminases (ALT, AST).

Treatment of Acute Viral Hepatitis B


• No specific antiviral treatment is required.
• Offer supportive management and counselling.
• Offer a follow up plan at 4 or 6 weeks’ intervals for a clinical and laboratory re assessment
for evidence of symptoms recovery and biochemical remission.
• Re-test at 6 months to assess seroconversion status or progression to chronicity
Chronic Hepatitis B infection.
Defined as persistence of hepatitis B surface antigen (HBsAg) for six months or more after acute
infection with HBV.

Clinical presentation
• Usually asymptomatic
• Right upper quadrant abdominal pains.
• Fatigue, malaise, anorexia, low grade fever; jaundice is frequent in severe disease.
• Ascites, variceal bleeding, encephalopathy, coagulopathy, and hypersplenism.
• Urticaria, arthritis, vasculitis, polyneuropathy, glomerulonephritis, thyroiditis

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Investigations

• HBsAg, HBsAb, HBeAg, HBeAb, HBV DNA PCR


• LFT, RFT, FBP, HIV,
• Alfa Feto Protein (AFP)
• Colour Doppler ultrasonography or duplex Doppler ultrasonography or real time
ultrasonography.
• CT scan
• Fibroscan (if available)

Treatment of Chronic Hepatitis B infection


Pre Treatment Considerations – Who to Treat:
• Patient in chronic active/ Reactivation phase characterized by elevated liver enzymes ALT
>2X ULN, HBeAg +ve, viral load >20,000.
• ALT > 2X ULN, HBeAg –ve, HBeAb –ve, viral load>2000(mutant strain).
• Patients with evidence of fibrosis development (APRI score >2)/cirrhosis should receive
treatment irrespective of age, and viral loads.
• Adults aged > 30 years with three determinations of persistently abnormal ALT levels
above ULN made at unspecific intervals during 6-12month period with DNA viral load >
20,000 IU/ml irrespective of HBeAg status.
• Patients co-infected with HIV

Pre Treatment Considerations – Who not treat:


• Treatment should not be given to patients with persistently normal ALT levels and APRI
score < 2 regardless of age and HBeAg status.
• Immunotolerant patients characterized by high viremia with normal liver chemistry, age
less than 30 years old require no treatment. Re assess after 24weeks interval.
• Patient in latent or inactive phase characterized by low viremia, normal liver chemistry with
or without HBeAg sero-conversion requires no treatment. Re assess after 2 weeks’
intervals.

Pharmacological Treatment
(For eligible adults with no contraindications to tenofovir)
A: tenofovir (TDF) (PO) 300mg 24hourly; for at least 48weeks;

Note
• Re-asses at 24 weeks for evidence of biochemical and viral replication remission.
(Normalization of ALT, viral suppression to undetected level and seroconversion to anti-
HBe).
• Offer a consolidated TDF therapy for extended 48 weeks for patients with evidence of
HBeAb sero-conversion and biochemical remission at the end of the first 48 weeks. For
patients still with detectable viral load and or not yet seroconverted to HBeAb, continue
with Tenofovir 300mg daily dose and reassess every 6 to 12 months for HBV DNA,
HBeAg/Ab status
• Absolute Contraindications to Tenofovir in patients aged < 12 Years
OR
S: entecavir in the following groups: Children and adolescents between age 2 to 18 years
weighing between 10kg and 32kg

Adults with renal insufficiency (CrCl<49ml/min

Entecavir dose Considerations


• Children age 2 to 18 years weighing between 10kg and 32kg - 0.5mg (PO) 24hourly
• Adults naive to nucleoside therapy (PO) 0.5mg 24hourly
• Adults with Lamivudine resistance/previous exposure; and decompensated cirrhosis -
1mg (PO)
• Adults with renal insufficiency (CrCl<49ml/min); dose should be adjusted according to
calculated GFR
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A: Tenofovir (PO) 300mg 24hourly for patients who have treatment failure with other
Nucleotides analogues with low resistance barrier (i.e. Lamivudine) OR Interferon based
therapy.

Note
• Lamivudine should not be prioritized due to their low resistance barrier. Interferon based
therapy is not recommended in our setting due to undesirable side effects, route of
administration and high cost.

When to Stop Treatment


• Patient who has been put on Nucleotides analogues therapy without evidence of cirrhosis
or APRI< 2 should be given a follow up plan.
• Patients who are HBeAb sero-converted after 48 weeks of consolidation therapy, with
persistently normal ALT and undetectable DNA levels should stop treatment and
monitored closely
• Patients with evidence of HBsAb sero-conversion after completing consolidated therapy
regardless of their DNA and HBeAg status should stop treatment.
• Treatment in patient with Liver cirrhosis or significant Fibrosis is indefinitely

Monitoring and evaluation of therapeutic response and toxicity.


• HBsAg, HBeAb, HBeAg, HBV DNA, AFP, ALT should be monitored pre, during, and post
treatment patients. PLUS (Fibrosis assessment by APRI scores) at 24/ 48weeks interval
• Renal functions in adults and growth development in children should be monitored
annually for renal toxicity for patient on Tenofovir and Entecavir respectively.
• Abdominal Ultrasound (AUS) and Alpha Feto Protein (AFP) should be done at 24- 48
weeks’ interval for HCC surveillance.

Note
Screening all close contacts is important. All at risk individuals eg. Healthcare workers, men who
have sex with men, patients on hemodialysis, prisoners, children born to mothers with HBV and
patients requiring multiple transfusions, patients with non-B viral hepatitis should be tested for HBV
and vaccinated if found negative for HBsAg and no evidence of natural immunity to HBV.

HBV in Pregnancy
All Infants and Neonates should have mandatory vaccination according to the recommended
National EPI schedule. Neonates born to mothers infected with HBV and HBeAg positive, should
receive at birth dose of hepatitis B immunoglobulin (HBIG) and HBV Vaccine, and then follow up
with EPI program schedule at 6weeks. During pregnancy, prevention of HBV transmission from
mother to childshould follow similar protocols as per adults with HBV infection.HBsAg positive
pregnant mothers with VL >200,000 IU/ml should receive TDF at 3rd trimester until 6months post-
natal period.

Pharmacological Treatment
• First dose for the infant: Hepatitis B vaccine born to HBsAg-negative mothers
• Medically stable infants weighing ≥2,000 grams: 0.5 ML (IM) within 24h of birth
• Preterm infants weighing <2,000 g: 0.5 mL (IM) 1 month after birth or at hospital discharge

First dose for the infant: Hepatitis B vaccine born to HBsAg-positive mothers
B: hepatitis B vaccine (HBV) (IM) 0.5 mL within 12hours of birth

205
AND
S: hepatitis B immune globulin (HBIG) (IM) 0.5 mL within 12hours of birth

Note
• Mother's HBsAg status unknown: 0.5 mL IM within 12 hour of birth AND HBIG 0.5ml(IM); if
newborn wt <2 kg, determine mother's HBsAg status as soon as possible and, if she is
HBsAg-positive, also administer HBIG for infants weighing 2 kg or more (no later than age
1 week)

For the HBV positive pregnant mother


A: tenofovir (PO) 300mg 24hourly (from third trimester to 6 months post-delivery for the
mother)

Post exposure prophylaxis (PEP)


HBIG and HBV vaccine should be given to individuals who are HBsAg negative exposed to HBsAg
positive focus within 24hours followed by active standard schedule to complete 3 doses.
S: hepatitis B immune globulin (HBIG) (IM) 0.06 mL/kg once
AND
B: hepatitis B vaccine (HBV) (IM) 1 mL (20 mcg) at 0, 1, and 6months

Note:
• HBIG and HBV Vaccine should be given at different intramuscular sites PEP should be
given in <24hours, may not be effective after 72hours of exposure.

10.4.2.3 Hepatitis C virus (HCV)


Hepatitis C virus (HCV) is a small enveloped RNA virus and a member of the family Flaviviridae.
HCV comprises six genotypes and hundreds of subtypes with variable geographical distribution and
bears significance in determining the rate of liver disease progression, development of HCC and
specific therapeutic responses.

Clinical presentation
• Initial symptoms of HCV are often • Myalgias,
extrahepatic, most commonly • Pruritus,
involving the joints, muscle, and • Sicca syndrome.
skin. • Sensory neuropathy
• Arthralgias,
• Paresthesias,

Symptoms characteristic of complications from advanced or decompensated liver disease are


related to synthetic dysfunction and portal hypertension, such as the following:
• Mental status changes (hepatic encephalopathy), Ankle edema and abdominal distention
(ascites), Hematemesis or melena (variceal bleeding)
Signs in patients with decompensated liver disease include the following:
• Hand signs: Palmar erythema, Dupuytren contracture, asterixis, leukonychia, clubbing
• Head signs: Icteric sclera, temporal muscle wasting, enlarged parotid gland, cyanosis
• Fetor hepaticus, Gynecomastia, small testes
• Abdominal signs: Paraumbilical hernia, ascites, caput medusae, hepatosplenomegaly,
abdominal bruit, Ankle edema, Scant body hair, Skin signs: Spider nevi, petechiae,
excoriations due to pruritus
Other common extrahepatic manifestations include the following:
• Cryoglobulinemia, Membranoproliferative glomerulonephritis, Idiopathic thrombocytopenic
purpura, Lichen planus, Keratoconjunctivitis sicca, Raynaud syndrome, Sjögren syndrome
• Porphyria cutanea tarda, Necrotizing cutaneous vasculitis

206
Investigations
General baseline studies in patients with suspected HCV include the following:
• FBP, LFT, RFT TSH, T3
• Screening tests for coinfection with HIV or HBV
• Screening for alcohol abuse, drug abuse, or depression
• Pregnancy testing
Tests for detecting HCV infection include the following:
• Hepatitis C antibody testing:
• Qualitative and quantitative assays for HCV RNA PCR
• HCV genotyping
• Serologic testing (essential mixed cryoglobulinemia is a common finding)

Treatment
Use pangenotypic drugs which are efficacious, safe and cost-effective.
Who to treat
• Confirmed cases of Hepatitis C irrespective of clinical stage of the liver disease
• Patients with HCC who are eligible for liver transplant if feasible.
• Liver transplant patients if MELD score is < 18 (pre transplant) or >18 (post-transplant)
Who not to treat
• HCC patients who are not eligible for liver transplant.
• Patient with limited life expectancy due to ESLD (by MELD score or Child-Pugh), or non-
hepatic related comorbidities.

Pharmacological Treatment
All individuals diagnosed with HCV infection who are ≥ 12 years old are eligible for treatment
children (<12 years old), the treatment should be deferred until they reach that age.
S: ledipasvir (PO) 90mg 24hourly for 12-24weeks
AND
S: sofosbuvir (PO) 400mg 24hourly for 12-24weeks
AND
S: ribavirin (PO) given in two divided doses *<75kg of Body weight =1g/day; >75Kg of
Body weight =1.2g/day for 12weeks (in treatment naive patients) OR for 24 weeks (in
treatment experienced patients) for genotypes 1, 4, 5 & 6.
OR
S: sofosbuvir (PO) 400mg daily AND ledipasvir (PO) 90mg daily AND ribavirin if a patient
has been previously exposed to other antivirals.

Note
• Due to complexity and variability of HCV management, care and treatment should be done
at the tertiary level facility
• Ribavirin is contraindicated in patients with anaemia (HB<8.5g/dL), and the dose should be
reduced if HB <10g/dL
Sofosbuvir is contraindicated if eGFR < 30ml/min/1.73m2

When to stop medications


• Ribavirin regimen should be stopped if patients’ HB drops to < 8.5g/dl during follow up
schedules.
• If there’s adverse drug reaction
• When there are ALT flares or massively increased ALT (>10 X UNL)
• If there’s evidence of drug to drug interactions- consider switching with medication with a
less interacting potential

207
Clinical monitoring and follow up
• Assess treatment adherence, tolerance and toxicity at 4 weeks after treatment initiation.
• Treatment toxicity
• Stop Ribavirin if HB drops to <8.5
• Stop all DAAs if ALT >10 X ULN and other causes have been ruled out
• Stop Sofosbuvir if eGFR drops to < 30ml/min/1.73m2

10.4.2.4 Hepatitis D Virus


Hepatitis D virus (HDV) is a defective RNA virus belonging to genus of delta virus that requires the
helper function of Hepatitis B (HBV) for virion assembly, release and transmission, and therefore the
infection does not occur in the absence of hepatitis B virus. The routes of HDV transmission are
similar for HBV the most important being sexually, percutaneous or parenteral exposure to blood or
blood products.

Investigations
Serology assays for HDV immunoglobulin titres for IgM and IgG are diagnostic for acute and post
exposure/chronic infections respectively. Real time PCR for HDV RNA is confirmatory.

Treatment
There is no specific treatment for acute or chronic HDV infection.

Note
The more risk population includes health care workers, transfusion recipients and haemophiliacs,
PWID, and immigrants of endemic areas. Nucleotide sequences of HDV obtained worldwide
indicates the existence of eight genotypes, with genotype 1 being detected worldwide. HDV
Antiviral nucleotide analogues for HBV have no or limited effect on HDV replication and Pegylated
interferon alpha is the only drug effective against HDV now and more than one year of therapy may
be necessary as most of patients relapses after discontinuation of therapy.

10.4.2.5 Hepatitis E Virus


Hepatitis E virus (HEV) belongs is a RNA virus belonging from a family Hepadna viridae under
Genus Hepevirus and acute liver infection. The virus has at least 4 different types: genotypes 1, 2, 3
and 4. Genotypes 1 and 2 have been found only in humans. Genotype 3 and 4 viruses circulate in
several animals (including pigs, wild boars, and deer) without causing any disease, and occasionally
infect humans.

Clinical presentation
Prodromal-phase symptoms include the following:
• Myalgia, Arthralgia, Fever with mild temperature elevations
• Anorexia, Nausea/vomiting, Weight loss. Dehydration, Right upper quadrant pain
Icteric-phase symptoms may last days to several weeks and include the following:
• Jaundice, Dark urine, Light-colored stool, Pruritus
Other features include the following
• Malaise (most common), Arthritis, Pancreatitis
• Aplastic anemia, Thrombocytopenia
• Neurologic symptoms of polyradiculopathy, Guillain–Barré syndrome, Bell palsy, peripheral
neuropathy, ataxia, and mental confusion
• Membranoproliferative glomerulonephritis and membranous glomerulonephritis

Investigations
Serology assays for HEV immunoglobulin titres for IgM and IgG are diagnostic for acute and post
exposure/chronic infections respectively. Real time PCR for HEV RNA in serum and particularly in
stool is confirmatory.

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Treatment
There is no specific treatment for cure or reversing the course of acute hepatitis E. The disease is
usually self-limiting; hospitalization is generally not required except for patients with fulminant
hepatitis or for symptomatic pregnant women where severity of infection is usually high and
associated with high rates of fetal loss and mortality especially in third trimester.
Note
• The virus is shed in the stools of infected persons and enters the human body through the
intestine. It is transmitted mainly through contaminated drinking water. Usually the infection
is self-limiting and resolves within 2–6 weeks. Rarely the infection can lead to fulminant
hepatitis with acute liver failure.
• The virus causes sporadic cases and major epidemics of viral hepatitis and occurs in
resource poor population with unhygienic conditions and through ingestion of
contaminated water and food.

10.4.2 Portal Hypertension


This is high blood pressure in the hepatic portal system which includes the portal veins and its
branches which drains from most of the intestines to the liver. It is indicated when the hepatic
venous pressure gradient exceeds 7mmHg, while liver cirrhosis remains the most common cause
which in our local setting is commonly caused by chronic viral hepatitis followed by heavy alcohol
intake.

Clinical presentation
• Ascites, Splenomegaly
• Esophageal varices, and hematemesis
• Swollen veins of the anterior abdomen (caput medusa) and hemorrhoids

Investigations
• Radiological evidence of shrunken liver, with typical features of cirrhosis.

10.4.2.1 Ascites
Ascites is the pathologic accumulation of fluid in the peritoneal cavity, and its most common cause is
cirrhosis.

Pharmacological Treatment
C: spironolactone (PO) 50mg – 400mg 24hourly incrementally till ascites resolves
OR
S: eplerenone (PO) 50mg 24hourly
AND
B: furosemide (PO) 40mg–160 mg 24hourly or in divided doses incrementally till ascites
resolves
AND
A: propranolol (PO) 40mg–160mg 12hourly daily incrementally target heart rate 55-60bpm.

OR
C: carvedilol (PO) 6.25mg 24hourly, increase to 6.25mg (PO) 12hourly unless persistent
arterial hypertension, SBP should not decrease <90mmHg.
AND
S: albumin 25% (IV) – in refractory ascites and large volume paracentesis. Give 25g stat,
repeat at 15–30min Interval at Max Dose of 250g/48hourly

Note
• Consider discounting βB if SBP <90 or MAP ≤82 mmHg, serum Na <120 mEq/L, AKI,
HRS, SBP, sepsis, severe alcoholic hepatitis, poor follow-up.
• Large-volume paracenteses (LVP; >5 L fluid removal): give 6–8g albumin per L fluid
removed (above 5 L) as colloid replacement is associated with decreased risk of post-
paracentesis circulatory dysfunction and possibly decreased mortality.

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10.4.2.2 Spontaneous Bacterial Peritonitis
Spontaneous bacterial peritonitis is an acute bacterial infection of ascitic fluid in the absence of a
contagious cause of infection (e.g., intestinal perforation or abscess)

Clinical presentation
• Fever and chills • Ascites that does not improve
• Abdominal pain or discomfort following administration of diuretic
• Worsening or unexplained medication
encephalopathy • Worsening or new-onset renal
• Diarrhea failure
• Ileus
Investigations
Diagnosis of Spontaneous bacterial peritonitis is based on the demonstration of an absolute number
of polymorphonuclear cells in ascitic fluid equal to or greater than 250/mm3

Pharmacological treatment

Community Acquired Spontaneous bacterial peritonitis


B: ceftriaxone (IV) 1g 12-24 hourly for 5- 10days
OR
B: amoxicillin-clavulanic acid (FDC) (IV) 1-2g 6-8hours for 5-10days
OR
C: ciprofloxacin (IV) 200mg 12hourly for 5–10days
AND
S: administration of albumin dose is 1.5 g/kg on day 1 and 1 g/kg on day 3

Nosocomial Spontaneous bacterial peritonitis Treatment


S: meropenem (IV) 1gm 8hourly for 5-7days

Spontaneous bacterial peritonitis prophylaxis


Prophylaxis should be continuous until the disappearance of ascites (i.e., patients with alcoholic
hepatitis), death, or transplant.
A: ciprofloxacin (PO) 400mg 24hourly for 10-14days
OR
A: co-trimoxazole (PO) 960mg 24hourly for 10-14days

10.4.2.3 Bleeding Esophageal Varices


Esophageal varices are collateral veins within the wall of the esophagus that project directly into the
lumen. Acute variceal bleeding is a fatal complication in patients with liver cirrhosis. In patients with
decompensated liver cirrhosis accompanied by ascites or hepatic encephalopathy, acute variceal
bleeding is associated with a high mortality rate.

Pharmacological Treatment
S: octreotide (SC) 50–100µg 8hourly for 3days (infusion 50µg/hour for 72hours up to
5days)
OR
S: terlipressin: Adult (body weight up to 50 kg): Initially 2 mg every 4 hours until bleeding
controlled, then reduced to 1 mg every 4 hours if required, maximum duration 48 hours.
Adult (body weight 50 kg and above): Initially 2 mg every 4 hours until bleeding controlled,
reduced if not tolerated to 1 mg every 4 hours, maximum duration 48 hours
AND
Band ligation of beeding esophageal varices (EVL); 3 – 6 shoots per session.
OR
Sclerotherapy (Histo Acryl Glue Inj. 5 %;( mixed with Lipiodol at a ratio 1:1) Ethanolamine oleate
5%); given 2 -5ml per varix up to 20ml per session.

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AND
B: ceftriaxone (IV) 1g 24hourly for 7days

Note
Blood transfusion (PRBC, PLT concentrates and FFP) when required.

10.4.2.4 Hepatic Encephalopathy (HE)


Hepatic encephalopathy (HE) is defined as “a condition which reflects a spectrum of
neuropsychiatric abnormalities seen in patients with liver dysfunction after exclusion of other known
brain disease.”

Clinical presentation
Stage Symptoms
I Mild confusion, agitation, irritability, sleep disturbance, decreased attention
II Lethargy, disorientation, inappropriate behavior, drowsiness
III Somnolent but arousable, slurred speech, confused, aggressive
IV Coma

Pharmacological Treatment
S: L-Ornithine L-Aspartate (IV) 10g 8hourly daily for 3-5days
THEN
S: L-Ornithine L-Aspartate (PO) 9g 24hourly in divided doses for 4–12weeks
AND
C: lactulose solution (PO) for bowel cleansing when required

Episode of HE (grade 2 or higher)—enemas:


A: 0.9% sodium chloride 300mL in 1000mL water 2hourly until there is clinical
improvement
Episode of HE (able to tolerate oral administration)—(PO): 45mL every hour until there is bowel
movement and clinical improvement
Outpatient therapy: 15-45mL 8-12hourly until there are 2-3 bowel movements per day
AND
A: metronidazole (PO) 400mg 8 hourly for 7days
AND
B: ceftriaxone (IV) 1g 12 hourly for 7days (if evidence of spontaneous bacterial peritonitis)

Fluid deficit correction and electrolytes replacements as appropriate (screen for and correct all
precipitants of HE as shown in the table below).

Table 10.2: Precipitants of HE


Hyponatremia Vomiting
Gastrointestinal bleeding Diarrhea
Infection Sedative drugs (narcotics, sleep aids,
antihistaminics)
Surgery Alkalosis
Dehydration Azotemia
Fluid restriction Hypokalemia
Diuretics Excessive protein intake
Excessive paracentesis Constipation

10.4.2.5 Hepatorenal Syndrome


Hepatorenal syndrome (HRS) is the development of renal failure in patients with advanced chronic
liver disease and, occasionally, fulminant hepatitis, who have portal hypertension and ascites.

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Table 10.3: Pharmacological treatment
Vasoconstrictor Recommended Dosage
S: terlipressin Bolus Initially 0.5 mg (IV) 4-6hourly. If no response by day
3 can increase the dosage to 1mg 4-6hourly.
Maximum dosage is 2mg 4-6hourly. Maximum
OR duration 14days.
Continuous Initially 2mg/day. If no response by Day 3, can
infusion increase the dosage to 4mg/day. Maximum dosage
is 12mg/day. Maximum duration 14days.
S: norepinephrine Continuous 0.5-3mg/hour continuously to achieve an increase in
infusion mean arterial pressure of 10 mmHg. Treatment is to
be continued until serum creatinine concentration is
< 1.5mg/dL, or < 133µmol/L.
S: Albumin must be given concomitantly with any of the vasoconstrictors at a dosage of 20-40
g/day.

10.4.3 Biliary Tract Diseases


Cholestasis is a pathologic state of reduced bile formation or flow which can be hepatocellular
(Intrahepatic), where an impairment of bile formation occurs or ductular (extra hepatic), where
impedance to bile flow occurs after it is formed. Intrahepatic causes of cholestasis include viral
hepatitis, alcohol, primary biliary cirrhosis, drug toxicity, Hodgkin’s lymphoma and pregnancy.
Extrahepatic causes include choledocholithiasis, carcinoma, and ascariasis of the biliary tree.

Clinical presentation
• Jaundice,
• Dark urine,
• Pale stools, and
• Generalized body itching/pruritis.

Investigations
• Laboratory evidence of elevated serum levels of total bilirubin, direct bilirubin, alkaline
phosphatase, gamma-glutamyl transferase, and transaminases. WITH
• Supporting radiological evidence of dilated intra or extra hepatic biliary radicles.

Pharmacological Treatment
Definitive treatment:
Identify and treat specific cause

Supportive treatment:
S: cholestyramine (PO) 4–16g/day
OR
S: ursodeoxycholic acid (PO) 20–30 mg/kg/day

Note
• Surgical intervention is indicated for extra hepatic cholestasis.

10.4.3.1 Cholelithiasis
Cholelithiasis involves the presence of gallstones which are concretions that form in the biliary tract,
usually in the gallbladder. Choledocholithiasis refers to the presence of one or more gallstones in
the common bile duct (CBD). Treatment of gallstones depends on the stage of disease.

Clinical presentation
• Asymptomatic in majority of patients.
• Biliary pain (episodic RUQ or epigastric pain), pain radiating to scapula;
• Pain precipitated by fatty foods; nausea

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• Physical exam: afebrile, and/or RUQ tenderness or epigastric pain
• Nonspecific symptoms (eg, indigestion, dyspepsia, belching, or bloating)

Investigations
• Full Blood count
• Liver function panel
• Pancreatic enzymes (Amylase, Lipase)
• Abdominal radiography (upright and supine) – to exclude other causes of abdominal pain
• Ultrasonography
• CT scan –superior for demonstrating stones in the distal CBD
• MRI with MRCP
• Scintigraphy (HIDA) scans
• Endoscopic retrograde cholangiopancreatography (ERCP)
• Percutaneous transhepatic cholangiography (PTC)

Complications
• Cholecystitis
• Choledocholithiasis leading to cholangitis or gallstone pancreatitis
• Mirizzi syndrome
• Cholecystenteric fistula stone erodes through gallbladder into bowel
• Gallstone ileus: SBO (usually at term ileum) due to stone in intestine that passed through
fistula
• Gallbladder carcinoma

Non-pharmacological Treatment
• Asymptomatic gallstones – Expectant management
• Symptomatic gallstones – definitive surgical intervention (cholecystectomy)

Pharmacological Treatment
A: paracetamol (PO) 1g 8hourly for 5days
OR
A: ibuprofen (PO) 400mg 4-6hourly for 3-5days
OR
B: tramadol (PO) 50mg 12hourly for 3-5days
AND
S: ursodeoxycholic acid 8-10mg/kg/day divided once to three times up to 6months

Note
Cholecystectomy (open or laparoscopic) for asymptomatic gallstones may be indicated in the
following:
• Those with large (>2 cm) gallstones
• Nonfunctional or calcified (porcelain) gallbladder on imaging studies and at high risk of
gallbladder carcinoma
• Those with spinal cord injuries or sensory neuropathies affecting the abdomen
• Sickle cell anemia patients- difficult to distinguish between painful crisis and cholecystitis
• Cholecystectomy, Cholecystectomy, Endoscopic sphincterotomy, Extracorporeal
shockwave lithotripsy

10.4.3.2 Choledocholithiasis
Gallstone lodged in common bile duct (CBD). Occurs in some of patients with gallbladder stones;
can form de novo in CBD.

Clinical presentation
• Asymptomatic • Jaundice,
• RUQ pain, • Pruritus,
• Epigastric pain due to obstruction • Nausea.
of bile flow which leads to increase
in CBD pressure,

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Investigations
• LFT, • ERCP, if ERCP unavailable or
• Amylase unsuccessful
• Lipase. EUS/MRCP
• Abdominal (RUQ) Ultrasound

Non-pharmacological Treatment
ERCP & papillotomy w/ stone extraction (± lithotripsy)
Cholecystectomy typically within 6 weeks unless contraindication

Pharmacological Treatment
S: cholestyramine (PO) 4-8g 12hourly when required for itching.

Complications
Cholangitis, cholecystitis, pancreatitis, stricture

10.4.3.3 Cholecystitis
Cholecystitis is inflammation of the gallbladder that occurs most commonly because of an
obstruction of the cystic duct by gallstones (stone impaction in cystic duct leads to inflammation
behind obstruction causing GB swelling and secondary infection of biliary fluid).

Acalculous cholecystitis: Occurs in critically ill. GB stasis and ischemia (without cholelithiasis)
leading to necroinflammation.

Clinical presentation
• RUQ/epigastric pain, radiating to right shoulder/back, nausea, vomiting, fever
• Signs of peritoneal irritation may be present
• Patients with acalculous cholecystitis may present with fever and sepsis alone
• RUQ tenderness, Murphy’s sign, palpable gallbladder, jaundice
• The absence of physical findings does not rule out the diagnosis of cholecystitis.

Investigations
• FBP, LFT, amylase, lipase
• Ultrasonography RUQ ultrasound: high Sensitivity and specificity for stones but need
specific signs of cholecystitis: GB wall thickening >4 mm, pericholecystic fluid and a
sonographic Murphy’s sign
• Radiography
• Computed tomography (CT)
• Magnetic resonance imaging (MRI)
• Hepatobiliary scintigraphy (HIDA)
• Endoscopic retrograde cholangiopancreatography (ERCP)

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Pharmacological Treatment
In acute cholecystitis, the initial treatment includes bowel rest, IV hydration, and correction of
electrolyte abnormalities

A: paracetamol (PO) 1g 8hourly daily ORD: paracetamol (IV) 1g 8 hourly daily (for
analgesia
AND
C: metoclopramide (IV/PO) 10mg 12hourly daily (for intractable vomiting)
AND
S: piperacillin + tazobactam FDC (IV) 4.5g 6-8 hourly 7-10 days (for severe/complicated
cases)
OR
B: ceftriaxone (IV) 1-2gm 24hourly for 7-10days
OR
C: ciprofloxacin (IV) 200-400mg 12hourly for 7-10days
AND
B: metronidazole (IV) 500mg 8hourly for 7-10days

In cases of uncomplicated cholecystitis, outpatient treatment may be appropriate.


A: ciprofloxacin (PO) 500mg 12hourly for 7days
AND
A: metronidazole (PO) 400mg 12hourly for 7days

Note
• Laparoscopic cholecystectomy (standard of care for surgical treatment of cholecystitis)
others include ERCP.
• Endoscopic ultrasound-guided transmural cholecystostomy, Endoscopic gallbladder
drainage.

10.4.3.4 Cholangitis
Bile duct (BD) obstruction leads to infection proximal to the obstruction, etiologies include BD stone,
malignant (biliary, pancreatic) or benign stricture, infection with fluke (Clonorchis sinensis,
Opisthorchis viverrini)

Clinical presentations
• Charcot’s triad: RUQ pains, jaundice, fever/chills; present in three quarter of patients
• Reynolds’ pentad: Charcot’s triad + shock and altered mental status; present in 15% of
patients

Investigations
• Ultrasound, RUQ USS often demonstrates dilation
• FBP, LFT, amylase, lipase
• Blood cultures
• ERCP; percutaneous transhepatic cholangiogram if ERCP unsuccessful

Pharmacologic Treatment
B: ceftriaxone (IV) 1-2g 24hourly for 7-10days
OR
S: piperacillin+tazobactam FDC (IV) 4.5g 6-8hourly for 7-10days (for severe/complicated
cases)
OR
S: meropenem (IV) 1g 8 hourly for 7-10days
AND
C: metronidazole (IV) 500mg 8hourly for 7-10days
Alternatively
C: ciprofloxacin (IV) 200-400mg 12hourly for 7-10days
AND
B: metronidazole (IV) 500mg 8hourly for 7-10days

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Note
• About 80% respond to conservative treatment and antibiotics then, 20% require urgent
biliary decompression via ERCP (papillotomy, stone extraction and/or stent insertion)
• If sphincterotomy cannot be performed (larger stones), decompression by biliary stent or
nasobiliary catheter can be done; otherwise, percutaneous trans hepatic biliary drainage or
surgery

216
CHAPTER ELEVEN
OBSTETRICS, GYNECOLOGY AND CONTRACEPTION
11.1 Bleeding in Pregnancy
Bleeding during pregnancy is common, especially during the first trimester. Bleeding can sometimes
be a sign of something serious, therefore it is important to know the possible causes and take
adequate measures.
11.1.1 Abortion
It is a spontaneous loss of a fetus before it is viable (has the potential to survive outside the womb).
The World Health Organization (WHO) defines it as expulsion or extraction of an embryo or fetus
weighing 500mg or less, approximately at or less than 24 weeks of gestation. In Tanzania abortion
is defined as loss of pregnancy before 28 weeks of gestations. Clinical features will depend on the
types of abortion.

11.1.1.1 Threatened Abortion


Clinical presentation
• Mild vaginal bleeding
• Mild/no lower abdominal pain
• Cervix is closed on digital examination

Investigation
Check Hb level

Management of threatened abortion in Dispensary & Health Centre


• Adequate bed rest at home
• Avoid strenuous activities and sexual intercourse until all the symptoms have subsided
• Schedule a follow up within 7 days
• Tell the woman to come immediately if;
o Bleeding becomes heavy
o Experiences offensive discharge
o Severe abdominal pain

Referral
Refer to higher-level health facility with adequate expertise and diagnostics if:
• Bleeding recurs
• Experiences fever
• Experiences offensive discharge
• Experience severe abdominal pain

In higher level health facilities:


• Take thorough history and perform investigations to establish the causes
• Perform ultrasound to confirm pregnancy, gestational age, foetal viability and potential
causes of abortion.
• Admit the patient and manage appropriately
• Encourage bed rest
• For unexplained recurrent miscarriage (3 consecutive abortions) or PRL due to luteal
phase defect manage with

Pharmacological Treatment
S: dydrogesterone (PO) 40mg stat then 10mg 24hourly until the bleeding stops for
threatening abortion
OR 10mg 24hourly from conception up to 20weeks for luteal phase defect.

11.1.1. 2 Inevitable Abortion


Abortion is said to be inevitable when it is not possible for the pregnancy to continue and the cervix
is dilated, but all the products of conception are in situ.

Clinical presentation
• Moderate or severe per vaginal bleeding
• Moderate or severe lower abdominal pain

217
• Membranes may be intact or ruptured with leakage of
• The uterine fundal height may correspond with gestational age
• The cervix is dilated

Management of inevitable abortion in Dispensary & Health Centre (B-EMONC facilities)


• Apply Airway, Breathing, Circulation and Dehydration (ABCD) principles of resuscitation

A: compound sodium lactate (IV) OR 0.9% sodium chloride (IV) depending of amount of blood
loss.
• Perform Manual Vacuum Aspiration (MVA) if gestation age is below 12 weeks
Augment the process by administering A: oxytocin 20 IU in 500mls RL/NS at 40–60
drops/minute if gestation age is above 12 weeks
• Manage as incomplete abortion if after augmentation some products of conception remain
in the uterus
• Manage as complete abortion if all products of conception are expelled

Referral: Refer to hospital if MVA is not possible and/or bleeding is persisting or severe to
necessitate blood transfusion.

Management of inevitable Abortion in the Hospital


• Apply Airway, Breathing, Circulation and Dehydration principles of resuscitation
• Obtain blood samples for Hb, grouping and cross–matching
• Give compound sodium lactate (IV)OR 0.9% sodium chloride aim at replacing 3 times the
amount of estimated blood loss.
• Give blood transfusion if indicated
• Perform Manual Vacuum Aspiration (MVA) if gestation age is below 12 weeks
• Augment the process by administering oxytocin 20IU in 500mls RL/NS at 40–60
drops/minute if gestation age is above 12 weeks
• Manage as incomplete abortion if after augmentation some products of conception remain
in the uterus
• Manage as complete abortion if all products of conception are expelled

11.1.1.3 Incomplete Abortion


Abortion is said to be incomplete when after expulsion some of the products of conception get
retained in the uterine cavity.

Clinical presentation
• Severe Cramping lower abdominal pain
• moderate to severe PV bleeding
• Fundus smaller than dates
• The cervix is dilated and products of conception may be felt on or through the cervix on
digital examination

Management of incomplete abortion in dispensary & health centre (B-EMONC facilities)


• Apply Airway, Breathing, Circulation and Dehydration principles of resuscitation
• Check hemoglobin level
A: compound sodium lactate (IV) OR 0.9% sodium chloride depending on amount of blood
loss
• If feasible Perform digital evacuation of products of conception to miminize the PV bleeding
• Perform MVA if gestation age is below 12 weeks

Pharmacological treatment in place

In place where uterine evacuation is accessible give;


A: oxytocin (IM) 10 IU
OR
A: misoprostol (sublingual) 600µg

After evacuation give:


A: erythromycin (PO) 500mg 8hourly for 5days

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OR
B: amoxicillin + clavulanic acid (FDC) (PO) 625mg 8 hourly for 5days
AND
A: metronidazole (PO) 400mg 8hourly for 5days
AND
A: paracetamol (PO) 1g 8hourly for 5 days

Referral: Resuscitate the patient and to hospital level with an escort of a nurse if bleeding continues

Management in a Hospital
• If patient is in shock, shout for help, mobilize resources
• Apply ABCD principles of resuscitation
• Obtain blood for HB, grouping and cross–matching
• Blood transfusion if indicated
• Give compound sodium lactate (IV) OR 0.9% sodium chloride aim at replacing 3times the
amount of estimated blood loss
• Digital evacuation of products of conception if feasible to minimize the PV bleeding
• MVA if gestation age is below 12 weeks
• Evacuate uterus in theatre with sharp curette under general anesthesia if pregnancy was
more than 12 weeks

Pharmacological Treatment
After evacuation give:
A: erythomycin (PO) 500mg 8hourly for 5days
OR
B: amoxicillin + clavulanic acid (FDC) (PO) 625mg 8hourly for 5 days
AND
A: metronidazole (PO) 400mg 8hourly for 5 days
AND
A: paracetamol (PO) 1g 8hourly for 5days.
AND
A: ferrous sulfate + folic acid (FDC) (PO) 1 tab 24hourly for 4 weeks

Patient education.
• Counsel and educate the patient on possible reasons for abortion and future fertility
• Provide family planning counseling and give appropriate contraceptive method before the
patient leaves the facility premises.
• Provide linkage to other reproductive and non reproductive health services depending on
patient needs

11.1.1.4 Complete Abortion


Abortion is said to be complete when the Products of conception are completely expelled

Clinical presentation
• Minimal or no PV bleeding
• Uterus smaller than dates and often well contracted.
• Cervix may or may not be closed
• The patient may be in Shock due to severe bleeding

Pharmacological Treatment
A: erythromycin (PO) 500mg 8hourly for 5days
OR
B: amoxicillin + clavulanic acid (FDC) (PO) 625mg 8hourly for 5days
AND
A: metronidazole (PO) 400mg 8hourly for 5days
AND
A: ferrous sulfate + folic acid (FDC) (PO) 1 tablet 24hourly for 4weeks

If patient is in shock;
• Shout for help and mobilize resources
• Apply ABCD principles of resuscitation

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• Give compound sodium lactate (IV) OR 0.9%sodium chloride (IV) 3litres or more in the first
hour
• Insert an indwelling urethral catheter
• Give ampicillin (IV) 1g and metronidazole (IV) 500mg stat
• Obtain blood for HB,

Referral: Resuscitate the patient and referto hospital with an escort of a nurse

Management in a hospital
• If patient is stable continue as above;
• If patient is in shock, perform as above and give blood transfusion if indicated

Patient Education
Provide counseling, education and FP services as in incomplete abortion above

11.1.1.5 Septic Abortion


Abortion is said to be septic when It is complicated by infections.
Clinical presentation
• Moderate to severe Abdominal pain following abortion
• Fever may be present
• Foul smelling PV discharge which may be mixed with blood.
• May be in shock
• Tender uterus with or without rebound tenderness
• Cervix is usually open

Management of septic abortion in dispensary & health centre


• Apply ABCD principles of resuscitation
• Give compound sodium lactate (IV) OR sodium chloride (IV) 0.9% in case of hypotension
or shock. Avoid IV fluid in case of chronic anaemia.
• Insert an indwelling urethral catheter
• Obtain blood for Hb or FBC
• Perform Ultrasound if feasible

Pharmacological Treatment
C: amoxycillin + clavulanic acid (FDC) (IV) 1.2g 8hourly for 24-48hours
AND
B: metronidazole (IV) 500mg 8hourly for 24–48hours

Referral: Resuscitate and immediatelyrefer the patient to hospital with an escort of a nurse.

Management in the Hospital:


• Full Blood Count (FBC)
• Draw Blood for culture and susceptibility testing
• Check abdominal pelvic ultrasound as appropriate
• IV RL/NS depending on individual patient needs
• Give blood transfusion if indicated
• Evacuate the uterus with sharp wide curette under general anesthesia

Pharmacological Treatment
Treat as above and when the patient is stable continue with;
B: amoxicillin+ clavulanic acid (FDC) (PO) 625mg 8hourly for 7days
A: metronidazole (PO) 400mg 8hourly for 7days

If no response with the above antibiotics within 3 days; adjust according to culture and sensitivity
results or switch to
D: ceftriaxone + sulbactam (FDC) (IV) 1.5g 12hourly for 5days
AND
B: metronidazole 500mg (IV) 8hourly for 5days
AND
A: ferrous sulfate +folic acid (FDC) (PO) 1tablet daily for 4weeks then reassess.

220

Patient Education
• Counsel educate and provide appropriate contraceptive method.

11.1.1.6 Molar Pregnancy


A molar pregnancy is a gestational trophoblastic disease which grows into a mass in the uterus that
has swollen chorionic villi. These villi grow in clusters that resemble bunches of grapes. Once
diagnosed it should be treated right away.

Clinical presentation
• Vaginal bleeding
• Uterus that is bigger than gestational age.
• Exaggerated pregnancy symptoms (Severe nausea and vomiting)
• Vaginal discharge of tissue that resemble grapes
• Heavy PV bleeding when the mole abort spontaneously

Management of Molar pregnancy at the dispensary and Health centers


• Apply Airway, Breathing, Circulation and Dehydration principles of resuscitation
• Check hemoglobin level
• If the patient is actively bleeding, catheterize, Establish Iv line and Give IV RL/NS 2lts at a
rapid rate

Referral: Resuscitate and refer the patient to higher level facility with a nurse escort for appropriate
management

Management of molar pregnancy at the Hospital


• Apply Airway, Breathing, Circulation and Dehydration principles of resuscitation
• If the patient is patient is actively bleeding or in shock shout for help and mobilize
resources
• Cheek HB, Blood grouping and Cross matching
• Perform quantitative serum Beta Human Chorionic Gonadotropin (bHCG)
• Check abdominal pelvic Ultrasound to confirm the diagnosis (Snowstorm appearance)
• Infuse compound sodium lactate (IV) OR 0.9% sodium chloride (IV) as needed
• Initiate blood transfusion if indicated
• Perform suction curettage in operating theatre
• Perform other investigations as appropriate (chest X ray, RFT, LFT, Chemistry panel)

Follow up for Molar pregnancy after Molar Evacuation


• Check weekly bHCG until when it becomes normal(5-10mIU/ml) for 3 weeks consecutively
• Then check monthly bHCG and pelvic ultrasound for 12 months
• Advice the patient to use effective contraception during follow up (preferably COCs)

11.1.1.7 Missed Abortion


This happens when a Fetus less than 24weeks die in utero, but it’s not expelled out

Clinical presentation
• History of amenorrhea
• Regression of the pregnancy symptoms
• Uterine size smaller than dates
• Mild of no PV bleeding

Management of a missed abortion at the dispensary and Health center

Referral: Referto higher level health facility with adequate expertise and diagnostics/equipment

Management of missed abortion at the hospital


Investigations
• Abdominal pelvic ultrasound
• Full blood count, Blood Grouping and cross matching
• Clotting indices (PT, APTT, INR)

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Pharmacological Treatment
Induce abortion with misoprostol if it is more than 12 weeks
A: misoprostol (PV) 100mcg 8hourly to max. 400mcg followed by sharp curettage in case of
incomplete abortion
Evacuate by Dilatation and Curettage (D&C) if the GA is less than 12weeks

Note
Avoid misoprostol in case of previous uterine scar

After evacuation give


A: metronidazole (PO) 400mg 8 hourly for 7days
AND
B: amoxicillin+ clavulanic acid (FDC) (PO) 625mg 8hourly for 7days

Patient education.
Counsel and provide appropriate contraception.

11.2 Ectopic Pregnancy


Ectopic pregnancy (EP) is defined as a pregnancy in which the implantation of the embryo occurs
outside the uterine cavity, most frequently in one of the two fallopian tubes or, rarely, in the
abdominal cavity.

11.2.1 Un-ruptured Ectopic Pregnancy


Clinical presentation

• History of amenorrhea
• PV Sport bleeding in early pregnancy
• Unilateral Abdominopelvic pain. Unilateral(localized) abdominal tenderness

Management of Un-ruptured ectopic pregnancy

Referral: Patients should be referred to higher level facilities with equipment and expertise
• At higher level facilities un-ruptured EP may be managed surgically or pharmacologically
depending GA and available expertise

Pharmacological Treatment
S: methotrexate (IV) 50mg/M2 single dose
OR
S: methotrexate 2.5mg (PO) 24hourly for 5days (in case IV methotrexate is not available)

Perform weekly pelvic ultrasound to ensure regression of Gestation sac

Note
Contraindications of methotrexate include a ruptured ectopic, ectopic mass greater than 3.5 cm, fetal
cardiac activity, high level hCG value (10,000 IU), breastfeeding and immunodeficiency

11.2.2 Ruptured Ectopic Pregnancy


Clinical presentation
• History of amenorrhea
• Acute generalized abdominal-pelvic pain
• Hypotension
• Fast and weak pulse
• Abdominal distension and tenderness with rebound tenderness

Management of ruptured ectopic at the dispensary and Health Center (B-MONC facilities)
• Apply ABCD principles of resuscitation
• Perform abdominal pelvic ultrasound if available
• Check Hb
• Start compound sodium lactate (IV) OR 0.9% sodium chloride (IV) infuse at a rate of
500mls per hour

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Referral: Ectopic pregnancy is an obstetric emergency, resuscitate and refer the patient
immediately, with an escort by skilled attendant.

Management of Ectopic pregnancy at the Hospital (C-EMONC facilities)

• Perform abdominal pelvic/Transvaginal ultrasonography


• Hb level
• Grouping and cross-matching
• compound sodium lactate (IV) OR 0.9% sodium chloride (IV) depending on amount of blood
loss
• Blood transfusion if indicated depending on the blood loss
• Perform Emergency laparotomy

11.3 Antepartum Hemorrhage


It is the bleeding from the birth canal after the 28th week of gestation but before the onset of labour.
The main forms are placenta praevia and abruption placenta. Other rare cause may include VASA
previa, heavy show and gynecological malignancies (cervical cancer)

11.3.1 Placenta Praevia


• It is an obstetric complication in which the placenta embeds itself partially or wholly in the
lower segment of the uterus. It is an obstetric emergency which should be managed in a
facility offering CEMONC services

Clinical presentation
• Sudden onset of bright red fresh painless bleeding after 28weeks of gestation

Management
• If partial PP and asymptomatic – Bed rest at home and follow up every 2weeks
• If complete placenta praevia
o Admit for close monitoring and observation
o Perform ultrasound to localize the placenta
o Perform FBP, Coagulation tests, Blood grouping and cross matching. Keep at least 2
units of blood ready in the bank for transfusion in case of acute bleeding
o Consider Blood transfusion if indicated
o Avoid vaginal digital examination
o If ˃34weeks and no PV bleeding or contraction, expectant management
o Deliver by Cesarean section preferably at 37–38 weeks of gestation
o Deliver by caesarean section by C/S any time incase of onset of labour or severe Pv
bleedingc
o Partial or marginal placenta praevia: Carefully perform amniotomy for vaginal delivery
if the head is engaged.

Pharmacological management
D: dexamethasone (PO) 6mg 12hourly for 48 hours if pregnancy is ˂34weeks for fetal lung
maturation
B: nifedipine (PO) 20mg 8hourly until labour symptoms subside

11.3.2. Placental Abruption


It is PV bleeding due to premature separation of a normally situated placenta in pregnancy after 28
weeks of gestation.
Clinical presentation
• Vaginal bleeding of dark colored blood or clots. Sometimes bleeding can be concealed
• Abdominal pain is moderate to severe but may be absent in revealed AP
• The uterus may be enlarged and very tender
• Fetal demise or fetal distress may be present

Management of Abruptio Placenta at Dispensary and Health centre.


• Apply the ABCD principles of resuscitation

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• Insert large bore cannula IV line, start rapid infusion with RL/NS
• Insert Urethral catheter
Refer: resuscitate and referimmediately to the hospital with an escort of a skilled health attendant

Management of Abruption Placenta at the hospital


Investigations
• Ultrasound: Fetal wellbeing, placenta localization and evidence of retro placental clot
• Full blood count and cross–match
• Renal function test, Liver function test and electrolytes
• Fibrinogen tests if available, D-dimer, PT, PTT, INR

Note
The diagnosis of placental abruption is mainly clinical

Maternal resuscitation
• Apply the ABCD principles of resuscitation
• Insert two (2) large bore IV lines and give Normal Saline/Ringers Lactate. Replete
crystalloids at ratio of 1 unit of blood loss: 3 unit of crystalloids
• Blood Transfusion is usually necessary
• Give oxygen supplementation at a flow of 6L/min
• Insert a urinary catheter to monitor input/output
• If Disseminated Intravascular Coagulation: Give fresh frozen Plasma 1 Unit/hour, give
whole blood 2–4 units
• Monitor blood pressure, pulse, bleeding, hourly, full blood count, clotting profile every 2
hours

Obstetrical Management
• If the foetus is alive and viable: emergency Caesarean section
• If the foetus is dead: Normal vaginal delivery is preferable if no contraindication for vaginal
delivery (eg uterine scar)
• Perform artificial rupture of membrane,

If no spontaneous labour: induce with Oxytocin infusion 5IU in 500 ml NS beginning with 10
drops/min increase the rate after every 20min until optimal contractions are achieved.
• Do active management of third stage of labour and uterine massage
• Emergency Caesarean section should be considered if:
o Worsening of maternal condition
o Failure/Non progressing vaginal delivery

Prophylactic antibiotics
C: amoxycillin + clavulinic acid (FDC) (IV) 1.2gstat
AND
B: metronidazole (IV) 500mg stat.
11.4 Obstructed Labour
Also known as labour dystocia, is when despite adequate uterine contractions the baby does not exit
the pelvis during due to being physically blocked. Obstructed may commonly be caused by; big
baby, narrow maternal pelvis, malpresentation and malpositions.
Clinical presentations
• Prolonged labour (˃8hours of • Severe caput succedaneum
active labour) • Maternal dehydration (neglected
• Delayed second stage of labour obstructed labour)
(˃1hour) • Bundl’s ring (sign of neglected
• Fetal distress obstructed labour)
• Severe moulding (3+)

Management of obstructed labour at B-EMONC facilities


• Insert IV line with and start RL/ DNS infusion 2L
• Insert urethral catheter
• Check Hb

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• Encourage the patient to lay in left lateral position

Management of Obstructed labour at the C-EMONC facilities


• Optimize hydration by RL/NS 2lt before caesarean section
• Ensure the patient is catheterized,
• Perform Hb estimation
• Perform emergency caesarean section.

Pharmacological treatment
A: compound sodium lactate (IV)/sodium chloride (IV) 0.9%to ensure adequate hydration
OR
A: ampicillin (IV) 2g within 30m before CS, continue 2g 24hourly for 3days
OR
B: ceftriaxone (IV) 1g stat within 30min before CS, continue 1 g 24hourly for 3days
OR
C: amoxycillin + Clavulinic acid (FDC) (IV) 1.2g within 30min before CS, continue 1.2g
8hourly for 3days
AND
B: metronidazole (IV) 500mg within 30min before CS, continue 500mg 8hourly for 3days.

11.5 Postpartum Hemorrhage (PPH)


It is abnormal uterine bleeding following delivery through 6 weeks (42 days). It is sub classified in to
Primary and Secondary PPH

Primary PPH
It is typically loss of more than 500 ml of blood from the genital tract after vaginal delivery or more
than 1000 ml after Caesarean section in the first 24 hours. OR it is any amount of blood loss after
delivery that would result in to haemodynamic instability.

Management of PPH at Dispensary and Health centre

• Insert 2 large bore cannula IV line, start rapid infusion with compound sodium lactate or
sodium chloride
• Start oxytocin (IV) 20IU in 500mls NS at a rate for 20drops per minute
• Ensure no retained placental tissues
• Clamp or ligate bleeding perineal tears if any.
• Massage the uterus
• Insert Urethral catheter

Referral: If bleeding continues, immediately refer the patient to the hospital an escort of a skilled
health attendant. Maintain IV infusion during transfer.

Management of PPH at the hospital


• Shout for help and mobilize resources
• Obtain blood samples for Hb, blood grouping and cross matching
• Insert 2 large bore cannulas and start infusing compound sodium chloride or sodium
chloride (IV) rapidly
• Blood Transfusion depending on amount of blood loss
• Start oxytocin (IV) 20IU in 500mls compound sodium lactate/0.9% sodium chloride (IV)
titrate at 20 drops per minute OR misoprostol (PO) 1000mcg or per rectal
• Perform other manoeuvres (balloon tamponade, TAH, Illiac artery ligation, B-Lych suture)
including surgical interventions depending on patient condition and available expertise.

Prevention of PPH –Active management of Third Stage of Labour (AMSTL)


Ensure no remaining second twin
A: oxytocin (IM)10IU
OR
A: misoprostol (PO) 600mcg

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Controlled cord traction (CCT) is recommended for vaginal births. Sustained uterine massage is not
recommended as an intervention to prevent PPH in women who have received prophylactic
oxytocin.

Prevention of PPH in Caesarean sections


A: oxytocin (IV/IM) 10IU is the recommended uterotonic drug for the prevention of PPH in
Caesarean section
Cord traction is the recommended method for the removal of the placenta in Caesarean
section

11.6 Prelabour Rupture of Membranes (PROM)


It is the rupture of membranes (breakage of the amniotic sac) before the onset of labor. If rupture
occurs before 37weeks it is called preterm prelabour rupture of membranes (PPROM). Prolonged
PROM is a case of premature rupture of membranes in which more than 24 hours have passed
between the rupture and the onset of labour. Prolonged PROM for more than 18 hours is a risk of
ascending infection which can lead to chorioamnionitis (infection of chorion, amnion and amniotic
fluid.

Clinical presentation
Leakage of watery fluid per vagina confirmed by performing a sterile speculum examination.

Management of PROM at the dispensary and health center


Give the following antibiotics for prophylaxis against chorioamnionitis
A: erythromycin (PO) 500mg 8hourly for 7days
AND
A: metronidazole (PO) 400mg 8hourly for 7days

Referral: Referto the hospital for further evaluation and management

Management of PROM at the hospital


Investigations
• Ultrasound for fetal wellbeing, amount of liquor and gestation age.
• Perform a sterile speculum examination to confirm leakage
• Perform HVS for culture and susceptibility testing
• Urinalysis

General Management
If PROM at term: Delivery within 24 hours
Assess Bishop’s Score and Induce Labour accordingly with
A: misoprostol (PO) 25mcg 8hourly (Max 3doses) if unfavorable cervix.
OR
A: oxytocin (IV) 5IU in 500ml of D5% titrate beginning with 10dpm if favourable cervix

Monitor FHR vigilantly during the process of IOL. Deliver by C/S if vaginal delivery is
contraindicated, fetal distress or failed induction of labour.

For Preterm PROM:


If no sign of infection, wait for foetal maturity and give

B: dexamethasone (IM) 6mg 12hourly for 48 hours if pregnancy is ˂34weeks for fetal lung
maturation
AND
B: nifedipine (PO) 20mg 8hourly for 7 days for tocolysis

Monitor for infection (FBP, RCP, Pulse, Fever) and fetal wellbeing (fetal movement, FHR, obstetric
ultrasound)
Administer prophylactic antibiotics
A: metronidazole (PO) 400mg 8hourly 10days.
AND
A: erythromycin (PO) 500mg 8hourly for 10days

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OR
B: amoxicillin + clavulanic acid (FDC) (PO) 625mg 8hourly for 10days

Deliver irrespective of gestation age in case of infection

If there are signs of infections-pyrexia, foul smelling liquor (chorioamnionitis)

A: metronidazole (PO) 400mg 8hourly for 5-7 days


AND
C: amoxycillin + clavulanic acid (FDC) (IV) 1.2g 8hourly for 5-7days
OR
D: ceftriaxone + sulbactam (FDC) (IV) 1.5g 12hourly for 5-7 days
11.7 Antenatal Care
11.7.1 Anaemia in Pregnancy
It is hemoglobin levels less than 11 g/dl in early pregnancy and less than 10.5 g/dl in the 2nd and
3rd trimester of pregnancy. Mild anemia– hemoglobin: 8–11g/dl; Severe anemia– hemoglobin<7g/dl.
Iron deficiency anemia during pregnancy has been associated with an increased risk of low birth
weight, preterm delivery and perinatal mortality.

Clinical presentation
• Tiredness, weakness, palpitations and dyspnea
• Exercise intolerance
• Pallor of skin and mucous membranes
• Dizziness, faintness, headache
• Intermittent claudication (ache, cramp, numbness or sense of fatigue)

Note
Some patients with anaemia in pregnancy may be asymptomatic

Investigations
• Full blood count and blood cross-match - red cell morphology
• Red blood cell electrophoresis if haemoglobinopathies suspected
• Blood smear for malaria
• Stool and urine analysis
• HIV test

Non-pharmacological Treatment
• Iron rich diet (fish, eggs, fruits and vegetables etc.)
• Prevent and early treatment of malaria
• Investigate and treat associated worm infestations

Pharmacological Treatment

Prophylaxis in Antenatal Care


A: ferrous sulfate(PO) 200mg 8-12hourly
AND
A: folic acid (PO) 5mg 24hourly

Note:
• Ferrous sulfate should be taken in a full stomach and avoid taking it with tea/coffee
• Where vomiting is experienced reduce dosage to tolerable level

If Hb is <7g/dl in 1st and second trimester give:


A: ferrous sulphate + folic acid (FDC) (PO) 1 tab 12hourly for 4 weeks.
AND
A: vitamin B (PO) 12hourly for 4 weeks

If HB is ˂7g/dl in 3rd trimester or in case of signs for severe anaemia (features of heart failure)
• Refer/admit the patient for blood transfusion at least 2 units of Packed RBCs

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• Continue with ferrous and folic acid as above after blood transfusion

11.7.2 Hypertensive Disorders in Pregnancy


Hypertension is blood pressure (BP) 140/90 mmHg or greater, measured on two occasions at least
four hours apart or elevated systolic BP >30mmHg, or diastolic BP 15mmHg from the baseline.

Chronic Hypertension
This is hypertension that is present at the booking visit or before 20 weeks or if the woman is already
hypertensive before conception. Most women with chronic hypertension are asymptomatic. New
onset chronic hypertension should have further evaluation to find underlying cause e.g. renal artery
stenosis, chronic renal disease, Cushing syndrome etc.

Pharmacological Treatment
A: methyldopa (PO) 250–500mg 8hourly
AND
B: nifedipine (PO) 20mg 12hourly

Pregnancy induced hypertension (gestation hypertension)

Gestational hypertension or pregnancy-induced hypertension (PIH) is the development of new


hypertension in a pregnant woman after 20 weeks of gestation without the presence of protein in the
urine or other signs of preeclampsia. Usually disappears within 12 weeks postpartum

Non-pharmacological Treatment
• Adequate rest at home and avoid strenuous activities
• Eat a normal balanced diet and plenty of oral fluids
• Schedule antenatal visits every 2 weeks up to 32 weeks and every week thereafter
• Recommend to deliver in the hospital and should be delivered at 37 completed weeks of
gestation

Pharmacological Treatment
For mild hypertension 140–159 mmHg systolic and/or 90–109 mmHg diastolic.
A: methyldopa (PO) 250–500mg 8hourly
OR
B: nifedipine (PO) 20mg 12hourly
OR
C: labetalol (PO) 100mg 12hourly a day

Severe hypertension
Severe hypertension is Blood Pressure (BP) of 160/110 mmHg or higher. Admit the patient to
hospital
A: methyldopa (PO) 500mg 8hourly
AND
C: hydralazine 10mg (slow IV) stat (over 4-5 minutes); recheck the BP after 20 minutes if
DBP is more/equal to 110mmHg give another dose of hydralazine (IV slowly) 5–10mg.
AND
B: nifedipine (PO) 20mg 12hourly
OR
C: labetalol (PO)100mg 12hourly

Note
Ensure slow administration and monitor closely for hypotension if using hydralazine.

Referral: Refer to the next level facility in case there is no improvement

11.7.3 Pre-eclampsia
Is diagnosed when blood pressure is ≥ 140/90 mmHg after 20 weeks of pregnancy plus proteinuria
of 300 mg per 24 hours or >2+ on urine dipstick. Or elevation of BP in pregnancy with features of
end organ damage (eg pulmonary edema, renal or liver damage)

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Diagnostic Criteria
• Most patients are asymptomatic, but symptoms may include headaches, dizziness, blurred
vision, and epigastric pain.
• Blood pressure of ≥ 140/90 mmHg
• Proteinuria (≥ 300mg per 24 hours)
• Generalized edema may be present (not a necessary criteria)

Investigations
• Urine for Proteinuria (qualitative/quantitative 24-hour urine collection)
• Obstetric Ultrasound and biophysical profile
• Urea, creatinine, electrolytes, liver function test and uric acid
• FBP and clotting profile
• Fundoscopy

Non-pharmacological Management
Pregnancy < 37 weeks of gestation
• Hospitalization and close monitoring
• Bed rest
• Monitoring BP, urine output, proteinuria, fetal movement and fetal heart beats (every day)
• ˂34weeks

Pregnancy >37 weeks of gestation: admit and deliver accordingly.

Pre-eclampsia with Severe Features:


This is diagnosed when BP ≥ 160/110 mmHg (especially diastolic ≥110 mmHg), or BP of
≥140/90mmHg with features of end organ damage eg severe headache, epigastric pain, blurring of
vision +/_vomiting, pulmonary oedema, renal or liver damage, features of haemolysis and low
platelets

Pharmacological Treatment
C: hydralazine (IV) 5mg in 10ml sterile water over 4minutes’ initial dose. Followed by
boluses 5–10mg as needed every 20 minutes until when the diastolic BP is less than
110mmHg)
AND
A: methyldopa (PO) 500mg 8hourly
AND
A: nifedipine (PO) 20mg 8hourly until BP is stabilized
OR
if hypertension is refractory to hydralazine
C: labetalol (IV bolus)10–20mg stat repeat each 10–20 minutes, with doubling doses not
exceeding 80mg in any single dose for maximum total cumulative dose of 300 mg.
Antenatal corticosteroids (dexamethasone Inj. 6mg 12hourly for 48hours) if pregnancy
Prophylaxis for Seizures
Anti-convulsion treatment of choice is magnesium sulfate.

A: Magnesium sulfate (IV) 1g hourly in 250mils of RL (OR 5g of 50% MgSO4 4 hourly or


alternate buttock) for 24 hours if GA is ≤34 weeks or until 24 hours post-delivery if GA
is≥34 weeks (Refer to eclampsia section)

Obstetrical Management
If at term deliver immediately when stable, preferably vaginal delivery

11.7.4 HELLP syndrome


It is a life-threatening complications of pre-eclampsia characterized by Haemolysis, Elevated Liver
enzymes and Low Platelets
Diagnostic criteria
• Haemolysis
o Abnormal peripheral smear
o Total bilirubin > 1.2 mg/dL

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o Lactic dehydrogenase > 600 U/L
• Elevated Liver Functions
o Serum glutamic oxaloacetic transaminase > 70 U/L
o Lactic dehydrogenase > 600 U/L
• Low Platelets
o Platelets < 1,000,000/mm3

Management of HELLP syndrome


The management is the same as for severe pre-eclampsia

11.7.5 Eclampsia
Eclampsia is a condition peculiar to pregnancy and post-partum periods, characterized by elevated
BP and tonic-clonic convulsions which are not caused by epilepsy, severe malaria, meningitis,
hypoglycemia or other causes of convulsions. Majority (50%) occur preterm. Eclampsia may occur
without prior elevation of BP.

Diagnostic Criteria
• Signs of severe pre-eclampsia (BP > 160/110mm Hg)
• Loss of consciousness
• Tonic-clonic seizures, coma
Investigations
• Full blood count and crossmatch • Blood smear to exclude malaria
• Ultrasound for GA and fetal viability • Blood sugar estimation to exclude
• Urea and creatinine + electrolytes hypoglycemia.
• Liver enzymes tests • Lamber puncture may be indicated
• 24h urine collection for proteinuria to exclude meningitis
• Clotting profile

Pharmacological Treatment
Manage with antihypertensive as in pre-eclampsia with severe features AND
A:magnesium sulfate (IV)
Loading dose: magnesium sulfate (IV) 4g of 20% (MgSO4) slowly over 5minutes.
If having 50% MgSO4 dilute it to make it 20% MgSO4 by Drawing 8mls of 50% MgSO4 and adding
12mls water for injection to make it 20mls of 20% of MgSO4 and
OR
Draw 10mls (5gms) of 50% MgSO4 into each syringe 1ml of A: 2% lignocaine in each syringe then
give deep IM into each buttock. Continue with maintenance dose until 24hours post-delivery or since
the last episode of convulsion: With MgSO4 infusion 1g per hour (in 200–300 ml of Ringer’s Lactate),
or MgSO4 5g undiluted 50% of MgSO4 injection (add 1ml of lignocaine 2%) apply deep intra-
muscular (IM) injection into each buttock every 4hrs for about 24 hours after delivery or the last
seizure whichever come last.16

Note
The magnesium sulfate infusion should only be given if patellar reflexes are present, respiration rate
is ≥ 12 per minute, and urine output is >100mls in 4 hours.

If convulsions recur within 15 minutes give;


A: magnesium sulfate 2g. Draw 4mls of 50% of MgSO4 (2gm), add 6mls of water for
injection to make it 10mls of 20% MgSO4 then give IV slowly over 5 minutes

Features of Magnesium Sulphate toxicity


• Respiratory depression (˂16cycles/min
• Reduced urine output(˂30mls/hour)
• Loss of deep tendon reflexes
In case of magnesium sulphate toxicity
• Stop magnesium sulphate administration
• A: calcium gluconate (IV) 1g slow bolus in 2 to 3 minutes

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Obstetrical management
Patients with eclampsia should be delivered within 12hours after the onset of seizures, even if the
foetus is premature. Expectant management is contraindicated. If not in labour, and no
contraindications, induce labour with misoprostol 50µg (PO) ,4hourly or 25µg vaginally and repeat
8hourly up to a total of four doses maximum
• If failure of induction or contraindication to vaginal delivery, immediate Caesarean section
is indicated

Prevention of pre-eclampsia and eclampsia


• Ensure effective antenatal care
• Calcium supplementation calcium supplementation at doses of 1.5–2.0g elemental
calcium/day) for those at high risk of developing pre-eclampsia.
• Low-dose acetylsalicylic acid (aspirin, 75 mg) is recommended for the prevention of pre-
eclampsia in women at high risk of developing pre-eclampsia.

11.7.6 Antiphospholipid Syndrome (APS) in Pregnancy


It is an autoimmune disease characterized by the presence in maternal circulation of one or more
auto antibodies against membrane phospholipids. It is an acquired condition. Antiphospholipid
syndrome (APS) is characterized by venous or arterial thrombosis and/or an adverse pregnancy
outcome. APS occurs either as a primary condition or in the setting of an underlying disease, usually
systemic lupus erythematosus (SLE).

Clinical presentation
• Recurrent pregnancy adverse outcome e.g. (miscarriages) recurrent
miscarriage, intrauterine growth restriction, early severe pre-eclampsia and preterm birth.
• Unexplained venous thrombosis (DVT) or arterial thrombosis (Stoke) or myocardial
infarction
• thrombocytopenia (common finding but among the clinical classification criteria)

Classification with APS requires one clinical and one laboratory manifestation:
Clinical
• A documented episode of arterial, venous, or small vessel thrombosis
• 1 or more unexplained deaths of a morphologically normal fetus ≥ 10-week GA
• 3 or more unexplained consecutive spontaneous abortions before the 10th weeks of GA
with anatomic, hormonal or chromosomal causes excluded
• Eclampsia or severe pre-eclampsia according to standard definitions, or recognized
features of placental insufficiency

Laboratory:
• Anti-cardiolipin IgG and/or IgM measured on 2 or more occasions, not less than 12 weeks
apart;
• Anti-β2 glycoprotein I IgG and/or IgM measured on 2 or more occasions, not less than 12
weeks apart
• Lupus anticoagulant detected on 2 occasions not less than 12 weeks apart.
Pharmacological Treatment

A: acetyl salicylic acid (PO) 75-120mg 24hourly beginning as soon as the pregnancy is
confirmed throughout pregnancy
AND
C: unfractionated heparin (SC) 5000–10000
OR
S: low molecular weight heparin (SC) 30–40mg 24hourly

Patients with Thrombosis such as stroke or pulmonary embolism need therapeutic


anticoagulation.
C: unfractionated heparin (SC) 5,000 bolus and subsequent 15,000–20,000 doses at
12hourly intervals

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OR
S: low molecular weight heparin (SC) 1mg/kg 12hourly

Note
• Warfarin should be avoided in pregnancy due the risk of teratogenicity
• The aPTT needs to be checked and is best done midway between the 12hourly doses,
24hourly.
• A target of 1.5–2.5 times the control should be aimed

Referral
Refer immediately to a level where expertise and monitoring for treatment through laboratory testing
is available.

11.7.7 Deep Vein Thrombosis in Pregnancy


Deep vein thrombosis (DVT) and acute pulmonary embolism (PE) are two manifestations of venous
thromboembolism (VTE. The risk of VTE is increased in pregnancy by about five timesbecause of a
more hyper-coagulable state. VTE contributes to significant maternal morbidity and mortality. The
mainstay of therapy for DVT is anticoagulation, provided there is no contraindication

Clinical presentation
• Pain on the affected limb
• Swelling or redness of the calf or thigh
• Homan’s sign (pain in the calf in response to dorsiflexion of the foot)

Investigations
• Venous doppler ultrasound
• Venography (CT MRI)
• Fibrin degradation product (FDP) or D-dimer

Prevention of DVT
• Early passive and active ambulation in women undergoing major obstetric surgery
• Compressive stockings in women ≥100kg undergoing obstetric surgery
• LMWH prophylaxis 5000IU within 1-hour post-surgery to at risk women.

Pharmacological Treatment
B: unfractionated heparin (SC) 5,000 bolus and subsequent 15,000–20,000 doses at
12hourly intervals (under supervision of a specialist)
OR
S: low molecular weight heparin (SC) 1mg/kg 12hourly
OR
C: warfarin (PO) 5mg 24hourly (in delivered women) consider bridging warfarin with
Heparin for 5days as it takes longer to act. Warfarin to be continued up to 6weeks
postpartum

Note
Check PTT every 4hours and PTT should be maintained at 1.5–2.5 X control. Once steady state has
been achieved measure PTT levels daily. Change heparin to SC route after 5–10days

Referral: Immediate referral to a hospital with expertise and monitoring of the treatment through
laboratory testing is recommended.

11.7.8 Pulmonary Embolism in Pregnancy


It is a blockage, usually a blood clot that prevents oxygen from reaching the tissues of the lungs; it
can be life-threatening

Diagnostic Criteria
• Acute onset of shortness of breath • Low grade fever
(dyspnea) • Tachypnea
• Pleuritic chest pain • Diminished oxygen saturation
• Cough and/or hemoptysis • Diminished breath sounds

232
Investigations
• Venous Doppler ultrasound • CT scan, MRI
• Pulmonary angiography • D-dimer

Non-pharmacological Treatment
Respiratory support and Oxygen supplementation

Pharmacological Treatment
B: unfractionated heparin (UFH) is the treatment of choice
Loading dose 150 U/kg (or minimum of 5000 U) followed by
Initial infusion 15–25 U/kg/hour (or minimum of 1000U/hourly)

Note
Check PTT every 4 hours and adjust infusion to maintained PTT at 1.5–2.5 x control. Once steady
state has been achieved measure PTT levels daily. Change heparin to SC route after 5–10 days to
avoid formation of hematoma.

Referral
Immediate referral to a health facility where expertise and monitoring of the treatment through
laboratory tests is available is recommended.

11.7.9 Vomiting in Pregnancy and Hyperemesis Gravidarum


It is excessive nausea and vomiting in early pregnancy requiring hospital admission and rehydration.

Clinical presentation
• Weight loss • Dehydration
• Excessive Nausea and vomiting • Altered general status (fast pulse,
typically in early pregnancy restlessness)

Investigations
• Full blood count • Liver function tests
• Blood for urea, electrolytes and • Thyroid function tests
serum creatinine • Obstetric ultrasound to exclude
• Urinalysis, micro urine and culture, multiple pregnancy and GTD
ketonuria

Non-pharmacological Treatment
• Nil per oral (nothing by mouth) for • Emotional support
24–48 hrs. • Rest and Lifestyle adjustment
• Input/output monitoring for 24–48 • Ensure adequate hydration and
hrs. Frequent small carbohydrate meal
• Monitor electrolytes for 24hrs
• Counselling and Reassurance

Pharmacological Treatment
A: compound sodium lactate with 5% dextrose and 0.9%sodium chloride according to daily
needs and severity.
AND
C: vitamin B1 (IV)100mg 24hourly mix in intravenous rehydration solution
AND
C: metoclopramide (IM) 5–10 mg 8hourly till vomiting stops.
OR
A: promethazine (IM) 12.5 mg 12hourly a day
OR
B: pyridoxine + doxylamine (FDC) (PO) 10mg/10mg 8hourly till vomiting stops

Referral: Depends on the status of the patient, refer to a hospital if vomiting is intractable and if
there is a need for high volume replacement.

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11.7.10 Heartburn in Pregnancy
Heartburn (also called acid indigestion or acid reflux) is a burning sensation that often extends from
the bottom of the breastbone to the lower throat. It is caused by some of the hormonal and physical
changes in pregnant women.

Non-pharmacological Treatment
Pregnant women should avoid:
• Food and beverages that cause gastrointestinal distress
• Tobacco and alcohol
• Do not eat big meals, instead eat several small meals throughout the day
• Drinking large quantities of fluids during meals
• Do not eat close to bedtime, they should give themselves 2–3 hours to digest food before
they lie down
• Sleep propped up with several pillows or a wedge.

Pharmacological Treatment
A: compound magnesium trisilicate (PO) as needed until when the heartburn subsides.
OR
A: omeprazole (PO) 20–40mg 24hourly
OR
C:pantoprazole (PO) 40mg 24hourly

11.7.11 Other Medical Disorders in Pregnancy


Other medical disorders in pregnancy/other gynecological disorders include diabetes mellitus,
glucose intolerance, malaria, HIV/AIDs complications, Pelvic Inflammatory Diseases (PID) etc. All
these complications are discussed under specific disease chapters.

11.7.12 Stimulation of Labour and Myometrial Relaxation


Myometrium stimulants should be used with great care before delivery especially in porous women.
Use in obstructed labour should be avoided.

Oxytocic’s are indicated for: –


• Augmentation of labour • Uterine stimulation after delivery for
• Induction of labour management of PPH due to uterine
• Active management of third stage atony
of labour.

Induction of Labour
Indications/Contraindications
• The indication for induction must be documented, and discussion should include reason for
induction, method of induction, and risks, including failure to achieve labour and possible
increased risk of Caesarean section5
• If induction of labour is unsuccessful, the indication and method of induction should be re-
evaluated.

Pre-induction assessment
• Health care providers should assess the cervix (using the Bishop score) to determine the
likelihood of success and to select the appropriate method of induction.
• The Bishop score should be documented.
• Care providers need to consider that induction of women with an unfavorable cervix is
associated with a higher failure rate and increased rate of operative deliveries.

Post-dates induction
• Women should be offered induction of labour between 41+0 and 42+0 weeks as this
intervention may reduce perinatal mortality and meconium aspiration syndrome without
increasing the Caesarean section rate
• Women who chose to delay induction >41+0 weeks should undergo twice-weekly
assessment for fetal wellbeing

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Options for Cervical Ripening/Induction: Unfavorable Cervix
• Intracervical Foley catheters are acceptable agents that are safe both in the setting of a
vaginal birth after Caesarean section and in the outpatient setting
• Double lumen catheters may be considered a second-line alternative

Pharmacological Treatment
A: misoprostol (PO) 25µg 2 hourly for 24hours or Misoprostol (PV) 25µg 6hourly for
24hours can be considered a safe and effective agent for labour induction with intact
membranes and on an inpatient basis.
OR
S: dinoprostone (PV) 3mg 6hourly a total of 2doses

Note
• Misoprostol should not be used in the setting of vaginal birth after Caesarean section due to
the increased risk of uterine rupture.
• Oxytocin should be started no earlier than 4hours after the last dose of misoprostol.

Options for induction with a favourable cervix


• Amniotomy should be reserved for women with a favorable cervix. Care should be given in
the case of unengaged presentation because there is a risk of cord prolapse.
• After amniotomy, oxytocin should be commenced early in order to establish labour.
• In the setting of ruptured membranes at term, oxytocin should be considered before
expectant management.
• Women positive for group B streptococcus (GBS) should be started on oxytocin as early
as possible after ruptured membranes in order to establish labour within 24 hours.
• Both high- and low-dose oxytocin may be considered within a hospital protocol.
• Because of the various concentrations, oxytocin infusion rates should always be recorded
in mU/min rather than mL/hr.
• Oxytocin induction maybe considered in the hospital setting of vaginal birth after
Caesarean section.
• For induction of labour use: Oxytocin IV, the dose will depend on parity.

Primigravida
A: oxytocin (IV) 5IU in 500mls of 0.9% sodium chloride the initial dose should be
8-10drops/Minute, the titration may be gradually increased at intervals not shorter
than 20 minutes and increments of not more than 5drops/minute, until a
contraction pattern similar to that of normal labour is established. The
recommended maximum rate is 40d/m.

Multiparous
A: oxytocin (IV) start with low dose e.g., 2.5IU in 500mls of fluid titrate as above.
Regulate the dose according to response.

Note
• Induction of labour with uterotonic drugs requires vigilant monitoring
• Induction of labour should only be attempted at hospitals with capacity to perform Caesarea
section

Augmentation of Labour
If labour progress is not optimum labour augmentation is necessary. Can be achieved by:
A: oxytocin as above
OR
Artificial rupture of membranes (ARM) and oxytocin. If membranes are already ruptured and no
labour progress the steps above should be followed; rule out obstruction before augmenting labour
with oxytocin.

Myometrial stimulation after delivery


A: oxytocin (IM) 10IU after delivery of the infant; when no response give oxytocin (IV
infusion) 20 units in 500mls of NS running at 10–20 drops per minute.
OR
C: ergometrine (IM) 0.25–0.5mg after delivery of the infant, in the absence of myometrium

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contraction and to prevent postpartum hemorrhage.
OR
A: misoprostol (PO/PV) 800–1000µg

Note
Use Ergometrine cautiously in cardiac and hypertensive disease patients

Myometrium relaxation (Tocolysis)


It is done to relax the uterus in order to:
• Relieve fetal distress immediately • Prevent uterine rupture
prior to Caesarian section • Perform external cephalic version
• Stop uterine contractions in
premature labour

Pharmacological Treatment
B: nifedipine (PO) 20 mg stat, followed by 10–20mg 6–8hourly
OR
B: salbutamol (PO) 4mg stat, when required (maximum daily dose 32mg)

Note
• β -stimulants should never be used if the patient had an antepartum hemorrhage
• β -stimulants are contra-indicated for cardiac disease and severe anemia in
pregnancy

11.7.13 Rhesus Incompatibility


Incompatibility between an infant’s blood type and that of its mother, resulting in destruction of the
infant’s red blood cells (hemolytic anemia) during pregnancy and after birth by antibodies from its
mother’s blood circulation.

Investigations
• Maternal Blood group+ Rhesus factor
• Paternal blood group+ Rhesus factor
• Infant Cord blood at delivery for grouping, FBC, Coombs test to detect maternal antibodies
and Total Billirubin

Prevention of Rhesus isoimmunisation

If the mother is Rhesus negative give


C: anti D immunoglobin 300microgram within 72hours of delivery
Antepartum
C: anti D immunoglobulin (IM)at 28-32weeks of gestation

Abortion in Rhesus negative mother give


C: anti D immunoglobulin 100microgram (IM) within 72hours of abortion

Note
For the management of other medical conditions in pregnancy e.g. Malaria, Peripartum
cardiomyopathy, Diabetes and Renal disease in pregnancy refer to specific chapters in this
guideline.

11.8 Postpartum Care


11.8.1 Mastitis
It is the inflammation of the breast usually associated with breastfeeding.

Clinical Presentation
• May develop rapidly,
• Breast becomes red and swollen, tenderness, warmth and burning sensation
• Fever

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Non-pharmacological Treatment
• Drinking plenty of liquids and resting
• Feed the baby more frequently and ensure adequate emptying.
• Expressing the milk more often in non-breastfeeding mothers.

Pharmacological Treatment
C: flucloxacillin + amoxycillin (FDC) (PO) 500mg 12hourly for 5-7days
OR
B: amoxycilling + clavulic acid (FDC)(PO) 625mg 12hourly for 5-7days
AND
A: ibuprofen (PO) 500mg 8hourly for 5days
OR
A: paracetamol (PO) 500–1000mg 8hourly for 5days

11.8.2 Puerperal Sepsis


It is the infection of the uterus and surrounding tissues within 6 weeks postpartum manifesting as
postpartum metritis, postpartum endometritis parametritis, peritonitis or septicaemia.
Clinical presentation
• Fever
• Foul smelling lochia
• Lower abdominal pain or generalized abdominal pain and tenderness
• Delayed involution

Investigations
• Full blood picture and Cross Matching
• Check LFT, RFT, Electrolytes
• Blood culture in case of suspected septicaemia
• Abdominal pelvic ultrasound

Management of Puerperal sepsis at Dispensary and Health Center


A: Establish IV line and give compound sodium lactate/0.9% sodium chloride 2l
then continue as required
AND
B: amoxicillin + Clavulanic acid (FDC) (PO) 625 12hourly for 5days
AND
A: metronidazole (PO) 400mg hourly for 5days
AND
A: gentamycin (IV) 80mg 12hourly for 24-48hours.

Referral: resuscitate and refer immediately to hospital for further investigations and management.
Management of puerperal sepsis at the hospital
• Blood transfusion in anaemic
• Plan interventions eg (laparotomy, uterine evacuation etc) appropriately.
• Continue with the above antibiotic for 5-7 days
• Adjust drugs depending on the Culture and susceptibility results or if not available and
there is no improvement after 3 days of treatment with above antibiotics switch to:

B: metronidazole (IV) 500mg 8hourly for 5-7days


AND
D: ceftriaxone + sulbactam (FDC) (IV) 1.5g 12hourly for 5-7 days
OR
S: piperacillin + tazobactam (FDC) (IV) 4.5g 12hourly for 5-7days

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Prevent Puerperal infections by
Observation of aseptic technique when performing all obstetric procedures including Pelvic
examinations during labour. Administration of prophylactic antibiotics within 1hour before performing
a caesarean section or manual removal of Placenta.

C: amoxycillin + clavulanic acid (FDC)(IV) 1.2g stat


OR
D: ceftriaxone + sulbactam (FDC) (IV)1.5g stat
AND
B: metronidazole (IV) 500mg stat

11.8.3 Abnormal Uterine Bleeding (AUB)


It is the uterine bleeding after menopause, in between menstrual periods or abnormally heavy and or
prolonged menstrual bleeding. Abnormal uterine bleeding (AUB) is a common condition affecting
women that has significant social and economic impact.

The causes of AUB are classified and summarized into an Acronym; PALM-COEIN
• P-Polyps
• A-Adenomyosis
• L-Leiomyosma
• M-Malignancy
• C-Coagulopathy
• O-Ovulatory dysfunction
• E-endometrial causes
• I-Iatrogenic
• N-Not yet Classified

Clinical presentation
Polyps
• Contact vaginal bleeding • Pelvic pain or heaviness
• Abdominal discharge

Adenomyosis
• Premenstrual uterine cramps • Heavy menstrual bleeding
• Dysmenorrhea

Leiomyoma
• Abdominal mass and distension • Lower abdominal pain and
• Heavy or prolonged menstrual discomfort
bleeding

Malignancy
• Presentation depend on type of • Foul smelling bloody or mucoid
malignant Vaginal discharge
• Abnormal intermenstrual or • Wight loss, loss of appetite, early
postmenopausal contact bleeding satiety
(cervical cancer)

Coagulopathy
• History of bleeding tendencies • Heavy and or prolonged
menstruation

Anovulatory dysfunction
• Irregular bleeding, often heavy • Infertility or subfertility

Endometrial causes
• Heavy or prolonged menstruation
• Irregular menstruation associated with endometrial hyperplasia

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Investigations
• Investigate according to the • Biopsy in case of suspected
possible cause of AUB basing on malignancy
clinical suspicion • Specific Tumor markers in certain
• A complete blood count (CBC) suspected malignancies e.g.
• Pregnancy test in reproductive age ovarian tumors.
to exclude pregnancy • Testing for coagulation disorders
• Examination under anaesthesia should be considered only in
and biopsy in case of malignancy women who have a history of
• Cervical and vaginal swab heavy menstrual bleeding
• Abdominal pelvic Ultrasound, CT beginning at menarche or who
scan, MRI, Xray as indicated have a personal or family history of
• LFT, RFT, Electrolytes abnormal bleeding
• Hysteroscopy, Cystoscopy,
Proctoscopy in case of suspected
malignancy
Pharmacological Treatment
The treatment will depend of the causative factor.
C: tranexamic acid (PO) 500 –1000mg 6–8hourly as required until the bleeding is
controlled
OR
A: combined oral contraceptives (PO) Useful for anovulatory bleeding.
OR
A: medroxyprogesterone acetate (PO) 5–10mg 24hourly for 10–14days initially and
repeated for 10days each month thereafter
OR
C: norethisterone (PO) 5mg 24hourly for 10days. Then 5mg 12hourly from days 19 to 26 of
the two subsequent cycles, should be given to prevent recurrence of the condition.
Surgical management
AUB due to organic causes may be amenable to surgical intervention. The decision regarding the
approach and the timing for surgical intervention should depend on final diagnosis, expertise and
other resources.
Referral
Immediately refer to the next level facility with capable for appropriate evaluation and
managementrecommend

11.8.4 Dysmenorrhea
It is a painful menstruation preventing normal activities and requires medication. There are 2 types
of dysmenorrhea:

Primary (no organic cause). Typically, pain occurs on the first day of menses, usually about the
time the flow begins.

Secondary (pathological cause) e.g., usually the pain is due to other underlying causes eg PID,
endometriosis, etc.

Pharmacological Treatment
A: ibuprofen (PO) 200–600mg 8hourly (maximum 2.4 g/day)
OR
A: acetylsalicylic acid (PO) 300–600mg 4hourly
OR
A: diclofenac (PO) 50–100mg 8–12hourly
OR
B: mefenamic acid (PO) 500mg 8hourly
AND
A: hyoscine butyl bromide (PO) 20mg 8hourly for 5days

Women with regular complaints can easily detect length of use during their periods (2–3days usually
enough). Treat the underlying condition if known

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Note
For primary dysmenorrhea patients may be advised to start taking ibuprofen one or two days
before menses and continue
for three to four days during menses to minimize painful menstruation

11.8.5 Endometriosis
It is the presence of endometrial glands and stroma in locations other than the uterine endometrium
and musculature. The common locations of endometriosis include the pelvis, small intestines,
bowels, appendix, anterior abdominal wall and incision scars

Clinical presentation
• Chronic pelvic pain, lower back • Dysfunctional uterine bleeding
pain and rectal pain • Infertility
• Dysmenorrhea
• Dyspareunia

Management at Dispensary and Heath center

A: ibuprofen (PO) 200–600mg 8hourly (maximum 2.4 g/day)


OR
A: acetylsalicylic (PO) acid 300–600mg 4hourly
OR
A: diclofenac (PO) 50–100mg 8–12hourly
OR
B: mefenamic acid (PO) 500mg 8hourly
OR
A: hyoscine butyl bromide (PO) 20mg 8hourly for 5days

Referral: Refer the patient with endometriosis to hospital for further investigations and management.

Management of endometriosis at Hospital


Investigations
• Abdominal pelvic/transvaginal • MRI
ultrasound • Laparoscopy
• CT scan

Pharmacological treatment of endometriosis


A: combined oral contraceptive pills (PO) 1 tab 24hourly for 3months
OR
A: medroxyprogesterone acetate (IM) 300mg monthly for 6months.
OR
S: danazol (PO) 200-400mg 12hourly depending on the severity. Continue RX to maintain
amenorrhea.
OR
S: Goserelin (IM) 3.6mg monthly for 4-6months

11.9 Contraception
11.9.1 Short term Contraceptive Methods
Short-term hormonal contraceptives
Before initiating hormonal contraceptives:
• Check blood pressure
• Perform vaginal examination (to check normal size of uterus)
• Check for contraindications like deep vein thrombosis

Follow up:
• Instruct women always to inform the doctor or nurse that they are on contraceptives while
attending clinic or hospital.

240

• Women on oral contraceptives need regular physical check-ups including blood pressure
measurement every six months
• Need to withdraw Contraceptives in:
o Pregnancy
o Severe headaches especially associated with visual disturbances
o Numbness or paresis of extremities
o Unexplained chest pain or shortness of breath
o Severe leg pains etc
o Deep vein thrombosis.

The recommended short-term hormonal contraceptives are:


A: ethinyloestradiol+norgestrel (FDC) (PO) 0.03mg/0.3mg 24hourly
OR
A: ethinyloestradiol+levonogestrel (FDC) (PO) 0.03mg/0.15mg 24hourly
OR
A: ethinyloestradiol+desogestrell (FDC) (PO) 0.03mg/0.15mg) 24hourly
OR
A: medroxyprogesterone acetate (IM) 150mg every three months
OR
A: levonorgestrel (PO).0.03mg 24hourly

Note
• Take the first pill on the 5th day of menstruation and then continue every day without
any interruptions
• Check blood sugar and hypertension after every 6 months
• Avoid use in women with severe hypertension and women without proven fertility

Post-coital contraception
The method is applicable mostly after rape and unprotected sexual intercourse where pregnancy is
not desired. Within 3 days (72 hours) of unprotected sexual intercourse, give:
A: levonorgestrel (PO) 1.5mg stat
OR
A: levonorgestrel (PO) 0.75mg 12hourly. 2 doses
OR
B:CuT380A Intrauterine Contraception Device (IUCD) may also be used.

Note
Emergency contraception should not be used as a routine method of contraception. Clients should
be advised to use regular effective contraceptive methods of their choice.

Barrier methods (condoms)


A: Male Condoms
A: Female Condoms
A correct use of both male and female condoms is required with every act of sexual intercourse for
greatest effectiveness.

Note
Condoms are the only contraceptives that can protect against both pregnancy and STIs

11.9.2 Long-term Contraceptive methods


Implant Contraceptives
Implants are contraindicated to:
• Severe hypertension • Sickle cell anaemia
• Thromboembolism • Genital bleeding
• Active liver disease • Severe headaches

The following are the recommended implants:


A: etonogestrel 68mg in single silastic capsule with applicator is implanted in the left upper
arm with local anesthesia. Is effective for 3 years
OR
A: levonorgestrel 75mg in two silastic capsules implanted subdermal in the left upper arm

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with local anesthesia. Is effective for 5 years and is recommended for women who have
completed their family or not ready for sterilization or those not able to take estrogen
containing contraceptives.

Note
Implants may be inserted during the immediate postpartum period, or after 4 weeks postpartum

Intrauterine Contraceptive Device


It is the devise containing copper or Levonorgestrel that is inserted in the uterus to prevent
pregnancy
B: CuT380A Intrauterine Contraception Device (IUCD) may also be used

It can be inserted during the immediate postpartum period, within 48hours postpartum or after 4
weeks postpartum

The contraindication to postpartum IUD includes


• Active postpartum haemorrhage
• Puerperal sepsis/chorioamnionitis,
active PID
• Allergy to copper
• Period within 48 hours and 4we

Note
Use the WHO Medical eligibility criteria (MEC) wheel on providing FP methods

11.9.3 Permanent (surgical) Contraceptive Methods


The available permanent contraceptive options include;

• Bilateral tubal ligation (female sterilization) for women who will not want more children
• Vasectomy for men who will not wat more children

11.8.4 Infertility
Infertility is a condition of the reproductive system defined by the failure to achieve a clinical
pregnancy after 12 months or more of regular unprotected sexual intercourse.
A detailed history taking, and physical examination are invaluable for the diagnosis for causes of
infertility

Investigation: Not every fertility test will be done for every case.

WOMEN: For women, fertility testing may include basic gynaecologic examination
• VDRL tests
• Urine routine and microscopic
• Cervical mucus examination
• Abdominal pelvic/Transvaginal USS
• HSG (hysterosalpingogram)for tubal patency
• Hysteroscopy-
• Diagnostic laparoscopy- This test is only done when symptoms point to possible
endometriosis, as part of treatment for blocked fallopian tubes, or in some cases of
unexplained infertility.
• Hormonal profile- FSH, LH, TSH, AMH, T3 & T4, Testosterone, prolactin, estradiol and
progesterone.

242

MEN: Perform the following
• Semen analysis
• VDRL tests
• Hormonal profile-FSH, Testosterone, but sometimes also LH, estradiol, or prolactin

Treatment will depend on the underlying cause

Non-pharmacological Treatment
• Weight reduction in obese clients.
• Educate the couple on the importance of having sexual intercourse during the fertile
window
• Try to avoid smoking/excessive drinking

Pharmacological Treatment
Ovulation stimulation;
C: clomiphene citrate (PO) 50mg 24hourly for 5days from the 2nd–5th day of
menstruation. (maximum 6 cycles)

Polycystic Ovarian Syndrome (PCOS)


A: metformin (PO) 500mg 8hourly is used for PCOS treatment, alone or along with fertility
drugs

Hyperprolactinemia
C: bromocriptine (PO) 2.5–5mg 24hourly until the prolactin level is within the normal range
OR
S: cabergoline (PO) 0.25–0.5mg once or twice weekly initially then the dose is gradually
increased monthly until prolactin levels normalize. Doses of less than 3mg per week are
usually enough to achieve this goal

Surgeries:
• Tubal surgery for Tubal blockage
• Myomectomy for uterine fibroids
• Ovarian drilling is a possible surgical treatment for PCOS–related infertility

Referral
Refer all patients with infertility to a gynecologist.

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CHAPTER TWELVE
SEXUALLY TRANSMITTED INFECTIONS
Sexually transmitted infections (STIs) — are generally acquired by sexual contact with a person who
has an STI. The organisms (bacteria, viruses or parasites) that cause sexually transmitted diseases
may pass from person to person in blood, semen, or vaginal and other bodily fluids. Reproductive
tract infections (RTIs) occur in the genital tract and affect both women and men. Some RTIs, such
as syphilis and gonorrhea, are sexually transmitted, but many are not. In women, overgrowth of
endogenous microorganisms normally found in the vagina may cause RTIs (yeast infection,
bacterial vaginosis).

Clinical Presentation
• Sores or bumps on the genitals or • Itching or irritation of the vulva or
in the oral or rectal area. vagina.
• Painful or burning urination. • Unusual vaginal bleeding.
• Discharge from the penis. • Pain during sex.
• Vaginal discharge that is abnormal • Lower abdominal pain
in colour, odour, amount or • Genital ulcers, sores or blisters
consistency. • Swelling, lumps or ulcer in the groin
area

12.1 STIs/RTIs Management Approaches


Management of STIs/RTIs can be done in either of the following approaches:
• Aetiological laboratory approach: By identification of causative agents through
laboratory methods and sensitivity pattern to the medicine to used, followed by disease-
specific treatment.

• Aetiological clinical approach: By targeting disease treatment based on suspected


causative agents diagnosed clinically. This is not appropriate at any health facility because
of its demands on the clinical acumen of the service provider and the danger of incorrect
diagnosis and, hence, insufficient treatment.

• Syndromic approach: This identifies clinical syndromes (symptoms and signs) followed
by syndrome-specific treatment that targets causative agents which cause the syndrome.

Management of STIs/RTIs using Aetiological Laboratory Approach


It identifies causative agents through laboratory methods, followed by disease-specific treatment.
This is the best approach to be used at a Health Facility (HF) which has a Laboratory capable of
doing the Laboratory Investigation and producing timely result(s) so as to enable the clinician to
prescribe medicine (s) according to the causative agent(s) and sensitivity pattern.

Management of STIs/RTIs using Syndromic Approach


This approach is recommended if the HF is not able to conduct appropriate Laboratory
Investigation(s) and producing timely result(s) to enable the clinician to prescribe the medicine in
accordance with causative agent(s).
Syndromic management of STIs is based on the diagnosis of defined symptoms and easily
recognizable clinical signs. Each syndrome can be caused by several different causative agents. For
each syndrome, a well-defined standard treatment which has been proven to be effective against
most endemic causative agents for the syndrome are used.

Syndromic approach of managing STIs/RTIs entails the service provider to follow laid down steps in
a flow chart which guides him/her in making rational management decisions for treating the client.
These are therefore known as treatment flow-charts. They may also be known as treatment
algorithms, treatment protocols or treatment decision trees. They guide the provider through a series
of decisions and actions that need to be made. Each decision or action is enclosed in a box, with
one or two routes leading out of it to another box, with another decision or action. Upon learning a
patient’s symptoms and signs, the service provider turns to the flow chart for the relevant syndrome

244

and works through the decisions and suggestions it guides to manage the client accordingly. Each
flow chart is made up of a series of three steps. These are:
• The clinical problem (the patients presenting symptoms and signs),
• The decision that needs to be taken,
• The action that needs to be carried out.

12.2 Urethral Discharge Syndrome (UDS)


UDS refers to the presence of abnormal secretions in the distal portion of the urethra.
Causes
• Neisseria gonorrhoeae and
• Chlamydia trachomatis.

Clinical Presentation
• Urethral discharge,
• Burning or painful micturition,
• Itchy urethra and increased frequency and urgency of micturition.

Note
• Persistent or recurrent symptoms of urethritis may be due to drug resistance, poor
compliance or re-infection. In some cases, there may be infection with Trichomonas
vaginalis (TV).
• Male patients complaining of urethral discharge and/or dysuria should be examined for
evidence of discharge. If none is seen per inspection, the urethra should be gently milked
from the ventral part of the penis towards the meatus.
• Delayed or inadequate treatment may result into orchitis, epididymitis, urethral stricture
and/or infertility.

Investigation(s) if the HF has a Laboratory capable of doing:


• Culture and Sensitivity • Quantitative or qualitative PCR
• Gram stain • Genetic sequencing
• ELISA

Management and Treatment of UDS (seeflow chart 12.1)

12.3 Vaginal Discharge Syndrome (VDS)


VDS refers to change of colour, odour and/or amount of vaginal secretions.
Causes
• T. vaginalis, • Neisseria gonorrhoeae
• C. albicans • Chlamydia trachomatis
• Bacterial Vaginosis

Clinical Presentation
• Abnormal vaginal discharge, • Increased frequency and urgency
• Burning or painful micturition, of micturition and/or painful coitus.
• Itchy vulva,

Note
• A spontaneous complaint of abnormal vaginal discharge is most commonly due to a vaginal
infection.
• T. vaginalis, C. albicans and Bacterial Vaginosis are the commonest causes of vaginal
infection while
• Neisseria gonorrhoeae and Chlamydia trachomatis cause cervical infection.
• The clinical detection of cervical infection is difficult because a large proportion of women with
gonococcal or chlamydia infections are asymptomatic.
• vaginal discharge is therefore highly indicative of vaginal infection, but poorly predictive for
cervical infection
• Due to the high prevalence of gonorrhea and chlamydia, all women presenting with VDS
should receive treatment for both vaginal and cervical infections.

245

• Delayed or inadequate treatment of VDS may result to endometritis, salpingitis, oophoritis or
ectopic pregnancy.
• Gonococcal or chlamydial cervical infection may be asymptomatic

Investigation(s) if the HF has a Laboratory capable of doing:


• Wet preparation • Pap test (Papanicolau test)
• Gram stain • ELISA
• Culture and Sensitivity • Quantitative or qualitative PCR
• Fluorescent Microscopy • NB starts simple to complex

Management and Treatment of VDS (see flow chart 12.2)

12.4 Lower Abdominal Pain Syndrome or Pelvic Inflammatory Disease (PID)


PID is defined as the inflammation of the uterus, fallopian tubes, ovaries and pelvic peritoneum. It is
also known as lower abdominal pain syndrome. It commonly occurs as a result of infection
ascending from the cervix. It can also occur as a result of trans-cervical procedure.
Causes
• Neisseria gonorrhoeae, • Anaerobic bacteria
• Chlamydia trachomatis and

Clinical Presentation
• Lower abdominal pain and • Menometrorrhagia,
tenderness, • Fever and sometime
• Painful micturition, • Nausea and vomiting.
• Painful coitus,
• Abnormal vaginal discharge,

Note
• Delayed or inadequately treated PID may lead to chronic lower abdominal pain,
• Pelvic abscess,
• Ectopic pregnancy,
• Dysmenorrhea and infertility.

Investigation(s) if the HF has a Laboratory capable of doing:


• Wet preparation • Pap test (Papanicolaou’s test)
• Gram stain • ELISA
• Culture and Sensitivity • Quantitative or qualitative PCR
• Fluorescent Microscopy

Management and Treatment of PID (see flow chart 12.3)

In-patient treatment of PID


All patients with PID who have fever or body temperature ≥ 380C should be admitted for closer care.
The recommended in-patient treatment options for PID are as follows:
Regimen 1:
A: cefixime (PO) 400mg 12hourly for 7-14days
AND
A: doxycycline (PO) 100mg 12hourly for 7-14days
AND
A: metronidazole (PO) 400mg 8-12hourly for 7-14days
OR
B: metronidazole (IV) 500mg 8-12hourly for 7-14days
Regimen 2:
A: ceftriaxone (IM) 1gm 24hourly for 5-7days
AND
A: doxycycline (PO) 100mg 12hourly for 7-14days
AND
A: metronidazole, (PO) 400mg 8-12hourly 7-14days
OR
A: metronidazole (IV) 500mg 8-12hourly 7-14days

246

Regimen 3:
S: clindamycin (IV) 900mg 8hourly for 7-14days
AND
A: gentamicin (IV) 1.5 mg/kg 6-8hourly 7-14days

Note
For all three regimens, therapy should be continued for two days after the patient has improved
and then be followed by doxycycline (PO) 100 mg 12hourly for 14days.
• Patients taking metronidazole should be cautioned to avoid alcohol.
• Doxycycline is contraindicated in pregnancy.

12.5 Painful Scrotal Swelling (PSS)


PSS is the inflammation of the epididymis and testis, often accompanied with scrotal pain, swelling
and tenderness. It is also known as epididymorchitis.
Causes
• Neisseria gonorrhoea and
• Chlamydia trachomatis

Clinical Presentation
• Scrotal pain, • Scrotal oedema
• Scrotal swelling and tenderness, • Fever

Note
Among the common complications of painful scrotal swelling include infertility and scrotal abscess.

Investigation(s) if the HF has a Laboratory capable of doing:


• Gram stain • Quantitative or qualitative PCR
• Culture and Sensitivity • Genetic sequencing
• ELISA

Management and Treatment of PSS (see flow chart 12.4)

12.6 Ano-rectal Syndrome (ARS)


Is defined as soreness, burning, itching or other irritation of the rectum together with redness in the
area of anus. Sometimes it is accompanied by diarrhea and it may occur as a toxic side effect of oral
administration of certain broad-spectrum antibiotics.
Causes
• Neisseria gonorrhoeae, • Herpes Simplex Virus.
• Chlamydia trachomatis, • Shigella spp., or
• Treponema pallidum • Entamoeba histolytica
Clinical presentation
• Purulent rectal discharge
• Mucous rectal discharge
• Watery rectal discharge
• Soreness, burning, itching or other irritation of the rectum together with redness in the area
of anus
• There may also be ineffectual straining to defecate (“tenesmus”), sometimes mistakenly
described as “constipation” by patients.
• The anus and rectum may be intensely painful, with external and internal ulceration
• Abdominal pain or cramping, abdominal swelling, distention or bloating;
• Bloody stool (blood may be red, black, or tarry in texture),
• Burning feeling,
• Change in bowel habits, constipation, diarrhea;
• Fecal incontinence (inability to control stools),
• Flatulence; pain, which may be severe, in the abdomen, pelvis, or lower back,

247

• Urgent need to pass stool and watery diarrhea including multiple episodes.
• A proctoscopic examination (which should be done, if feasible) will reveal rectal pus,
bleeding or ulceration.

Note
• Proctitis may be caused by Salmonella spp., Shigella spp., or Entamoeba histolytica as a
part of gastroenteritis, which may manifest as diarrhoea with fever, anorexia, and
abdominal cramps.
• Antibiotics that destroy normal intestinal bacteria and allow other bacteria to grow in their
place may also cause proctitis.
• Herpes proctitis may be mistaken for the rectal manifestation of ulcerative colitis or
Crohn’s disease.
• Proctitis typically causes painless bleeding or the passage of mucus (sometimes
mistaken for diarrhoea) from the rectum.
• All cases of proctitis in MSM should be treated for gonorrhoea and chlamydia infections.
• Symptoms of diarrhoea, bloody stools, abdominal cramping, nausea, and/or bloating
may indicate Giardia spp infection or amoebic dysentery.

Other non-STI causes of ARS include:


Anal fissure, Fecal impaction, Food intolerance, Gastroenteritis (bacterial and viral), Inflammatory
bowel disease (includes Crohn’s disease and ulcerative colitis), Neurological damage, and Perirectal
or perianal abscess.

Other symptoms might occur with rectal discharge includes gastrointestinal symptoms which vary
depending on the underlying disease, disorder or condition. These may include:
• Abdominal pain or cramping, abdominal swelling, distention or bloating; bloody stool (blood
may be red, black, or tarry in texture), burning feeling, change in bowel habits,
constipation, diarrhea; fecal incontinence (inability to control stools), flatulence; pain, which
may be severe, in the abdomen, pelvis, or lower back, urgent need to pass stool and
watery diarrhea including multiple episodes.

Investigation(s) if the HF has a Laboratory capable of doing:


• Wet preparation • Treponema palladium particle
• Gram stain agglutination (TPPA)
• Pap test (Papanicolaou’s test) • ELISA
• Culture and Sensitivity • Quantitative or qualitative PCR
• Rapid Plasma Reagin (RPR) • Genetic sequencing
• Fluorescent Microscopy

Management and Treatment of ARS(see flow chart 12.5.)

12.7 Oropharyngeal Syndrome


Oral sex can lead to oropharyngeal STIs (infections of mouth and throat).
Causes
• Human Papilloma Virus, • Chlamydia spp
• Herpes Simplex Virus, • Treponema pallidum
• N. gonorrhoea

Clinical presentation
• Pharyngitis, • History of unprotected oral sex

Investigation(s) if the HF has a Laboratory capable of doing:


• Wet preparation • Treponema pallidum particle
• Gram stain agglutination (TPPA)
• Pap test (Papanicolaou’s test) • ELISA
• Culture and Sensitivity • Quantitative or qualitative PCR
• Rapid Plasma Reagin (RPR) • Genetic sequencing

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• Fluorescent Microscopy

Management and Treatment of Oropharyngeal syndrome(see flow chart 12.6.)

12.8 Genital Ulcer Disease (GUD)


GUD is a loss of continuity of skin or mucous membrane producing one or more lesions in the
genital area.
Causes
• Treponema pallidum, • Herpes simplex virus type 2 (HSV)
• Haemophilus ducreyi, • Calymmatobacterium granulomatis.
• Chlamydia trachomatis,

Clinical presentation
• Ulcer • Vesicle
• Sore

Investigation(s) if the HF has a Laboratory capable of doing:


• Wet preparation • Rapid Plasma Reagin (RPR)
• Gram stain • ELISA
• Culture and Sensitivity • Quantitative or qualitative PCR
• Fluorescent Microscopy • Genetic sequencing
• Treponema palladium particle
agglutination (TPPA)

Management and Treatment of GUD (see flow chart 12.7)


12.9 Neonatal Conjunctivitis (Ophthalmia Neonatorum)
Ophthalmia Neonatorum (ON) means inflammation of the conjunctiva of a newborn baby of less
than 1 month of age.
Is a potentially sight threatening condition. If the baby is older, the cause is unlikely to be an STI.
Causes
• Neisseria gonorrhoeae
• Chlamydia trachomatis.
• Other non-STI causes of neonatal conjunctivitis include:
o Staphylococcus aureus,
o Streptococcus pneumoniae,
o Haemophilus and Pseudomonas spp,
o Viral, chemical and physical irritation.
Presentation
• Reddish conjunctiva,
• Oedema/swelling of the eyelids
• Purulent eye discharge

Prevention and control measures


• Screening of pregnant women,
• Early treatment of VDS in pregnant women
• Routine eye chemoprophylaxis in the newborn by providing
A: 1% oxytetracycline eye ointment to all newborns.

Note
Examine the neonate and exclude other congenital diseases

Management and Treatment of Neonatal conjunctivitis (see flow chart 12.8)


12.10 Inguinal Bubo (IB)
Inguinal and femoral bubos are localized enlargements of the lymph nodes in the groin area, which
are painful and may be fluctuant.
They are frequently associated with lymphogranuloma venereum and chancroid
Causes
• Chlamydia trachomatis

249

• Haemophilus ducreyi

Clinical presentation
• Localized enlargements of the • Fever
lymph nodes in the groin area, • Tenderness.
• Painful and may be fluctuant.
• Pain,

Note
• In many cases of chancroid an associated genital ulcer is visible, but occasionally may not
be.
• Non-sexually transmitted local and systemic infections (e.g. infections of the lower limb) can
also cause swelling of inguinal lymph nodes. These should therefore be ruled out.

Investigation(s) if the HF has a Laboratory capable of doing:


• Culture and Sensitivity
• ELISA
• Quantitative or qualitative PCR
• Direct Fluorescent Antibody (DFA)

Management and Treatment of Inguinal BUBO (see flow chart 12.9)

12.11STI/RTI flow charts


Steps in using the flow charts:
• Start by asking the patient for his/her symptoms.
• Find the appropriate flow chart, stated in the clinical problem box with “Patient Complaints
of.”
• The clinical problem box usually leads to an action box, which asks you to examine the
patient and/or take the history.
• Next, move to the decision box. After taking the history and examining the patient you
should have the necessary information to choose Yes or No accurately.
• Depending on your choice, there may be further decision boxes and action boxes.

Note
For the appropriate management of STIs/RTIs syndrome, drugs in the watch group (azithromycin,
cefixime and ceftriaxone) are the standard recommended for use as a first line treatment for the
most STIs/RTIs starting at the Dispensary level, therefore, should be used only for STIs/RTIs at
Primary HFs)

250

Flow Chart 12.1: Management of Urethral Discharge Syndrome (UDS)

251

Flow Chart 12.2: Management Of Vaginal Discharge Syndrome (VDS)

252

Flow Chart 12.3: Management Of Lower Abdominal Pain Syndrome (PID)

253

Flow Chart 12.4: MANAGEMENT OF PAINFUL SCROTAL SWELLING (PSS)

254

Flow Chart 12.5: MANAGEMENT OF ANORECTAL SYNDROME (ARS)


Patient complains of anorectal discharge or pain and discomfort in
the perianal area

1st Visit

Take history
Examine, the perianal area and do a proctoscopy if available to identify discharge

History of anal sex


No history of anal sex Other STI(s) found

Anorectal discharge or pain/ discomfort in the

perianal area confirmed

Use appropriate
• Find other cause of anorectal discharge, pain Flow Chart(s)
or discomfort and treat accordingly such as

Treat for Gonorrhoea and Chlamydia anogenital warts and herpes simples
A: Cefixime 400 mg PO stat • Provide health education

A: Azithromycin 1g PO start • Counsel on risk reduction

Provide health education
• Partner management

• Promote and provide condoms

Offer HIV counseling and testing

Incontinence, prolapse, etc


Refer to Surgeon

Appointment in 7 days

• Take history to assess treatment compliance & possible
re-infection.
• Examine

2nd
Visit
Persistent Anorectal discharge or pain/ No dischargeor pain/ Other STI(s)

discomfort in the perianal discomfort in the perianal

Use appropriate
Flow Chart(s)

Provide prolonged Chlamydia treatment and 2nd line for Cured, Discharge from clinic
gonorhoea:
A: Doxycyline 100mg PO 12 hourly for 7 days
A: Metronizadole 2 g PO stat
A: Inj. Ceftriaxone 1gm IM stat

255

FLOW CHART 12.6: MANAGEMENT OF OROPHARYNGEAL SYNDROME

256
Flow Chart 12.7: MANAGEMENT OF GENITAL ULCER DISEASE (GUD)

Patient complains of genital sore or ulcer


1st Visit

No ulcer/sore • Reassure
No vesicle • Provide health education
• Take history
No other STI • Counsel on risk reduction
• Examine


Ulcer/Sore found Only Vesicles present Other STI(s) found

Treat for Syphilis, Chancroid, LGV&(HSV-2 if history Treat for HSV-2 Use appropriate
of vesicles) Flow Chart(s)
• Keep clean and dry
A: Benz. Penicillin 2.4 MU i.m stat 1/2 in each

buttock B: Acyclovir tabs 400 mg 8 hourly for 7 days
A: Azithromycin 1g PO start B: Acyclovir cream

B: Acyclovir 400 mg PO 8 hourly for 7 days

• Ensure Compliance
• Provide health Education
• Counsel on risk reduction
• Partner management
• Promote and provide condoms
• Offer HIV counseling and testing
• Offer follow up date


2ndVisit Appointment in 7 days

Take History and Examine

No Improvement Other STI(s)


Cured

Treat with 2nd line drug: Discharge from clinic Use appropriate
A: Ceftriaxone 1gm IM stat Flow Chart(s)

1. Patients allergic to penicillin substitute with Erythromycin 500mg PO 6 hourly for 15 days

2. Do not give Acyclovir during pregnancy and breast feeding.

257
Flow Chart 12.8: MANAGEMENT OF NEONATAL CONJUCTIVITIS

258
FLOW CHART12.9: MANAGEMENT OF INGUINAL BUBOS (IB)

259

Table 12.1 Management of Mixed Infections
Mixed Sexually Drug treatment (new episode)
Transmitted
Infections
UDS + SSS Ceftriaxone (IM) 250mg stat AND Azithromycin (PO) 1g per week for
2weeks AND Metronidazole (PO) 2g stat AND Supportive therapy: to
reduce pain advice bed rest, scrotal elevation with a scrotal support (T-
bandage) and analgesics.
UDS + Balanitis Cefixime (PO) 400mg stat OR Ceftriaxone (IM) 250mg stat AND
Azithromycin (PO) 1g stat OR Doxycycline (PO) 100mg 12hourly for
7days AND Metronidazole (PO) 2g stat AND Clotrimazole cream, local
application 12hourly for 7days
UDS + GUS Cefixime (PO) 400mg stat OR Ceftriaxone (IM) 250mg stat AND Acyclovir
(PO) 400mg 8hourly for 7days AND Benzathine Penicillin* (IM) 2.4MU
stat AND Azithromycin (PO) 1g stat OR Doxycycline* (PO)100mg
12hourly for 7days AND Metronidazole (PO) 2g stat
VDS + LAP Ceftriaxone (IM) 250mg stat AND Azithromycin (PO) 1g per week for
2weeks AND Metronidazole (PO) 400mg 12hourly for 7–14days.
Clotrimazole pessary to be added, if vulva oedema, itching, excoriations
or curd-like discharge present
VDS + GUS (non- Cefixime 400mg stat OR Ceftriaxone (IM) 250mg stat AND Metronidazole
pregnant) (PO) 2g stat AND Benzathine Penicillin* (IM) 2.4 MU stat AND
Azithromycin (PO) 1g stat OR Doxycycline* (PO) 100mg 12hourly for
7days AND Acyclovir (PO) 400mg 8 hourly for 7 days. Clotrimazole
pessary to be added, if vulva oedema, itching, excoriations or curd-like
discharge present
VDS + GUS Cefixime 400mg stat OR Ceftriaxone (IM) 250mg stat AND Metronidazole
(pregnant, (PO) 2g stat AND Benzathine Penicillin* (IM) 2.4 MU stat AND
breastfeeding) Azithromycin (PO) 1g stat OR Erythromycin* (PO) 500mg 6hourly for
7days AND Acyclovir (PO) 400mg 8hourly for 7days. Clotrimazole
pessary to be added, if vulva oedema, itching, excoriations or curd-like
discharge present
LAP + GUS Ceftriaxone (IM) 250mg stat AND Metronidazole (PO) 400 mg 12hourly
for 7–14days AND Benzathine Penicillin* (IM) 2.4MU stat AND
Azithromycin (PO) 1g per week for 2weeks OR Doxycycline* (PO) 100 mg
12hourly for 7–14days AND Acyclovir (PO) 400 mg 8hourly for 7days
SSS + GUS Ceftriaxone (IM) 250mg stat AND Benzathine Penicillin* (IM) 2.4MU stat
AND Azithromycin (PO) 1g per week for 2weeks OR Doxycycline* (PO)
100mg 12hourly for 7–14days AND Acyclovir (PO) 400mg 8hourly for
7days
Note
In Penicillin-allergic patients: Give Doxycycline (non-pregnant women/men) or Erythromycin
(pregnant women) for 14days instead of 7days

12.8 Management of Other Common STI Conditions


Late Syphilis
This refers to Syphilis infection of more than 2years.
A: benzathine benzylpenicillin (IM) 2.4MU once weekly for 3 consecutive weeks.
AND
A: azithromycin (PO) 2g stat.

Syphilis in Pregnancy
Pregnant women should be regarded as a separate group requiring close surveillance to detect
possible re-infection after treatment has been given. It is also important to treat the sexual
partner(s).

260
A: benzathine benzylpenicillin (IM) 2.4MU, as a single dose
In case of late syphilis 3 doses of benzathine benzylpenicillin should be provided.

Congenital Syphilis
All infants born to sero-positive mothers should be treated with a single intramuscular dose of
benzathine benzylpenicillin,
50000IU/kg whether the mothers were treated during pregnancy (with or without penicillin).

Treatment regimens for early congenital syphilis (up to 2 years of age), and Infants with abnormal
cerebrospinal fluid:
A: benzyl penicillin (IV) 100000–150000IU/kg/day administered as 50000IU/kg/dose
12hourly, for the first 7days and every 8hourly thereafter for a total of 10days

For congenital syphilis in children 2 or more years


A: benzyl penicillin (IV or IM) 200000 – 300000IU/kg/day administered as 50000IU/kg
every 4–6hourly for 10–14days

The alternative regimen for penicillin allergic patients, after the first month of life
A: erythromycin (PO) 7.5–12.5 mg/kg 6hourly for 30days.

Syphilis and HIV Infection


All patients with syphilis should be encouraged to undergo testing for HIV because of the high
frequency of dual infection and its implications for clinical assessment and management.

Genital Warts (Venereal Warts)


Human papilloma virus (HPV) is a common sexually transmitted pathogen. Genital warts are
painless but may lead to serious complications. The removal of the lesion does not mean cure of the
infection. No treatment is completely satisfactory. Recommended regimens for venereal warts are as
follows:

Chemical Treatment (High level Health Facility Management)


D: Podophyllin 10–25% in compound tincture of benzoin, applied carefully to the warts,
avoiding normal tissue. External genital and perianal warts should be washed
thoroughly 4–6 hourly after the application of podophyllin. Podophyllin applied to warts
on vaginal or anal epithelial surfaces should be allowed to dry before removing the
speculum or anoscope. Treatment should be repeated at weekly intervals.

Other treatment approaches (Available at higher centres)


Cryotherapy with liquid nitrogen, solid carbon dioxide, or a cryoprobe. Repeat applications
every 1-2 weeks
OR
Electrosurgery
OR
Surgical removal

Treatment for Vaginal Warts


Recommended regimens for treatment of vaginal warts are:
D: cryotherapy (with liquid nitrogen)
OR
D: podophyllin 10–25% (allow to dry before removing speculum)

Treatment for Cervical Warts


Treatment of cervical warts should not be started until the results from a cervical smear test are
known

Management of Meatal and Urethral Wart


D: Cryotherapy
OR
D: podophyllin 10–25%
Note
Urethroscopy is necessary to diagnose intra-urethral warts, but they should be suspected in men
with recurrent meatal warts.

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CHAPTER THIRTEEN
SKIN DISEASES AND ALLERGIC REACTIONS

13.1 Bacterial Skin Infections


Bacterial skin infections can range fromimpetigo, folliculitis, furunculosis, erysipelas, cellulitis to
recurrent boils. All these skin conditions are caused by either Staphylococcus aureus alone or
together with streptococcus, but rarely streptococcus alone.
13.1.1 Impetigo
Is a contagious primary infection of the skin involving the stratum corneum of epidermis. It is
particularly common in children and people in disadvantaged areas.

Clinical presentation
• Polycyclic vesicles or blisters, which can contain pus
• Early lesions are isolated or confluent Erosions and yellowish crusts (“honey-colored”)

Fig 13.1 Impetigo

Note
Impetigo is a clinical diagnosis and the typical location in children is around orifices, especially
the mouth and nose.

Non-pharmacological Treatment
• Improve personal hygiene • Wash lesions with soap and water
• Hand washing • Remove crust

Pharmacological Treatments
A: Wet dressing with weak potassium permanganate (PP) soaks, 1:40000 (0.025%)
solution 12hourly for 3–4days. Each session to last for 15 to 20minutes
A: gentian violet paint (topical) 0.5% 12hourly for 5days
OR
C: mupirocin (topical) 2% 12hourly for 5–7days
OR
C: fusidic acid (topical) 12hourly for 5–7days

If severe or systemic symptoms are present (e.g. pyrexia) add an oral antibiotic:
A: phenoxymethylpenicillin (PO): Adult 500mg; paediatric 25mg/kg given 6hourly for 7days
OR
A: erythromycin (PO): Adult 500mg; paediatric 25—50mg/kg 8hourly for 10days
OR
B: amoxicillin + clavulanic acid 625mg (PO) 8hourly for 5days

13.1.2 Folliculitis
Folliculitis is an infection of the hair follicles commonly due to Staphylococcus aureus, and Gram-
negative bacteria such as Pseudomonas and Candida albicans.

Clinical presentation
Clinical features depend on risk factors, which may result into Pseudo-folliculitis, Carbuncles
aggregation and Furuncle (boil). The following are some of the clinical features:
• Scattered or extensive follicular
pustules

262

• Macular or papulo-erythematous • Permanent scars or scarring
lesions, mainly located on thighs, alopecia
buttocks, back and bearded area • Firm, broad swollen, painful,
• Papules and pustules fluctuant deep nodules
• Post-inflammatory • Multiple drainage tracts
hyperpigmentation • Fever and general body malaise
• Necrosis and suppuration with
discharge of necrotic core

Non-pharmacological Treatment
• Suspected irritants should be avoided
• In Pseudo-folliculitis (infection of the follicular opening) of the bearded area, shaving
should be stopped for several weeks until improvement occurs. Hair should be left to grow
to at least 1 mm long.
• Shaving with electric razors is preferred over manual razors for beard folliculitis. Cleaning
with water and soap

Pharmacological Treatment
A: potassium permanganate soaks, 1:40000 (0.025%) solution 12hourly for 3–4days. Each
session for 15 to 20minutes
Apply:
A: gentian violet paint (topical) 0.5% 12hourly for 5days
OR
C: mupirocin (topical) 2% 12hourly for 7-14days
OR
C: fusidic acid (topical) 2% 12hourly for 7-14days

Note
If severe, or systemic symptoms are present (e.g. pyrexia) add an oral antibiotic as above in
impetigo.

Fungal folliculitis
A: clotrimazole cream (topical) 12hourly for 4weeks
OR
C: miconazole cream (topical) 12hourly for 4weeks

13.1.3 Abscess
Abscess is a collection of pus caused by Staphylococcus aureus.

Clinical presentation
• Painful pus-filled nodule • Fluctuant palpable swelling
• Inflammatory erythematous plaque. • Fever is rare
• Lymphangitis and satellite nodes
may be experienced

Non-pharmacological Treatment
• By placing hot compresses over the swelling until it breaks

Surgical Treatment
• Incision and drainage

Pharmacological Treatment
Indicated in immunosuppressed patient, involvement of the face.
A: erythromycin (PO): Adult 500mg; paediatric 25–50mg/kg 8hourly for 7–10days
OR
C: flucloxacillin + amoxicillin (FDC) (P0): Adult 500mg; paediatric 25mg/kg 6hourlyfor 7–
10days

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13.1.4 Erysipelas and Cellulitis
Erysipelas is an acute superficial spreading infection commonly caused by Streptococci without pus
formation. Could also be due to Gram negative bacilli.

Clinical presentation
A prodrome of fever, chills, and malaise
• Locally, a large erythematous, swelling, well-demarcated, and usually raised lesion
• Regional adenopathy is frequent
• Superficial blistering secondary to edema,
• Superficial hemorrhage, may be sometimes be observed

Non-pharmacological Treatment
• Bed rest
• Elevation of the affected part
• Venous compression is recommended during the acute phase and subsequent weeks to
reduce the risk of lymphedema
• Prophylaxis of deep venous thrombosis (DVT) should be considered depending on
presence of other risk factors

Pharmacological Treatment
A: Weak potassium permanganate soaks, 1:40000 (0.025%) solution 12hourly for 3–
4days, with each session lasting for 15–20minutes
AND
A: silver sulfadiazine cream (topical) 12hourly 24hourly
OR
C: mupirocin (topical) 2% 12hourly for 5–7days
OR
C: fusidic Acid (topical) 2% 12hourly for 5–7days
AND
A: phenoxymethylpenicillin (PO): Adult 250–500mg; paediatric25mg/kg 6hourly for 5–
7days
OR
C: flucloxacillin + amoxicillin (FDC) (PO): Adult 500mg; paediatric 25–50/kg 6hourly for 5–
7days
AND
A: ibuprofen 400mg (OP) 6hourly for 5days

Referral: Referif there are local or general signs of severity of developing necrotizing fasciitis.

13.1.5 Paronychia
Paronychia is a painful infection that usually occurs at the nail fold. It may occur after injury or minor
trauma and is caused by Staphylococcus aureus. It may also occur as a result of fungal infection.

Clinical presentation
• Painful nail • Swelling
• Redness

Pharmacological Treatment
Acute Paronychia
B: amoxicillin with clavulanic acid (PO) 625mg 8hourly for 14days.
AND
C: mupirocin cream (topical) 12hourly for 14days
OR
S: clindamycin (PO) 300mg 12hourly for 14days

Chronic Paronychia (commonly due to fungal infection)


A: clotrimazole cream (topical) 1%, apply 12hourly for 14days
AND
A: fluconazole (PO) 200mg 24hourly for 14days
OR
D: itraconazole tablets (PO) 200mg 24hourly for 14days

264
Note
For acute paronychia incision and drainage may be needed

13.2 Fungal Skin Infections


13.2.1 Tinea Corporis (Body Ringworm)
Tinea corporis is a superficial fungal infection (dermatophytosis), commonly on the arms and legs,
but may occur on any part of the body
.
Clinical presentation
• Enlarging raised annular lesions with a central area of clearing
• Fine scales may be present
• Hair loss in areas of infection

Tinea corporis- before treatment Tinea corporis- after treatment

Investigation
Scraping edge of lesion for KOH

Pharmacological Treatment
A: benzoic acid compound ointment (topical) 12hourly up to 2weeks.
OR
C: miconazole cream (topical) 2%, apply thinly 12hourly a day. Continue for 5-7days after
clearing of lesions.
OR
C: terbinafine cream (topical) 12hourly for 2weeks

If extensive, use
C: terbinafine (PO) 250mg 24hourly for 2weeks

13.2.2 Tinea Capitis


Is a superficial fungal infection (dermatophytosis), on the scalp. It is quite common in children.

Clinical features
• Enlarging raised annular lesions with a central area of clearing
• Fine scales may be present
• Hair loss in areas of infection

Pharmacological Treatment
C: miconazole cream (topical) 2%, apply thinly 12hourly for 2weeks. Continue for 5-7days
after clearing of lesions
AND
A: griseofulvin (PO): Adult 500 mg; Paediatric 10-20mg/kg 24hourly for 6-8weeks
OR
C: terbinafine (PO): Adult 250mg 24hourly 6-8weeks; paediatric 62.5mg/ 10-20kg 24
hourly; 125mg/ 21-40 kg 24 hourly; 250mg/ 41kg 24hourly

13.2.3 Pityriasis Versicolor


It is a common fungal infection caused by yeast.

265

Clinical presentation
• Hypo/Hyper pigmented macules and confluent patches
• Lesions have fine scales
• Commonly occurs on the chest, back, arms and occasionally neck and face
Investigation
• KOH

Pharmacological Treatment
A: clotrimazole cream (topical) 12hourly for 2weeks
OR
C: miconazole nitrate cream (topical) 2% 12hourly for 2weeks
OR
C: ketoconazole shampoo 3times per week for 4weeks (if extensive)
AND
A: fluconazole (PO) 300mg stat
OR
D: itraconazole (PO)200mg 24hourly for 2weeks
13.2.4 Tinea Pedis (Athlete’s Foot) and Tinea Cruris
It is a common fungal infection of the toes and is often the source of infection at other sites
especially groin.

Clinical presentation
• Tinea pedis presents with erythema and maceration between the toes, sometimes
accompanied by painful vesicles.
• The chronic form is characterized by scaling, peeling on the soles.
• Tinea cruris-Itching and patches in the groin. Check for interdigital maceration for all with
tinea cruris.

Prevention and Non-Pharmacological Treatment


• Frequent change of socks/footwear, underwear.
• Use of cotton socks, underwear.
• Keep as dry as possible the spaces between toes after bathing always. Separating the
opposing skin surfaces (e.g. with a piece of gauze) will help speeding healing.

Pharmacological Treatment
A: clotrimazole cream (topical) 1% apply 12hourly for 2weeks
OR
C: miconazole cream (topical) 2%apply 12hourly for 2weeks
OR
C: terbinafine cream (topical) 24hourly for 14days
AND
A: gentian violet 24hourly for 14days for bacterial super infection
Alternatively
C: terbinafine (PO) 250mg 24hourly for 2- 4weeks
OR
D: itraconazole (PO) 200mg 24hourly for 2-4weeks

13.2.5 Candidiasis
It is a fungal infection mainly caused by yeast, Candida albicans. Candidiasis is usually precipitated
by prolonged use of contraceptive pills, AIDS, pregnancy,diabetes, prolonged use of antibiotics,
corticosteroid use, and being on immunosuppressive treatment

Clinical presentation (depending on the site of infection)


• Erythematous, moist exudate in the skin folds and accompanying satellite pustules
• Nail affection leads to painful swelling of the nail bed and folds, with pus discharge and is
made worse by contact with water
• Oral lesions are characterized by white, adherent mucosal plaques in buccal cavity
including the tongue

266

• Vaginal candidiasis is characterized by itchy, curd-like whitish vaginal discharge, dysuria
and dyspareunia
• Gastrointestinal candidiasis may be associated with painful swallowing (odynophagia).
Characteristic lesions are seen on endoscopy.

Pharmacological Treatment
Cutaneous candidiasis
A: clotrimazole cream (topical) 1% apply 12hourly for 2weeks
OR
C: miconazole cream (topical) 2% apply 12hourly for 2weeks
OR

Oral candidiasis
A: nystatin oral suspension - gurgle and swallow 6hourly a day
• Newborns: 200,000–400,000 Units for 24 hours
• <2 years old 400,000–1,000,000 Units for 24 hours
>2 years old 1,000,000–2,000,000 Units for 24 hours
OR
C: miconazole 2 % oral gel apply every 8hourly for 7days

Vaginal candidiasis
A: clotrimazole vaginal pessaries; insert one at night for 6days
OR
C: miconazole vaginal pessaries insert one at night for 3day
AND (if severe)
A: fluconazole (PO) 150mg stat

Gastrointestinal Tract (GIT) candidiasis


A: fluconazole (PO) 150mg 24hourly for 14days

13.2.6 Onychomycosis
It is defined as infection of the nail plate by fungus. Patients with diabetes or peripheral neuropathy
may be at a higher risk.

Clinical presentation
• Yellowish discoloration of the nail
• Subungual hyperkeratosis
• Over time lesions become more prominent and spread until the entire nail is affected

Investigations
• LFT before starting treatment and monitoring monthly.

Pharmacological Treatment
A: fluconazole (PO) 150-300mg once weekly for 6–12months
OR
C: terbinafine (PO) 250mg 24hourly for 6-8weeks. For toe nails the duration of treatment is
generally 12–16weeks.
OR
D: itraconazole (PO) 200mg 12hourly for 7days is given as pulsed dosing, of each month
for 6months

Note
terbinafine and itraconazole should not be used in pregnancy and while breastfeeding

13.2.7 Chromoblastomycosis
Chronic infection involving inoculated after minor trauma e.g. thorn prick.

Clinical presentation
• Nodule that progressively increases in into verrucous plaque

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Pharmacological Treatment
D: itraconazole (PO) 200mg 24hourly for 6-9months

13.2.8 Mycetoma (Madura Foot)


Is a chronic infection of skin and subcutaneous tissue? It can be caused infection by fungi or
bacteria. Once tests have established the etiology, the term Actinomycetoma is used for bacterial
form, while Eumycetoma is used for the fungal form. Clinical presentation depends on the affected
site and the disease can last for months to years.

Clinical presentation
• First lesion: nodule
• Localization: feet, legs, arms, buttocks, scalp, trunk
• Discharging sinuses where grains may be visible usually white yellow for Actinomycetoma
or black for Eumycetoma
• Pain before rupture of discharging sinus

Investigations
• KOH • Local Xray to rule infiltration of
• Biopsy underlying bone.

Treatment of Actinomycetoma (bacteria form)


Pharmacological Treatment
A: co-trimoxazole (PO) 480mg–960mg 12hourly for 5weeks
AND
S: amikacin 7.5mg/kg 12hourly for 5weeks
Alternatively
A: co-trimoxazole (PO) 480mg–960 mg 12hourly for 5weeks
AND
S: dapsone (PO): adult 100mg 24hourly for 2–4months; Paediatric 25–50mg 24hourly for
5weeks

Treatment of Eumycetoma (Fungi


form) Non-pharmacological Treatment
• Surgery where indicated
• Footwear and protective clothing in at-risk populations e.g. cattle herders
Pharmacological Treatment
D: itraconazole (PO) 200mg 12hourly for 5weeks or longer (up to a year).

Referral to surgeon
• Radical surgery for some cases.

13.3 Parasitic Infestations


13.3.1 Scabies
Scabies is an intensely pruritic and highly contagious infestation of the skin caused by mite
Sarcoptes scabies.

Clinical presentation
• Itchy vesicles and papules. Itching worse at night.
• Papules in between finger spaces, wrists, penis and scrotum.
• Someone else in the family is itching.

Non-pharmacological Treatment
• Treat all members of the household at the same time to prevent reinfection, regardless of
presence or absence of itching.
• Advise patients to bath and dress regularly and changing bed linen at the same time of
treatment.

Pharmacological Treatment
A: benzyl benzoate emulsion, BBE (25% for adults, 12.5% for children)
Adults and children over 2 years: Apply with fingers, from neck down to cover the whole-

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body surface, while paying attention to all skin folds. Leave emulsion in place for 6-8 hours
overnight.
Repeat the application after 7 days.
OR
C: lindane lotion (1%) to be applied as BBE above (do not use in children less than 1 year)
AND
C: betamethasone valerate cream (topical) 12hourly for the itch
AND
A: cetirizine (PO) 10mg 12hourly for 3- 4weeks
OR (if extensive, Norwegian scabies)
A: ivermectin (PO) 200microgram/kg stat then repeat after 1week

Should be in combination with the topical above

13.4 Viral Infections


13.4.1 Herpes Simplex
It is an acute viral infection caused by Herpes simplex virus hominis (types HSV1, HSV2 acquired by
close contact with an infected individual

Clinical presentation
• Preceding tingling sensation, discomfort and itching,
• Grouped vesicles forming on the skin, and mucous membranes, particularly the
buccal area, genitalia, conjunctivae, and cornea,
• Eczema herpeticum –herpes simplex infection in Atopic Eczema patients.

Pharmacological Treatment
B: acyclovir cream (topical) applied 4hourly for 7–10days
OR (especially if severe)
B: acyclovir (PO) 200mg 6hourly for 7–10days

For recurrent cases


B: acyclovir (PO) 400mg 12hourly for 6months up to 1year.

Note
Benefit of systemic acyclovir is optimum when given within the first 72hours of onset of symptoms

13.4.2 Chickenpox
It is a highly infectious disease caused by Varicella zoster virus (VZV)

Clinical presentation
• Red macular rash with a • Intense pruritus
central vesicle (blister) on the • Occasional regional
trunk, oral mucosa and scalp lymphadenopathy
• Pustules and crusting

Pharmacological Treatment
B: acyclovir (PO) 800mg 6hourly for 7days
AND
A: paracetamol (PO)1g 8 hourly for 4–5days
AND
A: calamine lotion (topical) 1% phenol, apply over the whole body 12hourly for 7days.

13.4.3 Herpes Zoster (Shingles)


It is due to resurgence or reactivation of the Varicella zoster virus infection which also causes
chickenpox.

Clinical presentation
• Severe burning pain

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• Grouped vesicles overlying erythematous skin following a dermatomal distribution;
typically, lesions do not cross the midline

Pharmacological Treatment
B: acyclovir (PO) 800mg 6hourly for 7–10days

Wound care
A: potassium permanganate soaks (1:4000) 12hourly for 3–4days
For Secondary infection (bacterial) apply
A: silver sulfadiazine cream (topical) applied 12hourly for 5days
OR
C: mupirocin 2% cream 12hourly for 5days

13.4.4 Post-herpetic Neuralgia


A complication of shingles (herpes zoster).

Clinical presentation
Intense pain described as burning, stabbing, or gnawing.

Pharmacological Treatment
A: amitriptyline (PO) 25mg at night, may be increased to 150mg at nightfor 4 weeks
OR
D: pregabalin (PO) 75-150mg 24hourly or divided doses for 2-4weeks

Referral: Refer immediately to Ophthalmologist in case of herpes zoster ophthalmicus for


atropinization

13.4.5 Molluscum Contagiosum


It is viral infection common in children and immunocompromised individuals.

Clinical presentation
• Skin coloured umbilicated papules
• It usually clears without treatment in 12-18months.

Molluscum contagiosum

Pharmacological Treatment:
A: benzoyl peroxide 24hourly for 4weeks
OR
S: tretinoin cream (topical) 2.5 % 24hourly for 4weeks

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Surgical treatment
C: Cryotherapy
D: Curatage

13.4.6 Viral Warts


Infection due to Human Papilloma Virusinclude; common warts, planar warts, and plantar warts, oral
warts.

Clinical presentation
• Verrucous papules on the body, palms, soles, genital and oral mucosa.
• Painful on applying pressure for warts on palms and soles.

Pharmacological Treatment
C: silver nitrate pencil 3times per week for 4weeks for plantar, common warts.
OR
S: tretinoin cream (topical) 2.5% 12hourly for 4weeks for planar warts.

Surgical treatment
C: Cryotherapy
D: Curatage
D: Excision of large warts

Note
For treatment of Genital warts refer to Sexually Transmitted Infections chapter 12

13.5 Eczema (Dermatitis) Conditions


13.5.1 Contact Dermatitis
It is a delayed hypersensitivity reaction following skin meeting a chemical. This may be a dye,
perfume, rubber, nickel, drugs, skin preparations containing lanolin, iodine, antihistamines,
neomycin etc.

Clinical presentation
• Red papulo-vesicular rash with • Blisters, draining fluid
ill-defined margins (weeping) and crusting, with
• Itching, which may be severe severe dermatitis
• Dry, cracked, scaly skin, if • Swelling, burning or
chronic tenderness

Investigations
Patch test
Non-pharmacological Treatment
Avoid contact with allergen

Pharmacological Treatment
A: potassium permanganate soaks, 1:4000 solutions 12hourly for 5days each session
lasting 15-20minutes (For weeping lesions weak)
AND (for mild cases)
B: betamethasone valerate 0.1% cream/ointment 12hourly for 4weeks
OR(for moderate cases)
S: mometasone furoate cream/ointment (topical) 12hourly for 4weeks
OR (IF severe cases)
D: clobetasol propionate 0.05% cream/ointment (topical) 12hourly for 4weeks

Note
A single application with occlusion at night is often more effective than multiple daytime
applications.

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13.5.2 Atopic Eczema
It is a dermatitis/Eczema on a background of atopy. Hence there is often a personal or family history
of atopic disease (asthma, hay fever or atopic dermatitis).

Clinical presentation
• Pruritus- face in children, flexures, of atopy
nape • Acute forms are weepy, chronic
• Chronic or chronic recurrent course forms are lichenified, scaly
• Positive personal or family history

Acute atopic eczema


atopic dermatitis-lichenified and scaly

Investigations
FBP, prick test, patch test, Ig E levels

Non-pharmacological Treatment
• Education about chronicity of problems
• Remove any obvious precipitant e.g. skin irritants or allergens (avoid irritants e.g.
medicated soap, wool and extremes of temperature).
• Generous use of emulsifiers (skin moisturizers)
• Bath oils/soap substitutes

Pharmacological Treatment
A: promethazine (PO) 25mg at bedtime increased to 50mg if necessary, for 2weeks
OR
A: cetirizine (PO) 10mg 24hourly for 2weeks
OR
C: loratadine (PO) 10mg 24hourly for 2weeks
AND
A: hydrocortisone 1% ointment (topical) 12hourly (if mild disease, or on face)
OR
C: betamethasone valerate cream/ointment (topical) 0.1% or 0.25% 12hourly for other
parts of the body.
OR (in severe cases)
D: clobetasol propionate cream/ointment (topical) 0.05% 12hourly for up to 8weeks
OR
S: tacrolimus ointment (topical) 0.03%/ 0.1% 12hourly not less than 1month

In case of skin atrophy on the face and in children >1 year


D: prednicarbate cream (topical) 0.1 % 24hourly for

For severe cases- Erythroderma


Extensive involvement of the whole body
• Patient needs admission
• Oral antibiotics as in impetigo
• Short course of systemic steroid therapy-

A: prednisolone (PO) 0.5 -1mg/ kg 24hourly for 1-2weeks then taper.

• For recalcitrant cases


S: methotrexate (PO) 7.5- 20mg weekly for not less than 3months
OR

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S: cyclosporine 3-5mg/kg/day up to 3months

• Phototherapy

Treat any infection (usually bacterial, but occasionally viral- eczema herpeticum).
Choice of skin preparations depends on whether lesions are wet (exudative) or dry/lichenified
(thickened skin with increased skin markings).
o If eczema is “weepy”, use saline baths or bathe in:
A: Potassium permanganate 1:4000 (0.025%) solution 24 hourly for 2-4 days until dry.
Where large areas are involved give a course of antibiotics for 5-10 days (as for impetigo)
o After the lesions have dried, apply an aqueous cream for a soothing effect.
Start with mild topical steroid cream for wet lesions and use ointment for dry skin lesions.
If the skin starts scaling (condition becomes chronic), add/apply an emollient such as: emulsifying
ointment or liquid paraffin.

Note
Potent topical corticosteroids may cause harmful cutaneous and systemic side effects especially if the
use is prolonged or involves extensive body surface. Striae, acne, hyperpigmentation and
hypopigmentation, hirsutism and atrophy may result. Therefore, avoid long term use; don’t use on
weepy or infected skin. Advise patients NOT to use them as cosmetics (eg for skin lightening purposes)

Example of Classes of Topical steroids;


Very Potent (0.05% clobetasol propionate), Potent (0.1% betamethasone valerate Mometasone
furoate), Moderately Potent (0.05% clobetasol butyrate), Mild (1% hydrocortisone)

13.5.3 Seborrheic Dermatitis


Chronic recurring inflammatory skin disorder associated with Malassezia species.

Clinical presentation
• Erythematous macules, • Scalp, face, chest, back axilla
plaques and groin
• Pruritus

Pharmacological Treatment
A: clotrimazole cream (topical) 12 hourly for 4-16weeks
OR
C: miconazole cream (topical) 12 hourly for 4-16weeks
AND
A: hydrocortisone cream (topical) 0.5% 12 hourly for 4-16weeks
OR
C: ketoconazole shampoo 3 times per week for not less than 3 months

13.6 Anaphylaxis
It is an acute and often life-threatening immunologic reaction, frequently heralded by scalp pruritus,
diffuse erythema, urticaria, or angioedema. Bronchospasm, laryngeal edema, hyperperistalsis,
hypotension, and cardiac arrhythmia may occur. Antibiotics (especially penicillins), other drugs, and
radiographic contrast agents are the most common causes of serious anaphylactic reactions.

Prevention and Non-Pharmacological Treatment


• If acute (existing for less than 3 months), exclude drug reactions (e.g. penicillin), or
infection
• Avoid precipitants

For management refer to emergency and critical care chapter.


13.7 Papulosquamous Disorder
13.7.1. Psoriasis
It is an inherited inflammatory condition of the skin

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Clinical presentation
• Thick, silvery white scaly plaques affecting mainly scalp, sacral region and extensor
body surfaces
• Usually symmetrically distributed, with a chronic relapsing course.
• Can involve joints

Note
Exclude precipitating factors e.g. alcohol, deficiencies of B12 or folate, stress, streptococcal
infections.

Non-pharmacological Treatment
Sun exposure to the lesions for half an hour or one hour daily may be of benefit

Pharmacological Treatment
C: crude coal tar 5% in Vaseline in the morning for not less than 3months
AND
C: salicylic acid 5% in Vaseline to de-scale, apply at night for not less than 3months
AND
C: betamethasone valerate ointment (topical) 0.25% 12hourly for not less than 12weeks.
OR
C: betamethasone dipropionate+ salicylic ointment (topical) 12hourly for not less than
4months

In severe disease
D: clobetasol propionate cream/ointment (topical) 0.05% 12hourly for not less than
4months

For extensive involvement > 20% body surface area and involvement of joints
ADD
S: methotrexate (PO) 7.5-20mg weekly for not less than 6months

Note
Systemic steroids should not be used in psoriasis due to their rebound effect.

13.7.2. Lichen Planus


It is an extremely pruritic chronic inflammatory skin condition.

Clinical presentation
• Primary lesions are violaceous, shiny flat-topped papules
• Coalesce and evolve into scaly plaques
• Distributed over inner wrists, arms and thighs as well as sacral area.
• Post inflammatory hyperpigmentation is common.
• Scarring alopecia may result from lichen planopilaris (severe)

Pharmacological Treatment
C: loratadine (PO) 10mg 24hourly for 2-4weeks
AND
C: betamethasone valerate ointment (topical) 0.1% 12hrly for 2–4 weeks
OR
D: clobetasol propionate ointment (topical) 0.05%–0.1% twice daily for 2–4weeks
AND
for extensive involvement
A: prednisolone (PO) 0.5-1 mg/kg 24hourly for 3-4weeks then taper

For recalcitrant cases


S: methotrexate (PO) 7.5- 20mg weekly for not less than 6months

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13.7.3 Acne
Acne is a multifactorial disease primarily of teenagers with follicular plugging and inflammation.

Clinical presentation
• Open and closed comedones
• Pustules, papules
• Nodular and cystic lesions involving the face, chest, shoulder and the back

Non-pharmacological Treatment
• Avoid underlying precipitating factor e.g. stress, nuts, chocolate, overuse of ointments
on skin, steroids, anticonvulsant drugs etc.
• Encourage a healthy lifestyle – exercise, sunshine exposure, etc.
• Use ordinary soap (harsh antibacterial cleansers or iodine-containing preparations
may aggravate the acne)
• Do not manipulate pustules and nodules

Pharmacological Treatment
Mild to moderate acne without scarring
Apply
A: benzoyl peroxide 2.5%–5% once nocte
OR
S: tretinoic acid cream (topical) 0.05% once nocte

Moderate acne with scarring-


A: doxycycline (PO) 100mg 24 hourly for 1–3 month
OR
A: erythromycin (PO) 250mg 6 hourly for 1–3 month
AND
A: benzoyl peroxide or topical retinoid as above.

Nodulocystic and/or conglobate acne


S: isotretinoin (PO) 0.025–0.5mg/kg 24hourly for at least 3–6months
AND
S: triamcinolone (intralesional) 40mg/ml for cysts stat

Acne fulminans
S: isotretinoin (PO) 0.025–0.5mg/kg 24 hourly for at least 4–6 months
AND
A: prednisolone (PO) 45mg stat then 5mg reduction daily up to 0mg.

Note
Isotretinoin is contraindicated in pregnant women.

13.8 Drug Reactions


Drug reactions can be classified in many ways. One useful approach is to separate predictable
reactions occurring in normal patients from unpredictable reactions occurring in susceptible patients.

Predictable adverse reactions;


• Over dosage (wrong dosage or defect in drug metabolism)
• Side effects (sleepiness from antihistamines)
• Indirect effects (antibiotics changing normal flora)
• Drug interactions (altered metabolism of drugs; most commonly involving the cytochrome
P-450 enzymes)

Unpredictable adverse reactions


• Allergic reaction (drug allergy or hypersensitivity; immunologic reaction to drug;
requires previous exposure or cross-reaction)

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• Pseudo allergic reaction (non-immunologic activation of mast cells).
• Idiosyncratic reaction (unexplained reaction, not related to mechanism of action,
without known or suspected immunologic mechanism).

Note
• 80% of allergic and pseudo allergic drug reactions are caused by Beta-lactam antibiotics,
aspirin, NSAIDs, andSulfonamides

13.8.1 Fixed Drug Eruption (FDE)


It is a cutaneous drug reaction that recurs at the same site with repeated exposure to the agent.

Clinical presentation
• Typically, red-brown patch or plaque
• Occasionally may be bullous
• common sites are genitalia, palms, and soles, as well as mucosa
• Often multiple. Starts with edematous papule or plaque later becomes darker
• Resolves with post-inflammatory hyperpigmentation

Note
• When confronted with hyper pigmented macule on genitalia, always think of Fixed Drug
Eruption

Non-pharmacological Treatment
• Avoidance of triggering drug;

Pharmacological Treatment
A: hydrocortisone (IV) 200mg 12hourly for 24hours
AND
B: betamethasone valerate cream (topical) 12hourly for 2weeks
OR
D: clobetasol propionate cream/ointment (topical) 0.05% 12hourly for 2- 4weeks

13.8.3 Stevens Johnson Syndrome (SJS) and Toxic Epidermal Necrolysis (TEN)
It is a life-threatening condition caused by reaction to drugs e.g. sulphur containing drugs. It causes
the skin to blister and peel off. Less than 10% of body surface area involved. Is referred to as SJS.
SJS progresses to Toxic Epidermal Necrolysis (TEN) with involvement of more than 2 mucosal
surfaces.

Clinical presentation
• Patients usually have prodromal with fever, malaise, and arthralgia’s
• Erosions, hemorrhage and crusts on lips, and erosions in mouth covered by necrotic white
pseudo membrane
• Involvement of the eyes: Erosive conjunctivitis, can lead to scarring
• Involvement of genitalia with painful erosions
• Sudden appearance of diffuse macules or diffuse erythema,
• Early sites of cutaneous involvement are the presternal region of the trunk and the face,
but also the palms and soles.
• Then prompt progression with widespread erythema and peeling of skin; skin lies in sheets
and folds on the bedding.

Pharmacological Treatment
• Identify and discontinue potential offending medications/drugs.
• Transfer patient to intensive care unit or critical care unit or burn unit.
• Wound care
• Keep warm
• Monitor fluid input and output –urine output 0.5-ml/kg/hour. Monitor electrolytes.
• Consultations – Ophthalmologist, Physician, Dermatologist

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SCORTEN SCORE for determining prognosis of patient

• Age >40years • Heart rate >120 beats/ min


• Malignancy • Blood urea nitrogen >28mg/dl
• Total body surface area affected • Serum glucose >250 mg/dl
>10% • Serum bicarbonate <20mEq per 1

Calculate SCORTEN on days 1 & 3 of hospital

stay Pharmacological Treatment


A: hydrocortisone (IV) 200mg 12hourly for 48hours
AND
A: prednisolone (PO) 1–2mg/kg 24hourly for 5–7days

Antibiotics in case of infection (as for treatment of sepsis)

Note
• Topical sulfur containing medications should be avoided.
• Systemic corticosteroids, if employed, should be used early to attempt to abort the immunologic
reaction (first 24 hours).

13.10 Pellagra
Is a disease caused by deficiency of nicotinic acid? Cardinal signs: diarrhea, dermatitis (sites
exposed to sun) and dementia.

Clinical presentation
• Casal’s necklace; hyper-pigmented scaling involving the neck region
• Hyper-pigmented scaly lesions on sun exposed areas

Pharmacological Treatment
Treat both adults and children
A: vitamin B complex (PO) 12hourly for 2months
C: nicotinamide (PO) 500mg 24hourly for 4weeks or until healing is complete;In children:
5mg/kg 24hourly for 4weeks or until healing is complete.

Note
The diet should be rich in deficient nutrients i.e. protein (meat, groundnuts, and beans)

13.11 Vitiligo
Is a condition presenting with patchy depigmentation of skin?

Clinical presentation
• Depigmented patches commonly on the face, neck, trunk and extremities
• Mucosal surfaces particularly oral and genital areas can also be depigmented

Pharmacological Treatment
There is no cure for vitiligo, but there are several treatments that can improve the condition.
C: betamethasone valerate ointment 0.1% 12hourly for 2–4 months
OR
S: tacrolimus 0.1% ointment 12hourly for facial lesions and children
AND
D: clobetasol propionate cream (topical) 0.05% 12hourly
OR
S: PUVA+ sun exposure

Note
Counsel the patient about the condition.

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13.12 Pruritic Papular Eruption (PPE)
A skin condition characterized by itchy papular eruptions on the extensor area of the upper and
lower limbs which is associated with HIV infection.

Clinical presentation
• Papular lesions on the • Excoriation
extensor areas • Lesions heal with
• Extremely itchy hyperpigmented scars

Pharmacological Treatment
C: betamethasone valerate cream (topical) 0.025% 12hourly for 3–4weeks
AND
A: cetirizine (PO) 10mg 12hourly for not less than 4weeks
OR
S: dapsone (PO) 100 mg 24hourly for not less than 4weeks

13.13 Oculo-cutaneous Albinism and Xeroderma Pigmentosum


These are recessive inherited oculo-cutaneous conditions.

Albinism characterized by the complete or partial absence of pigment (melanin) in the skin, hair and
eyes.

Clinical presentation
• Eye problems-photophobia, nystagmus, impaired vision
• Loss of pigment on skin and hair
• Freckles

Xeroderma Pigmentosum
Genetic disorder in which there is a decreased ability to repair DNA damage such as that caused by
ultraviolet light.
Clinical presentation
• Freckling in sun exposed areas • Changes in skin pigmentation
• Dry skin • Extreme photophobia

Non-pharmacological Treatment
• Counseling of parents that are genetic diseases
• People with Xeroderma pigmentosum should avoid sunlight as much as
possible.
• Patients are strongly advised to wear sun protective clothing (long sleeved shirt,
blouse, skirt and trousers and wide brimmed hats to prevent skin cancers)
• Sun protective glasses with special ultraviolet B (UVB) filters
• Advice on indoor income generating activities
• Cryotherapy of early lesions

Pharmacological Treatment
C: Sunscreen applications of SPF 30+ or above, applied twice a day at 8am and noon
AND
S: 5 Fluoro-uracil topical application of early lesions

Surgical treatment
• Excision of lesions
• Refer to oncologist in extensive involvements

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Note
Sunscreen lotions and creams contain physical and chemical products that absorb or scatter
ultraviolet rays that would otherwise cause damage to skin.
Uses of sunscreen;
• Albinism and xeroderma pigmentosum to prevent sunburn, and reduce risk of squamous
cell carcinoma, B cell carcinoma and melanoma.
• Skin conditions e.g. Lupus Erythematosus, dermatomyositis whereby ultraviolet light
exacerbates these conditions
• Normal use to prevent photoaging of the skin

13.14 Urticaria and Angioedema


Chronic recurrent whealing of the skin, with or without angioedema. Associated with atopy.

Clinical presentation
• Wheals which disappear within 24 hours
• With or without Swelling of tongue or lips
• Maybe precipitated by spices, food, food colourants, drugs.

Investigations
• FBP and ESR • Thyroid function test
• Stool for ova and parasite • Prick and patch tests
• Autoantibodies-ANA

Non-pharmacological Treatment
• Avoid precipitating factors e.g. NSAIDs, food, spices
• Treat any infection appropriately fungal, viral if suspect H pylori investigate and treat as per
gastrointestinal section.
• Deworm

Pharmacological Treatment
Antihistamine can be increased to maximum dose for not less than 12weeks

A: cetirizine 10mg 12hourly 4weeks can be increased up to 4 folds


OR
C: loratadine 10mg 24 hourly dose can be increased up to 4 folds
OR
S: desloratadine 5mg 24 hourly for not less than 16weeks
AND
D: montelukast 10mg 24hourly for not less than 16weeks

13.15 Connective Tissue Diseases


Are autoimmune diseases of unknown etiology that affects the skin, blood vessels and internal
organs.

Clinical presentation
Scleroderma
• Localized scleroderma- shiny plaques on the extremities, scalp, hands
• Systemic scleroderma- skin involvement, Raynaud phenomena, internal organ
involvement

Lupus erythematosus
• Discoid Lupus Erythematosus- hypo/depigmented plaques, follicular plugging on the
face mostly
• Systemic Lupus - malar rash, discoid rash, photosensitivity, oral ulcers, arthritis, serositis,
renal disease

Dermatomyositis
• cutaneous-gottrons papules, heliotrope rash
• proximal muscle weakness- inability to comb hair
• inability to rise when squats

279
Investigations
• FBP and ESR
• LFTS
• RFTS
• Urinalysis
• Autoantibodies- ANA, anti-dsDNA, anti-centromere, anti-scleroderma 70, Anti-
phospholipids, Anti- SM
• Creatine kinase levels
• Biopsy
• Monitoring liver, renal and blood count 3 monthly
• RBG every 3 months for patients on corticosteroids for long

Non-pharmacology Treatment
• Ophthalmology review before starting hydroxychloroquine and every 6 months after.
• Monitor blood pressure
• Use of sun protective factor (SPF) lotion and clothing especially for dermatomyositis and
Lupus.
• Keep extremities warm
• Physiotherapy
• Involve physician

Pharmacological Treatment
Deworm- Albendazole 400mg stat
Localized scleroderma:
D: clobetasol propionate cream / ointment (topical) 0.05% 12hourly

Systemic scleroderma
A: prednisolone (PO) 0.5-1mg /kg 24hourly for stabilizing then taper slowly
AND
S: methotrexate (PO) 7.5- 20mg weekly

Discoid Lupus Erythematosus


D: clobetasol propionate cream/ointment (topical) 0.05% 12hourly
AND
S: hydroxychloroquine (PO) 200mg 24hourly for not less 3months

Systemic Scleroderma

D: clobetasol propionate cream/ointment (topical) 0.05% 12hourly


AND
A: prednisolone (PO) 0.5- 1 mg 24hourly for 4weeks then taper to lowest level that is
effective.
AND
S: methotrexate (PO) 7.5- 20mg weekly
AND
A: omeprazole (PO)20mg 24hourly when needed for patients with gastritis, peptic ulcer
disease.

Dermatomyositis
A: prednisolone (PO) 1mg/ kg 24hourly for 12weeks till improvement then start tapering to
lowest effective dose
AND
S: methotrexate (PO) 7.5-20mg weekly for at least 6months

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13:16 Autoimmune Blistering Disease
Conditions in which autoantibodies target components of the skin and mucous membranes, leading
to blister and bullae formation. These include pemphigus vulgaris, foliaceous, vegetans, Bullous
pemphigoid, Dermatitis herpetiformis, Linear IgA.

Clinical presentation
• Tense or flaccid Vesicles and bullae on the skin and mucus membranes
• Vegetative plaques in axillae or groin

Linear IgA
Investigations
• Biopsy • FBP, LFT, RFT
• Immunofluorescence studies

Pharmacological Treatment
C: betamethasone cream/ointment (topical) 12hourly till improves
OR
D: clobetasol propionate cream/ointment (topical) 0.05% 12hourly till improves
AND
A: prednisolone (PO) 0.5-1mg/kg 24hourly for 2months then taper slowly to lowest
effective dose
AND in extensive involvement
S: methotrexate (PO) 7.5 – 20mg weekly for not less than 4months

Treatment of Dermatitis Herpetiformis /pemphigus foliaceous


S: dapsone (PO)100mg 24hourly for not less than 2months

13.17 Keloids
Excessive connective proliferation following an injury or spontaneously.

Clinical presentation
• Skin coloured nodules, plaques extending beyond the scar line commonly on
earlobes.

Pharmacological Treatment
S: triamcinolone (intralesional) 2.5-5mg/ml monthly for 4-6months for small – medium
sized keloids.

Surgical treatment
S: total excision or debulking of keloids Inj Triamcinolone 20mg intraoperatively and post
operatively for 3 months.

13.18 Folliculitis Decalvans


Characterized by pustules, papules, keloids and scarring alopecia on the nape of the scalp.

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Pharmacological Treatment
A: doxycycline (PO) 100mg 12hourly for 2-4weeks
OR
S: clindamycin (PO) 300mg 12hourly for 3months
AND
D: clobetasol propionate cream/gel (topical) 0.05% 12hourly for not less than 16weeks
ANDin recalcitrant cases
S: dapsone (PO) 100mg 24hourly for 6months

13.19 Infantile Haemangioma


Benign vascular tumor which appears at birth and continues growing till 9 months then starts
involuting.

Clinical presentation
• Red macule at birth haemangiomas (mainly facial),
• Grows progressively arterial, cardiac, eye, and sternal
• regresses from 9-12 months anomalies
• May be part of PHACES syndrome;
Posterior fossa malformation,

Indications for treatment


• If interferes with feeding
• If interferes with breathing
• If interferes with vision

Investigations
• FBG before initiating treatment and • Record heart rate and blood
serially after pressure before treatment
• ECG
Pharmacological Treatment
A: propranolol (PO) 1mg/kg divided into 3doses given 8hourly in 24hours.

Monitor heart rate and blood pressure 2hourly for 3days if tolerated
Increase the above-mentioned medication to 2mg/kg/day in 3divided doses till lesion regresses
Adjust with change in weight.

Note
Request your pharmacist to prepare the syrup.

13.20 Cysts
Slow growing cystic structures.
Include- Epidermoid cysts, Trichilemmal cysts, dermoid cyst

Treatment
• Excision
13.21 Skin Lightening
Skin lightening or skin bleaching is a cosmetic process that aims at lightening the dark areas of skin.
Some of the products used are strong topical corticosteroids e.g. clobetasol propionate,
hydroquinone, glutathione, lightening soaps, local concoctions etc. Melasma is a skin condition
whereby medical treatment is to lighten dark patches. However, in most situations women and men
desiring to have fairer skin go into great lengths to achieve this and end up with some reversible and
irreversible changes.

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Reversible conditions
• Tinea incognito – refer to treatment • Scabies – refer to scabies
of tinea treatment
• Steroid acne – refer to acne • Perioral dermatitis- Tacrolimus
treatment ointment

Irreversible conditions
• Stria
• Telangiectasia
• Atrophy
• Hirsutism
• Ochronosis
• Poor wound healing

Health Education
• Users should stop before they get
permanent irreversible changes.
• Use sunscreen lotion to protect
from ultraviolet damage.

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CHAPTER FOURTEEN
EYE DISEASES AND CONDITIONS

14.1 Major Blinding Eye Diseases


Eye Diseases are conditions affecting the eye. Diseases of most important are those leading to
blindness or visual impairment. Blindness is defined as a presenting visual acuity of less than 3/60
or central visual field of less than 10º in the better eye. The definition of blindness in children and
infantsis the same as that in adults though there are different methods for testing vision in young
children until when they are at preschool age when normal visual acuity chart can be used.The
common causes of blindness and visual impairment among adults are Cataract, Glaucoma,
Cicatricial Trachoma, Vitamin A deficiency (discussed under nutrition chapter) and other corneal
opacities, diseases of the Retina, uncorrected Refractive Errors and Low Vision. These are diseases
that affect both eyes however, they may be asymmetrical in their course. There are other eye
diseases that do not lead into blindness or visual impairment, these are also addressed in this
section. Patients presenting to eye clinic with uniocular eye complaint must have basic examination
of the fellow eye as well.

14.1.1 Cataract
Cataract is clouding of the lens of the eye which prevents clear vision. It may be as a result of
ageing process or secondary to trauma or inflammatory diseases. Children may be born with
cataract or develop cataract in the early ages of life.

Clinical Presentation
• Various degrees of vision • Cloudiness in the lens seen as a
impairment unilateral or bilateral white mark behind the pupil and iris
• History of trauma with a sharp seen with slit lamp microscope
object for traumatic cataract • Conjunctiva and cornea are clear
• History of red eye for secondary and the whole iris can be seen
cataract. clearly
• Glare and haloes around light • Obscured red reflex

Note
• Cataract may present in all age groups, blindness due to cataract is reversible
• Treatment is only by surgery
• Early treatment in children is mandatory
• White pupil in children may be a tumor in the eye, late referral may lead to permanent
loss of vision, squint, loss of eye or loss of life

Investigations For congenital cataract, the following


• Visual acuity additional investigations may be
• Slit Lamp Bimicroscopy ordered with Paediatrician
• Refraction depending on the consultation
density of cataract • ECG
• Dilated Fundoscopy • Echocardiogram
• B Scan if no fundal view • Haemoglobin
• A Scan • Full blood picture
• Biometry for Intraocular (IOL) • Chest X Ray
calculation • Blood grouping and Cross-
matching

Surgical Treatment
The only treatment available for Cataract is surgery. There are different cataract surgical procedures
depending on the causes of cataract, age of the patient and surgeons’ skills and equipment
availability.

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Pharmacological Treatment
Preoperative Treatment
A: amethocaine hydrochloride 1% Eye drops
OR
C: tetracaine 0.5% Eye drops
AND
C: tropicamide 1% +phenylephrine 2.5% (FDC) Eye drops
Alternatively
C: tropicamide 1% Eye drops
AND
A: iodine 2.5 – 5% Eye Drops
AND
A: lignocaine hydrochloride with adrenaline 2%, combined with hyaluronidase 1500IU, 5
mL, retrobulbar or Subtenon injection stat,

OR
A: lignocaine hydrochloride, combined with hyaluronidase 1500IU, 5mL, retrobulbar or
subtenon injection stat,
Intraoperative Treatment
A: adrenaline 0.5mL infusion in 500mL compound sodium lactate intracameral in during
the surgery
AND
C: trypan blue 0.06% injection, 0.4mL intracameral, stat
AND
S: sodium hyaluronate 1% Intracameral and topical stat
AND
S: acetylcholine chloride 1% Injection, 0.5ml intracameral stat
AND
B: dexamethasone phosphate 1.25mg intracameral injection stat
AND
A: gentamycin 1.25mg intracameral and subtenon injection stat
OR
B: ceftriaxone 5mg intracameral and subtenon injection, stat

In addition to the above intraoperative medicines, in children and patients with preoperative
ocular inflammatory conditions, use
S: triamcinolone acetone 20mg injection, Sub tenon, stat
OR
D: methylprednisolone 20mg injection, Sub tenon, stat

Postoperative Treatment
C:dexamethasone + chloramphenicol 0.1 – 0.5%, 1 -2 Drops in the operated eye, 2hourly
for 7days then 4hourly for days
OR
C: dexamethasone + gentamicin 0.1 - 0.3%, 1 – 2 Drops in the operated eye, 2hourly for
7days then 4hourly for 7days
AND
C: cyclopentolate 1%, 1 – 2 Drops in the operated eye, 12hourly for 14days
OR
B: atropine 1%, 1- 2 Drops in the operate eye, 24hourly for 14days
AND
C: acetazolamide (PO) 500mg, stat
AND
A: paracetamol (PO) 1 gm, 8hourly for 3days
THEN:

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D: prednisolone 0.5%, 1 – 2 Drops, 6hourly for 4weeks

Note
• Atropine is given to patients where excessive inflammation is anticipated such as cataract
surgeries in children, traumatic cataract and secondary cataract.
• Children may require longer term and more frequent topical steroids depending on their
postoperative response

Referral: Refer all cases to eye surgeon for cataract surgery, available at some of the Districts,
Regional, Zonal and National Hospitals. Children should be referred immediately to a Tertiary Health
Facility with capacity to operate children’s eyes safely.

14.1.2 Glaucoma
Glaucoma is a syndrome characterized by optic nerve damage and peripheral visual field loss which
may be associated with raised intraocular pressure. The main classes of glaucoma are open angle
glaucoma and angle closure glaucoma.

Note
Glaucoma may be congenital, primary or secondary to other secondary to ocular conditions

14.1.2.1 Primary Open Angle Glaucoma


Clinical presentation
• Painless loss of peripheral vision leading to absolute glaucoma as the end stage
• Affects mainly adults of 40 years of age and above
• Cornea and conjunctiva are clear
• Pupil in the affected eye does not react with direct light in advanced stage
• The optic nerve is always damaged, this can be seen through fundoscopy
• One eye may be affected more than the other
• First degree relatives of glaucoma patients are at increased risk

Note
• Primary Open Angle Glaucoma does not have symptoms in early stages, hence routine
intraocular pressure checkup and fundus examinations should be done in all people of 40
years and above by some qualified eye care personnel on annual basis.
• All suspected cases of glaucoma should be referred to qualified eye care personnel for
confirmation of diagnosis and commencement of treatment plan
• Surgical treatment is usually preceded by medical treatment
• Refilling of antiglaucoma may be prescribed by a middle cadre eye worker but annual
monitoring should be done at a centre where there is an Ophthalmologist
• For advanced and complicated Glaucoma, patients should be referred to a health facility
where there are Glaucoma Specialists

Investigations:
• Visual Acuity • Refraction
• Slit Lamp bimicroscopy • Visual Field Analysis
• Fundoscopy • Fundus Photography
• Tonometry • Pachymetry test
• Gonioscopy • Optical Coherent Tomography

Pharmacological Treatment
This is initiated after a diagnosis is reached by an ophthalmologist, refill of some medicines can be
done by Assistant Medical Officers in ophthalmology but with regular reviews at a health facility with
eye specialist. Medical treatment should be lifelong unless there are conditions necessitating other
interventions
C: timolol 0.25% or 0.5%, one drop in the affected eye, instill 12hourly.
OR

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D: betaxolol 0.25% or 0.5%, one drop in the affected eye, instill 12hourly. Use lower
strength in mild disease and those at risk of complications.

In patients who comply to treatment and there is no good response


ADD
D: latanoprost 0.005% one drop, 2hourly in the affected eye.
OR
D: prostamide bimatoprost 0.03%, one drop, 24hourly in the affected eye.

• These may be used as first-line in patients with contraindication of beta-blockers.


• They can be used as a second-line drug in patients on beta-blockers if the target IOP
reduction has not been reached.

In patients who are intolerant to prostaglandin analogue or are not responding give:
D: brimonidine tartrate 0.15–0.2%, one drop, 12hourly, in the affected eye.
OR
S: dorzolamide 20mg/mL, one drop, 8hourly in the affected eye

Failure to respond give:


C: pilocarpine hydrochloride 2% or 4%, instill one drop in the affected eye 6 hourly.

Note
Pilocarpine causes long-standing pupil constriction so it should not be used unless a patient is
prepared for glaucoma
surgery or as an alternative topical treatment for patients who are contraindicated for Timolol use.
Consult a specialist
before using it.

In severe cases or while waiting for surgery, use:


C: acetazolamide (PO) 250mg 6hourly

Note
• β-blockers are contraindicated to people who are known to have overt asthma as this
group of medication may cause an acute asthmatic attack within a short time following
instillation into the eye
• Brimonidine is contraindicated in children below 12years

Laser Treatment
• It may be indicated in addition to or instead of eye drops or surgery.
• Laser trabeculoplasty (Argon Laser Trabeculoplasty, Selective Laser Trabeculoplasty) or
cyclophotocoagulation are different options among others

Surgical Treatment
It is done in all patients with poor compliance and when medical treatment is not useful. There are
different surgical techniques depending on the age of the patients, patients’ response to surgical
treatment, surgeons’ surgical skills and availability of equipment. It is recommended that all
surgeries are done by Ophthalmologists after thorough assessment of the patients.
14.1.2.2 Angle Closure Glaucoma
This is also known as Congestive glaucoma and commonly affect people aged 40 years and above.
It affects more females than males.

Clinical Presentation
• Acute sudden onset of painful red • Shallow anterior chamber
eye in the affected eye • Fixed and semi-dilated pupil
• Severe headache and cloudiness
of the cornea

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• Severe elevated intraocular • It may be asymptomatic if IOP
pressure. raises slowly
• There is usually dramatic visual
impairment and vomiting may be
present

Note:
• Primary acute Angle Closure Glaucoma is an Ophthalmological Emergency
• Refer all patients with Congestive glaucoma to eye specialist after initial medical treatment
to lower Intraocular pressure

Investigations:
• Visual Acuity • Gonioscopy when cornea clear up
• Slit Lamp bimicroscopy • Visual Field Analysis for chronic
• Fundoscopy when cornea clear up disease
• Tonometry

Pharmacological Treatment
Institute therapy and then refer the patient to eye specialist at the Regional, Zonal or National
Hospital for investigations and proper management.
Try to achieve immediate IOP reduction

First-Line Treatment
C: acetazolamide (PO), 500mg immediately as a single dose followed by 250mg 6hourly

AND
C: timolol 0.25–0.5% eye drops, instill one drop 12hourly in the affected eye

Use the above combined treatment until you have achieved your target IOP reduction, then continue
with only Timolol eye drops for life unless patient has received surgical intervention and the IOP is
reduced to normal level.

Note
Manage the associated pain and vomiting

Second-Line Treatment
If the above measures fail, use as a short-term treatment, givesystemic osmotic agents:
C: mannitol 15–20% (IV)1.5–2mg/kg body weight to run slowly over 30–60minutes

These medicines have diuretic effects, so they are only used as a single dose. They are also used in
emergencies to prepare patients with high intraocular pressure for surgery as they lower intraocular
pressure rapidly.

Note
Acetazolamide is a Sulphur containing medicine, do not use in patients allergic to Sulphur.

Surgical Treatment
This is done at a centre with Eye Specialists and necessary diagnostic and treatment equipment.
Surgical or Later Peripheral Iridectomy will create a passage for the aqueous fluid from posterior
chamber to the drainage angle.

Referral: Management of advanced angle closure glaucoma is done by eye specialist. All patients
with Angle Closure Glaucoma should be referred to eye specialist for other management modalities.

14.1.2.3 Childhood Glaucoma


• Presents from birth to 5 years.
• It is a syndrome whereby the intraocular pressure is raised and cause abnormality of the
eyeball and visual disturbances including blindness.

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Clinical Presentation
• Patients presents with eyes bigger • Cloudy cornea,
than normal for age (buphthalmos) • Red conjunctiva though not severe.
• Photophobia • Decrease in visual acuity
• Tearing

Investigations
For children, examination is done under General Anaesthesia
• Tonometry • Fundoscopy
• Cornea Diameters • Gonioscopy depending on corneal
• Slit lamp examination visibility

Surgical Treatment
Treatment for congenital glaucoma is usually surgery, which is done by Pediatric Ophthalmologist or
Glaucoma specialist.

Referral: Refer any child who has the above-mentioned signs and you suspect that he/she is having
congenital glaucoma to a specialist at the National Hospital or Zonal Referral Hospitals where there
is Paediatric Eye team.

14.1.2.4 Secondary Glaucoma


This presents as a complication of other eye diseases such as uveitis, hypermature cataract, trauma
and retinal diseases. It may also be due to prolonged use of steroids.

Clinical Presentation
• Poor vision in the affected eye • Optic nerve damage
associated with • New vessels on the iris if the cause
• High intraocular pressure is retinal diseases

Investigations
• Visual Acuity • Refraction
• Slit Lamp bimicroscopy • Visual Field Analysis
• Fundoscopy • Fundus Photography
• Tonometry • Pachymetrytest
• Gonioscopy • Optical Coherent Tomography

Pharmacological Treatment
Management of these patients depends on the cause, but it includes medical, surgical and laser.
Institute these treatment as you refer these patients: -

C: acetazolamide (PO) 500mg immediately stat followed by 250mg 6hourly


AND
C: timolol 0.25–0.5% eye drops, instill one drop 12hourly in the affected eye.
Treatment of the preexisting eye disease is highly recommended.

Referral: Refer all patients suspected to have secondary glaucoma to a qualified eye specialist
available at the Regional, Zonal or National Hospital for proper assessment and definitive
management.

14.1.3 Trachoma
It is a chronic conjunctivitis caused by infection with Chlamydia trachomatis (bacteria). It is one of
the commonest causes of blindness worldwide. There is a chronic inflammation of the conjunctiva
leading to scarring of the upper eyelid tarsal plate, entropion and in turn of eyelashes.

289
Clinical presentation
• Photophobia in early stages or re- • In late stages, in-turned eyelashes
infection rub on the cornea leading to
• More than 5 Follicles in the upper corneal ulcers
tarsal plate seen as round and • Loss of vision due to corneal
white nodules in active diagnostic. scarring.

Clinical Stages according to World Health Organization


• Trachomatous Inflammation Follicular (TF) - Presence of at least 5 follicles on the upper
tarsal plate
• Trachomatous Inflammation Intense (TI) – There is intense inflammation, the conjunctival
blood vessels cannot be seen.
• Trachomatous Scarring (TS) – Presence of white scars in the upper tarsal plate
• Trachomatous Trichiasis (TT) – Presence of some eye lashes rubbing against the cornea
• Corneal Opacity (CO) – Presence of corneal opacity (scar) affecting the central cornea

Investigations
• Visual acuity
• Slit lamp bimicroscopy
• Conjunctival swab for dipstick test and or PCR

Non-pharmacological Treatment
• Face washing and total body hygiene to prevent transmission of disease from one person
to the other
• Environmental improvement/hygiene

Pharmacological Treatment
A: oxytetracycline eye ointment 3% 24hourly for 6weeks
OR
B: azithromycin (PO)1g stat- for preventive chemotherapy in mass treatment
campaign

Table 14.1: Dosage of Azithromycin in Children


Weight (kg) I-day regimen
< 15 20mg/kg 24hourly
15 – 25 400mg 24hourly
26 – 35 600mg 24hourly
36-45 800mg 24hourly
> 45 Dose as per adults

Note
Preventive chemotherapy in mass treatment campaign is conducted only once a year

Surgery
Surgical correction of entropion in TT patients. This procedure can be done at a Dispensary or
Health Centre and community level by a trained health worker.

Referral: Refer all patients with recurrent TT or lower Eyelid TT to Oculoplastic Surgeon at Regional
Referral or Zonal Referral Hospital for proper assessment and surgical management.

14.1.4 Diseases of the Retina


Main diseases of the retina that cause blindness are Diabetic Retinopathy, Diabetic Macular Edema,
Retinal Detachment and Age-related Macular Degeneration.

14.1.4.1 Diabetic Retinopathy


• It is a complication of diabetes mellitus in the eyes

290
• It is a chronic progressive sight-threatening disease of the retinal blood vessels associated
with the prolonged hyperglycemia and other conditions linked to diabetic mellitus such as
hypertension

Clinical Presentation
• Loss of vision in advanced stages, when there is retinal haemorrhage or cataract
• In early stages it may be asymptomatic
• Regular and annual screening at Diabetic or Eye Clinic is recommended for early
diagnosis.

Diabetic retinopathy is mainly grouped into three stages/presentations:


• Background diabetic retinopathy
• Diabetic maculopathy
• Proliferative diabetic retinopathy

Investigations
• Visual acuity with and without • Fundus photography
pinhole • Fluorescein Angiography
• Tonometry • Optical Coherence Tomography
• Dilated fundoscopy (Direct or
indirect ophthalmoscopy with or
without biomicroscopy)

Note
Dilate the pupils with combined
C: Tropicamide 1%/Phenylephrine 2.5% eye drops
OR
C: tropicamide 1% with
C: cyclopentolate 1% eye drops to screen

Table14.2 below gives a summary of the Stages of Diabetic Retinopathy at Eye Clinic, treatment
options and Follow up schedule. Treatment is done in consultation with Diabetologist and Physician
to ensure a good glycaemic and blood pressure control

Table 14.2: Treatment options for various grades of DR


Grade Treatment Options Follow-up
No retinopathy a. Patient counseling 9 -12monthly
b. Strict control of blood sugar,
pressure and lipids
Mild or Moderate Non-Proliferative a. No active treatment required 6-9monthly
Diabetic Retinopathy (NPDR) b. Patient counseling
c. Control of blood sugar, pressure
and lipids
Pre-proliferative DR
Severe NPDR * Close follow up for dilated fundoscopy 2-3monthly

Very severe NPDR * Partial scatter PRP therapy (maximum 3monthly


LASER burns 800 spots)
Mild Proliferative DR** Full scatter PRP minimum 1200 shots in 2monthly
(NVD/ NVE one sitting or/ and
No pre-retinal or vitreous Anti-VEGF injection***
hemorrhage
No Fibrovascular membrane <FVM>)
Moderate PDR ** Full scatter PRP up to Ora-serrata sparing 3monthly
(NVD/NVE, Moderate to severe the macula and away from the FVM ***
Vitreous hemorrhage with visible
fundus details for PRP, Pre-retinal
Hemorrhage
No FVM)

291
Severe PDR ** REFER To VR clinic
(NVD/NVE, Severe Vitreous
hemorrhage obscuring fundus
details/not visible for PRP,
Extensive FVM, Tractional Retinal
Detachment <TRD>
Macular traction)

* LASER treatment should also be considered in our settings in patients with severe and very severe
NPDR with the following situations as it has shown to reduce the rate of vision loss by half: -
i. Older type 2 diabetics
ii. Difficult retinal view
iii. Prior to cataract surgery
iv. Only eye situation where the first eye was lost due to PDR
v. Regular attendance to clinic for follow up is likely to be poor
vi. Difficult to examine patient due to other reasons.
** Monthly intra-vitreal anti-VEGF injections has been found to be effective on treatment for PDR
*** Mild and moderate PDR should be treated with full scatter PRP (minimum 1200 shots in one
sitting) or intravitreal anti-VEGF injection whichever is available, accessible and affordable. If both
are available and affordable then anti-VEGF injection is the treatment of choice provided the patient:

i. Is able to come for follow up at regular intervals- every month for 3 months and
then every 2 months for 3 months and then 3monthly
ii. Can afford the injections which may total up to 6 injections in the first year
iii. Has no contraindications to the injections?
If any one of the above does not apply, then the patient should have PRP done.

Treatment options for DME


Management of DME depends on the clinical stage of DME and treatment options available at the
facility where the patient has been attended.

Primary tests are required to be performed in order to grade the DME. Macula OCT for all diabetic
patients should be the baseline test to determine presence or absence of DME. Macular thickness of
equal or more than 400 microns should be considered as DME. Those facilities without this tool, the
clinical assessment will be the baseline test where the best corrected visual acuity will be the key
point for grading which will be matched with the clinical findings. Therefore, VA of less than 6/12
should be considered as DME case. It is important to exclude other causes of visual impairment
before concluding the presence of DME. Use of anti-VEGF has been found to be effective in the
treatment of DME.

Table14.3: Treatment options for various grades of DME


Grade Treatment option Follow up period
No DME Close observation review after 6 to
12months
Non-Centre Focal or Grid LASER 3-6months
involving DME
Centre involving 3 intravitreal anti VEGF injections at monthly interval Every 1 month
DME followed by 3 more injections at 6 weekly intervals.

After 6 injections, refer patient to VR clinic if


a. VA is not improving
b. There is clinically persistent DME

If anti VEGF injection is not available:


i. Grid LASER should be given for diffuse,
Exudative or edematous macular edema
ii. Focal LASER to areas of focal Exudative edema

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Pharmacological Treatment
For glycemic control give antioxidant in non-proliferative diabetic retinopathy
C: multivitamin +carotenoids (PO) 24hourly to a maximum of 3months

For intravitreal anti Vascular Endothelial Growth Factor (VEGF) in Proliferative Disease
S: bevacizumab, 1.25mg per 0.05ml, intravitreal injection, stat.
OR
S: ranibizumab, 0.5mg per 0.05ml, intravitreal injection stat.

Repeat after every month to a maximum of 3 months then 6weekly to complete 6 injections. Re-
assess on 3 monthly basis if there are signs of disease progression, restart treatment if any, with
close follow up.
AND
S: triamcinolone acetonide, 0.05ml, intravitreal injection, stat. Repeat after 3months if it is
necessary. This is indicated in Diabetic Macula Edema.

Surgical Treatment
• This is done in the proliferative stage
• It involves removal of vitreous and or blood, peeling of formed fibrovascular tissue and
reattachment of retina if the retina is detached
• It is combined with retinal photocoagulation
• The vitreous cavity may be filled with tamponade liquid such as silicon oil or expansile gas
like sulfur perfluoropropane or sulphur hexafluoride depending on the level of complication
• It may also be combined with pharmacological treatment (Anti VEGF) mentioned above

Laser Treatment
Laser photocoagulation: Extent and type of this treatment depending on the stage of the disease
• Focal Laser • Pan Retinal Photocoagulation for
• Grid Laser advanced disease

Note
• Ophthalmologists should work together with Physicians to holistically treat the diabetic
patient.
• Poorly controlled diabetes mellitus and diabetic retinopathy can lead to blindness
• All patients with diabetes mellitus regardless of their eye conditions, should have a
thorough eye examination by available eye care personnel or an eye specialist at least
once a year.
• Dilated eye examination and direct viewing of the retina by an ophthalmologist or
qualified eye care personnel is mandatory at initial diagnosis of Diabetes Mellitus and
as per recommended schedule by the attending clinician.
• Urgent referral of all diabetic patients with sudden loss of vision to eye specialist

14.1.4.2 Age Related Macular Degeneration


It is a disease condition characterized by progressive macular changes that are associated with
increase in age.

Clinical Presentation
• Drusens around macula area (yellowish excrescence in the retina)
• Affects elderly over 60 years
• Poor central vision, later can lead to blindness

Investigations
• Visual Acuity • Fundoscopy through a well-dilated
• Refraction pupil,
• Tonometry • Fundus photography

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• Optical Coherence Tomography • Fluorescein angiography.
and or

Pharmacological Treatment
• This depends on clinical presentation.
• Intravitreal injection in the affected eye

S: bevacizumab 1.25mg per 0.05ml stat


OR
S: ranibizumab 0.5mg per 0.05ml stat.

Give Antioxidant in non-proliferative Diabetic Retinopathy


C: multivitamin + Beta-carotenoids, Zinc Sulfate and Lutein, 1 tablet once daily to a
maximum of 3 months

Surgical Treatment
Type of surgery depends on the presentation/ stage of the disease.

Referral: Refer patients with Age Related Macular Degeneration to Vitreo-retinal Surgeons for
proper management

14.1.5 Refractive Errors


This is a condition where one presents with poor vision either at near or distance at any age. There
are mainly 4 types of refractive errors namely presbyopia, myopia, astigmatism and hyperopia. A
patient may have more than one type of refractive error.
14.1.5.1 Presbyopia
This is a disorder of refractive status commonly occurring in older people.

Clinical presentation
• It usually starts after the age of 40 years
• The main complaint is difficulty in reading/writing or doing near works
• Diagnosis is only through refraction. Attendance to heath facility is also a good opportunity
for screening of glaucoma and diabetic retinopathy

Investigations
• Visual acuity • Refraction
• Tonometry • Stereopsis test
• Fundoscopy • Colour vision test
Non-pharmacological Treatment
Convex lens spectacles for near vision.

14.1.5.2 Myopia (Short sightedness)


Thisis a condition whereby patient has difficulty seeing far objects.

Clinical presentation
• It is common in young age between • If not treated early, it may progress
5–25 years rapidly and lead to retinal
• The condition persists throughout complications
life • It is diagnosed through refraction.

Investigations
• Visual acuity • Colour
• Refraction • Strabismus assessment in all
• Fundoscopy children
• Stereopsis test

Non-pharmacological Treatment
Concave lens spectacles for constant wear.

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14.1.5.3 Hypermetropia (Long sightedness)
This is a condition where patients have difficulty in seeing near objects. It is less manifested in
children as they have a high accommodative power.

Clinical presentation
• Ocular strain
• Diagnosis in children should be reached after refraction through a pupil that is dilated

Investigations
• Visual acuity • Colour
• Refraction • Strabismus assessment in all
• Fundoscopy children
• Stereopsis test

Non-pharmacological Treatment
Convex lens spectacles for constant wear
Note
Spectacles should be given to: -
• Children who have only significant hypermetropia (more than +3.00 Diopter of Sphere both
eyes), all children who present with squint and have significant hypermetropia and children
with anisometropia
• Elderly who present with signs of ocular strain

14.1.5.4 Astigmatism
This is a condition where the cornea and sometimes the lens have different radius of curvature in all
meridians (different focus in different planes). Some myopic and hyperopic patients may have
astigmatism.

Clinical Presentation
• Poor vision at distance, • Diagnosis is reached through
• Photophobia refraction
• Headache (sometimes).

Investigations
• Visual acuity • Colour
• Refraction • Strabismus assessment in all
• Fundoscopy children
• Stereopsis test

Non-pharmacological Treatment
Cylindrical lenses spectacles for constant wear.
Note:
• Reassessment for all types of refractive errors is done annually and change the spectacles
of there are significant variation and improvement with new correction.
• All children with rapid progression of refractive errors need to be seen by Paediatric
Optometrist and Paediatric Ophthalmologist for further assessment

14.1.6 Low Vision


Low vision is irreversible visual loss that cannot be corrected with surgeries or spectacles resulting
in reduced ability to perform many daily activities. They have visual impairment even with treatment
and or standard refractive correction and

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Clinical presentation
Inability to
• Recognizing people in the streets, • Playing with friends.
• Reading black boards, • Visual acuity from less than 6/18 to
• Writing at the same speed as peers perception of light and a reduced
and central visual field.

Investigations
• Visual acuity • Fundoscopy
• Refraction • Low vision assessment
• Tonometry • Orthoptic Assessment

Non-pharmacological Treatment
• Assessment of the patients’ visual function
• Accurate refraction and provision of spectacles if indicated
• Low vision devices such as optical devices (magnifiers, telescopes) and or non-optical
devices (reading stands and or reading slits) as per assessment results.
• Surgical intervention is indicated e.g. if a patient has cataract

Referral: All children with low vision should be referred to high level health facility for proofer
assessment and management by a paediatric Eye Team

14.2 Painful Red Eyes


The eye conditions shown on Table 14.4 presents with an acute onset of red eyes: ocular trauma,
corneal ulcer, uveitis and conjunctivitis. The Table also summarizes the diagnostics of red eyes.

Table 14.4: Summary on diagnosis of Red Eyes

Disease Visual Affected Cornea Pupil Pain Discharge


Condition Acuity Eye
Allergic/ viral Good Both Clear Normal No Watery/mucoid
Conjunctivitis
Bacterial Good Both Clear Normal No Purulent
Conjunctivitis
Ophthalmia Poor +/- One/both Cloudy Normal +/- Yes Copious
neonatorum +/- purulent
Cornea ulcer Poor One/ both Gray Normal Yes Watery/purulent
spot
Uveitis Poor One/ both Clear or Small & Yes Watery
cloudy Irregular
Acute glaucoma Poor One Cloudy Mid Yes Watery
dilated

14.2.1 Ocular Trauma


These are eye injuries that may result from blunt or sharp objects or from chemical substances.The
management of these injuries is guided by history from the patient and ocular findings by the
clinicians. Classes of ocular trauma are as follows: -

14.2.1.1 Blunt Trauma/Perforating Eye Injury/Foreign Body


Establish the cause to determine the type of injury and whether there is penetration.

Clinical presentation
• Corneal abrasion/laceration with or without an imbedded foreign body.
• Eye lids may also be involved.

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Investigations
This is done after the first aid measures
• Visual acuity • Fundoscopy in blunt injury or
• Examine the injured eye with slit embedded foreign body
lamp or magnifier • B scan in embedded foreign body
• Fluorescein staining to reveal • CT Scan in suspected metal foreign
foreign body or corneal laceration body
• Tonometry in blunt injury

Non-pharmacological Treatment
• Provide first aid measures to the patients as per presentation
• If no penetration, irrigate the eye with clean water or Ringers Lactate to reduce chemical
substance in the eye
• Remove foreign body if visible with a cotton bud or surgical blade if shallow.

Pharmacological Treatment
At the primary care:

Corneal Abrasion:
A: chloramphenicol eye ointment 1%, 8hourly to the injured eye until no
fluorescein staining

Steps Guiding Management of Complicated Blunt Trauma


Complicated blunt trauma is a trauma where the vision is poor, patient’s experiences pain and there
is hyphaema. It is best managed by eye specialist as surgery may be required in the management.

Table 14.5: Steps guiding management of complicated blunt trauma


Findings Action to be taken
No hyphema, normal vision Observe
Hyphema, no pain Refer
No hyphema, normal vision, pain Paracetamol, observe for 2 days, refer if pain persist
Poor vision and pain Paracetamol, refer urgently
Hyphema, pain, poor vision Paracetamol, refer urgently

14.2.1.2 Deep Corneal or Scleral Injuries


These are corneal or scleral injuries caused by sharp objects.

Clinical presentation
• History of injury with a sharp object such as knife or wire
• Swollen eye
• Eye discharge

Investigations
• Visual acuity • Fluorescein staining to reveal
• Examine the injured eye with slit foreign body or corneal laceration
lamp or magnifier • Fundoscopy

Non-pharmacological Treatment
• Apply an eye shield or pad with no pressure and refer immediately

While waiting for referral, use the following in the affected eye:

Pharmacological Treatment
A: chloramphenicol 1% eye drop, 2 drops stat
OR
A: chloramphenicol 1% ointment, stat
AND

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B: atropine 1%, 1–2 drops stat
AND
A: tetanus toxoid (IM) 0.5ml stat as prophylaxis
AND
A: paracetamol (PO)1gm 4–6hourly to a maximum of 4 doses in 24hours, for 3days in
adults, the dosage in children is 10–14mg/kg 4–6hourly for 3days.

Referralindicated if
• Intraocular foreign body is suspected
• There is globe or intraocular penetration evidenced by:
o Poor vision,
o Distorted pupil
o Ocular contents of foreign body is seen
o Circumferential subconjunctival hemorrhage
o Hyphaema with or without raised intraocular pressure
• Conjunctival laceration requiring suturing (>1 cm)
• Laceration/perforation or diffuse damage to the cornea and sclera
• Chemical and thermal injuries
• Damage to ocular adnexa including eyelids
• Limited ocular movements

Surgical Treatment
This is done by a well-trained eye specialist at the District, Regional, Zonal and National hospitals. It
should be done within 48 hours of injury. Post-operative care should be monitored regularly for any
signs of endophthalmitis.

Note:
• Eye ointment should be applied very gently and in the lower fornix (behind the lower
eyelid).
• Do not apply pressure on the eye in perforating injuries of the eyeball
Delay in surgical management of the injury may cause irreversible blindness or may necessitate
removal of an eye

Referral: Immediately refer the patient to a health facility with eye surgeon at the District, Regional,
Zonal or National hospital depending on the staff availability.

14.2.1.3 Chemical Injuries/Burn


This is an Ophthalmological emergency. It occurs when chemicals such as acid or alkali (e.g.
household detergents, bleaching agents), snake spit, insect bite, traditional eye medicine, cement or
lime cause a damage to the eye.

Clinical presentation
• Diagnosis relies mostly with • Cloudiness of cornea with blurred
patients’ history vision
• Patients may present with • Loss of conjunctival blood vessels
photophobia • Traces of chemical substance such
• Inability to open the eyes as cement or herbs and blisters or
• Excessive tearing/watery eye loss of eyelid skin in open flame
injuries.
Investigations
• Visual acuity
• Slit lamp bimicroscopy
• Fluorescein staining

Non-pharmacological Treatment
If a patient gives you history of being in contact with the items mentioned above, the following
should be done:

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• Irrigate the eye with clean water or Ringers lactate continually for a minimum of 20–30
minutes to reduce chemical substances. Irrigate longer for severe alkali burn.
• Test the patients’ vision and examine the patient’s eye

Pharmacological Treatment
C: tetracaine 0.5% eye drops, instill 2 drops in the affected eye. Repeat irrigation if
possible. Evert the eye lids and remove the debris
AND
A: chloramphenicol 1% eye ointment, apply 6hourly to prevent infection for 3days.
AND
A: paracetamol (PO)1gm 4–6hourly to a maximum of 4 doses in 24hours, for 3days in
adults, the dosage in children is 10–14mg/kg 4–6hourly for 3days

Referral: Refer all cases within 12hours to eye specialist at high level health facilities for more care

14.2.2 Herpes Simplex Keratitis


It is an inflammatory condition of the cornea caused by Herpes Simplex Virus.

Clinical presentation
• Acute unilateral painful eye
• Blurring of vision
• Reduced corneal sensation
• Dendritic corneal ulcer seen on staining with fluorescein

Investigations
• Visual acuity
• Slit lamp bimicroscopy
• Fluorescein staining

Pharmacological Treatment
C: acyclovir 3%, ophthalmic ointment inserted in the lower conjunctival sac, 4hourly.
Continue for 3days after ulcer has been healed.
AND
B: acyclovir, (PO), 400mg 8–4hourly a day for 7–10days depending on initial response as
well as the extent of the ulcer.

Note
Topical corticosteroids are contraindicated in the treatment of dendritic ulcers

14.2.3 Corneal Ulcer


This is a painful red eye condition resulting from a raw discontinuity to the corneal epithelium. It may
be caused by infection (bacterial, viral e.g. Herpes simplex virus and measles, fungal, trauma
(physical or chemical) and nutritional (Vitamin A deficiency).

Clinical presentation
• Painful and red eye of acute onset • Gray/white spot on the cornea
• Excessive tearing staining with fluorescein
• Severe photophobia • Hypopyon (Pus or white cells in
• Poor vision anterior chamber)

Investigations
• Visual acuity
• Slit Lamp bimicroscope
• Corneal scrapping for Gram Stain and
• Corneal scrapping for Potassium Hydroxide staining
• Fluorescein sodium drops or a drop of local anesthetic on a fluorescein strip to assess the
pattern of the ulcer and measure the size of corneal defect.

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Pharmacological Treatment
While waiting for laboratory results, give:
C: ciprofloxacin 0.3%, ophthalmic drops, instill 1–2drops 1–2hourly for 3days then reduce
to 3–4hourly.
OR
D: ofloxacin 0.3%, ophthalmic drops, instill 1 drop 1–2hourly for 3days then reduce to 3–
4hourly

Give antifungal, if fungal infection is suspected or confirmed


S: natamycin 5%, ophthalmic drops, instill 1 drop 1–2hourly for 3–4days (specialist use
only). Then reduce to 1 drop 3-4hourly. Continue for 14–21days until resolution of infection
OR
S: econazole 2%, ophthalmic drops, instill 1 drop 1–2hourly for 3–4days (specialist use
only). Then reduce to 1 drop 3–4hourly. Continue for 14–21days until resolution of infection
OR
S: chlorhexidine 0.2%, ophthalmic drops, instill 1 drop 1–2hourly for 3–4days (specialist
use only). Then reduce to 1 drop 3–4hourly. Continue for 14–21days until resolution of
infection
Give antiviral if viral causes are suspected after the examination of the eye
C: acyclovir 3% eye ointment 5hourly a day until there is no corneal stain, then continue
with treatment 8hourly a day for a maximum of 10–14days

Note
Treatment may be changed depending on corneal scrapping results

Referral: Refer to the next level of care where there is an eye specialist when there is hypopyon
(white cells in anterior chamber)

14.2.4 Uveitis
This isInflammation of the uveal tissue (Iris, choroid and ciliary body) and its adjacent structures.
Majority of the cases are idiopathic whereby other cases are due to autoimmune diseases e.g.
Rheumatoid Arthritis, Viraland systemic diseases like Tuberculosis, Leprosy, and Syphilis.

Clinical presentation
It has three main clinical presentations namely acute, chronic and acute on chronic. The commonest
form is anterior uveitis. In acute type, patients present with: -
• Painful red eye • Loss of vision
• Excessive tearing • Cells in anterior chamber
• Severe photophobia • Irregular pupil with synechiae

Investigations Laboratory blood tests for bilateral and


• Visual acuity granulomatous uveitis: -
• Slit lamp bimicroscopic examination • FBC
anterior chamber • ESR
• Tonometry • Antinuclear Antibody
• B scan • VDRL
• Urinalysis • HIV Testing

Imaging: Chest X-Rays if Tuberculosis and Sarcoidosis are suspected.

Pharmacological Treatment
Treatment for uveitis is mainly steroids and specific treatment according to the cause. This should
be initiated in a facility where workup and close monitoring can be done.
Give:
Steroidal Anti-inflammatory medicines
D: dexamethasone 1% eye drops, 1–3hourly in the affected eye for 6weeks
OR

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D: prednisolone 0.5% or 1 % eye drops, 1–3hourly in the affected eye for 6weeks
AND
A: prednisolone (PO) 1mg/kg body weight, given in a tapering manner to maximum of 4–
6weeks
AND
D: triamcinolone (subtenon) 20mg stat, it can be repeated after 4 weeks if need arise.
AND
Pupil dilating eye drops
B: atropine eye drops or ointment 1% 12hourly in the affected eye
OR
C: cyclopentolate 1 % eye drops, 1–2drops 8hourly in the affected eye.
Treatment for uveitis is to be continued for a maximum of 6weeks

Note
• Treatment of uveitis must involve various specialists
• Acute uveitis is a serious problem and the patient should be referred urgently for specialist
treatment
• Recurrences may occur or acute disease may end up becoming a chronic uveitis

14.2.5 Conjunctivitis
This is an inflammation of the conjunctivae and one of the most common causes of red eyes. The
cause of conjunctivitis may be bacterial, viral or allergy. Clinical features and treatment guideline
depend on the type and cause of conjunctivitis.

Note
• If conjunctivitis is due to an infection, counsel on the importance of frequent hand washing,
use separate linen, towels and wash towels and avoid direct contact with infected materials
or individuals
• Contacts lenses should not be worn in patients with conjunctivitis until the condition has
resolved

14.2.5.1 Allergic Conjunctivitis


Clinical presentation
• Patients present with history of itching of eyes, sand sensation, and sometimes mucoid
discharge
• When examined,
o the eyes may be normal or slightly red,
o Conjunctival swelling in severe cases,
o Limbal hyperpigmentation and papillae of the upper tarsal conjunctiva.
o Normal iris, pupil and visual acuity.
o Corneal complications in very advanced stages

Investigations
• Visual acuity
• Slit lamp bimicroscopy
• Full blood picture
• Skin Allergic test

Non-pharmacological Treatment
Treatment of allergic conjunctivitis depends on the severity of the condition and age of the patient. In
mild cases where the eyes are white,
• Avoid allergens
• Cold water compresses for 10 minutes four times a day

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Pharmacological Treatment
Adults and children > 6 years of age:
C: oxymetazoline 0.025% drops 6hourly a maximum of 7days
If no response within 7days, use mast cell stabilizers such as:
C: sodium cromoglycate 2% eye drops, instill 6hourly per day (Doctor initiated)
Use may be seasonal (1–3 months) or long term.

Children 2–6 years of age:


A: chlorpheniramine (PO) 0.1 mg/kg/dose 6–8hourly
If no response within 7days use
C: sodium cromoglycate 2% eye drops, instill 6hourly per day (doctor initiated)
o Use may be seasonal (1–3 months) or long term for the prevention of further
attack, depending on the patient’s exposure to the allergen.

Persistent allergic Conjunctivitis in adults and children of >2 years of age:


For long term use:
Children 2–6years
A: cetirizine (PO) Adult; 10mg. Children below 6year 5mg 24hourly
o Use may be seasonal (1–3 months) or long term

Note
Do not give antihistamine to children under 2 years of age as its effectiveness at this age group has
not been proven.

Referral: Refer to eye specialist for further specialized care in case of the following:
• Moderate to severe allergic conjunctivitis
• No response
• Persons wearing contact lenses
• Children <2 years of age

At the specialized centre, the following treatment may be added depending on the patient’s
presentation:
Short term steroid eye drops (in severe cases with involvement of the cornea, apart from mast cell
stabilizers, give
D: dexamethasone 0.1%, 6hourly for a maximum of 14days.
OR
D: prednisolone 0.5%, 6hourly for a maximum of 14days.

In very severe form of allergic conjunctivitis, give steroid injection


D: triamcinolone acetonide (subtenon) 20mg stat
OR
D: methylprednisolone sodium acetate (subtenon) 20mg stat

14.2.5.2 Viral Conjunctivitis


The commonest causative organism is adenovirus. It may be unilateral but usually bilateral

Clinical presentation
• It may be associated with upper respiratory tract infection
• Presents with morning crusting and watery eye discharge
• A burning, sandy or gritty feeling in the eyes
• Diffuse pink or red conjunctiva due to subconjunctival hemorrhages
• Photophobia if the cornea is involved
• Normal visual acuity
• Preauricular lymphadenopathy
• It appears in epidemics so there will be history of contact with patients with similar eye
condition
• It is usually is self-limiting, but the irritation and discharge get worse on 3 – 5 days before
getting better and symptoms can persist for 2–3 weeks.

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Non-pharmacological Treatment
• Advise on correct cleansing or rinsing of eyes with clean water
• Cold compresses for symptomatic relief

Pharmacological Treatment
Children > 6 years and adults
C: oxymetazoline 0.025% eye drops, instill 1–2drops 6hourly for a maximum of 7days.
AND
A: paracetamol (PO) Adult; 1g. Pediatric 10–15 mg/kg/dose 6hourly when required.

Note: Viral conjunctivitis is very contagious so patients and members of the family should be
alerted

Referral: Refer all patients to a centre with eye specialist if there is


• No response after 5 days
• Unilateral red eye for more than one day
• Suspected herpes conjunctivitis
• Loss of vision
• Irregular pupil
• Haziness of cornea
• Persistent painful eye

14.2.5.3 Bacterial Conjunctivitis


Purulent conjunctival inflammation caused by bacterial infection

Clinical presentation
It is characterized by:
• Mucopurulent discharge from one • Conjunctiva redness more at the
or both eyes fornices
• Sore, gritty or scratch eyes and • Eyelids may be swollen
swollen lids • Matting of eye lashes in the
morning with eyelids stuck shut
Non-pharmacological Treatment
• Educate patient on personal hygiene to prevent spread
• Educate patient correct application of ophthalmic ointment
o To wash hands thoroughly before applying ophthalmic ointment
o Not to share the ophthalmic ointment and drops
• Eye swabs for Gram stain and for culture and sensitivity may be needed to tailor down
treatment.

Pharmacological Treatment
A: chloramphenicol 1%, ophthalmic ointment, applied 8hourly for 5days.
OR
C: ciprofloxacin 0.3%, ophthalmic drops, instill 1drop, 4hourly for 2days. Then reduce
frequency to 1 drop 6hourly for 5days
OR
D: ofloxacin 0.3%, ophthalmic drops, instill 1 drop 4hourly for 2days. Then reduce the
frequency to 1drop 6hourly for 5days
AND
A: paracetamol (PO) Adult 1g. Children 10–15 mg/kg/dose 6hourly when required. Adults:

Referral: Refer to eye specialist if no improvement after 2days of treatment


14.2.5.4 Ophthalmia Neonatorum/Neonatal Conjunctivitis
This is acute bacterial infection of the eyes that affect newborn baby during the first 28days of life.
The infection is acquired from mother’s birth canal secretions. It is characterized by inflammation of

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the conjunctivae, sticky eyes to abundant purulent discharge and eyelids oedema. Causative
organisms are Neisseria Gonorrhea, Chlamydia spp and Staphylococcus spp.

Clinical presentation
• Patients present with massive edema and redness of eyelids and with purulent and
copious discharge from the eyes, clinical presentation ranges from mild (small amount of
sticky exudates) to severe form (profuse pus and swollen eye lids) depending on the
causative organism
• There is usually rapid ulceration and perforation of corneal which eventually leads to
blindness if treatment is delayed
• It usually presents 3–4days of life
• Late and mild presentation is due to Staphylococcus or undefined
• Treat parents of a neonate with purulent discharge appropriately

Investigations
• Pus swab for Gram Stain
• Pus for Culture and sensitivity
• Vaginal swab for Gram stain and culture and sensitivity

Non-pharmacological Treatment
Cleanse or wipe eyes of all newborn babies with a clean cloth, cotton wool or swab, taking care not
to touch or injure the eye

Pharmacological Treatment
Screen women in the antenatal clinics and treat both parents for Sexually Transmitted Diseases. In
Ophthalmia neonatorum, prevention is better than cure.
A: Apply chloramphenicol 1% eye ointment, both eyes, to all newborn babies as
soon as possible after birth.
OR
A: povidone iodine 2.5 % Eye Drops, both eyes

Sticky eye(s) without purulent discharge:


A: chloramphenicol 1% eye ointment, apply 6hourly for 7days

Purulent discharge
Mild discharge without swollen eyelids and no corneal haziness:
A: compound sodium lactate eye wash, immediately then 2–3hourly until
discharge clears
AND
B: ceftriaxone (IM) 50mg/kg immediately stat
Given at District Hospital (Treatment to be initiated by Clinical Eye Care Professional eg. Assistant
Medical Officer in Ophthalmology)

Abundant purulent discharge and/or swollen eyelids and /or corneal haziness:
A: compound sodium lactate eye wash, immediately then hourly until referral
AND
B: ceftriaxone (IM) 50mg/kg immediately stat

Referral: To high level health facilities for proper management.

Note
• Ceftriaxone should not be used in neonates that are seriously ill or are jaundiced
• Ceftriaxone should not be administered if calcium containing intravenous infusion e.g
Compound Sodium Lactate is given or is expected to be given

Treat both parents of newborns who develop purulent conjunctivitis after 24 hours of birth for N-
gonorrhea and Chlamydia with

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B: ceftriaxone (IM) 250mg stat
(For ceftriaxone IM injection: Dissolve Ceftriaxone 250mg in 0.9 mL Lidocaine
1% without adrenaline)
AND
B: azithromycin (PO) 1g stat

Note:
For more details on prevention and treatment see the “Neonatal Conjunctivitis (NC) Flow chart
number 12.7 under the Sexual Transmitted disease chapter

Referral: Urgently
• Neonates with abundant purulent discharge and/or swollen eyelids and/or corneal
haziness and
• Neonates unresponsive to treatment within 2days.
14.3 Structural Abnormalities of the Eye
These includes:
• Squint: eyes are looking in different directions; one eye appears to be turned in or out, in
children or in adult. Refer urgently all children who present with squint to Paediatric Eye
Tertiary Centre
• Ocular surface disease: The most common ocular surface diseases are pterygium and
Squamous cell carcinoma of the conjunctiva.
• Eyelids abnormalities: eyelashes rubbing on cornea (trichiasis), inturned eyelids
(entropion), eyelids bent out too much (ectropion), drooping eyelids (ptosis), inability to
close the eyes (lagophthalmos)

Referral: Refer all patients to health facilities with eye specialist for surgical intervention

Note: Abnormal tissues excised from eye patients should be subjected to pathology examination for
proper diagnosis
14.4 Ocular Oncology
14.4.1 Retinoblastoma
It is the commonest childhood malignant tumor of the eyes. It is diagnosed between the first 1–
3years of life. It has a lower survival rate after diagnosis hence, monthly screening of all under-five
children is important for timely referral and management.

Clinical presentation
• White pupil reflex (leukocoria) • Ocular/periocular inflammation
• Squint • Secondary glaucoma
• Rarely vitreous hemorrhage • In late stages proptosis and
• Hyphema hypopyon

Investigations
• Visual acuity • Examination under
• Tonometry anaesthesia
• Fundoscopy • Histology of an enucleated
• B Scan eye in advanced disease
• CT Scan of the head • Cerebral Spinal Fluid analysis
in advanced disease

Non-pharmacological Treatment
Staging and treatment is done in specialized centres in consultation with Pediatrician and
Oncologist. The following are treatment modalities:
• Enucleation of the affected eye and the eye is taken for histology
• External beam radiotherapy
• Plaque radiotherapy
• Cryotherapy and laser photoablation

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Table 14.6: Classification of Retinoblastoma and recommended treatment options according
the classification of Retinoblastoma (ICRB)
Group Clinical features Recommended Treatment options
A All small tumors (3 mm or less) - Focal therapy (cryotherapy or Transpupillary
that are only in the retina and are thermotherapy (TTT).
not near important structures such - TTT is indicated for posterior located tumors.
as the optic disc or the foveolar TTT use Diode Laser (810nm) or 1064nm or
i.e. Not less than 3 mm from the 532nm. Tumor is heated until it turns slightly
foveolar and 1.5mmfrom the optic gray. Complete tumor regression can be
disc. achieved by using 3-4sessions
- Do not exceed 5 minutes per session to avoid
complication such as Cataract.
- Cryotherapy is done to a small tumor at
equatorial and peripheral retina. Under GA
place the probe precisely on the sclera, directly
behind the intraocular focus of the tumor. apply
triple freeze/thaw at 3week intervals until
complete tumor regression.
Note: Administer cryotherapy or TTT 3-6 hours prior
to chemotherapy if systemic treatment is indicated.
Focal therapy synergistically increases drug
penetration to the tumor
B Tumor of > 3mm, close to the - 6cycles of standard dose chemotherapy are
optic disc or foveola indicated to allow adequate tumor reduction.
No subretinal fluid Note: Standard dose is a combination of Carboplatin,
Vincristine and Etoposide (VEC).
Do not perform focal therapy if tumors are located in
the macular and juxtapupillary areas.
- If focal therapy is indicated chemotherapy
should be given within 6hr of focal therapy to
increase drug penetration to the eye and tumor
C Well-defined tumors - 6cycle of standard dose Chemotherapy is
with small amounts of subretinal indicated.
or - Chemotherapy should be given within 6 hours
vitreous seeding (tumor cells of focal therapy (cryotherapy or TTT or
floating within the vitreous cavity) Subtenon Carboplatin)depending on site and
response to treatment.
NOTE: Vitreous seeding is one of - Chemotherapy cycles are given at 3 weeks
the most challenging situations intervals, every cycle is preceded by EUA and
for eye-preservation therapy and focal therapy.
is the primary reason Note: Do not perform focal therapy if tumors are
for treatment failure following located in the macular and juxtapupillary areas
conservative management of - vitreous seeding can be managed by
retinoblastoma. plaque radiotherapy (need license), External
beam Radiotherapy, Enucleation or intravitreal
chemotherapy (Melphalan). Melphalan salvage
about 60% of eyeball with vitreous seeding (8-
10µg is safe dose)
D Large or poorly defined tumors - If unilateral Enucleate.
occupying up to 50% of the globe - If bilateral Start 3 cycles of chemotherapy
with widespread vitreous or - If no response and no visual potential enucleate
subretinal seeding. the worse eye.
There is retinal detachment up to - If there is response complete 6cycles of
50% of the globe systemic chemotherapy.
- Local radiation for persistent vitreous seeds
may be indicated (plaque therapy or Intravitreal
Melphalan)
Note: Focal therapy should be given prior to
chemotherapy for every cycle.
- Chemotherapy should be given within 6 hours
of focal therapy to increase drug penetration to
the eye and tumor
E The tumor is very large with one Enucleation with minimal manipulation is indicated for
or more of the following features: - All group E with no visual potential,
- - If all known effective treatment has failed

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• No visual potential Note: Optic nerve length should not be less than
• Tumor in the anterior 17mm to minimize the chances of leaving tumor at
segment surgical site. Also, when performing enucleation: -
• Tumor in or on the ciliary • Take care not to perforate the globe
body • Use primary orbital implant to achieve excellent
• Neovascular glaucoma cosmetic appearance
• When there is no direct • If histopathology results are positive for high risk
visualization of an active factors, 6cycles of Chemotherapy is indicated as
tumor (Vitreous for Group D above.
hemorrhage, cataract or Histopathological features in retinoblastoma are
hyphema) considered high-risk factors (HRF) for tumor
• Phthisical or pre-phthisical progression and metastasis, thus their presence
eye becomes an indication for adjuvant chemotherapy
• Orbital cellulitis-like (HRF) includes:
presentation i) Scleral extension
• Total RD of more than 50% ii) Post-laminar optic nerve invasion
iii) Disease at the cut margin of optic nerve
iv) Massive choroidal invasion of more than 3mm
v) Anterior chamber extension
• If no HRF no need of chemotherapy.
• Prosthesis and protective glasses are indicated
for all children who have been enucleated
EOE Orbital RB • 3–6 cycles of high dose chemotherapy- followed
by enucleation if tumor regressed significantly
• External Beam Radiotherapy and adjuvant
chemotherapy for a total of up to 12 cycles
NOTE: Exenteration is not encouraged at this stage
since aim of treatment is for palliation.
Distance CNS involvement RB- where Palliative care according to the National Palliative
metastasis Ct/MRI proved CNS extension or Care Guideline
cerebral-spinal fluid is positive for
RB cells
Metastatic RB where bone Palliative care according to the National Palliative
marrow biopsy is positive Care Guideline

Pharmacological Treatment
Systemic chemotherapy is instituted by Oncologists and or paediatrician. Ophthalmologist institute
intravitreal chemotherapy if need be.

Referral: Refer to Oncology Section in this document for details of Chemotherapy in Retinoblastoma
treatment.

Note
Close follow up is very important due to the following: -
• There is a chance of developing retinoblastoma in the fellow eye
• The risk is diminished with increase in age
• Also watch for secondary tumors like osteosarcoma

Referral: Refer all children presenting with a white pupillary reflex, squint or acute painful red eye to
some qualified eye care personnel/ophthalmologist.

14.4.2 Squamous Cell Carcinoma of Conjunctiva


Invasive squamous cell carcinoma of conjunctiva is the major and most common ocular malignancy
of the eye. The tumor typically occurs on the bulbar conjunctiva, originating at the limbus, and often
spreads onto the cornea, globe, orbit and nasolacrimal system. The cancer is a slow growing tumor
of middle-aged to elderly people.
Clinical presentation
• It manifests usually as a fleshy vascularized mass at the limbus. (temporal or nasally)
• In advanced stage, it may intrude the eyeball and extend to other ocular adnexa structures

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• Definitive diagnosis is by histopathological assessment of excised tissue

Investigations
• Visual acuity • Fundoscopy
• Slit lamp Bimicroscopy • Histology examination of the
• Tonometry excised mass

Non-pharmacological Treatment
• Check for HIV status of the patient as recurrences occurs most frequently in HIV positive
patients
• Close follow up of patients for at least the first 12 months postoperatively to look for
residual or recurrent tumors

Pharmacological Treatment
D: 5-fluorouracil (5FU) 50mg/mL, on a sponge, on the surgical bed for about 2.5minutes
then wash off with compound sodium lactate solution.
OR
D: mitomycin C 0.2mg/mL, on a sponge, on the surgical bed for about 2.5minutes then
wash off with compound sodium lactate solution.
AND
C: dexamethasone + chloramphenicol eye drops, 0.1%–0.5 %, 6hourly, for 3–4weeks
OR
C: dexamethasone + gentamicin eye drops, 0.1–0.3%, 6hourly, for 3–4 weeks
(These are post operatively until the wound is healed)
THEN
D: 5-fluorouracil (5FU) 1% eye drops, 4times daily for 2–3weeks

Note
• 5-fluorouracil (5FU) is used after the excision wound has healed
• 5 FU eye drops may cause watery eye, discomfort or eye inflammation, manage
accordingly

Surgical Treatment
• It depends on the tumor size, location, focality, and invasiveness
• Surgical excision of the mass with clear margin of 4 mm without touching the tumor is
recommended, followed with topical adjunctive cryotherapy and or chemotherapy to the
residual conjunctival and scleral bed
o Double - four freeze-thaw cycles of cryotherapy to the remaining
conjunctival margins, bed and limbus.
o For tumors that are adherent to the sclera, perform a superficial sclerectomy
and use cryotherapy to the base.
• A large or multicentric squamous conjunctival mass should be managed by a surgeon
experienced in treating such lesions
• Removal of the eyeball and adnexa may be indicated for advanced stage
• Radiotherapy if required, for palliation after removal of the eye.

Referral:
• All suspicious cases of Squamous Cell Carcinoma of Conjunctiva must be referred to
eye specialist for proper evaluation and management.
• Refer all patients with advanced Squamous Cell Carcinoma of the conjunctiva to
Oncologist

14.5 Dry Eye


It occurs when there is inadequate tear volume or function.

Clinical presentation
• Feelings of dryness, grittiness, burning and foreign body sensation, usually worse during
the day

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• Stringy discharge, redness and transient blurring of vision are also common. Exclude
allergic conjunctivitis

Investigations
• Visual acuity • Schirmer Test
• Slit lamp bimicroscopy • Tear break up test

Non-pharmacological Treatment
• Control symptoms since the condition is not curable
• Educate patients to avoid unprescribed eye medications which may worsen the dryness
and control their environmental factors by e.g. blinking frequently during visual attentive
tasks, avoid air conditioners

Pharmacological Treatment
Tear substitutes give:
C: hydroxypropyl methylcellulose 0.7%, ophthalmic drops, 1drop, 6hourly.

14.6 Herpes Zoster Ophthalmicus


Occurs when Varicella Zoster Virus reactivates in the trigeminal ganglion and passes down the
ophthalmic division of the trigeminal nerve

Clinical presentation
• Presents with painful vesicular rash in the trigeminal V1 area–vesicles on the tip of the
nose indicate nasociliary branch involvement and increases the risk of ocular involvement
• Some patients develop conjunctivitis, keratitis, uveitis, retinitis and cranial nerve
involvement (oculomotor and optic nerves)
• Later, chronic ocular inflammation, loss of vision, post herpetic neuralgia
• All patients should be offered HIV testing

Investigations
• Visual acuity • Fluorescein staining
• Slit lamp bimicroscopy • HIV Testing
• Corneal sensation test

Pharmacological Treatment
B: acyclovir (PO) 800mg 4hourly for 7–10days
AND
A: amitriptyline (PO) 25mg at night for 3months.

Note:
• Treatment should be initiated within 3 days of the onset of symptoms, except in HIV infected
patients who should be treated if there are active skin lesions
• Management of Herpes Zoster is Multidisciplinary so consult physician for proper management
of the patient.

Referral
Refer to eye specialist in case of: -
• Vesicles on the tip of the nose
• Fluorescein staining of the cornea shows corneal ulceration
• Decreased vision
• Red eye (uveitis or keratitis)
• Cranial nerve palsies

14.7 Endophthalmitis
It is an infection of the ocular cavity. It is an ophthalmic emergency that can cause blindness that
may occur secondary to bacteraemia (endogenous infection) or following penetrating eye injury of
surgery

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Clinical presentation
• Loss of vision, may be associated with pain in the affected eye
• Blood culture should be done to identify the source and how it can be treated (for
bacteraemia)
• In post injury or surgery, culture of specimens of aqueous or vitreous humour should be
done

Investigations
• Visual acuity • B Scan
• Slit lamp bimicroscopy • Vitreous Tap for Gram stain,
• Tonometry Culture and sensitivity
• Refraction

Pharmacological Treatment
Refer immediately to an ophthalmologist for treatment

Endogenous Endophthalmitis
Specialist initiated; vitrectomy often required
B: ceftriaxone (IV) 2g 24hourly for 7days

Adjust antibiotics according to culture and sensitivity


AND
D: ceftazidime (intravitreal) 2.25mg stat repeat after 16–24hours
AND
S: vancomycin (intravitreal) 1mg stat repeat after 72hours

Administer using separate 1 ml tuberculin or Insulin syringes

Post-Surgical endophthalmitis
Specialist initiated; vitrectomy often required
D: ceftazidime (intravitreal) 2.25mg stat repeat after 16 – 24hours
AND
D: vancomycin (intravitreal)1mg stat repeat after 72hours
Administer using separate tuberculin on Insulin syringes

In addition, if there is soft tissue involvement or as a prophylaxis after a penetrating injury:


A: ciprofloxacin (PO) 750mg 12hourly for 7days.

14.8 Retinitis
It is seen in advanced HIV infection with CD4 count of less 100 cells/mm3. Management of these
patients is done in consultation with treating physicians.

Diagnostic Criteria
• Presents with characteristic retinal appearance of necrosis (white exudates and
haemorrhages at the edge of the exudates
• Visual loss is irreversible

Pharmacological Treatment
S: ganciclovir (intravitreal) 2mg once a week
Once immune function has been restored with antiretroviral therapy, (CD4 > 100) and the features of
active retinitis has been cleared, maintenance Ganciclovir can be stopped but monitor for
recurrence.

Referral: Refer to Ophthalmologist for confirmation of diagnosis and treatment.

14.9 Orbital Cellulitis


Orbital cellulitis is an infection of the soft tissues of the orbit posterior to the orbital septum. It may be
a continuum of preseptal cellulitis, which is an infection of the soft tissue of the eyelids and

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periocular region anterior to the orbital septum. Orbital cellulitis may result from an extension of an
infection from the paranasal sinuses or other periorbital structures such as the face, globe, or
lacrimal sac, direct inoculation of the orbit from trauma or surgery or as a haematogenous spread
from bacteremia

Clinical presentation
• Fever, malaise, and a history of • Orbital pain and tenderness are
recent sinusitis or upper respiratory present early
tract infection • Swollen eyelids, chemosis,
• Proptosis and ophthalmoplegia are hyperemia of the conjunctiva, and
the cardinal signs of orbital resistance to retropulsion of the
cellulitis. globe may be present
• Conjunctival chemosis, • Purulent nasal discharge may be
dyschromatopsia, and relative present
afferent pupillary defect • For very ill children, vision may
• Decreased vision difficult to evaluate in very ill
• Elevated intraocular pressure children with marked edema
• Pain on eye movement

Investigations
• Visual acuity • CT Scan of the orbits and
• Slit lamp bimicroscopy paranasal sinuses with Contrast
• Tonometry and
• Fundoscopy • MRI will help differentiating it with
• Full Blood Count and ESR other diseases but also identifying
• Blood culture the source or extension of the
• Assessment of purulent nasal disease
discharge or from the abscess
(Swab for Gram Stain)

Non-pharmacological Treatment
• Patients must be hospitalized
• Adequate hydration
• Lower the temperature
• Daily evaluation and monitor the vital signs
• Management of orbital cellulitis is done with consultation from other medical team
(Neurosurgical (if brain extension is seen), ENT (for involvement of sinuses), Paediatrician
(for paediatric patients) and Physicians

Pharmacological Treatment
The antibiotic will be tailored when the laboratory results are out
Adults, give:
B: ampicillin + cloxacillin (FDC) (IV) 1g stat then 500mg 6hourly for 2weeks
AND
A: gentamicin (IV) 160mg 24hourly for 7days
AND
B: metronidazole (IV) 500mg 8hourly for 7days
AND
S: vancomycin (IV) 15–20 mg/kg 8–12hourly

Children more than one-month old give:


B: ampicillin + cloxacillin (FDC) (IV) 50 mg /kg 8hourly for 7–14days
AND
A: gentamicin (IV) 7.5mg/kg, 24hourly for 5 -7days
AND
B: metronidazole (IV) 7.5–15mg/kg 6hourly for 7–10days
AND
S: vancomycin (IV) 10mg/kg 6hourly for 7–10day

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Note: Individual dose not to exceed 1g
Children less or equal to one-month old give:
B: ampicillin + cloxacillin (FDC) (IV) 25–50mg/kg 8hourly for 7–14days
AND
A: gentamicin (IV) 5mg/kg 24hourly for 5–7days

Steroidal anti – inflammatory medicines


To be given after 48 hours of antibiotic therapy. Give:
A: prednisolone (PO) 1–2mg/kg 24hourly to be tapered slowly.
AND
Adults:
A: ibuprofen (PO) 400–800mg 6–8hourly; not to exceed 3.2 g 24hourly
OR
A: paracetamol (PO) 1g 4–6hourly to a maximum of 4 doses 24hourly, for
3days
Children:
A: ibuprofen (PO) 30–40mg/kg per day in 3–4doses
OR
A: paracetamol 10–14 mg/kg for 3days

Note
Do not use ibuprofen in patients with bleeding disorders or peptic ulcers

Surgical Treatment
Surgical drainage is only indicated when there is:
• A decrease in vision
• Development of an afferent pupillary defect
• Progression of Proptosis despite appropriate antibiotic therapy
• The size of the abscess does not reduce on CT scan within 48–72hours after appropriate
antibiotics have been administered
• If brain abscesses develop and do not respond to antibiotic therapy, then craniotomy is
indicated
• Presence of a drainable fluid collection is evident on CT scan in patients older than
16years

14.10 Visual Problems


Visual problems may be due to refractive errors, damage to the eye or optic nerve. This may be an
indication of underlying diseases such as diabetes or hypertension.

Investigations
• Assess ocular alignment
• Determine visual acuity accurately in both eyes by Snellen chart
• If vision is diminished, (less than 6/12), perform the following: -

Pin hole test


o Make a hole of about 1mm wide in a piece of dark/black paper – you can push a
hole in a paper or card with a pen tip
o Ask the patient to look through this hole at the Snellen chart
o If vision improves, this means that the patient has a refractive error

Red Reflex Test


The patient looks past the examiners head focusing on a distant target.
o With the ophthalmoscope at 0 (zero) the examiner keeps close to his eye and
then focuses the beam of light so that it falls on the pupillary area of the cornea
o The examiner stands about 60cm away from the patient.

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o In normal individuals, the examiner should be able to see a red or pink colour
(reflex) through the pupil which comes from the retina.

Significance of absent red reflex


If there is history of trauma or diabetes, the absence of a red reflex is probably due to:
• Retinal detachment
• A vitreous hemorrhage
• Mature cataract

If there are cataracts, one usually sees:


• Black shadows against the red reflex in immature cataract, or
• Absence of red reflex in mature cataracts

In a >50years of age with no history of trauma, diabetes or previous eye disease, an absent red
reflex is often due to cataract formation, especially with decreased visual acuity.

Fundoscopy

Note
Associated diabetes or hypertension should be adequately managed with referral, as surgery can
only be considered with appropriately managed systemic disease

Referral
Urgent within 12–24 hours
• Sudden loss of vision in one or both eyes
• Pain or redness in one eye only especially with visual and pupillary abnormalities
• Recent proptosis of one or both eyes or enlargement of the eye (buphthalmos) in children
• Hazy cornea in children
• Unilateral watery eye

Within days
• Squint of recent onset
• Suspected or previously diagnosed glaucoma
• Double vision following recent injury might indicate orbital fracture
• Leukocoria (white reflex from the pupil) especially in children
• Squint at an age if not previously investigated by ophthalmologist
• Visual loss in patients with systemic disease such as diabetes

Non-urgent referral
• Cataracts in adults
• Refractive errors in teenage and adults
• Longstanding blindness–first visit to health facility

14.11 Onchocerciasis (River Blindness)


Onchocerciasis is a tissue parasitic infestation caused by a filarial worm, Onchocerca volvulus. The
microfilariae invade lymphatic system, subcutaneous and deep tissues producing acute
inflammation and chronic inflammation at a later stage.

Clinical presentation
• Skin inflammation with papules • Skin nodules under the bony
• Subcutaneous nodules prominent areas
• Atypical skin lesions (scarred, • Microfilaria in anterior chamber
saggy, hanging areas of skin, • Scleritis and Keratitis leading to
leopard skin) Impaired vision as well as
blindness.
Investigations
• Visual acuity
• Rapid diagnostic test (OV-16 - Onchocerciasis IgG)

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• Skin snip for microscopic examination
• Slit lamp eye examination.
• B Scan

Pharmacological Treatment
Treatment is done in consultation with dermatologists and infectious disease specialists.
Apart from WHO recommended mass treatment campaign to community at risk with annual
preventive chemotherapy which polarize/paralyze the worm, treatment depends on individual patient
presentation.
A: ivermectin (PO) 0.15mg/kg once every 12months for 12–15years

Note:
• Patients with heavy ocular infestation require retreatment every 3 to 6 months.
• Treatment will only arrest progression of the clinical features but not reverse them.

Dosage guidelines based on body weight


Weight Dosage
15-25kg 3mg
26-44 kg 6mg
45 -64 kg 9mg
65- 84 kg 12mg
85kg or more 0.15mg/kg

Surgical treatment
Nodulectomy: It is done mostly for nodules located in the scalp to minimize the ocular complications.

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CHAPTER FIFTEEN
EAR, NOSE AND THROAT DISEASES
Ear, Nose and Throat (ENT) is a specialty in medicine that deals with medical and surgical
management of disorders affecting the ear, nose, throat, and the neck. Symptoms and diseases
affecting this area are common and commonly lead to patients seeking medical care.

15.1 Ear Condition


15.1.1 Circumscript otitis Externa (Furunculosis)
This is a localized infection of the hair follicle on the outer one-third of the external auditory canal. It
is caused by Staphylococcus aureus.

Clinical presentation
• Ear pain that is severe and disproportional to the visible lesion
• Reduced hearing
• Localized swelling on the external auditory canal
• There may be a purulent discharge if the swelling ruptures

Non-pharmacological management
• Aural toilet if there is otorrhea (ear suctioning under direct vision).
• Instruct the patient to keep the ear dry and avoiding scratching

Pharmacological management
B: ampicillin+cloxacillin (FDC) (PO) Adults: 500mg 8hourly for 7 to 10days. Children:
15mg/kg hourly for 7 to 10days
OR
C: amoxycillin + clavulanic acid (FDC) (PO) Adults: 625mg to 1g 12hourly for 7 to 10days.
Children ≤ 3 months: 30mg/kg/day in 2 divided doses for 7-10 days. Children >3 months:
25mg/kg/day in 2 divided doses for 7 to 10 days.
AND
A: paracetamol (PO) Adults: 500mg to 1g 4 to 8hourly as needed. Children ≤ 10kg:
10mg/kg 4 to 8 hourly as needed. Children >10kg: 15mg/kg 4 to 8 hourly as needed
OR
A: ibuprofen (PO) Adults: 200 mg to 400mg 4 to 8hourly as needed. Children ≥ 6 months:
5mg to 10mg/kg 4 to 8hourly as needed OR combined ibuprofen and paracetamol

Surgical management
• Incision and drainage

15.1.2 Diffusewer Otitis Externa (Swimmer’s ear)


This is an inflammation of the entire external auditory canal. It can be caused by bacteria, fungus or
both.

Clinical presentation
• Itchy, dry and scaly ear canal and painful ear
• There may be a water or purulent discharge, debris and reduced hearing
Pain may become extreme when the ear canal becomes completely occluded with edematous skin
and debris.

Non-pharmacological management
• Aural toilet at least once a week (ear suctioning under direct vision using microscope or
endoscope).
• Instruct the patient to keep the ear dry and avoiding scratching.

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Pharmacological management
C: ciprofloxacin ear drops 2 to 4drops each ear 6 to 8hourly for 14days.
OR
C: cream with combination of gentamicin or Neomycin+ Clobetasol or betamethasone or
beclometasone + miconazole or clotrimazole. Dosage: Apply pea size in external auditory
canal once per week for 4 to 6weeks.
OR
D: chloramphenicol+beclomethasone dipropionate+ clotrimazole + lignocaine ear drops
(FDC)
2 to 3drops each ear 6 to 8hourly for 14days.
AND
A: ciprofloxacin (PO) 500mg Adults and children above 12 years 12 hourly 7 to 14 day
OR
B: amoxycillin +clavulanate (FDC) (PO) Adult 625mg to 1g 12hourly: Paediatric ≤ 3 month
30mg/kg/day in 2 divided doses. Paediatric˃ 25mg/kg/day in 2 divided doses for 7-14days
AND
A: paracetamol (PO) Adult 1g: Pediatric ≤ 10kg 10mg/kg 4. Paediatric >15mg/kg 6 to 8
hourly as needed.
OR
A: ibuprofen (PO) 200 mg to 400mg 8 hourly as needed. Paediatric ≥ 6 months: 5mg to
10mg/kg 4 to 8hourly as needed
OR
D: diclofenac+ paracetamol (PO)(FDC)Adults: 50mg diclofenac and 500mg paracetamol
4 to 8hourly as needed.

15.1.3 Necrotizing Otitis Externa


This is a life-threatening infection that affects the external auditory canal and base of the skull. It is
common to elderly diabetic patients and other immunosuppressive conditions. Most common
causative organism is Pseumonas aureginosa. Controlling the underlying cause of
immunosuppression is of paramount importance.

Clinical presentation
• Ear pain, discharge, fullness and hearing impairment
• May present with facial nerve paralysis or other cranial nerves palsy.
• Presence of granulation tissues at the junction between the bony and cartilaginous parts of
external auditory canal
• Necrosis of external auditory canal

Non-pharmacological management
• Aural toilet at least once a week (ear suctioning under direct vision using microscope or
endoscope).
• Instruct the patient to keep the ear dry and avoiding scratching

Investigations
• culture and sensitivity of discharge

Pharmacological management
C: ciprofloxacin ear drops 2 to 4 drops each ear 6 to 8hourly for 14days
AND
B: ceftriaxone (IV) 1 to 2 g 12hourly for 7days.
For Children:
B: ceftriaxone (IV) 50 to 100mg/kg 24hourly for 7 day
OR
C: ciprofloxacin (IV) 400mg for 5 to 7days THEN 500mg (PO) 12hourly for 4 to 6weeks
days.
OR
S: meropenem (IV) (culture and sensitivity test is required) 500mg to 2g 8 hourly for 7
to 14days.
For Children ≥ 3 months:

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S: meropenem (IV) (culture and sensitivity test is required) 10mg/kg 8 hourly for 7 to
14days.
AND
A: paracetamol (IV) 500mg to 1g 4 to 8hourly as needed.
For Children ≤ 10kg:
A: paracetamol (IV) 10mg/kg 4 to 8hourly as needed.
ForChildren >10kg:
A: paracetamol (IV) 15mg/kg 4 to 8hourly as needed.
OR
A: ibuprofen (PO) 200 to 400mg 4 to 8hourly as needed.
For Children ≥ 6 months:
A: ibuprofen (PO) 5mg to 10mg/kg 4 to 8hourly as needed
OR
C: diclofenac+ paracetamol (PO) 50mg diclofenac and 500mg paracetamol 4 to 8hourly as
needed

Surgical management
Serial surgical debridement under local anesthesia(LA) or general anesthesia (GA).

Note: Necrotizing otitis externa is an emergency therefore treatment should be vigorous including
the treatment of underlaying immunodeficiency. Consider referral to tertiary facility for specialized
care.

15.1.4 Herpes Zoster Oticus (Ramsay Hunt syndrome)


This is a viral infection of external, middle and inner ear caused by reactivation of Varicella Zoster
virus in the geniculate ganglion.

Clinical presentation
• Vesicular rash of the ear • Ear pain
• Facial nerve paralysis • Ear discharge

Non-pharmacological management
Instruct the patient to keep the ear dry and avoiding scratching

Pharmacological management
A: prednisolone (PO) 60mg 24hourly for 5days then taper down to 50mg 24hourly for next
5days. Children: 1mg/kg 24hourly for 5days then taper down by half for the next 5days.
AND
B: acyclovir (PO) 800mg 4-8hourly for 7-14days.
For Children birth to 3 months:
B: acyclovir (IV) 10-20mg/kg 8hourly for 7-14days
For Children from 3 months to 12 years:
B: acyclovir (PO) 40-80mg/kg 6hourly for 7-14days
For Children more than 12 years
B: acyclovir (PO) 40-80mg/kg 6hourly for 7-14days
AND
B: acyclovir 5% cream.: Apply on the lesions 12 hourly.
AND
B: ampicilin+cloxacilin (FDC) (PO) 500mg 8hourly for 10-14 days.
For Children:
B: ampicilin+cloxacilin (FDC) (PO) 15mg/kg 6 hourly for 7-14 days
OR
B: amoxycillin+clavulanate (FDC) (PO) 625mg to 1g 12 hourly for 7-14 days.
ForChildren ≤ 3 months:
B: amoxycillin+clavulanate (FDC) (PO) 30mg/kg/day in 2 divided doses for 7-14 days.
For Children >3 months:
B: amoxycillin+clavulanate (FDC) (PO) 25mg/kg/day in 2 divided doses for 7 to 14 days
OR
A: paracetamol (PO) 500mg to 1g 4 to 8 hourly as needed.
ForChildren ≤ 10kg:
B: amoxycillin+clavulanate (FDC) (PO) 10mg/kg 4 to 8 hourly as needed.

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For Children >10kg:
B: amoxycillin+clavulanate (FDC) (PO) 15mg/kg 4 to 8 hourly as needed
OR
A: ibuprofen (PO) 200 to 400mg 4 to 8hourly as needed.
For Children ≥ 6 months:
A: ibuprofen (PO) 5mg to 10mg/kg 4 to 8hourly as needed
OR
C: diclofenac (PO) 50 mg 4 to 8hourly as needed.75 mg (IM) 8hourly as needed
OR
A: paracetamol + ibuprofen (PO) 400mg ibuprofen and 325mg paracetamol 4 to 8hourly as
needed.
For Children:
A: paracetamol + ibuprofen (PO) 100mg ibuprofen and 162.5mg paracetamol 4 to 8hourly
as needed

15.1.5 Pre-auricular Sinus Tract Infection


This is an infection of the pre-auricular sinus tract. May present with pre-auricular abscesses. Most
common causative organism is Staphylococcus aureus.

Clinical presentation
• Ear pain, sinus discharge
• Pre-auricular Swelling
• Fever, headache

Pharmacological management.
B: ampincillin+cloxacillin (FDC) (PO) 500mg 8hourly for 7-10days.
For Children:
B: ampincillin+cloxacillin (FDC) (PO) 15mg/kg 6 hourly for 7-10days
OR
B: amoxycillin+clavulanate (FDC) (PO) 625mg to 1g 12hourly for 7-10days
For Children ≤ 3 months:
B: amoxycillin+clavulanate (FDC) (PO): 30mg/kg/day in 2divided doses for 7-10days
For Children >3 months:
B: amoxycillin+clavulanate(FDC)(PO) 25mg/kg/day in 2divided doses for 7-14days
AND
A: paracetamol (PO) 500mg to 1g 4-8hourly as needed.
For Children ≤ 10kg:
A: paracetamol (PO) 10mg/kg 4-8hourly as needed.
For Children >10kg:
A: paracetamol (PO) 15mg/kg 4-8hourly as needed
OR
A: ibuprofen (PO) 200 mg to 400mg 4-8hourly as needed.
For Children ≥ 6 months:
A: ibuprofen (PO) 5mg to 10mg/kg 4-8hourly as needed
OR
C: diclofenac (PO) 50 mg 4 to 4-8hourly as needed. THEN 75 mg (IM) 4-8hourly as
needed
OR
C: diclofenac+ paracetamol (FDC) (PO) 50mg diclofenac and 500mg paracetamol 4-
8hourly as needed

Surgical management
• Incision and drainage of the abscess
• Excision of the sinus tract two to three weeks after incision and drainage i.e. when the
sinus tract is dry.

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15.2 Trauma of the Pinna
15.2.1 Hematoma of the Pinna

Clinical presentation
• History of trauma
• Fluctuant, tender pinna swelling

Pharmacological Treatment:
B: ampicilin+cloxacillin (FDC) (PO) 500mg 8hourly for 7-10days
Children: B: ampicilin+cloxacillin (FDC) (PO) 15mg/kg 6hours for 7-14days
OR
B: azithromycin (PO) 500mg 24hourly for 3days.
For Children:
B: ampicilin+cloxacillin (FDC) (PO) 10mg/kg 24hourly for 3days
AND
A: paracetamol (PO) 500mg to 1g 4-8hourly as needed.
ForChildren ≤ 10kg:
A: paracetamol (PO) 10mg/kg 4-8hourly as needed
For Children >10kg:
A: paracetamol (PO) 15mg/kg 4-8 hourly as needed
OR
C: ibuprofen (PO) 200 mg to 400mg 4-8hourly as needed.
ForChildren ≥ 6 months:
C: ibuprofen (PO) 5mg to 10mg/kg 4-8hourly as needed

Surgical management
• Incision and evacuation of hematoma
• Tight wound dressing to prevent re-accumulation of hematoma

15.2.2 Laceration of the Pinna


Lacerative trauma of the pinna with tear of skin and cartilage through and through.
Non-pharmacological management
• Skin to skin stitching of the wound, avoid through and through stitching this my
compromise blood supply to the cartilage.

Pharmacological management
B: ampincillin+cloxaccillin (PO) 500mg 8 hourly for 10 -14 days
ForChildren:
B: ampicillin+cloxacillin (PO) 15mg/kg 6hourly for 7 -14day
AND
A: paracetamol (PO) 500mg to 1g 4-8hourly as needed

ForChildren ≤ 10kg:
A: paracetamol (PO) 10mg/kg 4-8hourly as needed

For Children >


A: paracetamol (PO) 10kg: 15mg/kg 4-8hourly as needed
OR
A: ibuprofen (PO) 200mg to 400mg 4-8hourly as needed
For Children ≥ 6 months:
A: ibuprofen (PO) 5mg to 10mg/kg 4-8hourly as needed.
OR
C: diclofenac+ paracetamol (PO) 50mg diclofenac and 500mg paracetamol 4-8hourly as
needed

15.2.3 Ear Keloid


This is abnormal proliferation of scar tissue that forms at the site of cutaneous injury and grows
beyond the original margins of the scar. Most common causes are ear piercing, trauma or surgical
incisions.

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Clinical presentation
• Swelling of the involved area of the ear, most commonly ear lobe

Non-pharmacological management
• Use of pressure therapy e.g. pressure clips

Pharmacological management- Intra-lesional steroid injection


D: betamethasone (Intra-lesional) 6-12mg depending on the size of the lesion weekly for 4
weeks before excision and 4weeks after excision
OR
D: triamcinolone acetonide (Intra-lesional) 40mg depending on the size of the lesion
weekly for 4weeks before excision and 4weeks after excision

Surgical management
• Total keloidectomy+/-Steroid injection. (SHOULD BE DONE BY SOMEONE WITH
EXPERTISE)

15.2.4 Cerumen Impaction


Usually occurs following the use of cotton buds which hinder the natural movement of cerumen
outwards
Clinical presentation
• Reduced hearing • Itching
• Ear pain • Tinnitus
• Ear fullness

Pharmacological management
A: hydrogen peroxide 3% ear drops2-4drops each ear 6-8hourly for 7days.

Non-pharmacological Treatment:
• Remove using cerumen hook, syringing or suctioning under direct vision

Note
Patient should be educated on cleansing mechanism of the ear and not to use cotton bud.

15.2.5 Foreign Body in the Ear


Usually happens in children. Common foreign bodies include beads, stones and seeds (bean,
maize, orange). In adult’s foreign bodies include cotton bud and insect

Non-pharmacological Treatment:
• Restrain the child • An insect should be killed (by soaking
• Remove using a cerumen hook under the ear canal with normal saline or spirit)
direct vision (if the child cannot be before removal
restrained, sedation is advised)

Note
Do not attempt to remove ear foreign body if you don’t have proper instruments and expertise.

15.2.6 Traumatic Tympanic Membrane/ Ear Drum Perforation.


Clinical presentation
• History of trauma direct or indirect
• Ear bleeding +/-discharge
• Ear pain/otalgia

Non-pharmacological Treatment
• For indirect trauma avoid ear drops and water in the ear
• For direct trauma aural toilet can be done then ear drops instilled

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Pharmacological management
A: hydrogen peroxide 3% ear drops 2-4drops each ear 6-8hourly for 7days
AND
A: ciprofloxacin ear drops, 2-4drops each ear 6-8hourly for 14days
AND
A: ciprofloxacin (PO) 500mg Adults and children above 12years 12hourly for 5-7days
OR
C: ciprofloxacin (IV) 400mg 12hourly for 5-7days then for 5-7days
AND
A: paracetamol (PO) 500mg to 1g 4-8 hourly as needed.
For Children ≤ 10kg:
A: paracetamol (PO) 10mg/kg 4-8 hourly as needed.
For Children >10kg:
A: paracetamol (PO) 15mg/kg 4-8 hourly as needed
OR
A: ibuprofen (PO) 200 mg to 400mg 4-hourly as needed.
For Children ≥ 6 months:
A: ibuprofen (PO) 5mg to 10mg/kg 4-8 hourly as needed
OR
C: diclofenac+paracetamol (PO) 50mg diclofenac and 500mg paracetamol 4-8hourly as
needed

15.3 Otitis Media (Acute or Chronic)


It is an inflammation of the middle ear cavity. It is considered acute when the inflammation is of less
than 2 weeks’ duration, and chronic when the inflammation is of more than 2 weeks’ duration with
tympanic membrane perforation.

Clinical presentation
• Examine the pinna
• Using an otoscope carefully examine the external auditory canal and the tympanic membrane

15.3.1 Acute Otitis Media


Clinical presentation
• Previous upper respiratory tract infection • Fever
• Painful ear • Hearing often reduced
• Restlessness • Inflamed, bulged tympanic membrane

Non-pharmacological Treatment:
• Acute otitis media should be treated with analgesics, antibiotics and/or paracentesis/
(Myringotomy) to reduce pain and to obtain pus for culture and sensitivity)

Pharmacological Treatment:
B: amoxicillin+clavulanic acid (PO) 375–625mg 12hourly for 10days
OR
A: azithromycin (PO) 500mg 24 hourly for 5days (for patients who are allergic to penicillin) For
Children
A: azithromycin (PO) 10mg/kg 24hourly for 5days
OR
B: ceftriaxone (IV) 1 to 2 g 12hourly for 10days.
For Children:
B: ceftriaxone (IV) 50 to 100mg/kg 24hourly for 10days
OR
C: clarithromycin (PO) 500mg 12hourly for 10-14days.
ForChildren ≥ 6 months:
C: clarithromycin (PO) 15mg/kg/day in 2divided doses for 10-14days
OR
S: cefixime (PO) 400mg 24hourly for 10-4days

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For Children ≥ 6 months to 12 years (weight below 45kg):
S: cefixime (PO) 8mg/kg 24hourly for 10-14days
AND
A: paracetamol (PO) 500mg to 1g 4-8hourly for 3days.
For Children ≤ 10kg:
A: paracetamol (PO) 10mg/kg 4-8hourly for 3days
For Children >10kg:
A: paracetamol (PO) 15mg/kg 4-8 hourly for 3days.
OR
A: ibuprofen (PO) 200mg to 400mg 4-8hourly as needed.
For Children ≥ 6 months:
A: ibuprofen (PO) 5mg to 10mg/kg 4-8hourly as needed
OR
C: diclofenac+ paracetamol (PO) 50mg diclofenac and 500mg paracetamol 4-8hourly as
needed

Note: For antibiotics, treatment periods shorter than 10 days increase the risk of treatment failure

Referral
• Children with high fever, severe ear pain, headache, altered state of consciousness
• A chronically discharging ear that persists in spite of proper treatment.
• Foul smelling ear discharge
• Mastoiditis
• Otitis in the normal (or better hearing) ear combined with permanent hearing loss in the other
ear

15.3.2 Chronic Suppurative Otitis Media


This is a perforated tympanic membrane with persistent drainage from the middle ear for more than
2-6 weeks. Most common causative organisms are Pseudomonas aeruginosa, Staphylococcus
aureus, Proteus species, Klebsiella pneumonia, and diphtheroids.

Clinical presentation
• Discharge of pus from the ear
• Perforated tympanic membrane
• Reduced hearing

Non-pharmacological Treatment:
• Keep ear dry/avoid water into the ear
• Aural toilet – ear suctioning under direct vision(otomicroscopy/endoscopy), removal of debris
• Ear wicking regularly, with a dry cotton wick at home

Pharmacological Treatment
C: ciprofloxacin ear drops, three drops12hourly for 14days
A: hydrogen peroxide 3% ear drops: 2 to 4 drops each ear 6-8hourly for 14days
OR
A: boric acid ear drops: 2-4 drops each ear 6-8hourly for 14days
OR
D: ofloxacin ear drops: 2 to 4 drops each ear 6-8hourly for 14days
AND
A: ciprofloxacin (PO) 500mg 12hourly for 10days

ForChildren:
A: ciprofloxacin (PO) 10–20mg/kg 12hourly for 10days

Surgical management
• Mastoidectomy • Tympano-mastoidectomy
• Endoscopic tympanoplasty • Ossiculoplasty

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Note
Treatment of shorter than 10 days will result into treatment failure
Avoid ototoxic drugs(gentamycin , neomycin and quinine) if there is TM perforation

15.3.3 Mastoditis with Sub-Periosteal Abscess


It is due to infection of the mastoid air cells in the middle ear, a complication of chronic suppurative
otitis media. It presents as a fluctuant painful swelling on the post auricular area. The overlying skin
is also inflamed.

Non-pharmacological Treatment
Aspirate the swelling before incision and drainage, and then refer for mastoidectomy at a
zonal/national hospital

Pharmacological Treatment:
C: ciprofloxacin ear drops, 3drops, 12hourly for 14days
AND
A: ciprofloxacin (PO) 500mg 12hourly for 10days; Children 10–20mg/kg 12hourly for
10days

Investigations
• Culture &sensitivity
• CT SCAN-Temporal Bone

Surgical management
• Incision and drainage • Tympano-mastoidectomy
• Mastoidectomy/Drainage • Ossiculoplasty
mastoidectomy

Note
Treatment shorter than 10days will result into treatment failure

15.3.4 Otitis Media with Effusion


It is a multifactorial, inflammatory condition in the middle ear with serous or mucous accumulation
without ear discharge. It is a residual condition after acute otitis media and rhino sinusitis with
Eustachian tube dysfunction.

Diagnostic Criteria
It is often discovered by chance.
• Little or no ear pain
• Gradual loss of hearing
• No ear discharge
• Aural fullness

Non-pharmacological Treatment
• Close follow-up
• Valsava maneuver
• Encourage chewing

Pharmacological Treatment
D: fluticasone propionate (50mcg/spray) nasal spray. Adults and adolescents more than
12years: 2sprays in each nostril 24hourly as needed. Children 4-1years: 1spray in each
nostril 24hourly as needed.
OR
S: mometasone (nasal spray) Adults and adolescents from 12years: 1 sprays in each
nostril 24hourly as needed. Children 6-11years: 1spray in each nostril 24hourly as needed
AND
B: ephedrine (0.5% and 1%) nasal drop, Adults and children above 12years: Instill 1 to 2
drops in each nostril, not more than 4 times a day for 3 to 5 days

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Note
Otitis media with effusion with hearing loss that does not improve after 3months should be
referred to a specialist for myringotomy and grommets insertion

Surgical management
Myringotomy+grommet insertion (microscopic/endoscopic) +Adenotonsilectomy (In children)
15.4 Hearing Loss
A child with hearing loss should be detected and intervention started immediately after delivery. New
born hearing screening is done using an otoacustic emission machine. Any child suspected of
hearing loss (usually presenting with delayed speech development) should be referred to a
zonal/national hospital immediately since early intervention has a better outcome.

15.4.1 Sensorineural Hearing Loss (SNHL)


Loss of hearing that results from defective function of cochlea or auditory pathway. It may be
congenital or acquired.
Clinical presentation
• Hearing impairment as confirmed by hearing assessment tests.

Investigation
• Distraction Test/Free Field Test – • Auditory Brainsterm Response
for children (ABR)
• Tympamomery • CT-Scan/MRI for bone cochlea and
• Audiometry auditory nerve assessment for pre
• Otoacoustic emission(OAE) cochlea implantation

Non-pharmacological management (Rehabilitation)


• Avoiding exposure to noises • Bone-anchored hearing Aid(BAHA)
• Avoiding unnecessary use of • Cochlea Implantation (C.I), with
ototoxic drugs interval
• Digital programmable hearing aid- programming/troubleshooting –for
for mild to moderate SNHL severe and profound SNHL.
• Super power digital programmable • Speech therapy
hearing aid-for severe and • Sign language/lip reading
profound SNHL

Pharmacological management
C: calcium +vitamins 1tablets 24hourly for not less than 3months
Surgical management
Posterior tympanotomy for cochlear implantation

15.4.2 Sudden Sensorineural Hearing Loss


Clinical presentation
• Sudden onset of hearing loss 24-72 hours from onset, unilateral or bilateral.
• Tinnitus
Investigations
• Tympamomery
• Audiometry

Pharmacological management
A: prednisolone (PO) 60mg 24hourly for 5days then taper down to 50mg 24hourly for next
5days.
For Children:
A: prednisolone (PO) 1mg/kg 24hourly for 5days then taper down by half for the next
5days.
AND
C: calcium and vitamins 1tablet 24hourly for not less than 3months

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15.4.3 Otosclerosis
Otosclerosis is a bony overgrowth that involves the footplate of the stapes. As the overgrowth
develops, the stapes can no longer function as a piston, it become fixated. Conduction gradually
becomes worse until a maximal conductive hearing loss of 60 dB is reached.

Clinical presentation
• Hearing loss
• Dizziness
• Tinnitus
Investigations
• Tympanomety
• Pure tone Audiometry (PTA)
• CT- Scan -of temporal bone

Non-pharmacological management
• Hearing aids (H/A)-Digital Programmable Hearing Aids
• Cochlea implantation

Surgical management
• Stapedectomy
• Posterior tympanotomy for Cochlea Implantation

15.4.4 Peripheral Vertigo (Meniere’s disease and Benign Paroxysmal Positional


Vertigo(BPPV)
Clinical presentation
Meniere’s disease Benign Paroxysmal Positional Vertigo( PPPV)
Vertigo Vertigo
Nausea Nausea
Vomiting Vomiting
Tinnitus Directional specificity
Aural Fullness
Reduced Hearing
Reduced Hearing
Investigation
• Audiometry • MRI Brain-to rule out
• Vestibular test cerebellopontine angle (CPA)
• Video nystagmogram (vNG) tumours
• Video head impulse test (vHIT)

Non-pharmacological management (FOR BPPV)


• Epley maneuver • Vestiulr rehabilitation therapy
• Berbecure maneuver • Stabilometer

Pharmacological management (FOR MENIERES)


C: betahistidine (PO) 24-48mg 1 hourly for 14days. Maintanance dose 24mg 24hourly for
14days.
AND
B: intratympanic dexamethasone (IV) 4mg
AND
C: acetazolamide (PO) 250mg 24hourly for 14days

15.4.5 Vestibular Neuritis /Vestibular Neuronitis and Labyrinthitis


Clinical presentation
• Rapid onset severe vertigo, nausea, vomiting
• Spontaneous vestibular nystagmus

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• Gait instability

Pharmacological management
A: prednisolone (PO) 60mg 24hourly for 5days then taper down to 50mg 24hourly for next
5days.
For Children:
A: prednisolone (PO) 1mg/kg 24hourly for 5days then taper down by half for the next
5days.
OR
D: methylprednisolone (IV) 100mg 24hourly then taper to 10mg over 3weeks.

15.4.6 Vestibular Migraine


Clinical presentation
• Dizziness/Vertigo
• Moderate to severe temporal headache
• Sensory amplification e.g. hyperaccusis

Investigations
• Audiometry • MRI Brain-to rule out
• Vestibular test cerebellopontine angle
• Video nystagmogram(vNG) (CPA)tumours
• Video head impulse test(vHIT)

Pharmacological management
A: propranolol (PO) 40mg 12hourly for 14days
OR
C: amlodipine (PO) 10mg 24hourly for 14days

15.4.7 Tinnitus
Clinical presentation
• Perception of sound in proximity to the head in the absence of an external source

Non-pharmacological management
• Tinnitus masking

Pharmacological management
C: betahistidine (PO) 16-24mg 8hourly for 14days

For Children 5-12 years:


C: acetazolamide (PO) 250mg 24hourly 14days

15.4.8 Glomus Tumours


Paragangliomas are rare neuroendocrine tumors that arise from the extra-adrenal autonomic
paraganglia, small organs consisting mainly of neuroendocrine cells that are derived from the
embryonic neural crest and have the ability to secrete catecholamines

Clinical presentation
• Neck mass (at angle of • Hearing loss(conductive)
mandible) • Rising sun signs
• Pulsatile tinnitus

Investigations
• Audiometry • CT-angiogram
• CT-Scan-head & neck • MRI-neck

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Surgical management
• Glomus Tumour excision

15.4.9 Vestibular Schwannomas


Also known as acoustic neuromas, acoustic schwannomas, acoustic neurinomas, or vestibular
neurilemomas) are Schwann cell-derived tumors that commonly arise from the vestibular portion of
the eighth cranial nerve.

Clinical presentation
• Hearing loss
• Tinnitus
Investigations
• Audiometry
• MRI-brain (with gadolinium as contrast)

Non-pharmacological management
• Observation/watchful waiting
• Radiotherapy

Surgical management
• Tumour (schwanoma) excision
15.5 Nose/Paranasal Sinuses Conditions
15.5.1 Acute Rhinitis
It is a viral inflammatory condition in the nasal mucous membrane, usually part of a more wide-
spread infection of the upper respiratory tract.

Non-pharmacological Treatment
• Bed rest& warm drinks

Pharmacological Treatment
A: ephedrine nasal drops (1% for adults and 0.5% for children) 1–2drops into each nostril
6hourly for not more than 5days

15.5.2 Acute Non-Allergic Rhinitis


Clinical presentation
• Nasal blockage
• Post nasal drip
• Erythematous turbinate

Pharmacological management
B: ephedrine (0.5% and 1%) nasal drop, Adults and children above 12years: Instill 1-
2drops in each nostril, not more than 4times a day for 3-5days
OR
C: oxymetazoline (0.05%) nasal drops/spray Dosage for adults and children above 6years:
Instill 2 -3drops or sprays in each nostril 12hourly for 3-5days
AND
D: fluticasone propionate (50mcg/spray) nasal spray, Adults and adolescents more than
12years: 2sprays in each nostril 24 hourly as needed. children 4-11years: 1 spray in each
nostril 24hourly as needed
OR
S: mometasone nasal spray, Adults and adolescents from 12years: 1sprays in each nostril
24hourly as needed, children 6-11 years: 1spray in each nostril 24hourly as needed
A: prednisolone (PO), Adults: 60mg 24hourly for 5days then taper down to 50mg 24hourly
for next 5days. Children: 1mg/kg 24hourly for 5days then taper down by half for the next
5days.

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Note
Oral drugs to reduce swelling of the mucous membrane, antihistamines and antibiotics are not
indicated

15.5.3 Allergic Rhinitis


It is an irritation of the nasal mucosa by an allergen in a previously sensitized individual. Common
allergens include house dust (mite’s feaces), pollens, cockroach antigen, animal dander, molds (in-
door)

Clinical presentation
• Itchy nostrils, throat, eyes • Sneezing
• Watery nasal discharge • Post nasal drip
• Nasal congestion • Cough

Investigations:
• Anterior rhinos copy – watery nasal discharge, nasal congestion
• Total or specific IgE
• Skin prick Allergy test

Non-pharmacological management
• The main treatment of allergic rhinitis is the Avoidance of the triggers.
• Steaming
• Immunotherapy

Pharmacological Treatment:
A: ephedrine (0.5% and 1%)nasal drop, Adults and children above 12years: Instill 1 to
2drops in each nostril, not more than 4 times a day for 3-5days
OR
C: oxymetazoline (0.5%) nasal drops/spray, Adults and children above 6 years: Instill 2- 3
drops or sprays in each nostril every after 12 hours for 3-5days
AND
D: fluticasone propionate (50mcg/spray) nasal spray, Adults and adolescents more than
12years: 2sprays in each nostril 24 hourly as needed. children 4-11years: 1spray in each
nostril 24hourly as needed
OR
S: mometasone nasal spray, Adults and adolescents from 12years: 1 sprays in each
nostril 24 hourly as needed. children 6 to 11 years: 1 spray in each nostril 24 hourly as
needed.
AND
A: prednisolone (PO): 60mg 24hourly for 5days then taper down to 50mg 24 hourly for
next 5days. Children: 1mg/kg 24hourly for 5days then taper down by half for the next
5days.
AND
C: loratadine (PO), Adults: 10mg 24hourly for 30days. Children 2-6years: 5mg 24hourly for
14days. Children above 6 years: 10mg 24 hourly for 14 days
OR
S: desloratadine (PO)Adults: 5mg 24hourly for 30days. Children 2-5 years: 1.25mg
24hourly for 14days. Children 6 to 12 years: 2.5mg 24hourly for 30days
AND
S: montelukast, Adults: 10mg 24hourly for 30days.Children 1-15 years: 5mg 24hourly for
14days

15.6 Granulomatous Diseases of the Nose


15.6.1 Rhinoscleroma

Clinical presentation
• Rhinitis, Fetid rhinorrhea • Intranasal rubbery nodules
• Crusting, Nasal bleeds • Dysphonia

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• Fibrosis, Nasal deformity

Non-pharmacological management
• nasal douching with saline solution

Pharmacological management
A: ciprofloxacin (PO), Adults and children above 12years: 500mg 12hourly for 4-12weeks.
Continue treatment for at least 2days after signs and symptoms have disappeared.
OR
S: cefixime (PO), Adults: 400mg 24hourly for 4-12weeks. Children ≥ 6months to 12years
(weight below 45kg): 8mg/kg 24hourly for 4-12weeks
AND
A: prednisolone (PO) Adults: 60mg 24hourly for 5days then taper down to 50mg 24hourly
for next 5days. Children: 1mg/kg 24hourly for 5days then taper down by half for the next
5days.

Surgical management
• Rhinoplasty

15.6.2 Tuberculosis of the Nose

Clinical presentation
• Nasal pain • Mass in the nose
• Nasal bleeing • Nasal deformity

Investigations
• Nasal mucosal scraping for AFB/gene expert
• Skin biopsy for Histology and AFB

Pharmacological management
Refer TB Program

15.6.3 Syphilis of the Nose

Clinical presentation
• Nasal discharge • Ulceration of nose
• Nasal crusting • Saddle nose
• Epistaxis

Investigations
VDRL

Non-pharmacological management
• Crusts Removal-Endoscopic

Pharmacological management
Refer STI chapter

15.6.4 Rhinosporiodiosis
Nasal disease caused by rhinosporidium seeberi
Clinical presentation
• Unilateral nasal obstruction • Pink or deep red polyp, strawberry
• Epistaxis like appearance, Bleeds easily on
• Local pruritus manipulation
• Rhinorrhea

329
Pharmacological management
S: dapsone (PO), Adults: 100mg 24hourly for 6months. Children1-2mg/kg 24hourly, not to
exceed 100mg 24hourly

Surgical management
Wide excision with wide area electro-coagulation of the lesion base

15.6.5. Mucormycosis
This is fungal infection of nose, caused by mucor, rhizopus species.

Clinical presentation
• Fever, Headache • Eshar of nasal mucosa
• Nasal congestion, Purulent nasal • Proptosis, Blindness
discharge
• Facial numbness

Pharmacological management
S: amphotericin B (IV): Adults, Test dose of 1mg IV infused over 20-30 minutes. Loading
dose of 0.25-0.5mg/kg infused over 2-6hours. Maintenance dose of 0.25-1mg/kg IV
24hourly for 3-6weeks. Dosage for children: Test dose of 0.1mg/kg not to exceed 1mg:
infused over 20-60minutes. Loading dose of 0.25mg/kg infused over 2-6hours.
Maintenance dose of 0.25/kg 24hourly to ensure a total dose of 30-40mg/kg is given over
3-6weeks

Surgical management
Endoscopic debridement of the necrotic tissues under general Anastasia(GA)

Note
High index of suspicion in patient with DKA and nasal symptoms

15.7 Other Conditions of the Nose


15.7.1 Nasal septal Abscess and Hematoma
Clinical presentation
• Nasal pain • Bilateral nasal blockage with boggy
• Fever septal mass
• History of trauma for septal hematoma • Aspiration will confirm the diagnosis
• Nasal swelling

Pharmacological management
B: ampicilin+cloxacilin (FDC) (PO) Adults: 500mg 8hourly for 10-14days. Children:
15mg/kg 6hourly for 7-14days
OR
B: amoxycillin+clavulanate (PO) Adults: 625mg to 1g 12hourly for 7-14days. Children ≤3
months: 30mg/kg/day in 2 divided doses for 7-14 days. Children >3 months: 25mg/kg/day
in 2 divided doses for 7-14 days
AND
A: paracetamol (PO/IV), adults: 500mg to 1g 4-8hourly as needed. Children ≤10kg:
10mg/kg 4-8hourly as needed. Children >10kg: 15mg/kg 4 to 8hourly as needed.
OR
A: ibuprofen (PO) Adults: 200-400mg 4-8hourly as needed. Children≥6 months: 5-10mg/kg
4-8hourly as needed
OR
C: diclofenac+ Paracetamol (PO) Adults: 50mg diclofenac and 500mg paracetamol 4-
8hourly as needed

330
Surgical management
• Intranasal Incision and drainage
• Tight bilateral nasal packing or Suturing of mucoperichondrial to prevent re-accumulation

15.7.2. Choanal Atresia


This is failure of canalization of choanal OR is obliteration or blockage of the posterior nasal
aperture.
It can be unilateral or bilateral. If bilateral it is surgical emergency.

Clinical presentation
• New born presenting with cyanosis while at rest which improve on crying
• Thick nasal discharge on the defective nostril
• Failure to pass nasogastric tube
• Thread/cotton test

Investigation
• CT-SCAN-Paranasal sinuses(PNS)

Non-pharmacological management
• For bilateral choanal atresia put oropharyngeal airway then refer to specialized hospital.

Surgical management
• Choanal atresia release (open or endoscopic)

15.7.3 Nasal Turbinate Hypertrophy


Turbinate hypertrophy is a complication of allergic rhinitis
Clinical presentation
• snoring
• Nasal obstruction
• Nasal irritation
• Enlarged inferior or middle turbinate on rhinoscopy

Pharmacological Management
As for Allergic Rhinitis

Surgical management
Partial submucosal Turbinectomy – (open or endoscopic)

15.7.4 Nasal Bone Fracture


Clinical presentation
• History of nasal trauma • Nasal bleeding
• Deviation of nose or septum • Nasal obstruction

Pharmacological management (antibiotics & analgesics)-As for nasal septal abscess and
hematoma
Surgical Management-Closed reduction and alignment of nasal structures under LA or GA this
should be 1-2weeks if there is edema. Can be done using nasal speculum or endoscopically.

15.7.5 Nasal Septal Deviation (Non-Traumatic)


Clinical presentation
• nasal obstruction
• nasal dryness
• +/_Nasal bleeding

331
Surgical management
• Septoplasty –open or Endoscopic

15.7.6 Adenoid Hypertrophy


It is hypertrophy of the lymphoid tissues in the nasopharynx; presenting with mouth breathing,
snoring sleep apnea and otitis media with effusion. It is reported mainly in children.

Investigations: Nasopharynx lateral view X-ray.

Pharmacological Treatment:
A: cetirizine (PO) 10mg nocte for 2weeks. Children: 5mg nocte for 2weeks
AND
A: 0.9% sodium chloride nasal spray/drops 4hourly for 2weeks
AND
B: azithromycin (PO) 500mg 24hourly for 3days. Children: 10mg/kg 24 hourly for 3days
OR
B: amoxicillin+clavulanic acid (PO) (FDC) Adults: 625mg (500mg amoxicillin+125mg
Clavulanic acid) 8hourly for 7days
Children: 375mg (250mg amoxicillin+ 125 Clavulanic acid) 12hourly for 7days;
OR
S: cefixime (PO) Adults: 400mg 24hourly for 7-14days. Children ≥ 6months to 12years
(weight below 45kg): 8mg/kg 24hourly for 7-14days
OR
C: clarithromycin (PO), Adults: 500mg12 hourly for 7-14days. Children ≥ 6months:
15mg/kg/day in 2divided doses for 7-14days
AND
A: paracetamol (PO) 1gm 8hourly until fever is controlled: Children 10mg/kg body weight
8hourly until fever is controlled.

Surgical management
Adenotonsilectomy/Adenotomy+/-Myringotomy and Gromet insertion

Note
An adult with snoaring upper aerodigestive tumours and Obstructive Sleep Apnea (OSA)should be
considered.

15.7.7 Acute Rhinosinusitis


It is the inflammation of the mucosal lining of the nose and paranasal sinuses of not more than 12
weeks’ duration. In sinusitis of dental origin, anaerobic bacteria are often found.

Acute Purulent Rhinosinusitis


Bacterial infection with pus accumulation in one or more of the paranasal sinuses

Clinical presentation
• Nasal discharge (watery or • Ear pain and blockage
purulent) • Anterior rhinoscopy –
• Nasal congestion watery/purulent nasal discharge
• Post nasal dripping occasionally foul smelling
• Headache worsening on bending • Nasal congestion
forward and more in the morning • Plain paranasal sinuses X ray
(Water’s, Caldwell views)
• Fever
• Mucosal thickening; air fluid levels
• Facial pain

Pharmacological Treatment:
B: azithromycin (PO) 500mg 24hourly for 3days. Children: 10mg/kg 24hourly for 3days
OR
B: amoxicillin+clavulanic acid (PO) 625mg 8hourly for 7days Children: 375mg 12hourly for
7days;
OR

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C: clarithromycin (PO), 500mg 12hourly for 7-14days. Children ≥ 6 months: 15mg/kg/day
in 2divided doses for 7-14days
OR
B: ceftriaxone (IV) Adults: 1-2 g12hourly for 7 days. Children: 50 to 100mg/kg once for
7days
OR
S: cefixime (PO) Adults: 400mg 24hourly for 7-14 days. Children ≥ 6 months to 12years
(weight below 45kg): 8mg/kg 24hourly for 7-14days
AND (for fungal rhinosinusitis)
D: itraconazole (PO) Adults: 200mg 24hourly for 30days. Children: 50-100mg/kg once for
7days
OR
S: amphotericin B (IV) Adults: Test dose of 1mg IV infused over 20-30minutes. Loading
dose of 0.25-0.5mg/kg IV infused over 2 to 6 hourly. Maintenance dose of 0.25-1mg/kg
24hourly for 3-6weeks for children: Test dose of 0.1mg/kg not to exceed 1mg: infused
over 20-60minutes Loading dose of 0.25mg/kg infused over 2-6hours. Maintenance dose
of 0.25/kg 24hourly to ensure a total dose of 30-40mg/kg is given over 3-6weeks
AND
B: ephedrine (0.5% and 1%) nasal drop, Adults and children above 12years: Instill 1 to
2drops in each nostril, not more than 4 times a day for 3 to 5days
OR
S: xylometazoline (0.05% and 0.1%) nasal drops/spray, Adults and children above 6years:
Instill 2 to 3drops in each nostril 8hourly for 3 to 5days or1 to 2sprays in each nostril
8hourly for 3 to 5days
OR
D: fluticasone propionate (50mcg/spray) nasal spray, Adults and adolescents more than
12years: 2sprays in each nostril 24hourly as needed. Children 4-11years: 1spray in each
nostril 24hourly as needed
OR
S: mometasone nasal spray, Adults and adolescents from 12years: 1sprays in each nostril
24hourly as needed. Children 6-11years: 1spray in each nostril 24hourly as needed.
AND
A: paracetamol (PO) Adults: 500mg to 1g 4-8hourly as needed. Children ≤ 10kg: 10mg/kg
4-8hourly as needed. Children >10kg: 15mg/kg 4-8hourly as needed
OR
A: diclofenac (IM) Adults: 75mg 8hourly as needed
OR
C: diclofenac (PO) Adults: 50mg 4-8 hourly as needed
OR
C: ibuprofen (PO) Adults: 200-400mg 4-8 hourly as needed. Children ≥ 6 months: 5-
10mg/kg 4-8hourly as needed

Non-pharmacological management
• Saline nasal wash
• Steaming with or without Vicks

Note: Treatment periods shorter than ten days increase the risk of treatment failure

Referral: To ENT Specialists


• Children with ethmoiditis presenting as an acute periorbital inflammation or orbital cellulitis must
be hospitalized immediately (ophthalmology consultation should be sought)
• Adults with pronounced symptoms despite treatment
• If sinusitis of dental origin is suspected
• Recurrent sinusitis (>3 attacks in a year) or chronic sinusitis (duration of illness of >12 weeks)

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Surgical management
Surgery if associated with complications eg obital/periobital abscess, pottys puffy tumour, Brain
abscess and nasal polyposis etc.
• Frontal Trephination
• Open ethimoidectomy
• Functional Endoscopic Sinus Surgery (FESS)

15.7.8 Chronic Rhinosinusitis


Can be caused byBacterial or Fungal

Clinical presentation
• Anterior and/or posterior nasal mucopurulent drainage
• Nasal obstruction/nasal blockage/congestion
• Facial pain, pressure and/or fullness
• Hyposmia or Anosmia
• Halitosis

Investigations
CT Scan of paranasal sinuses (PNS)-gold standard-should be done after adequate medical
treatment with persistent symptoms.

Non-pharmacological management
• Saline nasal wash
• Steaming with or without vicks

Pharmacological Treatment: as for acute sinusitis BUT should be for 4-6 weeks

Surgical Management-Surgery if associated with complications eg obital/periobital abscess, pottys


puffy tumour, Brain abscess and nasal polyposis etc and Failure of disease resolution after
adequate medical treatment.
Frontal Trephination
OR
Caldwel Luc operation
OR
Open ethimoidectomy
OR
Functional Endoscopic Sinus Surgery (FESS)

15.7.9 Nasal Polyposis


This is mucosal change due to chronic mucosal inflammation. Ethmoidal polyp- This is a
complication of allergic rhinitis or chronic rhinosinusitis. Antrochoanal polyp benign tumor of the
maxillary sinus that prolapse to the nasal cavity.

Clinical presentation
• History of allergy or asthma
• Nasal congestion/blockage
• Nasal discharge
• Snoaring and mouth breathing
• Post nasal dripping

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Investigations
• Direct nasal Endoscopy (DNE) or Fiber optic nasopharyngoscopy
• Serum Total/specific IgE
• CT-Scan of paranasal sinuses (CT-PNS)

Pharmacological Management-As for allergic rhinitis/acute rhinosinusitis

Surgical management
i. Intranasal polypectomy
ii. Partial/Medial maxillectomy
iii. Functional Endoscopic Sinus surgey(FESS)

15.7.10 Nose Bleeding (Epistaxis)


Nose bleeding is a condition which is common in adults. It may be due to a local cause in the nasal
cavity (e.g. trauma, tumor, foreign body, septal varices, or septal deviation); or a systemic cause
(e.g. blood disorders, vascular disorders, renal failure, hepatic failure, or use of anticoagulants
(warfarin, heparin). Most cases of epistaxis are minor; do not require hospitalization. Patients with
significant nose bleeding do require hospitalization.

Non-pharmacological Treatment
• Stabilize the patient: put an open intravenous line, do blood grouping and cross matching
• Put the patient in a sitting position and advise the patient to pinch the soft part of the nose
gently for 5minutes
• Put on a gown, glasses, head light and sterile gloves and evacuate clots.Do a thorough
head and neck examination
• Cauterize septal varisces (if any) using a silver nitrate pencil
• Do an anterior nasal packing by introducing into the nasal cavity as far posterior as
possible sterile Vaseline gauzes (or iodine soaked gauzes if not available) or special
merocele pack,using a dissecting forcep (if bayonet forcep is not available)
• Put rolled dry gauze on the collumela and plaster it

If the patient is still bleeding


• Do a posterior nasal packing using a Foley’s catheter introduced through the nasal cavity
into the oropharynx, balloon it with normal saline up to 10–15cc while pulling it outward to
impinge on the posterior nasal choana, then do anterior nasal packing as above
• Put dry gauze on the nose to prevent necrosis of the collumela and fix the catheter on the
nose with an umbilical clamp
• Almost all of the nasal bleedings will be controlled by this way

Note: Remove the packs after 72 hours

Pharmacological Treatment (to prevent rhinosinusitis)


B: azithromycin (PO) 500mg 2 hourly for 3days. Children: 10mg/kg 24hourly for 3days
OR
B: amoxicillin+ clavulanic acid (PO) Adults: 625mg 8hourly. Children: 375mg 12hourly for
7days
AND
A: paracetamol (PO) 1gm 8hourly until fever is controlled Children 10 mg/kg body weight 8
hourly until fever is controlled
AND
A: ephedrine (0.5% and 1%)nasal drops, Adults and children above 12 years: Instill 1 to
2drops in each nostril, not more than 4times a day for 3-5days
OR
S: xylometazoline (0.05% and 0.1%) nasal drops/spray. Adults and children above 6
years: Instill 2 to 3drops in each nostril 8hourly for 3 to 5days or 1 to 2sprays in each
nostril 8hourly for 3 to 5days.
AND
C: tranexamic acid (PO/IM) Adults: 500mg 8hourly for 5 to 8days. Children: 25mg/kg 6 or
8hourly for 5-8days

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AND
C: silver Nitrate Stick-Apply on the lesion once IF the bleeding area is identified.

Note
Putting an ice cube on the forehead, extending the neck or placing a cotton bud soaked with
adrenaline in the vestibule will not help

Referral: refer the patient to the next facility with adequate expertise and facilities if:
• The patient is still bleeding repack and refer immediately
• Failure to manage the underlying cause, refer the patient

Surgical management
• Endoscopic electrical cauterization of the lesion for posterior nasal bleeding
• Ligation/Clipping/cauterization of bleeding vessel (open or endoscopic)

Note
Rule out systemic causes of epistaxis eg. renal, blood dyscrasias and liver failure.

15.7.11. Foreign Bodies in the Nose


This situation usually occurs in children.

Non-pharmacological Treatment:
• Restrain the child before removal using a cerumen hook, if the child cannot be restrained
sedation is advised

Note
A unilateral foul smelling nasal discharge in a child is due to a foreign body until proven otherwise

15.8 Throat Conditions


15.8.1 Pharyngotonsilitis
Pharyngotonsilitis is an acute inflammation of the pharynx and tonsils, which is characterized by
fever and a painful throat.

Pharmacological Treatment
B: azithromycin (PO) 500mg 24hourly for 3days. Children: 10mg/kg 24hourly for 3days
OR
B: amoxicillin+ clavulanic acid (PO)(FDC) Adults: 625mg 8hourly for 7days Children:
375mg 12hourly for 7days;
OR
C: clarithromycin (PO), Adults: 500mg 12hourly for 7-14days. Children ≥ 6 months:
15mg/kg/day in 2divided doses for 7-14days
OR
S: cefixime (PO) Adults: 400mg 24hourly for 7-14days. Children ≥ 6 months to 12 years
(weight below 45kg): 8mg/kg 24hourly for 7-14days
AND
A: paracetamol (PO) Adult 1gm 10mg/ kg body weight 8 hourly until the fever is controlled
OR
A: ibuprofen (PO) Adults: 200-400mg 4-8hourly as needed. Children ≥ 6 months: 5-
10mg/kg 4-8hourly as needed
OR
A: diclofenac (IM) Adults 75 mg 8hourly as needed
OR
C: diclofenac (PO) Adults: 50 mg 4-8hourly as needed
OR
C: diclofenac+ paracetamol (PO) (FDC) Adults: 50mg diclofenac and 500mg paracetamol
4-8hourly as needed

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Note
Refer the patient with tonsillitis to the specialist for tonsillectomy if
• Chronic tonsillitis
• Recurrent tonsillitis (>5attacks in a year or 3 or more attacks in 2 consecutive years)
• Obstructive tonsillitis (causing an upper airway obstruction)

Surgical management
• Tonsilectomy

15.8.2 Laryngitis
This is an infectious or non-infectious, acute or chronic inflammatory condition of the larynx. It
becomes chronic when the condition lasts for more than 3 weeks. The picture of the disease is
different in children and adults due to the small size of the larynx in children.
• Acute subglottic laryngitis occurs mainly in children under the age of seven, it is a viral
infection
• Edema of the mucous membrane of the subglottic space causes breathing difficulties,
especially on inspiration
• Laryngitis in children may require active treatment

15.8.3 Acute Laryngitis


Acute subglottic laryngitis occurs mainly in children under the age of seven, it is a viral infection.

Non-pharmacological Treatment
• Parents should behave calmly and avoid frightening the child
• Bed rest
• Keep the air damp and cool
• Give extra fluid

Pharmacological Treatment
A: adrenaline inhalation/nebulization effectively reduces symptoms

Table15.1: Doses of adrenaline Preparation


Age adrenaline(20 mg/ml) 0.9% Saline
0-6 months 0.1 ml 2 ml
6-12 months 0.15 ml 2 ml
>12 0.2 ml 2 ml
Note
The total fluid volume is inhaled in 5 minutes with the use of inhalator

AND
A: prednisolone (PO) Adults: 60mg 24hourly for 5days then taper down to 50mg 24hourly
for next 5days. Children: 1mg/kg 24hourly for 5days then taper down by half for the next
5days.
OR
A: hydrocortisone (IV/IM) Adults and children ≥ 12years: 100-500mg/dose IV/IM 4hourly as
needed. Children <12 years: 1-5mg/kg/day IV/IM divided 12hourly as needed
AND
B: amoxycillin + clavulanate (PO) (FDC) Adults: 625mg to 1g 12 hourly for 7-14 days.
Children ≤ 3 months: 30mg/kg/day in 2divided doses for 7-14days. Children >3 months:
25mg/kg/day in 2 divided doses for 7-14days
AND
A: cough suppressant Syrups-Dosage for adults: as instructed by a physician or
pharmacist.

Hospitalization
If severe symptoms persist or worsen after epinephrine inhalation, hospitalization is indicated.

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15.8.4 Chronic Laryngitis
Non-pharmacological Treatment:
• Voice rest • Refer to specialist for Rigid
• Stop smoking laryngoscopy (Endoscopy) OR
• Rehydration Fiber optic Nasolaryngoscopy

15.8.5 Acute Epiglottitis (AE)


Epiglottitis is an acute infectious inflammation of the epiglottis, supraglottic and hypopharynx which
occurs both in children and adults. It is commonly caused by Haemophilus influenzae. Epiglottitis is
a potentially lethal condition especially in children. Edema of the epiglottis may cause acute airway
obstruction.

Clinical presentation
• Throat pain and difficulty in • Patient prefers sitting posture with
swallowing an extended neck
• Drooling • Laborious inspiration
• Husky voice • Cough in some cases
• Fever often high and with chills • Anxiety

Investigations: Plain X-ray of the neck, lateral view characteristically presents with a positive thumb
sign (edematous epiglottis).

Non-pharmacological Treatment:
• Immediate hospitalization, preferably in the ICU
• Transportation: sitting, with oxygen supplementation
• Be prepared to treat respiratory failure (intubation or tracheotomy)

Pharmacological Treatment
B: azithromycin (PO) 500mg 24hourly for 3days. Children: 10mg/kg 24hourly for 3days
OR
B: amoxicillin+ clavulanic acid (PO)(FDC) Adults: 625mg 8hourly Children: 375mg 12hourly
for 7days;
AND
A: paracetamol (PO) 1gm 8hourly until fever is controlled. Children: 10 mg/kg body weight
8hourly

15.8.6 Non-infectious Chronic Laryngitis


[Laryngopharyngeal reflux disease (LPR) with Vocal cord nodules or Laryngeal polyp]
Clinical presentation
• Dysphonia or hoarseness • Globus sensation, Frequent throat
• Dry Cough clearing
• Dysphagia

Investigations - Rigid laryngoscopy (Endoscopy) OR Fiber optic Nasolaryngoscopy

Non-pharmacological Treatment
• Dietary modification, spice foods and feeding times
• Life style changes; avoid alcohol, tobacco
• Voice rest

Pharmacological Treatment
C: pantoprazole (PO) Adults: 40mg 24hourly for 8-12 weeks
Children ≥ 5 year:
C: pantoprazole (PO) 20mg 24hourly for 8-12 weeks
For <40kg
C: pantoprazole (PO) 20mg 24hourly for 8-12 weeks
For >40kg
C: pantoprazole (PO) 40mg 24hourly for 8-12 weeks

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OR
C: lansoprazole (PO) Adult 30mg. Paediatric ≥ 1 to 12years: <30kg 15mg;>30kg give
30mg 24hourly for 8 – 12 weeks.
OR
S: esomeprazole (PO) Adult 40mg. Paediatric ≥ 1 to 12 years 10-20mg. Paediatric >12
years 20-40mg 24 hourly for 8-12weeks.
C: antiacid liquid/mixture10-15mls 12hourly for 10-14days.
AND
A: prednisolone (PO): Adult 60mg 24hourly for 5days then taper down to 50mg 24hourly
for next 5days.
For Children:
A: prednisolone (PO): 1mg/kg 24hourly for 5days then taper down by half for the next
5days.
OR
D: triamcinolone acetonide. Adult (IM) 40-80mg stat. Children 6-12years: 0.2mg/kg stat
AND
C: loratadine (PO) Adults: 10mg 24hourly for 14days. Children 2-6years: 5mg 24hourly for
14days. Children above 6years: 10mg 24 hourly for 14days
OR
S: desloratadine (PO) Adults: 5mg 24hourly for 14days. Children 2-5years: 1.25mg
24hourly for 14days. Children 6-12 years: 2.5mg 24hourly for 14days

Surgical management
Direct laryngoscopy+microlaryngeal surgery (D/Scopy+MLS) to remove polyp or cyst-using
microscope or Endoscope with microdebrider/shaver

15.8.7 Recurrent Respiratory Papillomatosis (Laryngeal Papillomas)


It is the commonest benign laryngeal tumor of the larynx caused by Human papilloma virus (HPV),
occurring in both children and adults. It has a higher recurrence rate in children than in adults,
among adults it may turn into a malignancy.

Clinical presentation
• Hoarse voice, audible respiration (inspiratory stridor)
• Progressive difficulty in breathing
• Progressive inspiratory stridor
• On and off cough

Investigations
• Perform a thorough respiratory system examination
• Indirect laryngoscopy for papilloma croups on the larynx
• Rigid laryngoscopy (Endoscopy) OR Fiber optic Nasolaryngoscopy

Non-pharmacological Treatment
• If in distress, perform a tracheostomy first then refer

Referral: Refer the patient to the next facility with adequate expertise and facilities

Surgical management
• Tracheostomy if there is upper airway obstruction
• Direct Laryngoscopy under GA+microlaryngeal surgery(D/Scopy+MLS)
• D/Scopy+microdebridment

15.8.8. Foreign Bodies in the Throat


If the foreign body is suspected to be in the hypopharynx, esophagus, trachea or bronchus
• Take a thorough history and do a thorough physical examination
• Do chest X ray to confirm your diagnosis (though some foreign bodies are radiolucent)
• Refer to a next level hospital with facility for removal

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Surgical management
• Oesophagoscopy for oesophageal foreign body(FB)
• Bronchoscopy for airway FB

15.8.9 Subglottic Hemangioma


Congenital subglottic hemangiomas are vascular lesions that undergo a phase of rapid growth that
is initiated during the first few weeks to months of life. They may present as solitary lesions or as
part of a segmental hemangioma syndrome.

Clinical presentation
• Hoarseness of voice • Cyanosis
• Insipiratory stridor • Concomitant cervical facial
• Cough hemangioma

Pharmacological management
A: prednisolone (PO) Children: 1mg/kg 24hourly for 5days then taper down by half for the
next 5days.
AND
A: propranolol (PO) for children: Starting dose of 0.6mg/kg 12hourly for 1week, then
increase dose to 1.1mg/kg 12hourly for 2weeks; then Maintenance dose 1.7mg/kg
12hourly for at least 6months.

Surgical Management-Tracheostomy- if severe inspiratory stridor is present.

15.8.9 Laryngomalacia
This is the most common congenital anomaly of the larynx, characterized by partial or complete
collapse of supraglottic structures on inspiration. This is the most common cause of noisy breathing
in infancy. Gastroesophageal reflux disease (GERD) has been implicated.
Clinical presentation
• Insipiratory stridor relieved by lying • Difficult feeding
prone • Chocking on feeding
• Difficult breathing/dsypnoea

Investigations
• Fiber optic nasolaryngoscopy
• Microlaryngoscopy and bronchoscopy

Non-pharmacological management
• Sleep prone rather than supine
• Feeding modification
• Close observation of upper respiratory tract infections

Pharmacological management
For children 1-12years
S: esomeprazole (PO) 10-20mg 24hourly
For children >12years give
S: esomeprazole (PO) 20 - 40mg 24hourly
Surgical management
• Supraglotoplastly
• Tracheostomy for severe cases

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15.8.10 Vocal Cords Paralysis
It is due to total interruption of nerve impulse resulting in no movement of laryngeal muscles. Vocal
cord paralysis is a sign of disease and not a diagnosis by itself, vocal cord paralysis can be
unilateral or bilateral.

Clinical presentation
• Change in voice/hoarseness (for • Cough and aspiration
unilateral vocal cord paralysis) • History of neck
• Vocal fatigue surgery(thyroidectomy)
• Dyspnoea/upper airway obstruction • Neck or mediastinal tumors
• Stridor

Investigation
• Fiber optic nasolaryngoscopy
• Video stroboscopy

Non-pharmacological management
• Speech therapy

Surgical management: depends on the severity and desired outcome.


• Tracheostomy • Cordectomy
• Arytenoidectomy • Thyroplasty type i& ii
• Vocal cord lateralation through • Injection of Teflon paste
endoscopy • Muscle or cartilage implant

15.8.11 Infection of Thyroglossal Duct Cyst, Dermoid Cyst, Branchial Cleft


Cysts
Clinical presentation
• For Thyroglosal cyst- Midline upper neck mass which is cystic just below the hyoid bone. If
infected my present with tenderness. My also present as discharging sinus
• For branchial cleft cysts mass or discharging sinus along the anterior border of the
sternocleidomastoid muscle.

Investigation
• Neck USS

Pharmacological management
B: ampicillin+cloxaccillin (PO) Adult 500mg. Paediatric 15mg/kg 6-8hourly for 10-14days.
AND
B: cephalexin (PO) Adult 500mg 8hourly. Paediatric 75-100mg/kg/day divided in 4doses
for 7-14days
OR
B: amoxycillin + clavulanate (PO): 625mg to 1g 12hourly for 7-14days.
ForChildren ≤3 months:
B: amoxycillin + clavulanate (PO) 30mg/kg/day in 2divided doses for 7-14days.
For Children>3 months:
B: amoxycillin + clavulanate (PO) 25mg/kg/day in 2divided doses for 7- 14days

Surgical management
• Thyroglosal duct cyst excision (Sistrunk procedure)
• Branchial cyst/fistula excision

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15.8.12 Deep Neck Spaces Infections
Clinical presentation
• Truisms • Difficult breathing
• Induration and swelling below the • Neck stiffness/torticollis
angle of mandible • Neck swelling, mass, or
• Medial bulging of the pharyngeal lymphadenopathy
wall • Systemic toxicity with fever and
• Difficult swallowing rigors
(dysphagia/odynophagi)

Pharmacological management
B: azithromycin (PO) Adult 500mg 24hourly. Paediatric ≥ 6 months10mg/kg/day for 2 to 5
days
OR
A: metronidazole (PO) 400mg 8hourly for 7-14day. Children: 7.5-15mg/kg 8 hourly for 20–
30days
OR
B: metronidazole (IV) 500mg 8hourly. Children: 7.5-15mg/kg 8 hourly for 7-14days
OR
B: amoxycillin + clavulanate (PO) 625mg to 1g 12hourly for 7- 14days
For Children ≤ 3 months:
B: amoxycillin + clavulanate (PO) 30mg/kg/day in 2divided doses for 7-14days.
For Children >3 months:
B: amoxycillin + clavulanate (PO) 25mg/kg/day in 2 divided doses for 7-14days.
OR
C: clarithromycin (PO) 500mg 12hourly for 7-14 days.
ForChildren ≥ 6 months:
S: clarithromycin (PO) 15mg/kg/day in 2 divided doses for 7-14days
OR
C: ceftriaxone (IV) Adult 1-2g 12 hourly. Paediatric 50-100mg/kg 24hourly for 7days
AND
A: paracetamol (PO) 500mg to 1g 4-8hourly as needed.
For Children ≤ 10kg:
A: paracetamol (PO) 10mg/kg 4-8hourly as needed.
For Children >
A: paracetamol (PO) 10kg: 15mg/kg 4-8hourly as needed
OR
A: diclofenac (IM) 75mg 8hourly as needed

C: diclofenac (PO) 50mg 4-8hourly as needed,

15.8.13 Peritonsillar Abscess (Quincy)


Peritonsillar abscess is a collection of pus located between the capsule of the palatine tonsil and
the pharyngeal muscles.

Clinical presentation
• Severe sore throat (usually unilateral) with Fever
• "Hot potato" or muffled voice
• Pooling of saliva or drooling may be present
• Trismus, neck swelling and pain and may have ipsilateral ear pain
• Fatigue, irritability
• Swollen and/or fluctuant tonsil with deviation of the uvula to the opposite side
Pharmacological management
B: amoxycillin + clavulanate (PO) 625mg to 1g 12hourly for 7-14days.
ForChildren ≤ 3 months:
B: amoxycillin + clavulanate (PO) 30mg/kg/day in 2divided doses for 7-14days.

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For Children >3 months:
B: amoxycillin + clavulanate (PO) 25mg/kg/day in 2divided doses for 7-14days
OR
B: ceftriaxone (IV) 1- 2 g 12 hourly for 7days.
For Children:
B: ceftriaxone (IV) 50-100mg/kg 24hourly for 7days
OR
C: clarithromycin (PO) 500mg 12hourly for 7-14days.
For Children ≥ 6 months: 15mg/kg/day in 2divided doses for 7-14days
OR
S: cefixime (PO) 400mg 24hourly for 7-14days.
ForChildren ≥ 6 months to 12years (weight below 45kg):
S: cefixime (PO) 8mg/kg 24hourly for 7-14days

Surgical management
• Needle Aspiration
• Incision and drainage (LA/GA)
• Drainage/quincy tonsillectomy
• Interval tonsilectomy
15.9 ENT Neoplasms
15.9.1 Juvenile nasopharyngeal angiofibromas (JNA)
Are rare vascular tumors exclusively seen in adolescent males.

Clinical features
• Nasal bleeding
• Nasal blockage
• May present with eye protrusion

Investigation
CT-Scan (with contrast) PNS/Skull base-will show widening of sphenopalatine fissure and anterior
bowing of posterior wall of maxillary sinus.

Note
Never take biopsy for suspected case of JNA

Surgical treatment
Embolization of internal maxillary artery THEN
Excision of Angiofibroma (Open or Endoscopic/modified Denkers operation)

15.9.2 Salivary Gland Tumors


Salivary gland tumors include a heterogeneous group of lesions. Most salivary gland tumors are
composed of more than one cell type. Tumours may arise from major or minor salivary glands.
(Parotid, Submandibular, Lingual and minor salivary gland tumours)

Clinical presentation
• Painless progressive swelling of a given salivary gland.

Investigation
• Fine needle aspiration cytology (FNAC)
• Do not take incisional biopsy unless lesion is ulcerative.

Surgical management
-Partial or Total parotidectomy-for parotid tumours
-Submandibular gland tumor excision-for submandibular gland
-Sub lingual gland tumor excision
-Minor salivary gland tumors excision

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15.9.3 Parapharyngeal Tumours
Both benign and malignant tumors may arise from any of the structures contained in this space.
Among parapharyngeal space (PPS) tumors; 70-80% are benign, and 20-30% are malignant. Most
PPS tumors are of salivary or neurogenic origin.

Clinical presentation
• Sore throat • Snoaring
• Dysphonia • Tonsilar/pharyngeal mass
• Otalgia • Neck/submandibular mass

Investigation
• Fine neddle aspiration cytology (FNAC)
• CT SCAN-Neck&skull base
• MRI –Head and neck

Surgical Management
• Parapharyngeal tumour excision

15.9.4 Cancer of the Larynx


It is the commonest ENT malignancy. Risk factors include cigarette smoking, alcohol intake,
gastroesophageal reflux disease and human papilloma virus.

Clinical presentation
• Progressive hoarseness of voice
• Difficulty in breathing (inspiratory stridor)
• Hemoptysis

Referral: Refer the patient to the next facility with adequate expertise and facilities

Investigations
• Rigid Laryngoscopy (endoscopy) or Fiberoptic nasolaryngoscopy(diagnostic)

Surgical management
1. Direct Laryngoscopy +Biopsy under General Anaestesia (GA)
2. Tracheostomy
3. Total/Partial laryngectomy +/- neck dissection

Note
Any patient with progressive hoarseness of voice for more than two weeks should undergo
laryngoscopy

15.9.5 Sino-Nasal Malignancy


Is a malignancy of the nose and paranasal sinuses? Risk factors include wood dust (both soft and
hard), wielding dust, lather industry fumes, hydrocarbons fumes, and aflatoxin dust.

Clinical presentation
• Nasal bleeding • Cheek swelling
• Nasal discharge • Proptosis
• Nasal obstruction • Hearing loss
• Teeth loosening

Referral: Refer the patient to the next facility with adequate expertise and facilities

Investigations
• Biopsy-transnasal • Chest x –ray
biopsy/Endoscopic • Urinalysis-bence -Jones proteins
• CT-Scan –paranasal sinus (PNS)

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Surgical management
Total Maxillectomy-Open OR
Partial Maxillectomy-Open/Endoscopic

Note
Refer patient for adjuvant chemo and radiotherapy

15.9.6 Naso-Pharyngeal Malignancy


It is a malignancy which arises from the nasopharynx. Risk factors include genetic predisposition,
Epstein Bar virus, smoked and/or salted foods.

Clinical presentation
• Cervical lymphadenopthy, usually bilateral
• Nose bleeding
• Nasal blockage
• Hearing loss, tinnitus or ear pain

Referral: Refer the patient to the next facility with adequate expertise and facilities

Note
A patient presenting with cervical lymphadenopathy has nasopharyngeal carcinoma until proven
otherwise

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Investigations

• Biopsy-Transnasal/Endoscopic
• Fine needle aspiration cytology for neck mass
• CT-Scan-head and neck
• Chest x-ray
• Serology for Epstein Bar virus(EBV)

Treatment
• Radiotherapy

15.9.7 Oropharyngeal Malignancy


Oropharyngeal squamous cell carcinomas arise in the soft palate, tonsils, base of tongue,
pharyngeal wall, and vallecula.

Clinical presentation
• Sore throat
• Throat pain/painful swallowing
• Voice change (“hot potato” voice)
• Difficulty in breathing
• Oropharyngeal mass/ulcer

Investigations
• Rigid endoscopy
• Transoral biopsy
• Serology for HPV (human papilloma virus)
• CT-Scan or MRI -Neck

Management
• Surgery: open or transoral
• Definitive Management: Refer Malignancy chapter.

15.9.8 Hypo-Pharyngeal Malignancy


It is a malignancy which arises from the hypopharynx. Risk factors include cigarette smoking,
alcohol intake and gastroesophageal reflux disease.

Clinical presentation
• Progressive dysphasia • Difficulty in breathing (inspiratory
• Progressive odynophagia stridor)
• Hematemesis/hemoptysis • Excessive salivation/Pooling of
• Ear pain (referred otalgia) saliva
• Cervical lymphadenopathy

Referral: Refer the patient to the next facility with adequate expertise and facilities

Investigations
• Rigid Laryngoscopy (endoscopy) or Fiber optic nasolaryngoscopy(diagnostic).
• CT-Scan-head and neck
• Chest x-ray

Surgical managemrnt
1. Direct Hypopharyngoscopy +Biopsy under general anestisia(GA)
Definitive Management
• Chemoradiotherapy depending on histological results –Refer to oncology chapter

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15.9.9 Metastatic Lymphadenopathy and Neck Masses
Cervical lymph nodes are a common site of metastases for malignant tumors that originate at
primary sites in the head and neck. Primary lymphoma in neck nodes must be considered in any
differential diagnosis.

Clinical presentation
• Neck mass unilateral or bilateral
• Neck ulcer

Note
• An adult patient with neck mass, should be approached with a presumption of malignancy
until proven otherwise.
• Once the diagnosis of metastatic squamous cell carcinoma is made, a search for the
primary tumor must be performed. The probable primary site can often be identified by
history and physical examination; panendoscopy and directed imaging may be required.

Investigations
• Neck ultrasound
• Fine needle asypiration cytology(FNAC)
• Panendoscopy of upper aerodigestive areas (nose and paranasal sinuses, nasopharyngx,
oropharyngx, laryngx, hyponaryngx) and oesophagoscopy.
• Direct nasal endoscopy (DNE)
• Fiber optic nasolaryngoscopy
• Rigid laryngoscopy (endoscopy)

Note: Do not treat patient with cervical lymphadenopathy as a case of TB adenitis until
malignancy is ruled out and TB adenitis is proved.

Surgical management
• Biopsy for histology from suspected site
• Neck dissection: Radical or Modified Neck Dissection

15.10. Speech Disorders


Speech disorder refers to any condition that affects a person’s ability to produce sounds that create
words. This includes stuttering, apraxia, dysarthria can be caused by brain damage/stroke, muscle
weakness, hearing loss, dementia etc.

Investigations
• Audiometry • Auditory brainstem response
• Otoacoustic emission (OAEs) • Fiber optic nasolaryngoscopy

Non-pharmacological management
• Auditory verbal training-for post
cochlea implantation
• Speech therapy for aphasia,
stuttering, apraxia and dysarthria.
• Hearing Aids
• Cochlea implantation

Surgical management
• Posterior tympanotomy-for cochlea
implantation.

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CHAPTER SIXTEEN
ORAL AND DENTAL CONDITIONS

Oral diseases and conditions are common and range from dental caries, periodontal conditions,
dental abscess, acute bacterial infections, viral infections, fungal infections, traumatic injuries,
tumors, and lesions affecting the maxillofacial region (perioral, jaws and face). Before doing oral
examination or any dental procedures, patients should gurgle with hydrogen peroxide 3% or
povidone iodine 2% to minimize infectious agent’s contamination between patient and oral health
care provider.

16.1 Periodontal Conditions


16.1.1 Gingivitis
Inflammatory changes in the gingival develop within a couple of days of undisturbed bacterial growth
on the gingival margin of the erupted tooth in the oral cavity
Clinical presentation
• Gingival redness
• Swollen and shiny gingival tissue
• Increased tendency of the gingival to bleed on gentle probing or spontaneously, during
tooth brushing or even on touch and on biting bread and fruits.
• Bad breath from the mouth

Prevention and non-pharmacological Treatment


Proper oral hygiene care counselling.
Remove accumulated plaque and teach oral hygiene on systematic tooth brushing and other
adjuvant means of oral hygiene (dental flossing, tongue cleaning on the dorsal part, use of mouth
washes including saline mouth wash).

16.1.2 Periodontitis
This is the progression of the inflammation of gingival into the deep tissue affecting the periodontal
membrane causing periodontal pockets, introduction of infection and destruction of periodontium.
Clinical presentation
• Reddened, swollen gingiva • Loose/mobile teeth
• Easily bleeding gingival on gently • Bad breath from the mouth
probing • Gingival recession
• Periodontal pocket
Investigation
Orthopantomography (OPG) to determine extent of bone loss

Non-pharmacological Treatment
Instruct and guide the patients on proper oral hygiene for proper plaque control.
Plaque control by scaling and root planning.

Pharmacological Treatment
Mouth wash: Do not swallow
A: hydrogen peroxide (PO) 3% 6hourly for at least for 5days
OR
B: chlorhexidine gluconate (PO) 0.1% 12hourly at least for 5days
OR
Use antibiotics only in severe cases
A: metronidazole (PO) 400mg 8hourly for 8days
AND EITHER
A: amoxicillin (PO) 500mg 8hourly for 8 days
OR
A: doxycycline (PO) 100mg 12hourly for 10days

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16.1.3 Acute Necrotizing Ulcerative Gingivitis (ANUG)
It is a severe form of gingivitis and is characterized by rapid destruction of gingival tissue, particularly
in the interdental papilla. Patients usually present with soreness and bleeding of the gums and foul
smell test (fetor-ex ore/halitosis). It is common in malnourished children and immunocompromised
individuals especially patients with diabetes and HIV/AIDS.

Clinical presentation

• Painful swollen gingiva which bleeds easily and erythema of the gingival margins
• Yellowish-white ulceration of the gingival
• Fever, malaise, and regional lymphadenitis
• In some patients (especially malnourished children), ANUG may presents with
extensive destruction of the face and jaws in the severe form known as Cancrum Oris

Pharmacological Treatment
Professional cleaning with hydrogen peroxide 3% (under local anesthesia)
A: metronidazole (PO) 400 mg 8hourly for 5days
AND
A: amoxicillin (PO) 500mg 8hourly for 5days

16.1.4 Stomatitis
This is generalized inflammation of the oral mucosal (including the gingiva) due to different
etiologies such as infections, chemical burn, radiation, and allergy.

Clinical presentation
• Oral sores and ulceration

Pharmacological Treatment
Mouth wash (do not swallow)
A: hydrogen peroxide solution 3% (PO) 6hourly for at least 5days
OR
B: chlorhexidine 0. % topical oral gel 12hourly

Note
Mouth wash should not be used at the same time with the gel. Also, should not be swallowed.

Oral analgesics can be added


A: paracetamol (PO) 1gm 8hourly for at least 3days
OR
A: ibuprofen (PO) 400 mg 8hourly for at least 3days
OR
C: diclofenac (PO) 50 mg 8hourly for at least 3days

16.2 Dental Caries


Dental caries is caused by bacteria of the dental plaque which feed on sugary food substrates
producing acid as by-products which dissolve the minerals of the tooth surface.

Clinical presentation
Early stage–asymptomatic
• Intermediate stage: black/brown spot which may be visible on any surface of tooth
• Cavities developing on tooth surface
• Pain/toothache elicited by hot, cold, or sweet foods/drinks

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Late stage
• Pain may be spontaneous, intermittent, sharp, and severe, even interfering with sleep.
• Tenderness on percussion of the tooth

Investigation
Periapical x-ray of tooth/teeth may need to be done specially to confirm extent of caries for
treatment decision e.g. the caries contained in the dentine can be distinguished from pulpal caries.

Prevention
• Proper counseling to avoid frequent use of sugary foods and drinks
• Use fluoridated toothpaste to brush teeth at least twice a day
• Provide preventive measures to early lesions presenting as a spot on the enamel without
cavitation and softening

Non-pharmacological Treatment
Lesion with cavitation but confined to dentine–filling/restoration of teeth with suitable filling materials
(e.g. amalgam, composite, glass ionomer)
Perform endodontic treatment with combination of antibiotics wherever possible for tooth with lesion
involving the pulp (with or without periapical abscess otherwise tooth extraction is done

Pharmacological Treatment
Analgesics: for toothache
A: paracetamol (PO) 1gm 8hourly for 3days
OR
A: ibuprofen (PO) 400mg 8hourly for at least 3days
OR
C: diclofenac (PO) 50 mg 8hourly for at least 3days
Antibiotics for endodontic treatment
B: ampicillin + cloxacillin (FDC) (PO) 500mg 8hourly for 5days
AND
A: metronidazole (PO) 400mg 8hourly for 5days

16.3 Odontogenic and Non-Odontogenic Orofacial Infections


16.3.1. Periapical abscess
This clinical condition arises as a complication of inflammation of the dental pulp or periodontal
pocket. The condition may be acute and diffuse, chronic with fistula or localized and circumscribed.
It is in the apical aspect of the supporting bone.

Clinical presentation
• The patient complains of tooth ache
• Pain during intake of hot or cold foods/drinks
• Pain on bringing the tooth on occlusion
• Tenderness on percussion (vertical percussion)
• Swelling of gingiva around the affected tooth

Non-pharmacological Treatment
• For posterior teeth: Extraction of the offending tooth under local anesthesia (can perform
root canal treatment for posterior teeth instead of tooth extraction under good clinical
judgement)
• Perform Incisional and drainage under local anesthesia followed by analgesics.
For anterior teeth (incisors, canine and premolars): extraction is carried out only when root canal
treatment is not possible

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Pharmacological Treatment
A: paracetamol (PO) 1gm 6hourly for 3days.
AND
A: amoxicillin (PO) 500mg 8hourly for at least 7days
OR
A: erythromycin (PO) 500mg 8hourly for 7days (if allergic to penicillin)
AND
A: metronidazole (PO) 400mg 8hourly for 7days

16.3.2 Dental Abscess (Odontogenic Abscess)


Dental abscess is an acute lesion characterized by localization of pus (caused by polymicrobial
infection) in the structures that surround the teeth.
Clinical presentation
• Fever and chills
• Throbbing pain of the offending tooth
• Swelling of the gingiva and sounding tissues
• Pus discharge around the gingiva of affected tooth/teeth
• Trismus (inability to open the mouth)
• Regional lymph nodes enlargement and tender
• Aspiration of pus
Investigation
Pus for Gram stain, culture, and sensitivity if the patient doesn’t respond to initial antibiotic
treatment.

Non-pharmacological Treatment
• Incision and drainage and irrigation (irrigation and dressing is repeated daily). Irrigation is
done with 3%hydrogen peroxide followed by 0.9% sodium chloride.
• Supportive therapy carried out depending on the level of debilitation. Most patients need
rehydration and detoxification using 0.9% sodium chloride (IV) or compound sodium
lactate (IV).

Pharmacological Treatment
A: amoxicillin (PO) 500mg 8hourly for 5days
AND
A: metronidazole (PO) 400mg 8hourly for 5days.
In severe cases,
B: amoxicillin+ clavulanic acid (FDC) (PO) 625mg 8hourly for 5days
AND
A: metronidazole (PO) 400mg 8hourly for 5days.

If a patient is allergic to penicillin


A: erythromycin (PO) 500mg 8hourly for 5days
Where parenteral administration of antibiotics is necessary (especially when the patient cannot
swallow and has life threatening infection), consider the following
B: ceftriaxone (IV) 1gm once daily for 5days
AND
B: metronidazole (IV) 500 mg 8hourly for 5days
AND
A: gentamicin (IV) 80mg 8hourly for 5days

Note
Incision and drainage is mandatory in cases of deeper spaces involvement followed by a course of
antibiotics. The practice of prescribing antibiotics to patients with abscess and denying referral for
definitive care until pus has established or resolved has been found to lead to more problems for
orofacial infections therefore early referral for definitive care is important.

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16.3.3 Ludwig’s Angina
This is a serious life threatening generalized septic cellulitis of the fascia spaces found on the floor of
the mouth and tongue. It is an extension of infection from mandibular molar teeth into the floor of the
mouth covering the submandibular, sublingual, and submental spaces bilaterally.

Clinical presentation
• Brawny induration • Tissues may become gangrenous
• Tissues are swollen, board like, not with a peculiar lifeless appearance
pitted and no fluctuance on cutting
• Respiratory distress • Three fascia spaces are involved
• Dysphagia bilaterally (submandibular,
submental, and sublingual)
Non-pharmacological Treatment
• Incision and drainage is done (even in absence of pus) to relieve the pressure and allow
irrigation
• Only when the airway distress is significant and there is evidence that it is not relieved by
incision and drainage then tracheostomy is needed. Supportive care includes high protein
diet and fluids for rehydration and detoxification. During incision and drainage pus should
be taken for culture and sensitivity. Offending tooth should be removed at the same sitting
if the patient can open the mouth.

Pharmacological Treatment
B: ceftriaxone (IV) 1g 24hourly for 5days
OR
B: amoxicillin + clavulanic acid (FDC) (PO) 625mg8hourly for 5days
AND
B: metronidazole (IV) 500mg 8hourly for 5days

If allergic to penicillin use


A: erythromycin (PO) 500mg 6hourly for 5days
Once the patient can swallow, replace IV medication with oral treatment.

Note
For this condition and other life-threatening oral conditions consultation of available specialists
(especially oral and maxillofacial surgeons) should go parallel with life saving measures.

16.3.4 Pericoronitis
Inflammation of the soft tissues covering the crown of erupting tooth and occurs more commonly in
association with the mandibular third molar (wisdom) teeth.
Clinical presentation
• High temperature • Signs of partial tooth eruption
• Discomfort in swallowing and • Bad smell (Foetor-ox oris)
chewing • Trismus
• Well localized dull pain, swollen
and tender gum flap

Non-pharmacological Treatment
Excision of the operculum/flap (flapectomy) under local anesthesia.
Extraction of the third molar associated with the condition.
Grinding or extraction of the opposing tooth.

Pharmacological Treatment
A: hydrogen peroxide solution 3% (PO) 6hourly for 5days (Gurgle /rinse)
A: amoxicillin (PO) 500mg 6hourly for 5days

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AND
A: metronidazole (PO) 400mg 8hourly for 5days
If severe (rare) refer to treatment of dental abscess section

16.3.5 Osteomyelitis of the Jaw


Osteomyelitis is an infection involving all layers of bone in which widespread necrosis may occur. It
is rare in the maxilla due to the rich blood supply, but on occasions may affect the anterior palate
where the bone is thicker. It is more common in the mandible, usually because of dental infection,
trauma, or a blood-borne infection.

Clinical presentation
• In the initial stage there is no • Later as the bone undergoes
swelling necrosis the area becomes
• Malaise and fever very painful and swollen
• Enlargement of regional lymph • Pus ruptures through the
nodes periosteum and discharged
• Teeth in the affected area outside the skin surface
become painful and loose. through a sinus

Investigation
X-ray – OPG (Orthopantomography) or mandibular lateral oblique, water’s view for maxilla/midface.
The x-ray will show sequestra formation in chronic stage. In early stage features seen in x-ray
include widening of periodontal spaces, changes in bone trabeculation and areas of radiolucency.
Perform culture and sensitivity of the pus aspirate to detect the specific bacteria.

Non-pharmacological Treatment
Incision and adequate drainage to confirmed pus accumulation which is accessible.
Removal of the sequestrum by surgical intervention (sequestrectomy) is done after the formation of
sequestrum has been confirmed by X-ray.

Pharmacological Treatment
For acute osteomyelitis of the jaw
B: ampicillin + cloxacillin (FDC) (PO) 500mg 8hourly for 4-6weeks
AND
A: metronidazole (PO) 400mg 8hourly for 4-6weeks. If culture is available treat according
to results.

For chronic osteomyelitis of the jaw which sequestrectomy has been done
A: doxycycline (PO) 100mg 12hourly for 5days
OR
A: metronidazole (PO) 400mg 8hourly for 5days
AND
S: clindamycin (PO) 500mg 8hourly for 5days

16.4. Fungal Infections


16.4.1 Oral Candidiasis
This is a fungal infection of the oral mucosa caused by Candida infection mainly Candida albicans.

Clinical presentation
Features of candidiasis are divided according to the types as follows:

Pseudomembranous
• White creamy patches/plaque
• Cover any portion of mouth but more on tongue, palate, and buccal mucosa

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• Sometimes may present as erythematous type whereby bright erythematous mucosal
lesions with only scattered white patches/plaques

Hyperplastic
• White patches leukoplakia-like which are not easily rubbed-off.

Angular cheilitis (angular stomatitis)


• Soreness, erythema and fissuring at the angles of the mouth
• Commonly associated with denture mastitis but may represent a nutritional deficiency or it
may be related to orofacial granulomatosis or HIV infection

Pharmacological Treatment
A: nystatin suspension (PO) 100,000IU (1 ml) mixture held in the mouth for at least
3minutes before swallowing, 6hourly
OR
C: miconazole gel (PO) 25mg/ml 5–10mls in mouth –hold in the mouth for 60 seconds
before swallowing. The treatment should be continued for 5days after cure/clearance. Where topical
application has failed, or candida infection has been considered severe use.
A: fluconazole (PO) 150mg 24hourly for 7days
OR
D: itraconazole (PO) 200mg 24hourly for 7days

Note
Candidiasis has several risk factors; it is recommended that for HIV/AIDS patients with candidiasis,
refer to the Tanzania HIV/AIDS Guidelines.

16.5 Viral Infections


16.5.1 Herpes Simplex Virus
This is a viral infection commonly affecting the lips and perioral soft tissues presenting as
papulovesicular lesions which ultimately ulcerate. The primary infection affects mainly the gingiva
and palate.
Clinical presentation
• A prodromal of tingling, warmth or itching at the site usually precedes the recurrence
• About 12 hours later, redness appears followed by papules and then vesicles
• These vesicles then burst, weep, dry, scab and then heal
• The length of the cycle is variable 5–12days mean time being 7days

Non-pharmacological Treatment
• Adequate hydration
• Avoid salty and acidic drinks
• Cover lesions on the lips with Petroleum jelly and control any underlying cause

Pharmacological Treatment
This is an otherwise self-limiting condition but if persistent for 10days or recurrent infection use
medication:

For Herpes Labials


B: acyclovir cream applies 4hourly for 5days

For Herpes Stomatitis


B: acyclovir (PO) 200mg 6hourly for 5days
AND
B: acyclovir cream 12hourly for 5days

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In immunocompromised patients
B: acyclovir (PO) 400mg 6hourly for 5days

For oral facial lesions of herpes zoster treat with


B: acyclovir (PO) 400–800mg 6hourly for 5days

Pain control by analgesics


A: paracetamol (PO) 1g 8hourly for 3days
OR
C: diclofenac (PO) 50mg 8hourly for 3days
OR
A: ibuprofen (PO) 400mg 8hourly for 3days
16.6 Aphthous Ulceration
Aphthous or recurrent aphthous stomatitis (RAS) are painful recurrent mucous membrane
ulcerations. Usually affect the non-keratinized oral mucous membrane.
Clinical presentation
Minor Aphthous Ulcers
• Small round or ovoid ulcers 2–4 mm in diameter, surrounded by an erythematous halo and
some edema.
• Occurs in groups of only a few ulcers (i.e. 1–6) at a time.
• Found mainly on the non-keratinized mobile mucosa of the lips, cheeks, floor of the mouth,
sulci, or ventrum of the tongue.

Major Aphthous ulcers


• Painful ulcers on non-keratinized oral mucous membrane, they are large 1–3 cm edged
ulcers, and several may be present simultaneously.

Herpetiform ulcers
These occur in a group of multiple ulcers which are small (1–5 mm) and heal within 7–10days.

Pharmacological Treatment
B: chlorhexidine gluconate 0.1% mouthwash used 8hourly for 5days
OR
D: triamcinolone acetonide cream 0.1% apply 12hourly for 5days

If systemic therapy is required;


A: prednisolone (PO) 20mg 8hourly for 3days then dose tapered to 10mg 8hourly for
2days then 5mg 8hourly for other 2 days.
A: paracetamol (PO) 1gm 8hourly for 3days when required for pain.

16.7 Post Extraction Complications


16.7.1 Bleeding socket
Commonly due to disturbing the blood clot by the patient through rinsing or inadequate compression
on the gauze, though at times may be due to bony/tooth remnants.
Clinical presentation
Bleeding socket can be primary (occurring within first 24 hours post extraction) or secondary
occurring beyond 24 hours post extraction.

Primary Bleeding Socket


• Active bleeding from the socket
• Patient may be dehydrated and pale if has lost significant amount of blood
• Features of decreased pulse rate and volume, hypotension also if patient has lost
significant amount of blood

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Secondary bleeding
• The socket may show features of infection or trauma
Non-pharmacological Treatment
Give local anesthesia (lignocaine 2% with adrenaline 1 in 80,000 IU).
Clear any clot available and examine the socket to identify source of bleeding.
Suturing of the wound only when necessary (like significantly traumatized gingiva).
Give proper instructions to follow (bite on gauze pack for 30 minutes, not to rinse or eat hot foods on
that day at least for 12 hours and avoid disturbance to the wound).

Pharmacological Treatment
Analgesics may be needed:
A: paracetamol (PO) 1g 8hourly for 3days
OR
C: diclofenac (PO) 50mg 8hourly for 3days
OR
A: ibuprofen (PO) 400mg 8hourly for 3days
AND
C: tranexamic acid (PO) or (IV) 500 mg 8hourly for the first 24hours.

16.7.2 Infected Socket


A post extraction complication due to infection of the clot due to contamination (infected socket). The
condition is painful and if not managed well could lead to osteomyelitis.

Clinical presentation
• Severe painful socket 2–4days after tooth extraction
• Fever
• Necrotic blood clot in the socket
• Swollen gingiva around the socket
• Sometimes there may be lymphadenopathy and trismus (inability to open the mouth)

Non-pharmacological Treatment
Socket debridement under local anesthesia with lignocaine 2% and irrigate with hydrogen peroxide
3% followed with copious amounts of normal saline. The procedure of irrigation is repeated the 2nd
and 3rd day and where necessary can be extended to the 4th day if pain persists.

Pharmacological Treatment
Patient is instructed to rinse with 3% hydrogen peroxide or 2% povidone iodine 3–4 times a day.
antibiotics should be prescribed to prevent progression to osteomyelitis:
A: amoxicillin (PO) 500mg 8hourly for 5–7days
OR
B: azithromycin (PO) 500mg 24hourly for 3days
AND
A: metronidazole (PO) 400mg 8hourly for 5days
Investigation
Periapical X-ray of the socket may be necessary when there is limited improvement despite
treatment.

16.7.3 Dry Socket


This is a post extraction complication due to failure to form a clot (dry socket). The condition is very
painful, and it differs from an infected socket by lack of clotting and levels of severity of pain.

Clinical presentation
• Severe pain 2–4 days’ post- • Socket devoid of clot
extraction • Surrounded by inflamed gingiva
• Pain exacerbated by entry of air on
the site

356
Non-pharmacological Treatment
Treatment is under local anesthesia with lignocaine 2%, socket debridement and irrigation with
hydrogen peroxide 3% followed with copious amount of normal saline. The procedure of irrigation is
repeated on the 2nd and 3rd day and where necessary can be extended to the 4th day if pain
persists.

16.7.4 Oro-Antral Communication


Occasionally, the uncomplicated extraction of a tooth may fracture the thin floor of the sinus and
cause an oro-antral communication (OAC). More commonly, the communication is produced by
attempts to remove retained tooth root so that the antrum floor is perforated, or the apex displaced
into it.

Clinical presentation
• Air passing from the nose into the mouth and the surgeon will be able to see bubbling
through the communication when the patient is asked to breathe out.
• Blood from the wound, drinks and mouthwashes used to rinse the mouth may pass
through the sinus into the nose.

Non-pharmacological Treatment
Immediately on diagnosing a communication the tooth should be checked to ensure that it has been
completely extracted. All pieces of loose bone that might form sequestra are then gently removed.
The buccal plate of alveolar bone is trimmed if a flap has been raised but is otherwise left alone.
Buccal advancement flap is the operation of choice to repair the fistula (oro-antral communication)

Pharmacological Treatment
A: metronidazole (PO) 400mg 8hourly for 5days
AND
B: amoxicillin + clavulanic acid (FDC) (PO) 625mg 12hourly for 7days

16.8 Tooth Sensitivities


Teeth become sensitive because of worn enamel, or exposed tooth roots, cavity, gingival collapse, a
consequence of periodontitis, tartar (calculus) build-up, cracked or chipped tooth and recent filling.

Non-pharmacological Treatment
• Recommend brushing teeth with desensitizing toothpaste for sensitive teeth
• Desensitizing or bonding – apply bonding resin material or Glass Ionomer Cement to seal
the area around the tooth
• Root canal treatment – for severe, prolonged discomfort
• Prevent tooth-grinding (bruxism) by fabricating to the patient a mouth guard

Pharmacological Treatment
C: sodium fluoride 1.1 % +potassium nitrate 5% (fluoride gel or varnish), apply 12hourly

16.9 Tooth Eruption, Shedding and Edentulousness


16.9.1 Eruption of Teeth
Eruption of deciduous /primary teeth usually starts at five months of age. Symptoms associated with
it like fever and diarrhea are normal and self-limiting unless any other causes can be established.
The following conditions are usually associated with tooth eruption and should be referred to dental
personnel: eruption cysts, gingival cysts of the newborn and pre/natal teeth.

Note
“Nylon teeth” is a myth/belief existing in some traditions. These are conditions associated with the
eruption of deciduous/primary teeth

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16.9.2 Shedding of Deciduous Teeth
Phenomenon of losing deciduous/primary teeth occurring between ages of 5–12 years is a normal
physiological change. Deciduous teeth should be left to fall out themselves unless the teeth are
carious or there is any other indication. Parents should be counseled accordingly and be instructed
to assist their children to loosen the already mobile teeth and when there is no success, or the
permanent teeth are erupting in wrong direction should consult a dentist.

16.9.3 Edentulousness
It is the partial or full loss of natural teeth and subsequent resorption of the alveolar bone.

Diagnosis
Diagnostic cast, Periapical X-ray, OPG.

Non-pharmacological Treatment
• Design and fabricate dental prosthesis
• Dental prosthesis may be fixed, partial dentures and complete/full dentures
• Materials required in fabrication of these prostheses are: alginate impression materials,
silicone impression materials, implant system, gypsum dental stone, Acrylic resins
(monomer and polymer), porcelain, ceramic, metal alloys, wax etc.

16.9.3.1 Dental implant (s)


A permanent device that is biocompatible and bio-functional placed on or within the bone to provide
retention for fixed or removable prostheses.
Indications of Dental Implant(s)
• Single tooth replacement.
• Multiple teeth replacement.
• Retention of removable prosthesis in partially edentulous patient.
• Retention of over denture in completely edentulous patient (In mandible two 2 implants are
required for support and in maxilla 4 implants are needed to support the denture.
• Retention of fixed prostheses completely edentulous patient (In mandible 4 implants
needed and in maxilla - 6-8implants required).
• Retention of maxillofacial prosthesis.

Investigation
Radiographic examination
Maxillary and mandibular bone status may be evaluated in combination of periapical X-ray, occlusal
radiograph, panoramic radiograph, lateral cephalography, MRI and CT-Scan.

Surgiguids
They are custom made for each patient. They are used as guides for drilling in the optimum
locations implant placement then removed after placement.

Study cast
Evaluate occlusal centric relation, including any premature occlusal contacts, the relationship of the
edentulous area to the adjacent natural teeth and opposing arches.

Intra-operatively, the following should be observed to have a successful Implant


• Assess anatomical variation and abnormalities of vital structures so that implant should
never touch them.
• Maintain Sterility as interfere with Osseo-integration

Surgical technique
Adequate blood supply (proper incision design and flap reflection. Using sharp gradual series of drill
sizes with copious amount of irrigation by normal saline.

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Pharmacological Treatment after implant insertion
Mouth wash: Do not swallow
A: hydrogen peroxide 3% 6hourly for at least for 5days
OR
B: chlorhexidine gluconate 0.2% 12hourly at least for 5days
AND
A: metronidazole (PO) 400mg 8hourly for 8days
AND
A: amoxicillin (PO) 500mg 8hourly for 8days

16.10 Malocclusions
Malocclusion is any variation in the arrangement of teeth leading to abnormal occlusion to the extent
that may be functionally harmful or aesthetically objectionable.
Clinical presentation
• Class I malocclusion: Diagnosed when there is any occlusal abnormality or individual tooth
malocclusion in a case with normal arch relationship in anteroposterior plane.
• Class II malocclusion: Mesiobuccal cusp of upper first permanent molar occludes mesial to
the buccal developmental groove of the lower first permanent molar
• Class III malocclusion: The upper first permanent molar occludes distal to the buccal
developmental groove of the lower first permanent molar
• Skeletal malocclusions: These malocclusions are caused by defects in the underlying
skeletal structure itself.

Non-pharmacological Treatment:
• Preventive orthodontics
It includes parent counselling, caries control, space maintenance, managing exfoliation of deciduous
teeth, release of abnormal frenal attachments, treatment of blocked permanent first molars,
management of abnormal oral musculature and related habits.

• Interception orthodontics
o Correction of anterior or posterior cross bite, relieving crowding of the permanent
dentition, Space closure, treatment of anterior open bite, Deep bite, reverse overjet,
proclination of the upper labial segment and oral habits management by patient
education and monitoring or removable and fixed habit breaker
o For skeletal malocclusion: Use of extra oral appliances like reverse pull headgear
combined with an RME, high pull head gear and chin cups or functional appliances
are indicated for skeletal malocclusion in growing patients

• Definitive Orthodontic
Alignment of teeth in patient with dental alveolar malocclusion by using removable, clear aligner or
fixed appliances. Simple removable appliances are very useful in our local settings especially for
mild to moderate malocclusion in teenagers and include retainers or space maintainers.

16.11 Management of Maxillofacial Trauma


16.11.1 Traumatic Dental Injuries
It may result in loosening, displacement and or loss of teeth, fracture of teeth and or bone,
lacerations, and bleeding. The commonest causes are falls (in sports and play) at home or school
and motor accidents. Most affected are upper incisors.

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Clinical presentation

Type Presentation
Tooth Is an injury to supporting tissues of tooth, without displacement
concussion
Sublaxation Is the partial displacement, but is commonly used to describe loosening of a tooth
without displacement
Intrusion Is the displacement of tooth into its socket often accompanied by fracture of alveolar
bone
Luxation Is the displacement of tooth laterally, labially or palatally
Avulsion Is the complete loss of tooth from the socket

Soft tissue Injuries


Abrasion
Where friction between an object and the surface of the soft tissue causes a wound. This wound is
usually superficial, denudes the epithelium, and occasionally involves deeper layers.

Contusion/Bruising
Indicates that some amount of tissue disruption has occurred within the tissues, which resulted in
subcutaneous or sub mucosal hemorrhage without a break in the soft tissue surface.

Laceration
Is a tear in the epithelial and sub epithelial tissues? It is perhaps the most frequent type of soft tissue
injury, is caused most by a sharp object

16.11.2 Facial Bones Injuries


The commonest causes of fractured jaws are fights, road accidents, falls and sport. They occur
chiefly in males between 15-35years of age and twice as frequently in the mandible as in the
maxilla.
Initial assessment

The initial assessment should not concentrate on the most obvious injury but involve a rapid survey
of the vital functions to allow management priorities to be established.

The Mandible

The commonest sites of fracture in the mandible are the condyle neck, the angle, and the canine
region.

Middle third of the face

Fractures of the middle third of the face involve a complex of bones, which include the paired bones,
the maxilla, palatine, zygomatic, nasal, lachrymal and inferior conchae, together with the single
vomer and ethmoid bones.
Clinical presentation

Fracture site Clinical presentation


Bilateral condyle Pain, tenderness and swelling over both joints
Gagging on the posterior teeth and an anterior open bite, Restricted lateral
movements, Absence of movement of condyle heads
Body of the mandible Pain on moving jaw, Trismus
Movement and crepitus at site of fracture, Step deformity of lower border of
mandible, Derangement of the occlusion, Mental anaesthesia, Haematoma in
the floor of mouth and buccal mucosa
Zygomatic bone Depression of the prominence of the cheek, Step deformity in the infraorbital
ridge, Subconjunctival haemorrhage and diplopia, Infraorbital nerve
anaesthesia, Haematoma intraorally over the malar buttress, Blood in the
antrum, Trismus due to the coronoid process impacting against the displaced

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malar or zygomatic arch, Circumorbital ecchymosis
Le Fort I Floating palate, Blood in the antrum, Bilateral haematoma in buccal sulcus,
Deranged occlusion with anterior open bite
Le Fort II Gross swelling and, after oedema subside, dish – faced deformity,
Subconjunctival haemorrhage and diplopia, Bilateral infraorbital nerve
anaesthesia, Bilateral haematoma intraorally over malar buttresses,
Retroposed upper dental arch with anterior open bite
Le Fort III Gross swelling and, after oedema subside, dish – faced deformity
Subconjunctival haemorrhage and sometimes diplopia
Retroposed upper dental arch with anterior open bite
Cerebrospinal fluid leak from nose
Signs of head injury
Unilateral condyle Affected side
Pain in joint, worse on moving, Tenderness and swelling
Absence (or abnormality) of movements of
condyle head, Deviation of mandible towards this side, Gagging on molar
teeth
Opposite side
Open bite
Limitation of lateral excursion to that side

Investigation

Fracture sites Type of Investigation


Mandible OPG, Skull x-ray (lateral oblique and PA view)
Zygoma Skull x-ray (Occipitomental and submental vertex view), CT scan
Maxilla Skull x-ray (Occipitomental, submental vertex, lateral face view), CT scan.
Naso- ethmoidal complex CT scan

Non-pharmacological Treatment
• Intra-oral examination: Look for soft-tissue lacerations, dentoalveolar fractures and
damage to teeth.
• Check for tooth fragments which may be displaced in soft tissues.
• Examine traumatized teeth for mobility and check mobility.
• Suture for any soft tissue wounds.
• Extraction is a treatment of choice for significantly traumatized primary/deciduous teeth
with mobility and or displacement.

Reduction of fractures
In reducing fractures, the object is to rearrange the bone ends as accurately as possible. Although
the surgeon should attempt to get perfect reduction, the aim is to treat not a radiograph, but a
patient, and where displacement is acceptable and function is not impaired the patient should not be
subjected to unnecessary surgery.

Open reduction and rigid internal fixation (ORIF)


It is a standard treatment for most facial fractures. The technique relies on exposing the fractures
through intra -or extra oral incisions and accurate reduction of the bony fractures, which are then
held rigidly in place by the application of titanium plates for facial fractures,2 mm used in mandibular
fractures, 1.7 mm (low profile) and 1 mm used in mid - third fractures.

Intermaxillary fixation (IMF)


The mandible is immobilized by fixing it to the maxilla using arch bars and flexible wires of different
sizes 0.5, 0.6, 0.7 and 0.8mm. This establishes the occlusion and is an accepted part of the
treatment of maxillary fractures. It may be employed in mandibular fractures, particularly when one
or both condyles are involved.

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Note
Give tetanus toxoid (0.5% IU) if the patient has not received vaccination in the past 10 years.

Pharmacological Treatment
Pain control by analgesics
A: paracetamol (PO) 1g 8hourly for 3days
OR
C: diclofenac (PO) 50mg 8hourly for 3days
OR
A: ibuprofen (PO) 400mg 8hourly for 3days

Prophylactic antibiotics are indicated in cases of suspected contamination or extensive damage


B: ampicillin + cloxacillin (FDC) (PO) 500mg 8hourly for 5days

16.12 Tumours and Tumour-Like Conditions of Oral Cavity and Facial Region
16.12.1 Benign Odontogenic Tumors
Each tumour presents with different cardinal features radiologically and on histopathological
diagnosis.
16.12.1.1Ameloblastoma
Clinical Presentation
• Recognized between ages of 10 to 80 years
• 80% form in the mandible and 70% develop in the posterior molar region and often involve
the ramus
• Painless, slow growing tumor that may be solid or cystic
• Loosening of teeth, with roots resorption
• Gradual facial asymmetry due to enlargement and destruction of bone
• Continuous sheet of paper-thin bone covering the tumor

Investigation
Radiographically, the tumour presents with multilocular radiolucency, honeycomb, or soap bubble
appearance.

Note
Diagnostic confirmation of this tumour is through histopathology. Complete excision e.g. total
resection of the jaw, segmental resection plus bone grafting is the treatment of choice. Hence refer
the patient to a centre where there is oral and maxillofacial surgeon and histopathology Unit.

Calcifying odontogenic tumors


Clinical Presentation
• Most often found in the mandibular molar/premolar region, but 33% of cases are found in
the maxilla
• It is associated with an unerupted or impacted tooth in 50% of cases

Investigation
Radiographically these lesions can be radiolucent, but more characteristically are mixed lucent and
opaque masses, exhibiting a snow-driven appearance

Non-pharmacological Treatment
Complete excision of the tumour with border of normal lobe should be curative, but recurrence
follows incomplete excision.

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16.12.1.2 Amelobastic Fibroma
Clinical Presentation
• Slower growing tumor than the simple ameloblastoma and does not infiltrate between bone
trabeculae
• 75% of ameloblastic fibromas are found in the posterior mandible in the area of a
developing tooth. It is benign and expansile, growing as a pushing front rather than
invading surrounding tissues

Investigation
Radiographically this lesion appears as a uniocular or bilocular radiolucency, most often in the
posterior mandible. The radiographic appearance is identical to that of unicystic ameloblastoma, and
both lesions should be differential diagnoses because they affect similar age groups and have
similar clinical and radiographic appearances. Histologic examination differentiates the two.

Non-pharmacological Treatment
Conservative resection is effective, but if incomplete, recurrence follows

16.12.1.3. Adenomatoid Tumors (Adenoameloblastoma)


Clinical Presentation
• Two thirds of the cases occur in the anterior maxilla, one third occur in the anterior
mandible, and it is never found posterior to the premolars
• Two thirds of the cases are associated with an impacted tooth (usually the cuspid)
• Present with mild swelling or in association with a clinically missing tooth

Investigation
Radiographically this lesion generally appears as a well-demarcated radiolucency. In 75% of cases,
it is associated with an unerupted tooth, usually the canine. It may contain radiopaque flecks, which
represent calcified material.

Non-pharmacological Treatment
Enucleation is curative and recurrence is almost unknown.

16.12.1.4 Odontogenic Myxoma


Clinical Presentation
• Clinically indistinguishable from ameloblastoma
• The radiographic appearance of this lesion is not distinctive. It appears quite like
ameloblastoma (eg multilocular radiolucency).

Investigation
Confirmation is through histopathology

Non-pharmacological treatment
Wide excision is required.
16.12.2 Non Odontogenic Benign Tumours
(Benign Osteogenic Tumours, Arise from Bone)
16.12.2.1 Ewing’s tumor
Clinical presentation
• Painful swelling accompanied with fever.
• It is characterized by extraordinarily fast growth.

Investigation
Radiographically poorly defined solitary osteolytic lesion, irregular moth–eaten appearance which
may be undetectable in serial images for a long period. Histological diagnosis is needed.

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Pharmacological and Non-pharmacological Treatment
The initial treatment is wide excision, if not possible radiation should be considered. Combination
chemotherapy should be given.

16.12.2.2 Pregnancy Tumours


Clinical presentation
• They most commonly appear after first trimester, grow rapidly, and typically regress after
delivery.
• Found on the gingiva and arise predominantly.
• They are exophytic, lobulated, or smooth surfaced lesion with a red to purplish color and a
soft, spongy texture.
Non-pharmacological Treatment
Surgical intervention is often not required. However, pregnancy tumors can be removed during the
second trimester if they interfere with occlusion, are painful, bleed excessively, or are excessively
large. Lesions excised during pregnancy often recur. After delivery, pregnancy tumors typically
recede spontaneously but excision may be necessary for those cases which persist. Other non-
odontogenic tumors are Osteomas, Myxomas, Chondromas, Central giant cell and Fibro-osteoma.

16.12.3 Benign Soft Tissues Non-Odontogenic Tumours


Haemangioma
Clinical presentation
• Enlarged, vascular hamartoma appears as a painless, soft, smooth, or lobulated, sessile,
or pedunculated mass but may ulcerate and possibly hemorrhage if traumatized
• The lesions present with deep red or bluish red in color and moderately firm to palpation.
• May occur on tongue, lips, buccal mucosa, gingiva, palatal mucosa, salivary glands,
alveolar ridge, and jawbone.
• They occur early in life and may enlarge rapidly or progressively as the patient grows.

Non-pharmacological Treatment
Surgery can be beneficial if the lesion is small and has no risk of excessive bleeding. The potential
for severe hemorrhage caused by the vascular nature of the lesion must be considered.

Non-pharmacological Treatment of benign tumors


Enucleation or excision is the treatment of choice depending on the type. Can be hemi
mandibulectomy, total mandibulectomy, hemi maxillectomy or total maxillectomy. Followed with
reconstruction when necessary.

Pharmacological Treatment
S: bleomycin injection intralesional (sclerotherapy) under ultrasound guidance to cause
sclerosis of tissues. Surgery may follow if deemed necessary.

16.12.4 Malignant Soft and Bone


Tumours 16.12.4.1 Squamous cell carcinoma

Clinical presentation

• A sore in the mouth that does not heal (most common symptom).
• Pain in the mouth.
• Persistent lump or thickening of mucosa in the cheek.
• Persistent white or red patch on the tongue, gums, tonsils, or lining of the mouth.
• Difficult moving jaw or tongue.
• Difficult chewing or swallowing.
• Enlarged cervical lymph nodes may be present.

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Note
Take tissue biopsy of the lesion and send for histopathology investigation or refer the patient as
early as possible to a centre where there is oral and maxillofacial surgeon and Histopathology unit.
Treatment
Palliative; but this depends on stage of the tumor: stage I and II surgical excision (squamous cell
carcinoma) with wide margin then curative radiotherapy. Others, surgical excision, radiotherapy
followed by chemotherapy.

16.12.4.2 Lymphomas
These are group of neoplasms of varying degrees of malignancy which are derived from B-cells of
lymphoid tissues, the lymphocytes and histiocytes in any of their developmental stages.

Burkitt’s lymphoma (African Jaw Lymphoma)


Clinical presentation
• It shows close association and infection with the Epstein Barr virus. Confined almost
exclusively to children between 2–14years of age.
• Rapidly growing tumor mass of the jaws, destroying the bone and causing teeth loosening
with extension the maxillary, ethmoid and sphenoid sinuses as well as the orbit.
• Visceral organ involvement also occurs.

Note
Diagnostic confirmation is through histopathology; hence, it is emphasized to do early detection
and referral since Burkitt’s lymphoma responds very quickly on chemotherapy. (For detailed
management of malignant tumors please refer to the malignancy on chapter twenty-two)

16.12.5. Odontogenic and Non- Odontogenic Cysts


Odontogenic cysts
A group of jaw cysts that are formed from tissues involved in odontogenesis (tooth development).
Odontogenic cysts are closed sacs filled with fluid, and have a distinct membrane derived from rests
of odontogenic epithelium.

Non-odontogenic jaw cysts


A group of cysts arising from epithelial remnants of embryonic ducts left behind after embryonal
facial and jaw development; they are located deep within the tissues in the region of former epithelial
ridges, epithelial walls, and primary facial fissural and cleft structures. Some few examples of
frequently encountered cysts I orofacial regions are:

Dentigerous cyst
Dentigerous cysts, also called follicular cysts, are slow-growing benign and non-inflammatory
odontogenic cysts that are thought to be developmental in origin.

Clinical presentation
• Uninfected dentigerous cysts are painless and non - tender on palpation.
• Larger cysts cause a marked, smooth, rounded expansion of the bone, which may be
reduced to a thin layer of cortical plate.

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Investigation
Radiographically, they usually present as a well-defined and unilocular radiolucency surrounding the
crown of an unerupted or impacted tooth within the mandible.

Radicular (Apical) cyst


Radicular cyst is an inflammatory jaw cyst originating from epithelial remnants of the periodontal
ligament because of inflammation that is generally a consequence of pulp necrosis. The resulting
cyst commonly involves the apex of the affected tooth either by dental caries or trauma.

Investigation
Take OPG or Skull X-ray, the cysts appear as rounded, radiolucent areas sharply demarcated from
normal. Apical periodontal cysts are associated with the roots of dead teeth bone by a thin,
radiopaque, limiting line of compact or cortical bone.

Non pharmacological treatment


Dental cystectomy under local or general anesthesia.

Globulomaxillary cyst
The globulomaxillary cyst is a cyst that appears between a maxillary lateral incisor and the adjacent
canine. The globulomaxillary cyst often causes the roots of adjacent teeth to diverge.

Investigation
It exhibits as an "inverted pear-shaped radiolucency" on radiographs, or X-ray films.

Non-pharmacological Treatment
Dental cystectomy under local or general anesthesia.

Dermoid Cyst
Dermoid cysts are rare masses of the oral cavity derived from ectodermal elements. These are
benign, slow-growing tumors that are typically asymptomatic but cause complications of inflammation
or dysphagia, dystonia, and airway encroachment due to mass effects.

Clinical presentation
• Massive swelling of the floor of the mouth, which had displaced the tongue cranially.
• Painless slowly growing cystic lesion in the sublingual and or submental spaces.
• A dentigerous cyst may be suspected where a tooth is missing from the arch without any
history of previous extraction.

Non-pharmacological Treatment
Enucleation through an external approach below the mandible or intraorally though an incision in the
floor of the mouth.

Ranular Cyst
A mucous extravasation cyst involving a sublingual gland and is a type of mucocele found on the
floor of the mouth.

Clinical presentation
• Translucent, blue, dome-shaped, fluctuant swelling in the tissues of the floor of the mouth.
• The swelling is not fixed, may not show blanching, and is non-painful unless it becomes
secondarily infected.
• The usual location is lateral to the midline, which may be used to help distinguish it from a
midline dermoid cyst.

Non-pharmacological Treatment
Excision of sublingual salivary gland which is affected.

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16:13 Management of Oral Conditions during Pregnancy
The oral changes which are seen in pregnancy include gingivitis, gingival hyperplasia, pyogenic
granuloma, and salivary changes. Gastric acid secretion and the reflux of the acid into the oral cavity
leads to worsening of enamel erosion, increased caries risk, increased tooth mobility and loss.

For the first trimester (1-12weeks)


During the first trimester, it is recommended that the patients be scheduled to assess their current
dental health, to inform them of the changes that they should expect during their pregnancies, and to
discuss on how to avoid maternal dental problems that may arise from these changes.

Recommendations
Educate the patients about the maternal oral changes which occur during pregnancy.
Emphasize strict oral hygiene instructions and thereby, plaque control.
Limit dental treatment to a periodontal prophylaxis, normal filling, and emergency treatments only.
Avoid routine radiographs. They should be used selectively and only whenever they are needed.

For the second trimester (13-24weeks)


During the second trimester, the organogenesis is complete, and the risk to the foetus is low. The
mother has also had time to adjust to her pregnancy, and the foetus has not grown to a potentially
uncomfortable size that would make it difficult for the mother to remain still for long periods.

Recommendations
Maintenance of oral hygiene and plaque control.
It’s safe to perform scaling, polishing and curettage if necessary.
Active oral diseases should be controlled.
It’s safe to perform elective procedures i.e. Root canal, extraction, restorations.
Avoid routine radiographs. Use selectively and when they are needed.

For the third trimester (25-40weeks)


The fetal growth continues and the focus of the concern now, is the risk to the upcoming birth
process and the safety and comfort of the pregnant woman. It is safe to perform a routine dental
treatment in the early part of the 3rd trimester.

Recommendations
Maintenance of oral hygiene and plaque control.
It’s safe to perform scaling, polishing and curettage if necessary.
Active oral diseases should be controlled.
It’s safe to perform elective procedures.
The radiograph use should be minimized.
Procedures not to be performed after mid time of the third trimester.

Note
Pregnancy should not be considered as an absolute reason to deny required dental care. Pregnant
patients must be educated about the importance of maintaining good oral hygiene, expected
changes in the oral cavity and routine dental visits.

16.14 Temporal Mandibular Disorder and Chronic Orofacial Pain


Temporomandibular disorders (TMD) are disorders of the jaw muscles, temporomandibular joints,
and the nerves associated with chronic facial pain.

16.14.1 Chronic Orofacial Pain other than Temporomandibular Disorders


16.14.1.1 Trigeminal Neuralgia
A sudden, usually unilateral, severe, brief, stabbing, recurrent pain in the distribution of one or more
branches of the fifth cranial nerve.

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Clinical presentation
• Episodes of severe, shooting, or stabbing pain that may feel like an electric shock.
• Spontaneous attacks of pain triggered by things such as touching the face, chewing,
speaking, or brushing teeth.
• Pain in areas supplied by the trigeminal nerve, including the cheek, jaw, teeth, gums, lips,
or less often the eye and forehead.
• Pain affecting one side of the face at a time.

Note
For details of the Investigation and treatment refer a chapter eight (Central Nervous
System).

16.14.1.2 Persistent Idiopathic Orofacial Pain (a Typical Facial Pain, a Typical Odontalgia)
A persistent facial pain that does not have the characteristics of the cranial neuralgias and is not
attributed to another disorder.
Clinical presentation
• Poorly localized deep pain that does not follow anatomically defined patterns.
• Patients may have had multiple dental treatments to try and remove the pain.
• There is a female preponderance in the third to fourth decades.

Investigation
Thorough clinical history and examination
Take radiographs of the dentition preferable OPG

Non-pharmacological Treatment
Irreversible or invasive procedures should not be undertaken on teeth to try and relieve the pain if the
clinical picture, vitality testing or radiographic examination would not support the procedure.

Pharmacological Treatment
A: amitriptyline (PO) 25mg nocte 24hourly for 1month.
AND
A: carbamezepine (PO) 100mg 8hourly for 1month. Dosage can be increased up to 300mg
at the same frequency and duration.

16.14.2 Temporomandibular Disorders (TMDs)


A collective term embracing several clinical problems that involve the masticatory musculature, the
temporomandibular joint and associated structures, or both.

Clinical presentation
• Facial pain.
• Limitation of jaw motion.
• Muscle tenderness and stiffness.
• Along with any number of associated symptoms in the head, face, and neck region.

Non-pharmacological Treatment
Reassurance and counseling
Provide counseling to the patient on the natural history and course of temporomandibular disorders,
the role of stress and parafunctional habits such as clenching and grinding of the teeth, the
frequency of the problem in the population, and the self-limited nature of the disorder.

Heat application
Application of heat to the sides of the face with a heating pad, hot towel, or hot-water bottle. Vigorous
treatment may be achieved with ultrasound or short-wave diathermy heat treatments, which are
widely available in physiotherapy units.

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Fabrication of Intraoral Occlusal Orthotic Appliances
These devices are worn on the teeth like a retainer or a removable denture and are usually made of
processed, hard acrylic.

Physiotherapy
Perform manual manipulation, massage, and ultrasonography, which are helpful in reconditioning
and retraining the masticatory and the other cranio-cervical muscles that are usually involved in
temporomandibular disorders.
Pharmacological Treatment
A: amitriptyline (PO) 25mg nocte for 1month.
If the treatment is successful, maintenance dose should be given for 2-4months.

16.14.3 Osteoarthritis and Rheumatoid arthritis of TMJ


For details management of these two conditions, refer a chapter for disease of musculoskeletal
system

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CHAPTER SEVENTEEN
MUSCULOSKELETAL DISORDERS

17.1 Infections
17.1.1 Osteomyelitis
Osteomyelitis is an infection of the bone or bone marrow caused by pyogenic bacteria or
mycobacteria or fungi. This condition is most common in children under 12 years. Staphylococci
aureus are the most frequent responsible organisms. In patients with sickle cell disease Salmonella
species become more common pathogens than in healthy hosts. Can be classified as acute or
chronic depending on duration of symptoms.

Clinical presentation of acute osteomyelitis


• Fever, malaise severe pain at the site of infection, fatigue, irritability, restriction of movement
(pseudo paralysis of limb in neonates) local edema, erythema, and tenderness
• A history of recent trauma, surgery, or infection of another organ If the infection is close to a
joint there may be a ‘sympathetic’ effusion or concomitant septic arthritis.

Note
Risk Factor: Poor social economic status, immunosuppression and or malnutrition

Investigations
• Total and differential White Blood Cell • Polymerase Chain Reaction (PCR )
count for special case like Kingella kingae
• Erythrocyte sedimentation Rate species
• C- Reactive protein • Bone Scan using Technetium –99 in
• Urinalysis acute infection
• Urine for Culture and Sensitivity • Ultrasound
• Blood for culture and Sensitivity or • Plain X-ray
• Aspirated pus for culture and • CT scan in complex anatomical
sensitivity regions like shoulder, pelvic, spine
• Bone Biopsy for Culture and sensitivity

Pharmacological Treatment
B: cloxacillin (IV) 1–2g 6hourly then continue with ampicillin + cloxacillin (FDC) (PO) 500mg
8hourly to complete 3-6weeks course or until CRP and x ray become negative.
OR
C: ampicillin+sulbactam (FDC) (IV) 3g 6hourly for two weeks
THEN
B: amoxillin+clavulanate (FDC)(PO) 625mg 12hourly for 4weeks.
Patients with penicillin allergy consider.
S: clindamycin (IV) 60mg 6hourly for 2weeks then orally to complete 4-6weeks
AND
C: ciprofloxacin (IV) 400mg 12hourly for 2weeks then orally to complete 4-6weeks

For sickle cell patient if salmonella spp is suspected consider


C: ciprofloxacin (IV) 400mg 12hourly for 4weeks, you may change to oral after 2weeks

Surgical management
Surgical drainage and bone window recommended in all cases presenting with history lasting > 24
hours,

Clinical presentation of chronic osteomyelitis


A patient with a history of osteomyelitis who is experiencing a recurrence of pain, erythema, and
swelling in association with or without pus draining sinus

Investigations
• Total and differential White Blood • Erythrocyte sedimentation Rate
Cell count • C- Reactive protein

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• Stop antibiotic for two weeks before • Bone Scan using Technetium –99 in
bone biopsy for culture and acute infection
sensitivity • Plain X-ray
• Polymerase Chain Reaction (PCR ) • CT scan in complex anatomical
for special case like Kingella kingae regions like shoulder, pelvic, spine
species

Pharmacological management
B: amoxicillin + clavulanate (FDC) (PO) 625mg 12hourly for 6weeks

Surgical management
Extensive Surgical debridement of all devitalized tissue and dead bone, dead space filled with
antibiotic beads,
Antibiotics cement mixture
S: vancomycin at a dosage of 2–4g per 40g of cement

17.1.2 Septic Arthritis


Inflammation of a synovial membrane with purulent effusion into the joint capsule, often due to
bacterial infection, but can be caused by fungi and mycobacteria species. If not treated within 24 to
48hours may cause irreversible joint erosion, septicemia and can be fatal.

Clinical presentation
As for acute osteomyelitis however this time sign and symptoms will be localized around the affected
joint (refers Kocher’s criteria in standard text book for clinical diagnosis )

Pharmacological Treatment
Treat like acute osteomyelitis

Surgical drainage
• Open surgery – incision and drainage followed by meticulous irrigation
• Laparoscopic drainage

17.1.3: Gonococcal Arthritis


Pharmacological Treatment
A: benzyl penicillin (IV) 2.5–5MU 6hourly for 7days
AND
B: ceftriaxone (IV) 1g 12hourly for 7days
OR
S: cefepime (IV) 2g 12hourly for 7days

Note
• Adjust treatment basing on culture and sensitivity results.
• Repeat serial CRP, FBP, ESR starting 48hrs after initiation of appropriate treatment until
normalize

Surgical drainage
• Open surgery
• Laparoscopic drainage

17.1.4: Post Open Reduction and Internal Fixation or Arthroplasty Infection


• Early < 4/52 post surgery and late >4/52

Clinical presentation of Post arthroplasty infection


• Pain • Signs-sinus, effusion, wound
• Loss of ROM erythema
• Swelling • X rays –periosteal reaction,
• Local warmth subchondral bone resorption

371
Investigations
• Total and differential White Blood • Bone Scan using Technetium –99
Cell count in acute infection
• Erythrocyte sedimentation Rate • Plain X-ray
• C - reactive protein • CT scan in complex anatomical
• Aspirated pus for culture and regions like shoulder, pelvic, spine
sensitivity • Magnetic Resonance Imaging (MRI)
• Synovial or Bone Biopsy for Culture in Acute Stage
and sensitivity

Pharmacological management
General Principal: Start empirical treatment while awaiting culture and sensitivity results, adjust
drug according to laboratory results, and continue treatment until CRP become negative.
S: vancomycin (IV) 1g 12hourly for 6weeks
OR
S: clindamycin (IV) 600mg 8hourly for 6weeks
AND
D: ceftazidime (IV) 2g 12hourly for 6weeks
OR
S: cefepime (IV) 2g 12hourly for 6 weeks
OR
S: meropenem (IV) 500mg to 1g 8hourly for 6weeks

Surgical management:
• Post arthroplasty infection
Stage 1: Removal of prosthesis and replace with cement spacer or postalac and antibiotics for 6/52
Stage 2: Use of cement in re implantation and use -stemmed component

• Surgical site infection posts open reduction and internal fixation


Stage 1: Extensive surgical debridement, remove metal implant and replace with external fixation,
traction or orthosis
Stage 2: Revision surgery once CRP and other inflammatory marker become negative

Supportive treatment for bone and joint infection


• Rest and splintage of affected joint • Walking aid in case of pathological
for 48hrs fracture
• Nutritional support • Hydration
• Addressing the predisposing • Antipyretic for fever
condition • Analgesics for pain
• Physiotherapy to improve range of
motion of nearby joint

17.1.5: Tropical Pyomyositis


This is a condition whereby there is pyogenic infection of large muscle/muscles with extensive
necrosis of the involved muscle. This condition occurs more commonly in the tropics, affecting
immunocompromised individual than normal individual. The cause is uncertain since abscess
multiple pockets explored early are sterile but later culture of the pus usually yields Staphylococcus
aureus.

Clinical presentation
Fever and painful induration/fluctuation of one or more of the large muscles, mostly in the lower
extremities.

Investigations
• Complete blood count (CBC) • Plain X-ray
• Erythrocyte sedimentation rate (ESR • Muscle biopsy for culture and
• C – Reactive Protein test (CRP) sensitivity
• Ultrasound

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Pharmacological Treatment
Higher level facilities treatment should be guided by C/S results
Children
B: cloxacillin (IV) 1–2g 6hourly for 7-14days
OR
A: erythromycin (PO) 500mg 6-8hourly for 7-14days
OR
S: vancomycin IV 1g 12hourly for 7days
OR
S: clindamycin (IV) 600mg 8hourly for 7days

Adults
A: erythromycin (PO) 500mg 6-8hourly for 7-14days;
OR
B: amoxillin +clavulanate (FDC) (PO) 625mg 12hourly for 7-14days
OR
S: clindamycin (IV) 600mg 8hourly for 7days
OR
S: vancomycin (IV) 1g 12hourly for 7days

Surgical management
Incision and drainage and irrigation with copious amount of 0.9% sodium chloride

17.1.6: Necrotizing Fasciitis


Life threatening progressive rapidly spreading inflammatory infection located in deep fascia, most
commonly caused by Streptococcus species or polymicrobial

Clinical presentation of Necrotizing Fasciitis


• Early Sign and symptoms mimic • Late-stage multiple discoloration
acute osteomyelitis. develops a large are of gangrenous
• Foul smelling discharge skin,
• Presence of features of toxic shock
Investigations
• Complete blood count (CBC) • Plain X-ray
• Erythrocyte sedimentation rate (ESR • Muscle biopsy for culture and
• C – Reactive Protein test (CRP) sensitivity
• Ultrasound

Pharmacological Treatment
A: gentamycin (IV) 80mg 8hourly for 7days
AND
B: chloramphenicol (IV) 500mg 6hourly +/_S: clindamycin (IV) 600mg 8hourly for 7days
Alternatively
A: benzathine benzylpenicillin (IV) 2-4MU 6hourly for 7days
AND
S: clindamycin (IV) 600mg 8hourly +/- ciprofloxacin 400mg (IV) 8hourly for 7days
Alternatively
A: benzathine benzylpenicillin (IV) 2-4MU 6hourly for 7days
AND
S: clindamycin 600mg (IV) 8hourly for 7days
OR
S: vancomycin 1g 12hourly for 7days

Note
Adjust treatment basing on culture and sensitivity results Repeat serial CRP, FBP, ESR starting
48hours after initiation of appropriate treatment until normalize.

Surgical management
Serial extensive surgical debridement,
Skin grafting once the wound granulates with no sign of infection

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Supportive treatment
• Hydration • Antipyretic for fever
• Rest • Analgesics for pain
• Nutritional support • Physiotherapy to improve range of
• Addressing the predisposing motion of nearby joint
condition

17.2 Inflammatory Conditions


These are a group of diverse inflammatory conditions due to different causes which affect joints and
other musculoskeletal tissues.

General Guidelines
• The first-line treatment is a non-steroidal anti-inflammatory drug (NSAID). This group
includes medicines like aspirin, diclofenac and Ibuprofen, (provide dosage and scientific
proof) but does NOT include paracetamol
• NSAIDs should be used cautiously in pregnancy, the elderly, and patients with asthma and
liver or renal impairment.
• NSAIDS should be avoided in patients with bleeding disorders
• NSAIDS increases the risk of heart failure and stroke and should be avoided in patients with
cardiovascular diseases and those who are at high risk
• NSAIDs should be avoided in patients with current or past peptic ulceration.
• NSAIDs should be taken with food
• If dyspeptic symptoms develop in a patient on NSAIDs, try adding magnesium trisilicate
mixture. If dyspepsia persists and NSAID use considered essential antagonist
• Physiotherapy is a useful adjunct treatment in many inflammatory joint conditions

Referral: For patients with serious rheumatic disease and peptic ulceration should be referred to
higher level health facility with adequate expertise and facilities.

17.2.1 Rheumatoid Arthritis


Rheumatoid arthritis is an autoimmune condition whereby the immune system attacks the synovial
membrane of joints, initially of the small joints but progressively involving the big joints. It is a chronic
multisystem disease of unknown etiology.

Clinical presentation
Morning stiffness for >1hr, symmetrical swelling and inflammation of ≥ 3joints (Elbow, Wrist, PIP,
MCP, Ankle MTP) Rheumatoid nodule, subluxed joints.

Target population
Patients who
• Have at least1 joint with definite clinical synovitis (swelling)
• With synovitis not better explained by another disease

Table 17.1: Classification criteria for RA (score- based algorithm):


add scores of categories A-D, A score of ≥6/10 is needed for classification of patient as having
definite RA

Domain Category Point score


a
A Joint involvement (0–5 points)
1 large joint 0
2–10 large joints 1
1–3 small joints (large joints not counted) 2
4–10 small joints (large joints not counted) 3
>10 joints including at least one small joint 5
b
B Serology (at least one test needed for classification: 0–3 points)
Negative RF and negative ACPA 0
Low positive RF or low positive ACPA 2
High positive RF or high positive ACPA 3
C Acute-phase reactants (at least one test needed for classification;
c
0–1 point)
Normal CRP and normal ESR 0

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Abnormal CRP or abnormal ESR 1
D Duration of symptoms
<6 weeks 0
≥6 weeks 1

Investigations
Note
No test results are pathognomonic for RA instead they are potential identifier of disease progression
and monitoring of response to treatment.

• Full Blood Picture with differential • Antinuclear antibody Test


(FBP) • Liver Function test
• Erythrocyte Sedimentation Rate • Renal function Test
(ESR) • Other test depending on stage of the
• Rheumatoid factor (RF) disease and expert opinion.
• C-Reactive Protein (CRP) • Anti-citrullinated protein antibody
• Synovial Fluid analysis (WBC (more specific for Rheumatoid
>@2000/ mm³) arthritis)

Pharmacological Treatment
Non-steroidal anti-inflammatory drugs (NSAIDs) should be used in combination, corticosteroids or
with DMARDs and once DMARDs are effective, NSAIDs and corticosteroids can be reduced in dose
or discontinued.

Non selective COX1 and COX2 Inhibitors, until symptoms subside


A: ibuprofen (PO) 400–800mg 8hourly for 5days
OR
D: meloxicam (PO) 7.5mg–15mg 12 hourly for 5-14 days
OR
A: Piroxicam 20mg (PO) 24hourly or 10mg 12hourly for 5-14days
Selective COX 2 inhibitors
S: ketoprofen (PO) 50-75mg 8hourly for 7-14days
OR
S: dexketoprofen trometamol (PO) 12.5mg 6hourly or 25mg (PO) 8hrly for 7-14days
OR
Corticosteroid Therapy
A: prednisolone (PO) 40mg for 3days then taper over a course of 2 to 4 weeks
OR
D: triamcinolone (IM) 40mg every 6weeks may be supplemented by additional IM PRN 20-
100mg
OR
D: betamethasone dipropionate (Intralesional) 2mg + betamethasone sodium phosphate
(Intralesional) 10mg once ; not to exceed(4ml) 24hourly repeat every after 2 to 12 weeks,
maximum of 4 injections per year for a duration of 2years

Disease-Modifying Ant-rheumatoid Drugs or DMARDs


S: hydroxychloroquine (PO) 400-600mg 24hourly for 4-12 weeks followed by (PO) 200-400
mg 24hourly for 12 weeks
OR
D: sulfasalazine (PO) 0.5 – 1g 24hourly in two divided doses increase weekly to
maintenance dose of 2g/day (PO) for 12 weeks
OR
S: methotrexate (PO) may be taken with or without food 7.5mg dose weekly; increase PO
dose to optimum response however should not exceed 20mg/week for 12 weeks.

Note
• Repeat CRP and ESR after every two weeks to determine whether to increase dose or maintain or
taper down.
• Patient who are using NSAIDs for more than 2 weeks should be given proton pump inhibitors
• Combine oral corticosteroid or NSAIDS with one of the DMARDs to control inflammation
symptoms before DEMARDs become effective.
• Those on steroid should undergo RBG at least biannual.

375
Surgical treatment
• Synovectomy
• Tenosynovectomy
• Tendon realignment
• Reconstructive surgery or arthroplasty
• Arthrodesis
Rehabilitation
Orthotics and splints: Useful in decreasing pain and inflammation, improve function, reduce
deformity, and restore joint alignment. Well-padded shoes
• Walking aids
• Braces
Physiotherapy and occupational therapy
• 30 minutes of daily aerobic exercises at least four times a week
• Occupational therapy aims at enabling patient to cope with activities of daily life.

17.2.2: Juvenile Idiopathic Arthritis


Juvenile Idiopathic arthritis (JIA) is the most common chronic rheumatologic disease in children and
is one of the most common chronic diseases of childhood. JIA should be considered with arthritis
lasting for at least 6 weeks in children aged < 16 years. All the other causes should be excluded
including infections, malignancies and hematological conditions like sickle cell anemia.

Clinical presentation
History findings in children with JIA may include the following:
• Arthritis present for at least 6 weeks before diagnosis (mandatory for diagnosis of JIA)
• Either insidious or abrupt disease onset, often with morning stiffness or gelling
phenomenon and arthralgia during the day
• Complaints of joint pain or abnormal joint use
• History of school absences or limited ability to participate in physical education classes
• Spiking fevers occurring once or twice each day at about the same time of day
• Evanescent rash on the trunk and extremities
• Psoriasis or subtler dermatologic manifestations
Types of JIA include the following:
• Systemic-onset juvenile idiopathic arthritis
• Oligoarticular juvenile idiopathic arthritis
• Polyarticular juvenile idiopathic arthritis
• Psoriatic arthritis
• Enthesitis related arthritis
• Undifferentiated arthritis

Investigations
• ESR and CRP • Antinuclear antibody (ANA) testing
• Complete blood count (CBC) • ASOT and Anti-DNAse B test
• LFT • Urinalysis additional.
• Serum creatinine

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Non-pharmacological Treatment
• Psychosocial support
• Physiotherapy once the pain has subsided

Pharmacological Treatment
A: ibuprofen (PO) 10mg/kg/dose 6-8hourly (should be given if the duration of arthritis has
not reached 6 weeks)
AND
A: prednisolone (PO) 0.25-0.5mg/kg/day should be given in the initial stage of the
treatment, and for patients that are responding slowly to treatment, duration should be not
more than 6 months
OR
S: methotrexate (PO) 0.5mg/kg weekly (maximum 20mg)

Monitor for toxicity with FBP (leucopenia) and ALT (hepatotoxicity) every 1-3months.
Consider tapering and stopping treatment if the patient is in remission.
OR
D: Sulfasalazine (PO) 20-50mg/kg/day in two divided doses (maximum 2000mg/day)

17.2.3. Gout
Gout is a recurrent acute arthritis of peripheral joints which results from deposition, in and about the
joints and tendons, of crystals of monosodium urate from supersaturated hyperuricaemic body fluids.
The arthritis may become chronic.

Clinical presentation
• The main clinical features are those of an acute gouty arthritis, often nocturnal, throbbing
crushing or excruciating pain.
• The signs resemble an acute infection with swelling, hot red and very tender joints.
• The first metatarsophalangeal joint of the big toe is frequently involved

Investigation
• Serum uric acid level.

Non-Pharmacological Treatment
• In obese patient, reduce weight
• Avoid precipitants e.g. alcohol. Red meat
• Institute anti-hyperuricaemic therapy e adjust the dose depending on response to reduce
uric acid synthesis
• Prevention or reversal of deposition of uric acid crystals in males

Note: Aim is to maintain serum uric acid level below 8mg/dl (0.48mmol/l)

Pharmacological Treatment
Acute state
A: ibuprofen (PO) 400mg stat then 200mg 8hourly until 24 hours after relief of pain usually
3-5days.
OR
A: piroxicam 10–20mg (PO) once a day for 5days
OR
A: prenisolone (PO) is 40mg daily for 3days then taper for 2-4 weeks combined with NSAIDs
and proton pump inhibitor
OR
D: methylprednisolone Injection OR triamcinolone OR Betamethasone for monoarticular
flares (2vials for large joint and 1vial for small joints perday, repeat every after 2-12 weeks,
maximum of 4 injections per year for a duration of 2years)

Anti –hyperuricemic therapy for chronic cases


1st line
B: allopurinol (PO) 100mg 24hourly. This may be increased every 2-5weeks to until uric acid
level reaches 6mg/dl or less. Maximum of 600mg daily continue therapy for 6months.

377
2nd line
S: febuxostat (PO) 10mg 24hourly for 4weeks then 20mg 24hourly for 4weeks then 40mg
24hourly may increase to reaches 6mg/dl or less. Continue treatment for 6months.

Nutritional support
To prevent excessive accumulation of uric acid
• Use of low purine diet by restricting consumption red meat, fish, alcohol, stimulants,
and high protein foods to avoid exogenous addition of purines to the existing high
uric acid load is recommended
• Encourage consumption of alkalizing foods e.g. lemons, tomatoes, green beans,
fruits and milk products
• Intake of fluids about 3lts/day to enhance excretion of uric acid based on
assessment is recommended
• Moderate protein intake (0.8g/kg/day)
• Maintain adequate CHO intake to prevent ketosis
• Limit fat intake
• Avoid large and heavy meals late in the evening
• Encourage consumption of whole grains

17.2.4 Osteoarthritis
It is a common form of arthritis, characterized by degenerative loss of articular cartilage, subchondral
bony sclerosis, and cartilage and bone proliferation subsequent osteophyte formation. Gradual onset
of one or a few joints involved.

Clinical presentation
• Pain is the commonest symptom
• Specific clinical features depend on the joint involved e.g. enlargement of distal
interphalangeal joint (Bouchard’s nodes)

Investigation
• Plain X-ray of involved joint/ joints. • Diagnostic arthroscopy
• CT scan • Synovial fluid analysis

Non-pharmacological Treatment
• Rest the joint. Use crutches or walkers to protect weight bearing joints in severe cases.
• Crepe bandage or braces also can be worn during the active phase of disease.
• Reduction of weight in obese patients
• Physiotherapy exercise to the affected joints, TENS

Pharmacological Treatment
A: ibuprofen (PO) 400mg stat then 200mg 8hourly 7-14days
OR
C: diclofenac sodium (PO) 50mg 8hourly for 7-14days
OR
D: meloxicam (PO) 7.5-15mg 12hourly-24hourly for 7-14days
OR
S: dexketoprofen trometamol (PO) 12.5mg 4-6hourly or 25mg 8hourly for 7-14
OR
Topical non-steroidal anti-inflammatory drugs
A: diclofenac gel 12hourly for 2weeks

S: ketoprofen gel 12hourly for 2weeks

378
Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of peptic
ulcers or when giving NSAIDs for a duration of 2 weeks or more

A: omeprazole 20mg 24hourly


OR
C: pantoprazole 40mg 24hourly
OR
S: esomeprazole 40mg 24hourly
OR
C: lansoprazole 30mg 24hourly for 2-4 weeks
AND
B: tramadol (PO) 50mg 8houly for 7-14days
OR
B: tramadol+paracetamol (PO) 550mg 8hourly for 14days
OR
A: ibuprofen+paracetamol (PO) 900mg 8hourly for 14days
AND
A: prednisolone (PO) 5-10mg 24hourly for

Intra articular injection


D: methylprednisolone (Intra articular) 80mg/ml for large joint and 40mg/ml for small joints
per day repeat every after 2-12 weeks, maximum of 4injections per year for a duration of
2years.
OR
S: triamcinolone (Intra articular) 80mg/ml for large joint and 40mg/ml for small joints per day
repeat every after 2-12 weeks, maximum of 4injections per year for a duration of 2years.
OR
D: betamethasone (Intra articular) 12mg/ml for large joint and 6mg/ml for small joints per day
repeat every after 2-12 weeks, maximum of 4injections per year for a duration of 2years.
AND
A: 1% lignocaine 1-2mls.
AND
S: hyaluronic acid (Intra articular)16mg once per week for 3 consecutive weeks

Supplements
S: glucosamine sulfate1500mg +chondroitin sulfate 1200mg (FDC) (PO) taken with meal
once a day for 3-6months

Surgical management for advanced disease


• High tibia osteotomy for Varus • Joint fusion /arthrodesis for limb
deformities of knee joint salvage
• Fibula osteotomy for medial • Excisional arthroplasty
degeneration of the knee joint
• Total joint replacement

Note
For patient who are not fit for surgery consider nerve block option and or radiofrequency ablation.
Patient should be assessed every after two or four weeks to evaluate response to treatment and
disease progression

379
17.2.5 Heterotopic Ossification
Heterotopic ossification is defined as bone formation in no osseous tissues. Usually occurs in trauma
such as fractures and surgical procedures, the exact cause remains unknown.
Clinical presentation
• Pain and reduced ROM following trauma or post-surgical intervention.
• swelling and tenderness, which can mimic a low-grade infection.
• Bone in soft tissue starts to appear on plain radiographs 4 to 6 weeks after the
trauma/surgery,

Pharmacological Treatment
• Indomethacin 75- 150mg per day in single daily dose or divided dose 12hrly

Surgical management
Surgery is delayed for 6 months after the initial trauma/surgery to allow the bone to mature and a
distinct fibrous capsule to develop.

17.2.6 Tendinopathies
These are clinical syndrome characterized by chronic, localized tendon pain exacerbated by
mechanical loading. Caused mostly by tendon overuse and metabolic factors. Classified as Acute or
Chronic.

Clinical presentation
• Pain with palpation of the affected • Kinetic chain changes (muscle
part weakness, abnormal movement
• Pain during tendon loading which patterns or joint stiffness)
may be also referred pain. • Muscle spasm

Investigations
• MRI for tendinopathy involving deep tendon like around the shoulder joint
• Greyscale or color Doppler uss.

Non-pharmacological Treatment
• Physiotherapy (active exercise, stretching)
• Activity modification
• Correction of any biomechanical faults
• Reduction of aggravating activities
• Ice heat (chronic tendinopathy)
• Joint mobilization and friction (massage).

Pharmacological Treatment
Pain management in acute state
A: ibuprofen (PO) 400mg stat then 200mg 8 hourly
OR
C: diclofenac sodium (PO) 50mg 8hourly for 7-14days
OR
D: meloxicam (PO) 7.5-15mg 12-24hourly for 7-14days
OR
D: tramadol + paracentamol (PO) 550mg 8hourly for 7- 14days
OR
A: paracentamol + ibuprofen (PO) 900mg 8hourly for 7-14days

Topical analgesics can be added in cases of severe pain,


A: diclofenac gel applies 12hourly
OR
S: ketoprofen gel apply 12hourly

Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of peptic
ulcers or when giving NSAIDs for a duration of 2 weeks or more.

380

Proton pump inhibitors
A: omeprazole (PO) 20mg 24hourly
OR
C: pantoprazole (PO) 40mg 24hourly
OR
Corticosteroid Therapy
A: prednisolone (PO) 40mg 24hourly for 3days then taper down over 2-4weeks
OR
D: betamethasone (Intralesional) 12mg 24hourly; repeat every after 2-12 weeks, maximum
of 4 injections per year for a duration of 2years.
OR
S: triamcinolone 40mg per injection site once weekly not to exceed 40mg/day maximum of
3 injections in one year at interval of 1-3 weeks between injections.

Surgery
When no improvement after 6month of combined physiotherapy and medical treatment. Open
surgery or laparoscopic

17.2.7 Plantar Fasciitis


Planter Fasciitis is a degenerative disease of plantar fascia probably due to overuse trauma that
leads to micro tears. Depending on duration of symptoms it can be acute 4-6 weeks, subacute 6-12
weeks and chronic >12weeks with/without refractory.
Clinical presentation
• Pain in the medial side of the heel, most noticeable with initial steps after a period of
inactivity
• Paresthesia
• Tightness of Achilles tendon

Investigations
• Plain X-ray
• Ultrasound
• Nerve conduction and Electromyographic studies
• MRI in chronic with refractory.

Non-pharmacological Treatment
• Weight reduction
• Rest and activity modification
• Stretching/massage
• Ice
• Night splints
• custom orthotic (for client with Pes cavus or planus)
• Extracorporeal shock wave therapy (ESWT) (for subacute and chronic)

Pharmacological Treatment
Pain management in acute state
A: ibuprofen (PO) 400mg stat then 200mg 8hourly
OR
C: diclofenac sodium (PO) 50mg 8hourly for 7-14days
OR
D: meloxicam (PO) 7.5-15mg 12-24hourly for 7-14days
OR
D: tramadol and paracetamol (FDC) (PO) 550mg 8hourly for 14days
OR
A: ibuprofen and paracetamol (FDC) (PO) 900mg 8hourly for 14days

Topical analgesics can be added in cases of severe pain,


A: diclofenac gel apply 12hourly
OR

381

S: ketoprofen gel apply 12houry

Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of peptic
ulcers or when giving NSAIDs for a duration of 2weeks or more.

Proton pump inhibitors


A: omeprazole 20mg 24hourly for 2weeks or more
OR
C: pantoprazole 40mg 24hourly for 2weeks or more
OR
Corticosteroid Therapy
A: prednisolone (PO) 40mg 24hourly for 3days then taper down over 2-4 weeks
OR
S: triamcinolone per injection site 40mg once weekly not to exceed 40mg/day repeat every
after 2 to 12 weeks, maximum of 4 injections per year for a duration of 2 years
OR
D:betamethasone (Intralesional) 12mg 24hourly; repeat every after 2-12 weeks, maximum
of 4 injections per year for a duration of 2years
Surgery
• Open partial plantar fascia release with simultaneous release of first branch of lateral
plantar nerve or
• Endoscopic partial plantar fascia release

17.3: Metabolic Bone Diseases


17.3.1 Osteoporosis and Brittle Bone Diseases
Disease which is characterized by low bone mass, microtextural disruption and skeletal fragility and it
has no clinical manifestation until there is a fracture. Contrary to Brittle bone disease which are
inheritable with many different phenotypic presentation, however medication for the treatment of
these two disease are more or less similar.
Clinical presentation
• Presence of fragility fracture (spine, hip, wrist, humerus, rib and pelvis)
• Family history of osteoporotic fracture
• Bone pain

Investigation
• Complete blood count • Parathyroid stimulating hormone
• Dual-energy X-ray absorptiometry • Thyroid stimulating hormone
(DEXA) to measure spine and hip • Serum creatinine
bone density as reference point • Urea
• Serum 25-hydroxyvitamin D, • Serum electrolyte
• Serum Calcium

Diagnostic criteria
T-score chart based on the mineral density measurement by DXA. Osteoporosis is diagnosed when
a person’s BMD is equal to or more than 2.5 standard deviations below this reference measurement.
Status Hip BMD
Normal T-score of -1 or above
Osteopenia T-score lower than -1 and greater than -2.5
Osteoporosis T-score of -2.5 or lower
Severe osteoporosis T-score of -2.5 or lower, and presence of at least one fragility
fracture

382

Non-pharmacological Treatments
• Fall prevention.
• Diet containing Calcium/vit D.
• Exercise
• Cessation of smoking
• Exposure to sunlight

Pharmacological Treatment
Pain management
A: ibuprofen (PO) 400mg start then 200mg 8hourly
OR
D: meloxicam 7.5-15mg (PO) once-twice a day for 7-14days
OR
Topical analgesics can be added in cases of severe pain,
A: diclofenac gel applies 12hourly
OR
S: ketoprofen gel apply 12hourly

Note
• Consider concomitant use of gastro protective treatment in patients with preexistent history
of peptic ulcers or when giving NSAIDs for a duration of 2 weeks or more.

Proton pump inhibitors


A: omeprazole 20mg 24hourly for 2weeks or more
OR
C: pantoprazole 40mg 24hourly for 2weeks or more
OR
Calcium supplementation
B: Calcium 600mg + Vitamin D 800IU (PO) 24hourly for 3months then re-evaluate (1mcg of
Vitamin D=40IU)

Bisphosphonate treatment – should be given for a period of five years.


S: Ibandronate (IV) 3mg every 3months administered over 15-20minutes (treatment only)

17.3.2: Hypocholecalciferolemia (Vitamin D Deficiency)


This disease is characterized by hypocalcemia and or hypophosphatemia. The acceptable
concentration of Vitamin D is between 30-60ng/Ml.
Clinical presentation
Adult Children
Mild cases are generally asymptomatic Mild cases are generally asymptomatic
Bone pain and tenderness Bone pain and tenderness
Difficulty rising from a sitting position due to muscle Muscle weakness
weakness
Bone deformities (osteomalacia) Delayed achievement of motor milestones
Cognitive decline and dementia Fatigue and malaise
Inadequate dietary and supplemental vitamin D Rickets
intake

Investigations
• Serum calcium • Renal Function test
• Serum alkaline phosphatase • Dual –energy X-ray absorptiometry
• Parathyroid function test (Bone density scan
• Fasting serum phosphate
• Serum 25-hydroxyvitamin D,
(25(OH)D) levels

383

Table 17.3: Interpretation of Serum 25-hydroxyvitamin D, (25(OH) D) levels
Status Endocrine Society Guidelines
Deficient Below 20 ng/mL
Insufficient 21-29 ng/mL
Sufficient 30-60 ng/mL
Ideal 40-60 ng/mL
Considered safe <100 ng/Ml

Non-pharmacological Treatment
• Sunlight exposure • Protective waking
• Bracing • Isometric exercises

Pharmacological Treatment
Children1-18years
D:colecalciferol 2,000 IU 24hourly for 6weeks
OR
50,000IU once a week for 6weeks followed by maintenance therapy of 600-1000IU
24hourly for 3-6months then reevaluate by measuring serum 25(OH)D levels

Adults
D: colecalciferol 6000IU 24hourly or 50000IU once a week for 8weeks or 6000IU followed
by maintenance therapy of 1,500-2,000IU/day.

17.4: Condition which may require Amputation.


Amputation is the surgical removal of part of a limb or extremity such as an arm, leg, foot, hand, toe,
or finger. This is the treatment of choice for diseased limbs and devastating extremity injuries for
which attempts at salvage and reconstruction may be lengthy, emotionally, and financially costly and
have a less than satisfactory results.

Clinical Indication
• Trauma most common reason for • Vascular disease
extremity amputation • Metabolic diseases
• Infection • Congenital anomalies
• Tumor

Goals of amputation
• Preserve functional length. • Prevention of adjacent joint
• Preservation of useful sensibility contractures
• Prevention of symptomatic • Early prosthetic fitting
neuromas Early return of patient to work and recreation.

17.4.1: Diabetic Foot Ulcers


A common surgical complication in diabetic patients. Ulcers can be secondarily infected by
staphylococci, streptococci, coliforms, and anaerobic bacteria which can lead to cellulitis, abscess
formation, gangrene, and osteomyelitis.

Clinical presentation
The three main factors that lead to tissue necrosis in the diabetic foot are:
• Neuropathy
• Infection
• Ischaemia

Non-pharmacological Treatment
• Metabolic control • Relieve pressure: non-weight
bearing

384

• Smoking cessation is essential. • Frequent (e.g. weekly) removal of
• Wound care excess keratin and allow efficient
drainage of the lesion.

Pharmacological Treatment
B: ceftriaxone (IV) 1-2g 24hourly for 7-10days
AND
B: metronidazole (IV) 500mg 8hourly for 7-10days

Depending on culture results


S: piperacillin-tazobactam (IV) 4.5g 6-8hourly 7-10days (for severe/complicated cases)
OR
S: meropenem (IV) 1g 8hourly 7-10days

Surgical Management
• Surgical debridement
• Amputation depending Wagner’s classification

Table 17:4: Wageners Classification for Diabetic Foot Ulcers


ULCER GRADING DESCRIPTION
GRADE 0 No ulcer but high-risk foot
GRADE 1 Superficial ulcer
GRADE 2 Deep ulcer, no bony involvement or abscess
GRADE 3 Abscess with bony involvement (as shown by X-
ray)
GRADE 4 Localized gangrene e.g toe, heel etc
GRADE 5 Extensive gangrene involving the whole foot
Note
Grade 1-3 ulcers are termed non-gangrenous ulcers and Grade 4 and 5 ulcers are termed
gangrenous ulcers

17.5 Affection of the Brain and Spine


17.51 Low Back Pain
Low back pain is a common presenting complaint especially among the adult population. Severity
may range from mild, transient symptom to chronic and disabling pain. Causes of low back pain are
numerous and clues to the underlying cause can usually be found from a good clinical history and
physical examination. In some patients however, no cause will be found, and these people are
described as having nonspecific back pain.

Clinical presentation
Exclude specific causes of low back pain, for example, suspected or confirmed malignancies, spine
infection, spine trauma or inflammatory disease such as spondyloarthritis. (flag signs)
Acute low back pain (pain for <6 weeks’ duration)
Investigations
• Explain to people with acute low back pain with or without sciatica that their pain is likely to
resolve on analgesia and bed rest
• Do not routinely offer imaging for people with acute low back pain with or without sciatica in
absence of flag signs. Consider imaging only if the result is likely to change management.

Non-pharmacological Treatment
Self-management: Provide people with advice and information, tailored to their needs and
capabilities, to help them self-manage their low back pain.
• information on the nature of low back pain and sciatica
• encouragement to continue with normal activities upon pain relief.

385
Physical Exercise: Encourage exercise programmes (biomechanical, aerobics, or a combination of
approaches) based on individual needs, preferences, and capabilities.
Pharmacological treatment
The principles of pharmacological treatment include analgesics and muscle relaxants

A: ibuprofen (PO) 400mg stat then 200mg 8hourly


OR
C: diclofenac sodium (PO) 50mg 8hourly for 7-14days
OR
D: meloxicam (PO) 7.5-15mg 12hourly-24hourly for 7-14days
OR
For severe pain
A: diclofenac (IM) 75 mg 12hourly by deep IM injection for 1-3 days +/-
B: tramadol (IM) 100mg 12hourly by deep IM injection for 1-3days
THEN
C: diclofenac (PO) 50mg 8hourly for 7days +/-
B: tramadol (PO) 50mg 8hourly for up to 7days.

Topical analgesics can be added in cases of severe pain,


A: diclofenac gel applies 12hourly
OR
S: ketoprofen gel apply 12hourly

Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of peptic
ulcers or when giving NSAIDs for a duration of 2weeks or more

Proton pump inhibitors


A: omeprazole 20mg 24hourly for 2weeks or more
OR
C: pantoprazole 40mg 24hourly for 2weeks or more
OR
S: esomeprazole 40mg 24hourly for 2weeks or more
OR
C: lansoprazole 30mg 24hourly for 2-4weeks
Muscle relaxant
S: baclofen (PO) 5mg 8hourly initially, increase by 5mg/dose each after 3days up to 20mg
8hourly for up to 2weeks
OR
S: tizanidine (PO) initially 2mg 8hourly, increase gradually to 4mg per day every after 1-
4days, dose may be extended for 4weeks or more, to discontinue taper gradually; decrease
by 2-4mg daily.

Chronic Low Back Pain (pain for >6 weeks’ duration)


Investigations
• Plain Spine x rays
• Dynamic spine x Rays-Flexion/extension views
• Spine CT scan
• Spine MRI
• EMG can be considered for patients in whom the diagnosis is unclear after MRI

Non-pharmacological Treatment
Non Invasive treatment for chronic low back pain
Self-management: Provide people with advice and information, tailored to their needs and
capabilities, to help them self-manage their low back pain.

386

• information on the nature of low back pain and sciatica
• encouragement to continue with normal activities upon pain relief.

Physical Exercise: Encourage exercise programs (biomechanical, aerobics, or a combination of


approaches) based on individual needs, preferences, and capabilities.
Manual therapies: Consider manual therapy (spinal manipulation, mobilization, or soft tissue
techniques such as massage) for managing low back pain with or without sciatica, but only as part of
a treatment package including exercises.
Orthotics: Consider belts or corsets for managing chronic low back pain with or without sciatica in
selected cases
Psychological therapy: Consider psychological therapies using a cognitive behavioral approach for
managing low back pain but only as part of a treatment package including exercise, spinal
manipulation etc.

Pharmacological Treatment
The principles of conservative treatment include:
• External spinal immobilization and supportive treatment with analgesics, muscle relaxants,
bisphosphonates and bed rest
• Monitor for clinical or radiographic evidence of spinal instability and neurological
deterioration.

A: ibuprofen (PO) 400mg stat then 200mg 8 hourly


OR
C: diclofenac sodium (PO) 50mg 8hourly for 7-14days
OR
D: meloxicam (PO) 7.5-15mg 12hourly-24hourly for 7-14days
OR
For severe pain
A: diclofenac (IM) 75mg 12hourly by deep IM injection for 1-3 days +/-
B: tramadol (IM) 100mg 12hourly by deep IM injection for 1-3days
THEN
C: diclofenac (PO) 50mg 8hourly for 14 days +/-
B: tramadol (PO) 50mg 8hourly for up to 14 days.

Topical analgesics can be added in cases of severe pain,


A: diclofenac gel applies 12hourly
OR
S: ketoprofen gel apply 12hourly

Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of
peptic ulcers or when giving NSAIDs for a duration of 2 weeks or more

Proton pump inhibitors


A: omeprazole (PO) 20mg 24hourly for 2-4 weeks
OR
C: pantoprazole (PO) 40mg 24hourly for 2-4 weeks
OR
S: esomeprazole (PO) 40mg 24hourly for 2-4 weeks
OR
C: lansoprazole (PO) 30mg 24hourly for 2-4 weeks

For radicular symptoms add neuromodulators, neurovitamins and muscle relaxants:

Neuromodulator
D: pregabalin (PO) 75-150mg 24hourly for 4weeks (dose can be escalated based on
individual response)
AND
Neurovitamins
C: Vit B1+B6+B12 (PO) 24hourly for 4weeks
AND

387

Muscle relaxant
S: baclofen (PO) 5mg 8hourly initially, increase by 5mg/dose each after 3days up to-20mg
8hourly for up to 2 weeks
OR
S: tizanidine (PO) initially 2mg 8hourly, increase gradually (PO) to 4mg 24hourly every
after 1-4days, dose may be extended for 4weeks or more, to discontinue taper gradually;
decrease by 2-4mg daily

Invasive treatments for Chronic Low Back Pain


Non-surgical interventions
• Consider epidural injections of local anesthetic and steroid in people with severe refractory
pain.
• Consider referral for assessment for radiofrequency (RF) denervation for people with
chronic low back pain when non-surgical treatment has not worked for them and the main
source of pain is thought to come from structures supplied by the medial branch nerve and
they have moderate or severe levels of localized back pain, or surgical treatment is not
possible due to other comorbid conditions.
Surgical interventions
• Spinal decompression: Consider spinal decompression for people with sciatica when non-
surgical treatment has not improved pain or function and their radiological findings are
consistent with their symptoms. The surgical approach might entail an open or minimal
invasive technique based on patient factors, availability of resources and expertise.
• Spinal fusion: Consider spinal decompression and fusion with transpedicular screws and
rods, or interbody devices in unstable spine patients when non-surgical treatment has not
improved pain or function and their radiological findings are consistent with their symptoms.
The surgical approach might entail an open or minimal invasive technique based on patient
factors, availability of resources and expertise.
17.5.2: Cervical Degenerative Disorders
Cervical degenerative spine disorders (DSD)are common among the adult population. Clinical
characteristics include neck pain radiating to upper extremities related to compression and/or
irritation of one or more cervical nerve roots, resulting into varying degrees of sensory, motor and
reflex changes. Severity may range from mild, transient symptom to chronic and disabling pain.

Clinical presentation
• neck pain, dermatomal arm pain, scapular/periscapular pain
• upper limb paresthesias, numbness and sensory changes,
• muscle cramps, weakness, or abnormal deep tendon reflexes

Investigations
• Plain Spine x rays
• Dynamic spine x-Rays-Flexion/extension views
• Cervical Spine MRI
• EMG can be considered for patients in whom the diagnosis is unclear after MRI

Non-pharmacological Treatment
Non Invasive treatment for neck pain and radiculopathies
Physical Exercise: Encourage exercise programs based on individual needs, preferences, and
capabilities.
Manual therapies: Consider manual therapy (spinal manipulation, mobilization, or soft tissue
techniques such as massage) for managing pain as part of a treatment package including exercises.
Orthotics: Consider neck collars for managing neck pain with or without radicular symptoms
Psychological therapy: Emotional and cognitive factors (eg, job dissatisfaction) should be
considered when addressing surgical or medical/interventional treatment for patients with cervical
radiculopathy from degenerative disorders
Pharmacological Treatment
For mild to moderate pain
A: ibuprofen (PO) 400mg stat then 200mg 8hourly
OR

388

C: diclofenac sodium (PO) 50mg 8hourly for 7-14days
OR
D: meloxicam (PO)7.5-15mg 12-24hourly for 7-14days
OR
For severe pain
A: diclofenac (IM) 75 mg 12 hourly by deep IM injection for 1-3 days +/-
B: tramadol (IM) 100mg 12hourly by deep IM injection for 1-3days
THEN
C: diclofenac (PO) 50mg 8hourly for 14days +/-
B: tramadol (PO) 50mg 8hourly for up to 14days.

Topical analgesics can be added in cases of severe pain,


A: diclofenac gel applies 12hourly
OR
S: ketoprofen gel apply 12hourly

Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of peptic
ulcers or when giving NSAIDs for a duration of 2 weeks or more

Proton pump inhibitors


A: omeprazole (PO) 20mg 24hourly for 2-4 weeks
OR
C: pantoprazole (PO) 40mg 24hourly for 2-4 weeks
OR
S: esomeprazole (PO) 40m24hourly for 2-4 weeks
OR
C: lansoprazole (PO) 30mg 24hourly for 2-4 weeks

For radicular symptoms add neuromodulators, neurovitamins and muscle relaxants:


Neuromodulator
D: Pregabalin (PO) 75-150mg24hourly for 4 weeks (dose can be escalated based on
individual response)
AND
Neurovitamins
C: Vit B1+B6+B12 (PO) once daily for 4 weeks
AND
Muscle relaxant
S: baclofen (PO) 5mg three times a day initially, increase by 5mg/dose each after 3days up
to-20 mg 8hourly for up to 2 weeks
• OR

S: tizanidine (PO) initially 2mg 8hourly, increase gradually to 4mg 24hourly every after 1-
4days, dose may be extended for 4weeks or more, to discontinue taper gradually; decrease
by 2-4mg daily

Invasive treatments for Dervical Degenerative Disease


Non-surgical interventions
Consider transforaminal epidural steroid injections for severe symptoms while developing
interventional or surgical plan of management.

Surgical interventions
• Spinal decompression: Surgical intervention is recommended for cervical myelopathy and
suggested for relief of symptoms of cervical radiculopathy from degenerative disorders.
• The surgical technique (minimal invasive v/s open) approach via anterior/posterior or
combined, and the appropriate implants required will be guided by patient factors,
availability of resources and expertise.

389

17.5.3 Pyogenic Spondylodiscitis
Spinal infections constitute an important clinical problem that often requires aggressive medical and
surgical management to avoid serious complications and long-term sequelae. Common causative
agents are S. aureaus, E. coli and Proteus spp.

Clinical presentation
• Back pain, • Extremities weakness,
• Fever, • Numbness,
• Muscle spasms • Paresthesias

Investigations
• CBC, ESR, CRP • CT-guided biopsy or a surgical
• Blood and urine cultures biopsy is advisable if diagnosis is
• Spine Xrays uncertain Spine MRI with contrast
• Radionuclide bone scan
Pharmacological treatment
The principles of conservative treatment include:
• accurate microbiological diagnosis and treatment with appropriate antibiotics
• Treatment should include analgesics, antibiotics, muscle relaxants, bed rest and external
spinal immobilization with spinal orthotics
• Monitor for clinical/radiographic evidence of spinal instability and neurological deterioration

Pain management

A: ibuprofen (PO) 400mg stat then 200mg 8hourly


OR
C: diclofenac sodium (PO) 50mg 8hourly
OR
D: Meloxicam (PO) 7.5-15mg 12-24hourly for 7-14days
OR
For severe pain
A: diclofenac (IM) 75mg 12hourly by deep IM injection for 1-3 days +/-
B: tramadol (IM) 100mg 12hourly by deep IM injection for 1-3days

THEN
A: diclofenac (PO) 50mg 8hourly for 14 days +/-
B: tramadol (PO) 50mg 8hourly for up to 14 days.

Topical analgesics can be added in cases of severe pain,


A: diclofenac gel apply 12hourly
OR
S: ketoprofen gel apply 12hourly

Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of peptic
ulcers or when giving NSAIDs for a duration of 2 weeks or more

Proton pump inhibitors


A: omeprazole (PO) 20mg 24hourly for 2-4weeks
OR
C: pantoprazole (PO) 40mg 24hourly for 2-4weeks
OR
S: esomeprazole (PO) 40mg 24hourly for 2-4weeks
OR
C: lansoprazole (PO) 30mg 24hourly for 2-4weeks

390

For radicular symptoms add neuromodulators, neurovitamins and muscle relaxants:
Neuromodulators
D: pregabalin (PO) 75-150mg 24hourly for 4 weeks (dose can be escalated based on
individual response)
AND
Neurovitamins
C: vit B1+B6+B12 (PO) 24hourly for 4 weeks

AND
Muscle relaxant
S: baclofen (PO) 5mg 8hourly initially, increase by 5mg/dose each after 3days up to 20 mg
8hourly for up to 2 weeks
OR
S: tizanidine (PO) initially 2 mg 8hourly, increase gradually to 4mg 24hourly after 1-4days,
dose may be extended for 4weeks or more, to discontinue taper gradually; decrease by 2-
4mg daily

Antibiotic treatment
B: ceftriaxone (IV) 2g 12hourly for 4-6 weeks
OR
C: amoxicillin+clavulanate (IV) 1.2g 12hourly
AND
B: metronidazole (IV) 500mg 8hourly for 4-6 weeks
(shift to organism specific drugs after C/S results)

Surgical management for extensive debridement of the disc and vertebral bodies, and subsequent
autologous bone grafting via a least disrupting approach to the stabilizing element is preferred in the
following situations
• Failure to respond to conservative therapy.
• Significant or progressive neurologic deficits
• Large paraspinal abscess with local mass effect or septic embolization
• Progressive spine deformity with or without incapacitating spinal pain

17.5.4: Tuberculous Spondylodiscitis


Tuberculous spondylodiscitis, also called Pott’s disease is a common form of spinal infection that left
untreated can result in serious complications and long-term sequelae.

Clinical presentation
• Back pain, • Extremities weakness,
• Fever, • Numbness, paresthesia
• Muscle spasms • Spine deformity
Investigations
• CBC, ESR, CRP • Spine Xrays
• serology for HIV • Spine CT scan
• Chest x-rays
CT-guided biopsy or a surgical biopsy is advisable if diagnosis is uncertainSpine MRI with contrast

Pharmacolological treatment
The principles of conservative treatment include:
• antituberculous treatment in accordance with current national TB treatment guidelines
• supportive treatment with analgesics, muscle relaxants, bed rest and external spinal
immobilization with spinal orthotics

Monitoring for clinical and radiographic evidence of spinal instability and neurological
deterioration.
A: ibuprofen (PO) 400mg stat then 200mg 8 hourly
OR
C: diclofenac sodium (PO) 50 mg 8hourly
OR
D: meloxicam (PO) 7.5-15mg 12-24hourly
OR

391

For severe pain
A: diclofenac (IM) 75 mg 12hourly by deep IM injection
OR
B: tramadol (IM) 100mg 12hourly by deep IM injection for 1-3days
THEN
B: tramadol (PO) 50mg 8hourly for up to 14days.

For radicular symptoms add neuromodulators, neurovitamins and muscle relaxants:


Neuromodulator
D: pregabalin (PO) 75-150mg 24hourly for 4 weeks (dose can be escalated based on
individual response)
AND
Neurovitamins
C: vit B1+B6+B12 (PO) once daily for 4 weeks
AND
Muscle relaxant
S: baclofen (PO) 10-20mg 8hourly for up to 2weeks
OR
S: tizanidine (PO) 2mg to 4mg 8hourly for up to 2weeks

Surgical management
Surgical management for extensive debridement of the disc and vertebral bodies, and subsequent
autologous bone grafting with or without instrumented spine stabilization via a least disrupting
approach to the stabilizing element is preferred in the following situations;
• Failure to respond to pharmacological therapy.
• Progressive neurologic deficits from compromised neural structures.
• Large paraspinal abscess with local mass effect or septic embolization Progressive spine
deformity

17.5.5: Osteoporotic Vertebral Compression Fractures (VCFs)


Osteoporotic fractures are common in the elderly and in particular post-menopausal women.
Vertebral compression fractures (VCFs) are among the most common types of osteoporotic
fractures. Other causes of VCFs include primary or metastatic vertebrae tumors and chronic steroid
usage.

Clinical presentation
• Severe back pain • Paresthesia
• Extremities weakness, • Muscle spasms, Spine deformity
• Numbness,

Investigations
• CBC, ESR, CRP
• Serum calcium levels
• Spine X-rays
• Spine CT scan
• Spine MRI with contrast
• Radionuclide bone scan

Non-pharmacological Treatment
Consider referral for image guided vertebral cement augmentation procedures in patients with poor
response to medical treatment and spinal support.
• Vertebroplasty
• kyphoplasty
Surgical management—spinal decompression and instrumented stabilization in
• Progressive neurologic deficits from compromised neural structures.
• Progressive spine deformity with disabling pain.

392

Physical and occupational therapy
• strengthening back muscle, balance training
• consider 3-5sessions of weight bearing exercises such’s walking or jogging with each
session lasting 45-60minutes
• also encourage aerobic low impact exercises such as walking and bicycling

General measures
Behavioral modification
Counsel on smoking cessations, and moderation of intake of alcohol, caffeine and encouraged to
engage in physical activities

Fall prevention
• installing handrails in bathroom, halls, stairways
• ensures hallways,stairwells and entrance are well lighted
• encourage patient to wear sturdy, low heeled shoes.
• Use of walking aid

Pharmacological Treatment
The principles of conservative treatment include:
• External spinal immobilization and supportive treatment with analgesics, muscle relaxants,
bisphosphonates and bed rest
• Monitor for clinical or radiographic evidence of spinal instability and neurological
deterioration.

For mild pain provide one of the following NSAIDS as 1st line treatment
A: ibuprofen (PO) 400mg stat then 200mg 8hourly
OR
C: diclofenac sodium (PO) 50mg 8hourly for 7-14days
OR
D: meloxicam (PO) 7.5-15mg 12-24hourly for 7-14days
OR
For severe pain
A: diclofenac (IM) 75 mg 12 hourly by deep IM injection for 1-3 days +/-
B: tramadol (IM) 100mg 12hourly by deep IM injection for 1-3days
THEN
A: diclofenac (PO) 50mg 8hourly for 14 days +/-
B: tramadol (PO) 50 mg 8 hourly for up to 14 days.

Topical analgesics can be added in cases of severe pain,


A: diclofenac gel applies 12hourly
OR
S: ketoprofen gel apply 12hourly

Note
Consider concomitant use of gastro protective treatment in patients with preexistent history of peptic
ulcers or when giving NSAIDs for a duration of 2 weeks or more

Proton pump inhibitors


A: omeprazole (PO) 20mg 24hourly for 2-4weeks
OR
C: pantoprazole (PO) 40mg 24hourly for 2-4weeks
OR
C: lansoprazole (PO) 30mg 24hourly for 2-4weeks
OR
S: esomeprazole (PO) 40mg 24hourly for 2-4weeks

393

For radicular symptoms add neuromodulators, neurovitamins and muscle relaxants:
Neuromodulators
D: pregabalin 75-150mg 24hourly for 4weeks (dose can be escalated based on individual
response)
AND
Neurovitamins
C: vit B1+B6+B12 (PO) 24hourly for 4weeks
AND
Muscle relaxant
S: baclofen 5mg 8hourly initially, increase by 5mg/dose each after 3days up to 20 mg
8hourly for up to 2 weeks
OR
S: tizanidine initially 2mg 8hourly, increase gradually to 4mg per day every 1-4days, dose
may be extended for 4weeks or more, to discontinue taper gradually; decrease by 2-4mg
daily

Calcium supplementation
B: Calcium 600mg + Vitamin D800IU (PO) 24hourly for 3 months then re evaluate
(1mcg of Vitamin D=40 international unit)

Bisphosphonate treatment – should be given for a period of five years.


S: ibandronate (IV) 3mg every 3months administered over 15-20minutes (treatment only)
for 5years

17.6: Common Congenital Anomalies of Musculoskeletal System


17:6:1 Talipes equinovarus (congenital clubfoot)
Talipes equinovarus is one of the most common musculoskeletal birth defect affecting approx.
1/1,000 live births. If untreated it causes long-term functional disability. The condition can vary in its
degree of severity ranging from quite mild to very severe. It may present with other defects such as
spina bifida, arthrogryposis, multiplex congenita, congenital myotonic dystrophy, or diastrophic
dysplasia.

Clinical presentation
Birth deformities of the foot with
• Small foot and calf • Varus (tight tendoachilles, tibialis
• Cavus (tight intrinsics muscles) posterior, tibialis anterior)
• Adductus of forefoot (tight tibialis • Equinus (tight tendoachilles)
posterior)
Diagnosis
• Most clinical diagnosis
• Plain X-ray

Management
Non operative management - Ponseti method of serial manipulation and casting,
The goal is to rotate foot laterally around a fixed talus, order of correction follows acronym (CAVE) 1.
Cavus 2. Adductus3.Varus4. Equinus. Heel cord tenotomy needed in at least 80-90% of children.
Followed by Foot abduction orthosis (FAO). Non noncompliance to FAO is the biggest risk factor for
deformity recurrence

Table 17:5: Ponseti Method


Month Weekly serial casting (with knee • First correct cavus with forefoot SUPINATED (NOT
1-4 in 90° of flexion ) with forefoot pronated) by aligning the less varus forefoot with the
supination, then forefoot more varus hindfoot (pronation would increase cavus
abduction deformity)
• Secondly correct adduction and heel varus by
rotating calcaneus and forefoot around talus (head of
talus acts as a fulcrum) into forefoot ABDUCTION

394

Tendon Achilles lengthening • Equinus correction last with tendon Achilles
(Tenotomy) (TAL) at week 8 tenotomy
required in > 80-90% • Perform when foot is at least 60° abducted, heel is
in valgus and equinus persists
• Cast in maximal dorsiflexion for 3 weeks after
tenotomy

Month Foot abduction orthosis (FAO) • With FAO holding affected feet at least 60°external
4-8 • 23 hours a day for 3 months rotation and 30° in normal foot for unilateral cases
after correction
• night time/nap time only until • Feet are measured prior to tenotomy so FAO is
age 4 years available on the day of post-tenotomy cast removal

2-4 Tibialis anterior tendon transfer • 30-50% will need TA transfer with or without repeat
years (TA transfer) at 2-5 yrs of age TAL or gastrocnemius recession for recurrent
(30-50% will require) deformity
• Indicated if the patient demonstrates supination
during gait

Operative management
I. posteromedial soft tissue release and tendon lengthening for children of <2years
II. medial column lengthening or lateral column-shortening osteotomy, or cuboid
decancellation indicated for children older than 2years
III. talectomy-n severe, rigid recurrent clubfoot in children between 6-10yeras or those
with arthrogryposis

Note
Surgical management are complemented by serial casting and foot adduction orthosis

17.7: Musculoskeletal Tumour


Musculoskeletal tumors are tumors that develop in muscles, bones and nerves Bone tumors are
divided into primary and secondary (metastatic) tumours. Primary tumours arise from cells which
constitute the bone and are divided into benign and malignant types. Metastatic type is most
common cause of bone cancer, the most common primary sites being renal, thyroid, lung, prostate,
and breast.

Clinical presentation
• Dull and aching pain which worsen at night is deemed a ‘red flag’ symptom
• Swelling where the tumor is located
• Pathological fracture
• Fever, weight loss, anemia and general body malaise are late symptoms

Note
For detailed clinical presentations, investigations and management of specific bone tumor refer to
malignancy chapter

17:8 Angular Deformity of Limbs


17.8.1 Rickets
Refers to softening and weakening of bones in children, usually due to inadequate vitamin D. Vitamin
D promotes the body’s absorption of calcium and phosphorus. Extreme or prolonged lack of vitamin
D makes it difficult to maintain proper calcium and phosphorus levels in bones, which can cause
rickets.
Clinical presentation
• delayed growth,
• bow legs,
• weakness and pain in the spine,
• pelvis and leg

395

Pharmacological Treatment
Treatment may involve adding vitamin D or calcium to the diet,

17.8.2 Physiological Bowing/Knocked Knees


Is considered bending of knees at an early age due to early walking and overweight below the age of
2years

Diagnosis process
I. Diagnosis is mainly by physical examination – obvious varus/valgus deformity and
metaphysical widening.
II. Blood tests to measure the levels of calcium and phosphate in the blood (Refer to table
17:3.)
III. Bone X-rays to check for bone deformities.

Treatment
• First consultation: rule out if it’s physiological – bow legs at young age before the age of 3
years without signs of rickets
• If it’s physiological then consider follow up every 6 months +/- vitamin d supplements
• At the age of 3 years if deformity more than 8degrees consider–hemiepiphysiodesis at
around the age of 3years if the deformity is due to Blount’s disease consider
hemiepiphysiodesis/corrective osteotomy.

Note
For details on specific surgical option kindly refer to standard orthopedic text books.

396

CHAPTER NINETEEN
METABOLIC AND ENDOCRINE DISEASE CONDITIONS

19.1 Diabetes Mellitus


Diabetes mellitus is a clinical syndrome characterized by persistently high blood glucose values due
to deficiency or diminished effectiveness of insulin.

Classification
Diabetes mellitus can be classified as follows:
• Type 1 Diabetes Mellitus (T1DM) – due to autoimmune β-cell destruction
• Type 2 Diabetes Mellitus (T2DM) – due to a progressive loss of β-cell insulin secretion
frequently with underlying insulin resistance
• Gestational Diabetes Mellitus (GDM) – diabetes diagnosed in the second or third trimester of
pregnancy that was not clearly overt diabetes prior to gestation
• Specific types of diabetes – due to other causes e.g., monogenic, diseases of the exocrine
pancreas and drugs or chemicals.

Diagnostic Criteria
• Main clinical features of diabetes are thirst, polydipsia, polyuria, tiredness, loss of weight,
blurring of vision.
• Many people have no classical symptoms and may only present late with the symptoms
related to complications e.g., pruritus vulvae and balanitis due to infections, paraesthesia or
pain in the limbs, non-healing ulcers, and recurrent bacterial infections.

WHO diagnostic Criteria 2006


• Fasting plasma glucose level ≥ 7.0 mmol/L (126 mg/dL)
• Plasma glucose≥ 11.1 mmol/L (200 mg/dL) two hours after a 75 g oral glucose load in a
glucose tolerance test
• Symptoms of hypogycaemia and casual plasma glucose ≥11.1 mmol/L (200 mg/dL)
• Glycatedhemoglobin (HbA1c) ≥ 6.5%.

Diagnosis of gestational diabetes (WHO criteria 2013)


• Fasting plasma glucose 5.1–6.9 mmol/l
• 2–hour plasma glucose 8.5–11.0 mmol/l following a 75g oral glucose load.

Note
Fasting plasma glucose higher than 6.9 mmol/l or 2–hour plasma glucose higher than
11.0
mmol/l are considered overt diabetes rather than GDM

At risk screening
Early diagnosis and good control reduce the risk of costly complications and reduces the
deterioration of islet function in T2DM. The following people should therefore be screened with
fasting blood glucose or HbA1c at least yearly when they visit health facilities:
• Those aged ≥40 years
• Children and adults <40 years who are overweight or obese and who have two or more
additional risk factors for diabetes
• Individuals with impaired glucose tolerance or impaired fasting glucose or a history of a
cardiovascular event
• People on long-term steroids or immunosuppressants
• Women with a history of gestational diabetes mellitus or polycystic ovary syndrome
• All pregnant women at the first antenatal visit if overweight, have had gestational diabetes,
babies with birth weight >4 kg, previous stillbirths or neonatal deaths. Screening should be
repeated in the second trimester if negative.
• All women during the 2nd or 3rd trimester (for gestational diabetes).

Impaired glucose tolerance


For people with glucose intolerance the risk of T2DM and its associated mortality may be reduced
by:

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• dietary modification (see chapter on Nutrition)


• physical activity (see chapter on Nutrition)
• weight reduction
• medication with metformin.

Goals of diabetes management


Table 19.1: Goals for Optimum Management Of Diabetes
Diet Advise same as for people without diabetes
Body mass index Therapeutic goal is 5–10% weight loss for people who are overweight or
obese, but aim for BMI<25 kg/m2

Waist circumference <102 cm for men, <88 cm for women


Physical activity At least 30 minutes of moderate physical activity on most days of the
week (total ≥150 minutes/week)

Cigarette consumption 0 per day


Alcohol consumption Not more than 2 standard unit drinks (20 g) per day for men and 1 unit
for women
Blood glucose level Non-pregnant: 4–6 mmol/L fasting; 6–8 mmol/L postprandial
Pregnant: ≤5.0 mmol/L fasting, ≤6.7 mmol/L postprandial
Self-monitoring of blood glucose is essential to improve outcomes

HbA1c Target ≤7% (6.5–7.5%). Should be measured every three months until
stable, thereafter at least twice a year

Lipids Total cholesterol: <5.2 mmol/L


HDL-C: ≥1.0 mmol/L
LDL-C: <2.6 mmol/L
Triglycerides: <1.7 mmol/L

Blood pressure Target ≤140/90 mmHg


For those with albuminuria/proteinuria <130/80 mmHg

Urine albumin Spot collection: <20 mg/L

Urine albumin-to-creatinine ratio (UACR): women: <3.5 mg/mmol; men:


<2.5 mg/mmol

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Algorithm for the Glycemic Management of T2DM

STEP 1: Sick-looking Yes Admit patient.


Lifestyle changes: Severe symptoms
Consider insulin
Diet, Infections
Physical activity,

No
Stop smoking, &
Stop/reduce alcohol Recommend Llifestyle change
Wait T hree Months Continue to
Glycaemic goal met? monitor
Yes
No

STEP 2: Is Metformin contraindicated?


Oral monotherapy
No

Sufonylurea or
Y es

Metformin
Sulfonylurea Metformin

Start with low dose;


increase monthly as needed to
Yes Continue to
glucose target or maximum dose
monitor
Glycaemic control met?
No

Add another class of oral agents


STEP 3:
Start with low dose and increase
Oral combination
monthly as needed to glucose target
therapy
or until maximum dose
Yes Continue to
SU+Biguanides monitor
Glycaemic control met?
No

STEP 4: Continue above


Oral therapy Add bedtime Intermediate-acting Insulin
PLUS Insulin Continue to
Wait three months
monitor
Glycaemic control met?
Yes
No

STEP 5:
Insulin therapy in
Refer to secondary or tertiary care for
a secondary or
more than once daily Insulin therapy:
tertiary service

Non-pharmacological Management
Healthy lifestyles
Dietary control
• Objectives:
o To meet requirements for growth and development, physical activity, and
maintenance of desirable body weight. Majority of people with T2DM are overweight
or obese and need to lose weight.
o Attain and maintain near normal blood glucose levels to prevent hypo- and
hyperglycaemia and so minimize the onset of chronic complications.
o Attain optimum blood lipids and blood pressure control and so reduce the risk of
macrovascular disease.
• Appropriate measures

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o Each meal should consist of a variety of foods from the core food groups
(vegetables, fruits, whole grains, meat and proteins, dairy products)
o Distribute foods evenly throughout the day with small/light meals in between the
three main meals.
• Food composition
o Protein: 15-20% of total energy (1g/kg/day)
o Energy from carbohydrates: 45-60% of total calories
ü Less than 100gms carbohydrates per day is not advisable as it
leads to ketosis
ü The distribution and amount of carbohydrates between meals
should be synchronized with the action of insulin and drugs.
ü Distribute the food over three meals with snacks in between rather
than 1 or 2 large meals
ü Give more of carbohydrate as complex starches e.g. whole grain
cereals, whole grain bread, roots and stem tubers, because they
breakdown more slowly to releaseglucose.
ü Avoid simple sugars, sugar-sweetened beverages and honey.
o Fats should provide < 30% ofenergy
ü A lower fat intake of up to 20% or less of the daily energy in case
of obese adult with diabetes.
o Limit salt to less than 1 teaspoonful/day
o Limit fat intake
• Physical activity
o Aerobic (e.g. brisk walking) and muscle strengthening activities improve glucose
tolerance, energy expenditure, feeling of wellbeing and mood, work capacity, improved
blood pressure, lipid profiles and increased functional mobility in older people.
o Adjust medicine dosages and or food intake to avoid hypoglycaemia.
• No smoking
• Avoid or limit alcohol intake to one drink/day for women, two drinks/day for men.

Pharmacological Treatment
Treatment with oral hypoglycemics
• Review the blood glucose at follow-up clinic and adjust medicines as needed until blood
glucose is controlled.
• If lifestyle measures on their own failure achieve blood glucose control or blood glucose
levels are persistently high (fasting >11 mmol/l or random >15 mmol/l) initiate:
67267
A: metformin (PO) 500mg 12hourly with or after meals. Increase, as required, until a
maximum of 2000mg in 2–3 divided doses.

If Metformin is contraindicated, then use


A: glibenclamide (PO) 2.5–10mg 12hourly
OR
C: glimepiride (PO) 1–4mg 12hourly
OR
A: gliclazide (PO) 40–160mg 12hourly

• If the maximum dose of metformin does not result in adequate glycaemic control, either one
of the above sulphonylureas may be added, starting with the lower dose and increasing until
control is achieved or the maximum dose is reached.
• If a combination of both medicines is still inadequate, then insulin should be added as
detailed below in the section on insulin.

Note
• Activity of sulphonylureas is prolonged in both hepatic and renal failure
• Metformin is contraindicated in those with severe renal, liver and cardiac failure.
• The lower dosage is appropriate when initiating treatment in elderly patients with
uncertain meal schedules, or in patients with mild hyperglycemia
• Sulphonylureas are best taken 15 to 30 minutes before meals

Treatment with Insulin Injection in Type 2 Diabetes


Insulin injections are indicated in T2DM in the following conditions:
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• Initial presentation with fasting blood glucose more than 15 mmol/l
• Presentation in hyperglycaemic emergency
• Peri-operative period especially major or emergency surgery
• Other medical conditions requiring tight glycaemic control
• Organ failure: Renal, liver, heart etc,
• Diabetes not well controlled with diet or oral drugs
• Latent autoimmune diabetes of adults (LADA)
• Contraindications to oral drugs

Note
The maximum glucose lowering efficacy of oral drugs is usually evident by six months.
Therefore, the efficacy of any added therapy must be assessed within six months and
an alternative drug instituted in case of failure

Insulin injections should be initiated by a doctor able to fully instruct the patient in its use but insulin
will be available at lower health facilities for management of stable patients who require
prescription refills.

Table 19.2: Types of Insulin as per WHO Essential Medicine List


Type of Insulin Name Basal or short acting
A: Insulin–short acting (human)
Short acting Short acting
soluble

Intermediate acting A: Insulin–intermediate acting (human) Basal

Pre-mixed insulin A: Intermediate and short acting Basal + Short acting


insulin (70/30)

Insulin as substitution therapy


Oral medicines are discontinued (except metformin if patient is obese)
S: Pre-mixed insulin is introduced at a dosage of 0.2 IU/kg body weight and this is split into:
⅔ in the morning and ⅓ in the evening
• Inject 30 minutes before the morning and the evening meals for human insulins
• Inject 0 to 15minutes before meal for analog insulins.

Insulin as supplemental therapy


Oral medicines are continued
A: neutral protamine hagedorn (isophane) insulin administered at night before 22:00h at a total
daily dose of 0.1–0.2 IU/kg body weight.
• The oral medicines are continued (half maximum dose of sulphonylureas and
metformin dose of 2 g/day)
• Blood glucose levels are monitored.

Self-monitoring in patients with T2DM


Self-Monitoring Blood Glucose (SMBG) is usually recommended in the following patients:
• patients on insulin and glucose lowering agents that can cause hypoglycaemia
(sulphonylureas)
• when monitoring hyperglycaemia arising from illness
• with pregnancy and pre-pregnancy planning
• when changes in treatment, lifestyle or other conditions requires data on glycaemic
patterns
• when HbA1c estimations are unreliable (eg haemoglobinopathies)

TYPE 1 Diabetes Mellitus (Childhood


diabetes) Non-pharmacological Treatment
• Nutrition (refer to nutrition chapter)
• Exercise requirements are as for children without diabetes
• Psychological support is important to cope with this chronic illness.

Pharmacological Treatment
Total dose of insulin contains soluble and intermediate/long-acting insulin.

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• Give total dose of insulin
o pre puberty 0.5 IU/kg/day subcutaneously for life
o puberty 1-2 IU/kg/day subcutaneously for life
o after puberty < 2 IU/kg/day subcutaneously for life
• Divide total insulin dose as per recommended percentage below

Table 19.3: Recommended Insulin Dosage


Time Type of insulin Proportion
Break-fast Short acting 30% of total daily dose
Lunch Short acting 20% of total daily dose
Supper Short acting 10% of total daily dose
Bedtime Long/intermediate acting 40% of total daily dose

Note
• Diabetes in children is often misdiagnosed as some other condition – e.g. as pneumonia or
asthma (laboured breathing),
• Insulin should be given for life and the dose adjusted according to weight and glucose response
• Self-glucose monitoring by glucometer at home 3-4times/day
• Pre-mixed insulins not advised in children

Clinical monitoring of people with diabetes

Table 19.4: Clinical Monitoring of People with Diabetes


Initial visit 3 Month visit Annual visit
History and diagnosis • Relevant history History and examination
Physical examination • Weight – as at initial visit
• Height and weight • Blood pressure
• Waist/Hip circumference • Foot inspection Biochemistry as at initial visit
• Blood pressure • Blood Glucose
• Detailed foot examination • Urine protein
• Tooth inspection • Education advice
• Eye examination • Nutrition advice
• Visual acuity+ Fundoscopy • Review therapy
• ECG • HbA1c every six
• Biochemistry months
o Blood sugar
o Glycosylated Haemoglobin
(HbA1c)
o Lipid profile (TC, HDC, LDLC,
TG)
o Serum creatinine
o Urine: glucose, ketones, protein
• Education
• Nutritional advice
• Medication if needed
TC=Total cholesterol, HDLC=high density lipoprotein, LDLC= low density lipoprotein, G=Triglycerides

Surgery in diabetes
General measures
Correct pre-operative management depends on type of surgery (major or minor), type of diabetes
and recent diabetes control.
• Surgery should be delayed if possible if HBA1C >9% or blood glucose fasting >10 mmol/l or
random glucose > 13 mmol/l.
• Screen for nephropathy, cardiac disease, retinopathy and neuropathy and inform surgical
team.

If diabetes is well controlled and surgery is minor:


• If on diet or oral agent therapy, omit therapy on morning of surgery and resume therapy
when eating normally
• For T1DM, continue with normal dose of insulin

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If on insulin therapy or poor glycaemic control or major surgery:
• Use continuous IV insulin infusion
• Start at 8 am and stop when eating normally.
• Monitor blood glucose before, during and after surgery: aim for blood glucose levels of 6–10
mmol/l.

For major surgery (glucose-insulin potassium regimen)


• Once snack is missed, start an IV regimen irrespective of the size of the procedure
• Maintain insulin administration (hourly) to avoid lipolysis and ketoacidosis in patients with
restricted oral intake and thus prevent DKA
• Administer 5% dextrose in maintenance IV fluids AND
• Short-acting insulin (16 Units) + KCl 10mmol/L added to 500mls of 10% dextrose.
o Infuse at 80ml/hr IV.
o If obese or initial blood glucose is high (>14mmo/l) consider higher dose of insulin (20
Units)
o If very thin or usual insulin dose is very low, consider lower dose (12 Units)
• Monitor blood glucose levels hourly (aim for 6–10 mmo/l)
o If blood glucose is low or falling reduce dose by 4 Units
o If blood glucose is high or raising increase dose by 4 Units
• Patients receiving Multiple Daily Insulin Therapy (MDIT) should receive preoperative basal
insulin dose without interruption in the perioperative period. When oral intake is restricted,
regular insulin may be given every 4–6 hrs to control hyperglycemia. When a diet is
tolerated, the MDIT regimen should be resumed
• Post operatively: give 5–10% dextrose IV 1 litre + KCl 20ml + 2/3 of total daily dose of
insulin over 8hrs and repeat until able to take orally. Continue the infusion until 60 minutes
after the first meal.
• Resume usual therapy after first meal
• Check electrolytes daily.

19.2 Management of Diabetes During Religious Fasting


There are several types of fasting:
• Normal fast (the common fast): the person abstains from all foods but can take water for a
limited time.
• Total fast = total abstinence from both food and water. This should not go beyond a
maximum of three days and is not recommended for those people taking insulin
secretagogues or insulin.
• Partial fast = abstain from selected foods and drinks, or omit a certain meal each of the
fasting days.

Those with very poor glucose control should be discouraged from fasting
• A total fast is not recommended for anyone with diabetes. Adequate hydration is important
even during the period of fasting.
• For those on insulin, a partial fast is preferred to total or normal forms of fasting.
• Self-blood glucose monitoring is mandatory for people with diabetes who elect to fast.
o Once-a-day is adequate for patients on diet only or diet with metformin.
o At least 3 times a day in patients on insulin secretagogues
o More frequently if hyperglycaemia is marked and the urine tested for ketones.
• Consider terminating the fast if frequent hypoglycaemia or intercurrent infections.
• Vigorous activity should be avoided during period of fast.
• Ensure ready access to a healthcare provider during the period of fast.

Management of normal fasting for people treated with oral hypoglycaemic agents
• Fasting is possible in this situation.
• Usual dietary advice should be followed at this time.
• Patients on metformin, alpha-glucosidase inhibitors and thiazolidinediones (glitazones) can
continue taking the usual doses at the usual times.
• If on a second or third generation sulphonylurea (glibenclamide, gliclazide, glipizide,
glimepiride), this should be taken at the time of breaking the fast and not before dawn.

403
Management of normal fasting for T2DM patients on insulin
• If on once daily insulin before bed, this can be given as usual
• If on twice daily short- and intermediate-acting insulin:
o Before the dawn meal, give the usual evening dose of short-acting insulin without any
intermediate-acting insulin.
o Before the evening meal give the usual morning dose of short-acting and
intermediate-acting insulin.
• If on basal bolus regimen:
o Usual doses of the short-acting insulin can be given before the dawn and evening
meals, and usual doses of the intermediate-acting insulin can still be given at 10pm.
o Regular SBGM is essential to ensure prevention of hypoglycaemia
o Titration of doses should occur according to SBGM results.
• Neither the insulin injection nor the breaking of the skin for SBGM will break the fast.

Management of other fasting types


Table 19.4: Types of Fasting and Recommended Diabetic Treatment
Fasting regimen When to take antidiabetic
Treatment regimen
agents
Diet only Total, normal of partial fast Not applicable
Metformin, Thiazolidinediones Normal or partial fast With meals
Insulin secretagogues Partial fast Before meals
Sulphonylureas
Daily intermediate or long-acting Partial fast Before first meal
insulin
Multiple insulin doses using Avoid fasting Not applicable
intermediate and short acting insulin
Long-acting plus bolus fast acting Avoid fasting or partial fast Lantus am and analogue
insulin with meals

19.3 Hyperglycaemia in Pregnancy


Gestational Diabetes Mellitus (GDM) is any degree of glucose intolerance first recognized in
pregnancy. Diabetes in pregnancy refers to those with pre-existing diabetes, whether diagnosed or
not.

Screening at first antenatal visit


• Perform screening in all women at the first antenatal clinic attendance if they have:

o BMI > 25 kg/m2 o known impaired glucose


o previous history of GDM tolerance/impaired fasting
o previous big baby glucose.
o poor obstetric history o grand multipara
o family history of DM o glycosuria.

• Women in early pregnancy with levels of HbA1c≥6.5% or blood glucose levels fasting ≥7.0
mmol/l or two hours ≥11.1 mmol/l which are diagnostic of diabetes should be treated as
having pre-existing diabetes.
• Women with HbA1c 6.0–6.4%, fasting glucose 5.1– 6.9 mmol/l or two-hour glucose 8.6–11.0
mmol/l should be assessed to determine the need for immediate home glucose monitoring
and, if the diagnosis remains unclear, assessed for gestational diabetes by 75 g oral glucose
tolerance test (OGTT) at 24–28 weeks.

Screening later in Pregnancy


• All women with risk factors (see above) should have a 75 g OGTT at 24–28 weeks
• A fasting plasma glucose at 24–28 weeks is recommended in low-risk women

Non-pharmacological Treatments
• All women intending to become pregnant should:

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o Be encouraged to achieve excellent glycaemic control using glucose monitoring of both
fasting and postprandial values
o Be prescribed high-dose (5mg) pre-pregnancy folate supplementation, continuing up to
12 weeks’ gestation
o Have an eye exam and be informed of the risk of developing and/or progression of
diabetic retinopathy
o Have a kidney assessment (random urine albumin/creatinine ratio and serum
creatinine) and referred if urine protein ≥ 1g.
• A combined health-care team (obstetrician, diabetologist or internist, diabetes educator,
pediatrician/neonatologist) is required.
• Review SMBG, blood pressure and urine protein and ketones by dipstick at each visit and
eye examination in each trimester.
• Target glycaemia:
o Preprandial blood glucose 3.5–5.5mmol/L
o Postprandial blood glucose 5–7.5mmol/L
• Lifestyle management is the preferred means of managing gestational diabetes.
o Diet is based on the principles of optimal nutrition and controlled weight gain.
o Exercise can be helpful in lowering BG levels: the most acceptable form of exercise for
most women is walking in their normal daily routine.
• Glucose-lowering therapy should be considered in addition to diet where fasting or two
hours glucose levels are above target, for example, where two or more values per fortnight
are:
o fasting or preprandial ≥5.5 mmol/L, or two hours postprandial ≥7 mmol/L at ≤35 weeks
o fasting or preprandial ≥5.5 mmol/L, or two hours postrandial ≥8 mmol/L at >35 weeks
o any postprandial values are >9 mmol/L.
• When pharmacologic treatment of gestational diabetes is indicated, insulin and oral
medications are equivalent in efficacy, and either can be an appropriate first-line therapy.

Pharmacological Treatment
A: metformin 500 mg 12hourly, maximum 2000mg in 2–3 doses
OR
A: glibenclamide 2.5mg 24hourly to a maximum of 10mg daily

Note
Oral hypoglycaemics (except for metformin and glibenclamide) are contraindicated in pregnancy

Insulin
The rapid-acting insulin analogs (lispro and aspart) lower postprandial blood glucose and decrease
the risk of nocturnal hypoglycemia. Patients on lispro and aspart prior to conception may continue
them during pregnancy. Patients on regular insulin may be switched to lispro or aspart if 1–hour
postprandial blood glucose levels are above target and/or the patient is also experiencing pre-meal
or nocturnal hypoglycemia.

Postnatal Follow Up
• Women with gestational diabetes should be screened at 6–12 weeks postnatal to ensure
return to normal glucose tolerance. Thereafter, a 1–2 yearly follow up is recommended.
• Metformin and glibenclamide may be used even if a woman is breastfeeding. Encourage
women to breastfeed.
• If retinopathy, check eyes 1 year postpartum

19.4 Diabetes and HIV


The management of people with both diabetes and HIV need to consider the following:
• ARVs are associated with increased metabolic dysfunction, including insulin resistance,
dyslipidemia and lipodystrophy
• Protease inhibitors (PIs) increase insulin resistance and reduce insulin secretion by
interfering with GLUT–4 mediated glucose transport
• Standards of treatment and management of diabetes for patients with HIV are generally the
same as those for diabetic patients without HIV and patients who acquire HIV may continue
to be managed with the same drug therapy as before

405
• Sulfonylureas may not be effective in the face of severe insulin resistance. In case glycemic
control deteriorates, insulin should be initiated, rather than increasing dosage or number of
oral medications
• People who are on ARTs need to be screened for diabetes at least once a year and
especially if they have other CVD risk factors

19.5 Diabetes and Tuberculosis


Diabetes and tuberculosis are interlinked as follows:
• People attending TB clinics should be screened for diabetes and those attending diabetes
clinics should be screened for TB if presenting with symptoms.
• Diabetes may be associated with delayed sputum conversion (>60 days), higher probability
of tuberculosis treatment failure, higher recurrence and relapse rates, higher overall
mortality, higher rates of multi-drug resistance TB and more atypical presentation in
hyperosmolar hyperglycemic nonketotic coma or ketoacidosis
• For both conditions, controlling blood sugar, being more physically active, avoiding chronic
stress, getting enough sleep and maintaining ideal weight are recommended.

Review Drug Requirements


• Rifampicin is a potent hepatic enzyme-inducing agent, accelerates the metabolism of oral
hypoglycemic agents and shortens the plasma half-life of sulphonylureas
• Isoniazid antagonizes sulphonylureas, impairs insulin release and action and leads to
increased requirement of insulin and oral antidiabetic medication
• Therefore, people with diabetes may require an increase in dosage of antidiabetic
medication if they develop tuberculosis.

Use Oral Antidiabetic Medicines Carefully in Tuberculosis


• People with diabetes mellitus and tuberculosis should be treated with insulin injection, or in
case a diabetic with tuberculosis is on oral hypoglycemic agents, it may be necessary to
switch to insulin.
• Tuberculosis affects both the liver and pancreas: oral antidiabetic drugs are contraindicated
in hepatic disease, which is a common adverse effect of antituberculous therapy.
• Metformin produces weight loss, particularly in high doses, and it is also an anorectic.
• Marked weight loss and higher insulin and caloric needs in tuberculosis are other important
indications for reviewing oral antidiabetic therapy in diabetes mellitus.

19.6 Hypoglycaemia
Hypoglycaemia is defined as blood glucose <3.9mmol/L.

Diagnostic Criteria
• Hunger • Numbness around the lips and fingers
• Sweating • Headache
• Trembling or shaking • Confusion
• Anxiety • Lack of concentration
• Dizziness • Weakness
• Lightheadedness • Changes in behaviour (e.g. irritability,
• Palpitation tearfulness, crying), paraesthesiae.

Patients may also present with convulsions, seizures or coma due to delayed corrective action or
impaired hypoglycaemia awareness where the patient loses the ability to detect the early
symptoms of hypoglycaemia due to repeated episodes of mild hypoglycaemia or long duration of
diabetes leading to loss of adrenergic and glucagon response, with eventual loss of adrenergic and
neuroglycopaenic symptoms.

Non-pharmacological
Treatment for conscious Patients:
Quickly take a glass of a sugar-rich drink
OR
Eat one table spoon of sugar or honey
AND
Have a meal.
406
If symptoms persist after 5 minutes repeat the above.

Treatment for unconscious Patients:


C: 50% dextrose (IV) (40–50ml)
OR
C: 10% dextrose (IV) (200–300ml).
• Repeat if patient is not responsive or if after 15 minutes, the blood glucose is
still below 4mmol/l.
• Follow by 8–10 % glucose infusion. Use 5% dextrose if the higher
concentrations are not available.
OR
S: glucagon (IM or SC) 1mg stat

Note
If IV access is impossible, consider nasogastric tube or rectal glucose

On Recovery
• Give long-acting carbohydrate snack e.g. a piece of bread
• Identify the cause of hypoglycaemia and correct it
• If hypoglyceamia is a result of long acting suphonylureas, long- or intermediate acting insulin or
alcohol, frequently monitor blood glucose (2hourly) and give IV dextrose infusion (5–10%) for 12–
24 hours
• If patient is not responding look for another cause or refer.

19.7 Diabetic Ketoacidosis and Hyperosmolar Hyperglycemic States


These are acute metabolic complications of diabetes mellitus that may lead to severe dehydration,
altered level of consciousness and electrolyte imbalance. The presence of acidosis, ketonemia and
ketonuria in diabetic ketoacidosis (DKA) differentiates it from hyperglycemic hyperosmolar state
(HHS).

Symptoms
• Nausea/vomiting • Abdominal pain
• Shortness of breath • Fever
• Obtundation/drowsiness • Altered mental function
• Thirst/polyuria • Dehydration
• Fruity smellingbreath • Lethargy
• Confusion • Coma

Note
• When you suspect DKA, confirm diagnosis immediately
• All patients minimum should be admitted in hospital for intensive management

Table: 19.5: Diagnostic Criteria for DKA and HHS


Parameter Mild DKA Moderate DKA Severe DKA HHS
Blood Glucose >13.9 >13.9 >13.9 >30
Arterial PH 7.25-7.3 7.00-7.24 <7.00 >7.30
Serum bicarbonate 15-18 10-15 <10 >18
Urine ketones Positive Positive Positive Small
Serum ketones Positive Positive Positive Small
Serum osmolality Variable Variable Variable >320
Alteration in sensorium Alert Alert/drowsy Stupor/coma Stupor/coma

Investigations
Apart from the ones in the table above, check serum electrolytes, urea and creatinine.

DKA and HHS Treatment


Treatment of DKA and HHS is similar.
• Frequent monitoring of patients
• Improvement of circulatory volume and tissue perfusion

407
• Replacement of electrolyte losses (potassium)
• Administration of insulin
• Careful search and management of the precipitating causes
With proper treatment, the average time to resolution is between 10–18 hours for DKA and ~9–11
hours for HHS.

I. Fluid management protocol


• The first step - infusion of isotonic saline to expand extracellular volume and stabilize
cardiovascular status. Fluid replacement alone results in:
o Improvement of hyperglycemia, reduce insulin resistance
o lowering the plasma osmolality,
o reducing vasoconstriction and improving perfusion,
o restores renal perfusion
o Reduce insulin resistance by ↓ stress/counterregulatory hormone levels
• Both DKA and HHS patients have severe volume depletion -- estimated water deficit of
100mls/kg body weight
• Usual initial fluid → isotonic saline (0.9% NaCl)
• Optimal rate of fluid infusion depends on the clinical state of the patient. On average
15 to 20 ml/kg/hour (about 1000 ml/hour) max. <50ml/kg in the first four hours.

For children
o Detailed management of DKA is presented in the alogarithm for management of
paediatric diabetic ketoacidosis in low resource centre below.
o Give NS or RL for 48 hours
o Fluid Requirements = DEFICIT + 48 hours’ maintenance

Table: 19.6: Maintenance Fluid


Age Weight Maintenance fluid
(years) (kg) (ml/kg/hr)
<1 3-9 80
1-5 10-19 70
6-9 20-29 60
10-14 30-50 50
>15 >50 30

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Management of Diabetic Ketoacidosis in Low Resource Centre

Shock Dehydration 5-10% Dehydration <5%


Reduced conscious level Clinically acidotic Clinically well
Coma Vomiting Tolerating fluids

IV THERAPY THERAPY
Follow ABC concept
Correct over 48hrs by 0.9% NS Start with SC Insulin
Give IV Fluids
Add 20mmol KL in every 500mls Oral fluids e.g. ORS
Give 0.1IU/kg/hr as an infisuion

No Improvement No Improvement
OBSERVATION
Blood glucose 1-2 hourly
Neurological status 1hourly Neurological deterioration
Fluid input/output Reduced conscious level
Serum electrolytes 2hrs after starting IV Irritability
Reevaluate therapy then 4-6 hourly Signs of raised ICP
Fluid balance + IV therapy Headache
If acidosis manage Slowing heart rate
Check insulin dose and correct
Consider sepsis Blood glucose <14

Exclude hypoglycaemia
Change NS to 5% dextrose Possible cerebral oedema
Monitoring
INSULIN
Maintenance dose of insulin
Child who was on insulin can IMPROVEMENT MANAGEMENT
resume normal dose before DKA Clinically well Give manitol 0.1g/kg
Newly diagnosed start insulin as Drinking and tolerating food Transfer to ICU
shown in table Urine ketones may still be positive CT Scan when stable

II. Electrolyte management protocol


Almost all patients with DKA or HHS have a substantial potassium deficit.
• Acidosis –shift to extracellular
• Urinary losses related to the glucose osmotic diuresis
• Secondary hyperaldosteronism.
• Loss is high 3-10mEq/kg

Despite total body potassium deficit, concentration is usually normal or elevated due to
• insulin deficiency and hyperosmolality
• both result in potassium movement out of the cells
• Insulin treatment reverse distribution

Good approach checks ECG for signs of hyperkalemia (peaked T wave, QRS widening)
• Give KCL if signs absent and if K <5.3
• If Patient oliguric give KCL when K <4 or ECG signs of hypokalemia (U wave)

Table 19.7: Potassium Repletion in DKA and HHS


K+>5.2 mEq/L Do not give K+ initially, but check serum K+ with basic metabolic profile every
2h
K+<3.3 mEq/L Hold insulin and give K+ 20-30 mEq/hr until K+>3.3 mEq/L
K+ = 3.3-5.2 mEq/L Give 20-30 mEq K+ in each L of IV fluid to maintain serum K+ 4-5 mEq/L

Delay insulin treatment until the serum potassium is above 3.3 mEq/L
• insulin Rx worsen hypokalemia by driving potassium into the cells.
• To avoid possible arrhythmias, cardiac arrest, and respiratory muscle weakness

409
III. Insulin therapy management protocol
Continuous IV infusion of regular insulin is the treatment of choice
• Correct hypovolemic shock and hypokalemia if present, before starting insulin
• Low dose IV insulin for both DKA and HHS
• Serum potassium <3.3 mEq/L only contraindication for insulin
IV regular/Soluble insulin and rapid-acting insulin analogs are equally effective

Insulin therapy
• Lowers serum glucose concentration (↓ hepatic glucose production>> ↑ peripheral utilization)
• Diminishes ketone production (reducing both lipolysis and glucagon secretion)
• Augment ketone utilization.

Conventional Insulin Guidelines


Both HHS and moderate to severe DKA
• IV bolus of regular insulin (0.1 U/kg body weight) followed within 5 minutes by a continuous
infusion of regular insulin of 0.1 U/Kg/hour = 7 U/hour in a 70 kg patient
• Alternatively, omit bolus dose →continuous IV infusion of regular insulin at a rate of 0.14 U/kg
per hour (equivalent to 10 U/hour in a 70 kg patient)
o But bolus insulin is a priming dose, saturates insulin receptors full before continuous
insulin
o Avoid lag time in achieving steady state insulin levels
ü In practice -100iu in 100mls of NS titrate in 5-7cc/h in the first 24hours
ü Or 60iu in 60mls of NS titrate 6-7cc/hour in 24hours
• Insulin dosing same in DKA and HHS
• If plasma glucose does not decrease by 2.8-4.2mmol/l in the first hour, increase the infusion
rate of insulin by 50% to 100%
• Optimal rate of glucose declines 5.5mmol/l/hour
• Glucose drop not allowed to less than 14mmol/l during first 4-5hrs of treatment.
• It takes 12-24 hours to clear ketones from circulation after hyperglycemia is controlled
19.8 Diabetes and Cardiovascular Diseases
Diabetic patients are 2–4 times likely to develop cardiovascular diseases mainly due to
atherosclerosis and hypertension.
The clinical spectrum of cardiovascular diseases includes:
• Coronary heart disease
• Angina (which may be silent)
• Acute coronary artery syndrome
• Congestive cardiac failure
• Sudden death
• Cerebral vascular accident (stroke, transient ischaemic attacks and dementia)
• Peripheral vascular disease (intermittent claudication, foot ulcer and gangrene).

Assessment (annual)
• ECG, Chest X-Ray, if with symptoms/signs of heart failure.
• Peripheral vascular disease evaluation includes doppler and angiography of lower limbs.

Pharmacological Treatment
Acute coronary syndrome
All adults with T2DM and recent acute coronary syndrome and/or coronary stent should receive dual
anti-platelet therapy for 12 months after the event or procedure:
A: acetyl salicylic acid (PO) 75–100mg 24hourly
AND
D: clopidogrel (PO) 75mg 24hourly

Note
• acetyl salicylic acid is also indicated for primary prevention for people with T2DM >40years with
family history of ischaemic heart disease (IHD), cigarette smoking, obesity, proteinuria, or
dyslipidemia.
• It is contraindicated in peptic/duodenal ulcer, dyspepsia, heartburn, malignant hypertension,
haemorrhagic stroke.

410
Hyperlipidaemia
Statin therapy results in a significant decrease in CVD morbidity and mortality in T2DM and are
indicated in Type 2 diabetics > 40 years of age, or diabetes for > 10years
B: atorvastatin (PO) 10mg 24hourly. Dose may be increased to 80mg daily if required.
OR
S: rosuvastatin (PO) 10mg 24hourly. Dose may be increased to 40mg daily if required

Fenofibrate reduces incidence of retinopathy and need for laser surgery, peripheral neuropathy, and
improvement in proteinuria, suggesting a more generalized effect on microvascular disease
independent of dyslipidaemia.

• Fibrates:
o Should be used in mixed hyperlipidemias which have not responded adequately to diet
or other therapy.
o Are more effective in lowering triglycerides and increasing HDL, but less effective in
lowering cholesterol.
o Should be used with caution in combination with statins.
o Can enhance the effects of warfarin and antidiabetic agents
o Are contraindicated in patients taking Orlistat.
D: fenofibrate (PO) 67–267mg 24hourly

Hypertension
In people with T2DM, antihypertensive therapy with an angiotensin receptor blockers (ARB) or
angiotensin-converting enzyme inhibitors (ACEI) decreases the rate of progression of albuminuria,
promotes regression to normal albuminuria and may reduce the risk of decline in renal function.
Therefore:
• BP-lowering therapy in people with diabetes should preferentially include an angiotensin
converting enzyme inhibitor (ACEI) or angiotensin receptor blocker (ARB) e.g.
C: enalapril (PO) 10 – 40mg 24hourly, taken either as a single dose or two divided doses
(enalapril (PO) 5 mg–10mg 12hourly)
OR
C: losartan (PO) initial dose 50mg stat. Maintenance dose; losartan (PO) 25–100mg
24 hourly in single or 2 divided doses.

• The target level for optimum BP is controversial. It is reasonable to target BP levels of


<140/90 mmHg for people with diabetes, with lower targets for younger people and those at
high risk of stroke. The target BP for people with diabetes and microalbuminuria or
proteinuria remains <130/80 mmHg.
• Combining an ARB and an ACEI is not recommended.
• If monotherapy does not sufficiently reduce blood pressure add one of the following:
C: amlodipine (PO) 5–10mg 24hourly
OR
A: bendrofluazide (PO) 5mg 24hourly
• ACE-inhibitors and ARBs should be stopped pre-conception. Diltiazem (PO) 60mg 24hourly
may be a useful substitute.

19.9 Diabetic Peripheral Neuropathy


All patients should be screened for distal symmetric polyneuropathy starting at diagnosis of T2DM
and at least annually thereafter.

Diagnostic Criteria
• Unsteady gait
• Burning, aching pain or tenderness in legs or feet (occurring at rest or at night, not related to
exercise)
• Prickling sensations in legs and feet (occurring at rest or at night, distal>proximal, stocking
glove distribution)
• Numbness in legs or feet (distal>proximal, stocking glove distribution)
• History of previous foot ulceration and/or amputation.

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Investigations Test for:
• Sensation (10g monofilament or cotton wool)
• Vibration (128Hz tuning fork)
• Postural hypotension and pulse (tibial and dorsalis)
• Inspect foot for structural abnormalities and ulceration.

Pharmacological Treatment
It is difficult to treat. Some of the drugs used include:
D: pregabalin (PO) 75-150mg (24hourly–12hourly) for 4weeks

Tricyclic antidepressants may help


A: amitriptyline (PO) 25-75mg 24hourly
OR
C: imipramine (PO) 100mg 24hourly

Gastroparesis
Due to autonomic neuropathy
C: metoclopramide (PO) 10mg 8hourly
OR
D: domperidone (PO) 10mg 8hourly

Diabetic Foot:
Give foot care education and advice on appropriate footwear.

19.10 Diabetic Nephropathy


It is one of the most important causes of chronic renal failure. Persistent microalbuminuria is both a
marker for the development of overt nephropathy and cardiovascular risk. Patients with
microalbuminuria who progress to macroalbuminuria (>300 mg/24 h.) are likely to progress to end–
stage renal disease over a period of years. Patients with diabetes and chronic kidney disease (CKD)
should be treated with a comprehensive strategy to reduce risks of kidney disease progression and
cardiovascular disease.

Non-pharmacological Treatment
Patients with diabetes and CKD should be advised to:
Intensify management of modifiable risk factors:
• Stop smoking.
• Treat urinary infection aggressively.
• Avoid drugs toxic to the kidney.
• Consume an individualized diet high in vegetables, fruits, whole grains, fiber, legumes, plant-
based proteins, unsaturated fats, and nuts; and lower in processed meats, refined
carbohydrates, and sweetened beverages
• Undertake moderate-intensity physical activity for a cumulative duration of at least 150
minutes per week, or to a level compatible with their cardiovascular and physical tolerance

Pharmacological Treatment
• Renin–angiotensin system (RAS) inhibition is recommended for patients with albuminuria and
hypertension
• Most patients with T2D, CKD, and eGFR => 30 ml/min per 1.73 m2 would benefit from
treatment with both metformin and an SGLT2i.
• Patient preferences, comorbidities, eGFR, and cost should guide selection of additional drugs
to manage glycemia, when needed, with glucagon-like peptide-1 receptor agonist (GLP-1 RA)
generally preferred.
A: metformin (PO) 500mg or 850mg (12hourly – 24 hourly); usual maintenance dose: 1g
twice daily

SGLT-2 Inhibitors
S: empagliflozin (PO) 10–25mg 24hourly

• Advise contraception in women who are receiving ACEI or ARB therapy and discontinue
these agents in women who are considering pregnancy or who become pregnant.

412
• Monitor serum creatinine and potassium annually and more frequently if there is evidence of
renal impairment.
• Hyperkalaemia associated with the use of an ACEI or ARB can often be managed by
measures to reduce serum potassium levels rather than decreasing the dose or stopping the
ACEI or ARB immediately
o Avoid potassium-containing salt substitute or food products containing the salt substitute.
o Avoid drugs that can impair kidney excretion of potassium: over-the-counter nonsteroidal
anti-inflammatory drugs, supplements, and herbal treatments
o Avoid constipation by ensuring enough fluid intake and exercise.
o Consider diuretics treatment to enhance the excretion of potassium in the kidneys
especially when there is concomitant volume overload or hypertension.
o Consider oral sodium bicarbonate especially in patients with CKD and metabolic
acidosis.
• Metformin should not be used once the serum creatinine is > 200µmol/l.
• Treat blood pressure aggressively with target of <130/80 mmHg.
• Add diuretics if necessary (but in large doses inhibit insulin release).

19.11 Diabetic Retinopathy


It is one of the major causes of blindness. Poor glycaemic control, nephropathy, hypertension and
pregnancy, long duration of diabetes are among the risk factors. It is preventable and its progression
retarded by improved glycaemic control and blood pressure. Screening for early detection and laser
therapy can prevent blindness.

Screening for Diabetic Retinopathy


For all people with diabetes, yearly screening is necessary for early detection of ocular complications.
The screening should begin:
• Comprehensive eye examination in woman planning pregnancy, and during the first trimester,
preferably at booking of antenatal clinic (ANC). Further screening should be determined by
the degree of retinopathy detected at the initial appointment.
• Five years after the diagnosis of diabetes for individuals with Type 1 diabetes diagnosed after
puberty (around 14years).
• At puberty for individuals diagnosed with type 1 diabetes before puberty
• At the time of diagnosis of diabetes for individuals with type 2 diabetes
For each of the scheduled screening visits, detailed patient’s assessment should include a complete
ophthalmic examination in the following steps:
a. Take visual acuity (VA) without and with spectacles
b. If VA less than 6/9 take VA with pin hole
c. Dilate the pupil by using the mydriatic agents (Tropicamide)
d. Identify presence of cataract or other causes of media opacification.
e. Perform retinal evaluation by direct or indirect Ophthalmoscope or Fundus Photography
f. Identify retinal changes, document and if applicable grade the diabetic retinopathy and
maculopathy as shown in Table XX.
g. Explain the results of screening to the patient and schedule rescreening (Table XX).

Table 19.8:Grading of Diabetic Retinopathy for Screening at Community/ Diabetic Clinic:


Features and Outcome
Grade Features Outcome/action
R0 No disease Rescreen in12 months
R1 Mild background DR Including: micro-aneurysms, flame exudates, Rescreen in12months
>4 blot haemorrhages in one or both hemifields and/or cotton wool
spots
R2 Moderate background DR: >4blot haemorrhages in one Rescreen in 6months
hemifield
R3 Severe non-proliferative or pre proliferative DR: >4 blot Refer to Eye Clinic
haemorrhages in both hemi fields, intra-retinal microvascular
anomalies (IRMA),venous bleeding
R4 Proliferative retinopathy, Neovascularization of the Disc (NVD), Refer to Eye Clinic
Neovascularization Elsewhere (NVE), vitreous haemorrhage, retinal
detachment
M0 No macular findings Rescreen in 12months
M1 Hard exudates within 1–2 disc diameters of fovea Rescreen in 6 months

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M2 Blot haemorrhage or hard exudates within 1disc diameter of fovea Refer to Eye Clinic
P0 Photocoagulation Laser: Absent Refer to Eye Clinic
P1 Photocoagulation Absent/Present (Any PRP or evidence of Grid Refer to Eye Clinic
Laser
U Unclassifiable (When there is Cataract, small Pupil, Vitreous Refer to Eye Clinic
Haemorrage, Tractional Retinal Detachment or Corneal Opacity
KEY: R=Retinopathy; M=Maculopathy; P=Photocoagulation, U=Unclassified

At all times, remind patients to stop smoking and intensify blood pressure, lipids and glycaemic
control.

19.12 Thyroid Disorders


Thyroid disorders are conditions that affect the thyroid gland. There are specific kinds of thyroid
disorders that includes hypothyroidism, hyperthyroidism, goiter, thyroid nodules and thyroid
cancer.

19.12.1 Hypothyroidism
Hypothyroidism is a condition in which a person's thyroid hormone production is below normal.
Common causes of the disease are chronic autoimmune thyroiditis, post-surgery and post
radioactive iodine.

Diagnostic criteria
The symptoms depend on the deficiency of thyroid hormone, but can include:
• Increased cholesterol levels, • Memory loss
• Depression • Dry, rough skin
• Fatigue • Constipation
• Hair loss • Hoarse voice

Investigation
A blood test is used to confirm hypothyroidism

Indications for Treatment


• TSH level persistently >10mU/L; treat all patients due to, increased likelihood of progression
to overt disease and a higher risk of congestive heart failure, cardiovascular disease and
mortality.
• TSH levels (4.5–10mU/L); consider, treatment in patients younger than 65 with increased
cardiovascular risk (e.g., previous cardiovascular disease, hypertension, documented
diastolic dysfunction, atherosclerotic risk factors (dyslipidaemia, diabetes mellitus, smoker),
goitre, positive antithyroid peroxidase antibodies, evidence of autoimmune thyroiditis by
ultrasound, pregnancy, or infertility), particularly when TSH level is persistently >7mU/L.
• Levothyroxine therapy could be considered also for symptomatic middle-aged patients for a
short period of time. If a clear beneficial effect is observed, levothyroxine therapy could be
maintained.
• Persistently mildly increased TSH levels (>4.5–10mU/L) with positive Thyroid Antibody and
thyroid sonographic findings typical of autoimmune thyroiditis.

Pharmacological Treatment
Initial dose:
Clinical hypothyroidism–
D: levothyroxine 1.6–1.8µg/kg ideal body weight

Subclinical hypothyroidism–
D: levothyroxine 1.1–1.2µg/kg is recommended

• Take at least after 2hours fast, 30minutes before food intake. Alternatively, at bedtime (3 or
more hours after the evening meal).
• When initiating therapy in young healthy adults with overt hypothyroidism, consider beginning
treatment with full replacement doses
• Routine use of combined therapy with levothyroxine and triiodothyronine for hypothyroid
patients is not recommended

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• Assess TSH and adjust dosage when there are large changes in body weight, with aging, and
with pregnancy.
• There is no convincing evidence to support routine use of thyroid extracts, L-T3 monotherapy,
compounded thyroid hormones, iodine containing preparations, dietary supplementation, and
over the counter preparations in the management of hypothyroidism.

Monitoring
• TSH monitoring 6–8weeks after any levothyroxine dose change, and yearly life–long
monitoring once euthyroidism is achieved (target TSH 0.2–4.0um/l). FT4 can be measured in
early stages of treatment.
• In patients with central hypothyroidism, assessments of serum free T4 should guide therapy
and targeted to exceed the mid normal range value for the assay being used.
• Wait for TSH equilibration–TSH equilibration requires eight to 12 weeks after any thyroxine
dosage change. Once a stable dose is achieved–yearly TSH is sufficient.

In Pregnancy
When the elevation of the TSH level is confirmed, free T4 should be measured in order to classify
the hypothyroidism as clinical or overt (OH) and subclinical (SH).
• TSH > 2.5–10.0mU/L with normal free T4: SH.
• TSH > 2.5 –10.0mU/L with low levels of free T4: OH.
• TSH =10.0mU/L, despite the level of free T4: OH

Women in reproductive period should be euthyroid before conceiving, as the hypothyroidism is


associated with neural development. Dose may be doubled during pregnancy and returned to
normal dose after delivery

19.12.2 Hyperthyroidism
Hyperthyroidism is a condition in which an overactive thyroid gland is producing an excessive
amount of thyroid hormones that circulate in the blood. Graves' disease, multinodular goiter
(TMNG), inflammation of the thyroid gland (thyroiditis) and excessive iodine intake are the most
common cause of hyperthyroidism.

Diagnostic criteria
Hyperthyroidism can be suspected in patients with
• Tremors • A rapid heart rate
• Excessive sweating • An enlarged thyroid gland
• Smooth velvety skin • Frequent bowel movements
• Fine hair

Investigations
• Baseline complete blood count, including white count with differential, and a liver profile
(bilirubin and transaminases)
• Differential white blood cell count should be obtained during febrile illness and at the onset
of pharyngitis in all patients taking antithyroid medication. Routine monitoring of white blood
counts is not recommended
• Test for THS and T4
• When thyrotoxicosis is confirmed, if cause is not known request thyroid uptake scan

Note
Management of hyperthyroidism depends on the cause

19.12.3 Toxic Multinodular Goitre or Thyroid Antibody Positive


Patients with overtly Toxic multinodular goitre or Thyroid antibody are treated with either:

Non-pharmacological Treatment
S: Radio iodine (131-I) therapy
OR
S: Thyroidectomy

Note
Long term, low-dose carbimazole should not be used for either conditions except in some elderly

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Surgery
• Patients with overt hyperthyroidism should be rendered euthyroid prior to the procedure with
carbimazole pre-treatment (15–40mg daily, divided into 2–3doses a day for 4–8 weeks then a
maintenance dose of 5–15mg, taken once daily) with or without beta–adrenergic blockade
(e.g. propranolol 1—40mg 6hourly). Preoperative iodine should not be used in this setting.
• Following thyroidectomy for Toxic multinodular goitre, it is suggested that serum calcium or
intact parathyroid hormone levels be measured, and that calcitriol and oral calcium
supplementation (maximum 1,200mg of calcium per day in two divided doses) be
administered based on these results.
• Following surgery for Toxic multinodular goitre, thyroid hormone replacement should be
started at a dose appropriate for the patient’s weight (0.8µg/lb or 1.7µg/kg) and age, with
elderly patients needing somewhat less. TSH should be measured every 1–2months until
stable, and then annually.

Radioiodine
• Radioactive iodine therapy should be used for retreatment of persistent or recurrent
hyperthyroidism following inadequate surgery for Toxic multinodular goitre or Thyroid
antibody.

19.12.4 Grave’s Hyperthyroidism


Patients with overt Graves’ hyperthyroidism should be treated with:
Medicine Initial therapy for 4–6 Maintenance therapy
weeks (gradual reduction over 3–6 months from initial dose)
C: carbimazole 10–60mg/day in 2-3 5–10mg/day
divided dose Continue for approximately 12–18months, then taper or
discontinue if TSH is normal.

Beta Blockers are used for excessive sympathetic symptoms.


A: propranolol (PO) 40 to 120mg (24hourly or 12hourly)
OR
B: atenolol (PO) 50–100mg 12hourly

Factors which favour use of antithyroid medicines


• High likelihood of remission (patients, especially females, with mild disease, small goitres,
and negative or low-titre TSH-receptor antibody)
• Elderly or others with comorbidities increasing surgical risk or with limited life expectancy or
unable to follow radiation safety regulations
• Previously operated or irradiated necks
• Moderate to severe active Graves’ ophthalmopathy

Radioactive Iodine
Potassium iodide (B) should be given in the immediate preoperative period as 5–7drops (0.25–
0.35 mL) Lugol’s solution (8 mg iodide/drop) or 1–2 drops (0.05–0.1 mL) saturated solution of
potassium iodide (50 mg iodide/drop) three times daily mixed in water or juice for 10 days before
surgery

Factors which favour use of radioiodine


• Individuals with comorbidities • Contraindications to antithyroid
increasing surgical risk medicines use
• Patients with previously operated or • Females who are not pregnant and
externally irradiated necks are not planning a pregnancy in the
• Lack of access to a high-volume future (4–6months) following
thyroid surgeon radioiodine therapy

Surgery
Consider the following factors
• Symptomatic compression or large goitres
• Low uptake of radioactive iodine
• Thyroid malignancy is documented or suspected or large non-functioning nodule
• Coexisting hyperparathyroidism requiring surgery

416
• Females planning a pregnancy in <4–6months
• Patients with moderate to severe active Graves’ ophthalmopathy
• If a patient with Grave’s disease becomes hyperthyroid after completing a course of
carbimazole, consideration should be given to treatment with radioactive iodine or
thyroidectomy. Low-dose carbimazole treatment for longer than 12–18months may be
considered in patients not in remission who prefer this approach but evidence is that
remission rate in adults is not improved by a course of medicines longer than 18 months
• Whenever possible, patients with Grave’s disease undergoing thyroidectomy should be
rendered euthyroid with carbimazole.

19.12.5 Thyroid Storm (Crisis)


Thyroid storm is one of the most life-threatening endocrine emergencies, resulting from
exacerbation of manifestations of thyrotoxicosis.

Triggers of thyroid storm include:


• Antithyroid withdraw
• Acute infections
• Thyroidal or nonthyroidal surgeries
• Iodinated contrast dyes
• External beam radiation therapy.
• It should be considered in very sick patients if they present with recent history of
thyrotoxicosis and a recent history of precipitating factor.

Patients with thyroid storm (tachycardia, arrhythmias, congestive heart failure, hypotension,
hyperpyrexia, agitation, delirium, psychosis, stupor and coma, as well as nausea, vomiting,
diarrhoea, and hepatic failure) should receive a multimodal treatment including:

• Beta-adrenergic blockade • Volume resuscitation


• Antithyroid medicine therapy • Respiratory support
• Inorganic iodide • Monitoring in an intensive care unit.
• Corticosteroid therapy
• Aggressive cooling with
acetaminophen and cooling blankets

Thyroid storm is not a matter of thyroid levels increased beyond those of uncomplicated
thyrotoxicosis, but the systemic decompensation that occurs.

Table 19.7: Pharmacological Treatment


Medicine Dosing Comment
D: propylthiouracil* 500–1000mg load, then Blocks new hormone synthesis Blocks
250mg 4hourly T4–to–T3 conversion
C: carbimazole 40–60 mg/day Blocks new hormone synthesis
A: propranolol 60–80mg every 4hourly Consider invasive monitoring in congestive heart
failure patients
Blocks T4–to–T3 conversion in high doses.
Alternate medicine: esmolol infusion
B: iodine (saturated 5drops (0.25mL or 250mg) Do not start until 1hour after antithyroid medicines
solution of potassium (PO) 6hourly Blocks new hormone synthesis
iodide) Blocks thyroid hormone release

A: hydrocortisone 300 mg intravenous load, May block T4–to–T3 conversion


then 100mg Prophylaxis against relative adrenal insufficiency
8hourly Alternative medicine: dexamethasone

Note
In thyroid storm, propylthiouracil is preferred to carbimazole

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19.13 Cushing's Syndrome
Cushing syndrome is a clinical condition resulting from prolonged exposure to excessive
glucoccorticoids from either endogenous or exogenous sources. The most common cause of
Cushing’s syndrome is from the administration of exogenous sources.

Classification
Cushing syndrome can be divided into two categories based on pathophysiology, ACTH dependent
or ACTH – Independent
• ACTH-dependent States
o Pituitary Adenoma (Cushing’s Disease) 90-95%
o Ectopic ACTH Syndrome
• ACTH-independent States
o Adrenal adenoma
o Adrenal carcinoma
• Exogenous Sources
o Glucocorticoid intake
• Psychiatric Conditions (Pseudo-Cushing Disorders)
o Depression
o Alcoholism
• High Cortisol Secretion Rate without Convincing Clinical Features of Cushing Syndrome
• Pregnancy

Symptoms and signs of Cushing’s syndrome


• The symptoms and signs of Cushing's syndrome result directly from chronic exposure to
excess glucocorticoid
• Establishing the diagnosis is often difficult because none of the symptoms or signs are
pathognomonic of the syndrome.
• An important clinical clue to the presence of glucocorticoid excess is the simultaneous
development and increasing severity of several of these symptoms
• Common presenting symptoms include
o Central obesity
o Facial plethora
o Weakness of the proximal muscles
o Easily bruises and striae
o Hirsutism
o Glucose intolerance

Diagnosis of Cushing’s syndrome


At least two first-line tests should be abnormal to establish the diagnosis of Cushing's syndrome
• The low-dose dexamethasone suppression tests
• 24hrs urinary cortisol,
• Late night salivary cortisol
• Differential Diagnostic Testing to established, the cause of Cushing’s syndrome
o Morning serum ACTH
o High dose dexamethasone suppression test

Imaging diagnosis
• Pituitary CT - sensitivity of about 50% for identifying microadenomas
• MRI pituitary sensitivity up to 100%
• Adrenal ultrasonography/CT for suspected Adrenal source

Treatment of Cushing’s syndrome


Without therapy, Cushing’s syndrome is often fatal.
• Typically, due to CV, HTN or infectious complications.
• With therapy Symptoms improve over 2-12 months.

Definitive Therapy
Surgery by source when possible
• Adrenal source - Adrenalectomy
• Pituitary source - Transphenoidal resection
• Ectopic source - Tumor Resection

434
Medical therapy
S: metyrapone (PO) 30mg/kg, maximum dose 3,000mg, administered at midnight usually
with a snack
19.14 Prolactinoma
Are prolactin – secreting pituitary tumors

Classification
May present as Microprolactinomas (<10mm) or Macroprolactinomas (>10mm)

Clinical Presentation
Symptoms are due to hyperprolactinemia which include galactorhea, oligo/amenorrhea, infertility,
reduced libido, impotence and gynacomastia in male, headache and visual abnormality in large
adenomas.

Diagnosis
Serum prolactin levels
<100ng/ml possible prolactinoma
100-200ng/ml likely prolactinoma
>200 ng/ml –diagnostic of prolactinoma

Treatment
Proactinomas are unique among pituitary tumors in that first line treatment is medical not surgical.
The mainstays of management for prolactinomas are the dopamine agonist which are:
C: bromocriptine (PO) 2.5-20mg (24hourly or 12hourly)
OR
S: cabergoline (PO) 0.25-1mg (twice a week)

19.15 Diabetic Insipidus (DI)


DI is a disorder of water balance caused by non-osmotic renal loss of water leading to excretion of
large volume of dilute urine

Classification
Central DI: Is caused by either complete or partial deficiency of antidiurectic hormone (ADH)
secretion from the posterior pituitary gland
Nephrogenic DI: Is caused by end organ unresponsiveness of the kidney to ADH
Dipsogenic DI: Is caused by excessive and inappropriate fluid intake due to a defective in thirsty
mechanism

Clinical Presentations
Polyuria especially nocturnal

Diagnostic criteria
• Polyuria and urine osmolality of <300 for a given plasma osmolality
• Volume depletion and orthostatic hypotension may be found
• Plasma Sodium may be normal or elevated

Pharmacological Treatment
In case of water deficit - water replacement. Treating of the underlying defect
Central DI:
S: desmopressin (IV) 2-4 µg/day divided 12hourly
OR
S: desmopressin (PO) Initial dose 0.05mg 12hourly; effective range: 0.1-1.2mg divided 8-
12hourly
OR
D: desmopressin (Intranasal) 10-40µg (0.1-0.4mL) 24hourly, either as a single dose or
divided into 2 or 3doses; usual dose is 20µg (0.2mL) 24hourly in 2divided doses

Nephrogenic DI:
A: thiazide diuretic (e.g bendrofluazide (PO) 5mg 24hourly OR hydroclorothiazide 12.5-
25mg 24hourly)

435
19.16 Pheochromocytoma
Pheochromocytoma are neuroendocrine tumors arising from catecholamine producing chromaffin
cells of the adrenal medullar but about 15–20% are extra-adrenal in origin

Clinical presentation
• The classic symptoms of pheochromocytoma are due to episodic release of excess
catecholamines into circulation (Norepinephrine and Epinephrine)
• Typical symptoms
o headaches
o palpitations
o anxiety and diaphoresis
o hypertension which can be paroxysmal (∼48%) or persistent (∼29%).

Table: Biochemical Tests Comparisons


Test Sensitivity Specificity
Urine Catecholamine 83 88
Urine Total Metanephrines 76 94
Urine Catecholamines + Metanephrines 90 98
Urine VMA 63 94
Plasma Catecholamines 85 80
Plasma Metanephrines 99 89

Tumor Localization
• Anatomic localization of a catecholamine-secreting tumor should be performed only after
biochemical diagnosis has been confirmed
• Approximately 85% of catecholamine-secreting tumors are found in the adrenal glands, and
95% are found in the abdomen and pelvis
• Either CT or MRI are effective for localization of catecholamine-secreting tumors -sensitivity
89 vs 98% resp.

Management of Pheochromocytoma
• After definitive diagnosis, the mainstay of definitive therapy is complete surgical resection of
the tumor
• Prior to planned surgical intervention, the effects of excess catecholamines must be
ameliorated in order to avoid perioperative complications and improve outcome, by using α -
adrenergic antagonists

None selective α-antagonist


S: phenoxybenzamine (PO) 10mg 12hourly initially; increase to 20-40 mg 8-12hourly
OR

Selective α-antagonist
S: doxazocin (PO) 1-2mg 24hourly

Combined α + β blockade

19.17 Disorder of Sexual Development (DSD)


DSD formerly known as intersex conditions are classified on the basis of genetics and the state of
gonads. They may be caused by virilization 64XX or under virilization 46XY. As well as mosaism
(streak Ovary, Ovotestis, dysgentic testis). The most common DSD is Congenital Adrenal
Hyperplasia (CAH).

Diagnostic criteria
• Infant born with ambiguous or abnormal genitalia
• Infant with undescended testis, unilateral or bilateral
• Infant with hypospadias

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Investigations
• Serum electrolytes
• Chromosomal analysis
• Karyotyping in a male looking male with undescended testis and/or hypospadias whether the
genitalia appears normal or not
• Endocrine screening
• Antimurellian Hormone (AMH)

Non-pharmacological Treatment
Counseling of the parents on
• The condition
• Naming of a child and
• Gender assignment

Pharmacological Treatment
Depends on type of the DSD it is either CAH or other forms of DSD (Non CAH DSD)

CAH DSD
Salt losing in crisis-
• Bolus normal saline (0.9% NaCl) and maintenance,
• Hypoglycemic 2-4 ml of 10% dextrose

Long-term treatment
S: fludrocortisone (PO) 0.05-0.3mg 24hourly

Non CAH DSD


D: testosterone 50-400mg monthly for 3cycles, then asses +/-
D: testosterone cream

19.8 Obesity in Adults


Diagnosis
• Body mass index (BMI) = weight divided by height squared (weight in kg, height in meters)
• Ideal BMI is from 18.5-24.9: less than 18.5 is underweight, 25-29.9 is overweight and 30+ is
obese.
• Overweight/obesity increases risk of CVD, type 2 diabetes, pulmonary embolism, gallbladder
disease, colorectal cancer, osteoarthritis, chronic back pain and all-cause mortality, especially
for those with high blood pressure,hyperlipidemia, and hyperglycemia.
• Individuals living with obesity are subject to considerable stigma, which they may internalize
and experience as shame, depression and anxiety.
• As part of prevention of non-communicable diseases, for all adults attending health facilities,
height, weight and waist circumference should be measured at least yearly and appropriate
action taken:
o Everyone should be educated on the risks of overweight/obesity and the need to avoid
weight gain by adjusting food intake and engaging in regular physical activity
o Weight loss treatment is indicated for the obese or those overweight with increased
cardiovascular risk (e.g. diabetes, prediabetes, hypertension, dyslipidemia, elevated
waist circumference) or other obesity-related comorbidities.
o Evaluate diet, previous and current physical activity, and disorders of sleep, eating and
mood
o Assess the patient's medication regimen for drugs that may contribute to weight gain and
consider adjustments
o Determine diabetes and CVD risk
▪ High Blood Pressure
▪ Hyperlipidemia
▪ Hyperglycemia
▪ Elevated liver enzymes (Non-alcoholic liver disease)

Non-pharmacological Management
• Even modest, sustained weight loss of 3%–5% produce clinically meaningful reductions
in triglycerides, blood glucose, hemoglobin A1c, and the risk of developing type 2 diabetes.

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• Greater amounts of weight loss will reduce blood pressure, improve LDL-Cholesterol
and HDL-Cholesterol, and reduce the need for medications to control BP, blood glucose,
and lipids as well as further reduce triglycerides and blood glucose.
• Weight loss requires creating an energy deficit through caloric restriction, physical activity, or
both
o Aim for a loss of 5%-10% of baseline weight within 6 months (0·5 kg per week for 6
months: total about 8kg)
o Prescribe a diet to achieve energy deficit of ≥500 kcal/d: may be achieved with dietary
intake of 1200-1500 kcal/d for women and 1500-1800 kcal/d for men (25-30kcal/kg/day)
o The choice of diet should address a patient’s preference and ease of adherence and be
directed towards long-term lifestyle changes that include eating patterns that are
practical, achievable, and sustainable
o Use of very-low-calorie diets (<800 kcal/d) should be advised only under medical
supervision
o Proteins
▪ Aim for approximately 20% of total energy from good quality proteins, lean meats
and whole pulses
▪ Proteins induce a feeling of satiety and any excess is deaminated.
o Fats
▪ Aim for 20% or less of total energy from fats
▪ Avoid saturated fats to reduce the risk of heart problems
▪ Restrict or avoid fried foods
▪ Choose low fat milk.
o Carbohydrates
▪ Aim for 60% of energy from complex carbohydrates
▪ Whole grains, roots & tubers, e.g. sweet potatoes, yams
▪ Limit sugars and honey.
▪ Vegetables e.g. broccoli, mushroom, zucchini, cabbage, lettuce, cucumber, celery
▪ Fruits such as pineapple, apples, cherimoya, peach, grapefruit, watermelon

o Avoid
▪ Alcohol as it provides calories without nutrients, and excessive use is harmful in
many ways
▪ Omit fad diets and other unhealthy practices
• Tailored physical activity program
o Initially 30 min of moderate intensity 3-5 times per week
o eventually ≥60 min on most days; add muscle strengthening on at least two days/week
o Weight regain following weight loss is reduced by physical activity equivalent to 60 min
of brisk walking daily and lifestyle activity that increases energy expenditure throughout
the day without concern for the intensity or duration can be as effective for weight control
as jogging, swimming, or cycling.
• Offer behavioural support
o identify cues that prompt overeating or inactivity, and restructure thoughts and
behaviours to prompt healthy responses
o Advise patient to
▪ set goals that specify what, when, where, how, and for how long they will engage in
a selected activity
▪ keep detailed records of food intake, physical activity, and bodyweight
▪ eat breakfast regularly and maintain a consistent eating pattern across weekdays
and weekends
▪ engage family members for ongoing support
▪ participate for ≥6 months in a lifestyle program that assists participants in adhering
to a lower-calorie diet and in increasing physical activity
o For those who have lost weight, prescribe face-to-face or telephone-delivered weight
loss maintenance programs that provide regular contact (monthly or more frequently)
and helps participants to engage in high levels of physical activity (ie, 200–300
min/wk), monitor body weight regularly (ie, weekly or more frequently), and consume
a reduced-calorie diet (needed to maintain lower body weight).
• Facilitate referral to a specialist team (metabolic obesity clinic and/or metabolic surgery) if
patient:

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o is unable to achieve >= 5% weight loss at 3 months on a lifestyle intervention consisting
of reduced energy/low-energy diet, increased physical activity, and/or pharmacotherapy
o has a BMI ≥40 kg/m2 or BMI ≥35 kg/m2 with obesity-related comorbid conditions and
has not responded to behavioral treatment with or without pharmacotherapy to consider
bariatric surgery
o Monitor the patient's requirements for medication as weight loss progresses, particularly
for antihypertensive and diabetes medications that can cause hypotension and
hypoglycemia.

Pharmacological Treatment
Drug therapy may be considered for those with a BMI ≥30kg/m2, BMI ≥27kg/m2 with obesity-related
comorbid conditions, or if patient has not lost 0·5kg per week by 3–6months after lifestyle changes

S: orlistat (PO) 120mg 8hourly with each main meal containing fat (during or up to one
hour after the meal). It inhibits pancreatic and gastric lipase, reducing fat absorption by
approximately 30%

• Anti-obesity pharmacotherapy should be continued beyond 12weeks only if at least 5% of


initial body weight has been lost since starting medication and should be prescribed as an
adjunct to lifestyle interventions.

Innovative strategies for delivery and management of obesity care


Primary care should be enhanced with:
• patient registries and methods for systematic tracking to assess clinical interventions
(electronic health records)
• care teams to manage patients with chronic illnesses
• health information systems that support the use of evidence-based practices at the point-of-
care to provide longitudinal care for chronic illnesses.
• Electronic support
o text messaging to provide outreach, support for behaviour change to patients and
educational messages
o Blood pressure, blood glucose and wi-fi scales, which automatically transmit results from
machine to a server
o smartphones and tablets with weight loss applications to simplify monitoring of food
intake, physical activity, and weight
o interventions by telephone, study-specific website, and email
o Remote support offers flexibility to patients and practitioners and can be scaled up or
down according to patients’ needs.

Hospitals and health professionals as role models


• An overweight/obese health worker is less likely to counsel patients with obesity
• Provide healthy food choices for patients, employers, visitors, and communities, with pricing
incentives
• Label drinks sold in hospital cafeterias as red, yellow, or green to shift consumption towards
healthier beverages
• Prohibit fast food outlets in hospital premises

19.19 Physical Activity


• Physical fitness is the ability to perform physical activities without undue fatigue and is
achieved through proper nutrition, moderate to vigorous physical activity, and sufficient rest.
• Physical activity
o Improves insulin resistance, reduces HbA1c by 0.7% in Type II diabetes and protects
against the development of Type II diabetes
o Improves lipid profile, lowers blood pressure and helps maintain appropriate body
weight.
• Physical activities
o Include:
▪ Those associated with the performance of a job e.g. walking, hauling, lifting,
pushing, carpentry, farming, shoveling, packing boxes, etc.
▪ Those done during free time e.g. structured exercise as well as walking, hiking,
gardening, sport, dance, etc.

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o Require contraction of skeletal muscle and increased energy expenditure above the
resting level.
• The types of physical activity for optimal fitness include aerobic, muscle-strengthening,
stretching and coordination.

Aerobic Activities
• These improve the body composition (fat, muscle and bone) and cardiorespiratory fitness
• Examples:
o brisk walking, climbing stairs, cycling, swimming, dancing, jogging, running, washing
windows or car, sweeping floors or carpet, vacuuming, mopping, shoveling, digging
ditches, carrying heavy loads such as bricks
o Sports: badminton, golf, tennis, volleyball, swimming, basketball, football, jumping jacks,
jumping rope.
• For optimal effect, the activity has to be:
o Moderate intensity (a person doing moderate-intensity aerobic activity can talk, but not
sing, during the activity) or vigorous (cannot say more than a few words without pausing
for a breath).
o For at least 30 minutes per day at least five days per week.

Muscle-strengthening Activities
• These enable the major muscle groups of the body (the legs, hips, back, chest, abdomen,
shoulders, and arms) to do more work than they are accustomed and thus increase muscle
mass, strength and endurance.
• Examples: pull-down, pull-ups, push-ups, dips, abdominal crunch/curl-up, calf raises,
jumping, carrying heavy loads, and heavy gardening (digging or hoeing).
• For optimal effect:
o Each activity should consist of at least 8 repetitions of the movement (e.g. 8 push-ups)
o Each muscle group should be active on at least two days per week.

Stretching Activities
• Improve flexibility such as range of motion, e.g. ability to bend down to tie your shoe.
• Examples: neck flexions, arm rotations, trunk rotations, and stretching of muscles.

Coordination Activities
• Improve neuromuscular fitness such as balance, agility and proprioception necessary for
example to prevent falls in the elderly
• Examples: Standing on the toes of one leg.

Improving Exercise Adoption and Maintenance


As part of risk factor assessment in disease prevention, the physical activity level of all patients
attending health facilities should be assessed, followed by brief advice, if required, about
recommended levels.

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CHAPTER TWENTY
CARDIOVASCULAR DISEASE CONDITIONS
20.1 Prevention of Atherosclerotic Ischaemic Heart Disease and Stroke
Cardiovascular disease (CVD) prevention is a coordinated set of actions, at the population level or
targeted at an individual at risk of developing cardiovascular disease, that are aimed at eliminating or
minimizing the impact of CVDs and their related disabilities.

Diagnostic/screening Criteria
Major risk factors for ischaemic cardiovascular and cerebrovascular disease are:
• Diabetes mellitus
• Hypertension
• Central obesity: waist circumference ≥ 94cm (men) and ≥ 80cm (women)
• Dyslipidaemia (fasting levels): Total cholesterol > 5 mmol/L, or LDL> 3mmol/L, or HDL< 1
mmol/L in men and < 1.2mmol/L in women
• Smoking
• Age: Men >50 years, Women >60 years
• Family history of early onset cardiovascular disease; Male relatives <55 years and Female
relatives <65 year

Estimation of total cardiovascular risk is important for prevention of CVD in an individual, should be
adapted to his or her total CV risk: the higher the risk, the more intense the management should be
(See Table 20.1).

Table 20.1: Cardiovascular Disease Risk Classification and WHO Risk estimation
Very High Subjects with any of the following:
Risk • Documented CVD, clinical or unequivocal on imaging: previous AMI, ACS, coronary
revascularization and other arterial revascularization procedures, stroke and TIA, aortic
aneurysm and PAD. Unequivocally documented CVD on imaging includes plaque on coronary
angiography or carotid ultrasound. It does NOT include some increase in continuous imaging
parameters such as intima–media thickness of the carotid artery.
• DM with target organ damage such as proteinuria or with a major risk factor such as smoking
or marked hypercholesterolaemia or marked hypertension.
• Severe CKD (GFR <30mL/min/1.73m²).
• A calculated CVD Risk Score ≥10%.

High Risk Subjects with:


• Markedly elevated single risk factors, in cholesterol >8mmol/L (>310mg/dL) (e.g. in familial
hypercholesterolaemia) or BP ≥180/110mmHg.
• Most other people with DM (except for young people with type 1 DM and without major risk
factors that may be at low or moderate risk).
• Moderate CKD (GFR 30–59mL/min/1.73m²).
• A calculated CVD Risk Score ≥5% and <10%.
Moderate CVD Risk Score is ≥1% and <5% at 10years. Many middle–aged
Risk subjects belong to this category
Low Risk CVD Risk Score <1%

Non-pharmacological Treatment
General measures:
• Lifestyle modification (refer to table 20.2)

Table 20.2: The Summarized Preventive Measures to be Individualized on Targeted Goals


Risk factor goals and target levels for important cardiovascular disease risk factor reduction
1 Smoking No exposure to tobacco in any form.
2 Diet Reduce dietary sodium intake no more than 1000mmol/L (2.4gm sodium or 6gm
sodium chloride per day)
Low in saturated fat with a focus on wholegrain products, vegetables, fruit, and
fish.
Reduce alcohol intake to ≤ 2 units/day for men and ≤1 unit for women, not more
than 5 out of 7days per week (1 unit is equivalent to 25mL of spirits, 125mL of
wine, 340mL of beer or sorghum beer, or 60mL of sherry).
3 Physical activity At least 150minutes a week of moderate aerobic exercise (30minutes for

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5days/week) or 75minutes a week of vigorous aerobic exercise (15minutes for
5days/week) or a combination thereof
4 Body weight Body weight BMI 18.5–24.9kg/m²
Waist circumference <94 cm (men) or <80 cm (women)
5 Blood Pressure <140/90mmHg
6 Lipids Very high risk: <1.8 mmol/L (<70mg/dL), or a reduction of at least 50% if the
LDL–C is the baseline is between 1.8 and 3.5mmol/L (70 and 135mg/dL)
primary target High risk:<2.6mmol/L (<100mg/dL), o r a reduction of at least 50% if the baseline
is between 2.6 and 5.1mmol/L (100 and 200mg/dL)
Low to moderate risk:<3.0mmol/L (<115mg/dL)
HDL–C No target but >1.0mmol/L (>40mg/dL) in men and >1.2mmol/L (>45mg/dL) in
women indicate lower risk
Triglycerides No target but <1.7mmol/L (<150mg/dL) indicates lower risk and higher levels
indicate a need to look for other risk factors.
7 Diabetes HbA1c <7%. (<5.3mmol/l)

Recommended to repeat CV risk assessment every 5years, and more often for individuals with risks
close to thresholds mandating treatment.

Pharmacological Treatment: Forspecific pharmacological treatment for hypertension, diabetes,


dyslipidemia refer specific sections, respectively.
20.2 Management of Dyslipidemias
Lowering blood cholesterol levels using statins is recommended to reduce the impact of
cardiovascular morbidity and mortality

Clinical indication for lipid lowering medicine therapy


• Established atherosclerotic disease
• Ischaemic heart disease
• Peripheral vascular disease
• Atherothrombotic stroke

Note
Lipid lowering medicines should be administered in this setting even if the level of cholesterol is
normal
• Type 2 diabetics >40 years of age, or diabetes for >10 years,
• Existing cardiovascular disease,
• Chronic kidney disease (eGFR < 60mL/min).
• CV risks of more than >20% in 10years Such high-risk patients will benefit from lipid lowering
(statin) therapy irrespective of their baseline LDL levels.

Pharmacological Treatment
B: atorvastatin (PO) 20mg to 80mg 24hourly
OR
S: rosuvastatin (PO) 10mg-40mg 24hourly
AND
D: fenofibrate (PO) 120mg /160mg /200mg 24hourly

Note
• Criteria for initiating lipid lowering therapy are the same as for HIV uninfected patients. Fasting
lipid levels should be done 3months after starting lopinavir/ritonavir and atazanavir/ritonavir.
• Patients at high risk (>20% risk of developing a CVS event in 10years) should switch to
atazanavir/ritonavir and repeat the fasting lipid profile in 3 months.
• Concomitant use of Ezetimibe andAtorvastatin can lead to liver damage and rhabdomyolysis.
• Fenofibrate indicated Hypertriglyceridemia, in which statin alone is not enough to treat & lower
the hypertriglyceridemia.

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20.3 Chronic Stable Coronary Artery Disease (CSCAD) / ISCHAEMIC Heart
Disease (IHD)
Clinical history characterized by chest pain due to myocardial ischaemia usually inducible by
exercise, emotion, or other stress and reproducible, relieved by rest but may occur spontaneously
and stable in nature, occurs in high-risk patient.

Non-pharmacological Treatment
General Measures
• Lifestyle modification (refer to table 20.2).
• Annual control of lipids, glucose metabolism and creatinine are recommended in all patients with
known IHD.
• A resting ECG is recommended in all patients at presentation and during or immediately after an
episode of chest pain suspected to indicate clinical instability of CAD, Consider immediate
referral.
• A resting transthoracic echocardiogram is recommended in some patients for:
a) exclusion of alternative causes of angina
b) regional wall motion abnormalities suggestive of CAD
c) measurement of LVEF for risk stratification purpose
d) evaluation of diastolic function.
Consider referral if no echocardiogram available or unavailability of skilled personnel to perform
transthoracic.
• Stress ECG
• Stress Echocardiography; a) Physical (Exercise) Stress Echo; b) Dobutamine (Pharmacological)
Stress Echo performed to Orthopaedic related disorders pt who cannot walk on the Treadmill
machine).

Pharmacological Treatment
A: acetylsalicylic acid soluble (PO) 75–150mg 24hourly
AND
C: isosorbide dinitrate (PO) 20mg-40mg 12hourly

If nitrates cannot be tolerated, consider stepwise approach below.


S: ivabradine (PO) 2.5mg /5mg 24hourly

Step 1: add ß-blocker if not contraindicated:


B: atenolol (PO) 12.5/25mg 24hourly
OR
S: metoprolol tartrate (IV) 5mg 2min for max 3doses, then (PO) 50-100mg 12hourly
OR
C: metoprolol succinate (SR) (PO) 25–200mg 24hourly
OR
S: bisoprolol (PO) 2.5mg /10mg 24hourly
Consider long-acting calcium channel blocker, if a ß-blocker cannot be tolerated or contraindicated.

Step 2: add long-acting calcium channel blocker.


S: verapamil (PO) 60mg -120mg 8hourly 24hourly
OR
D: diltiazem (PO) 60mg 6 to 8hourlydaily; if suspects Prinzmetal Angina.

Key Points
• All patients with chronic stable angina are high-risk for cardiovascular events, lipid lowering
medicines should be initiated (See Section 20.2).
• Consider immediate referral to high level of care where there are adequate resources for the
case management.

Indications for Referral


• Angina or chest pain suspected to indicate clinical instability of CAD
• When diagnosis is in doubt/ failed medical therapy; no echocardiogram available or
unavailability of skilled personnel to perform transthoracic echocardiogram.

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Before referral when high likelihood of clinical instability of stable CAD consider giving:
A: acetylsalicylic acid(PO) 300mg stat.
AND
B: atorvastatin (PO) 80mgstat
AND
D: clopidogrel (PO) 300mg stat

20.4 Acute Coronary Syndrome


20.4.1 Unstable Angina (UA)
Unstable angina is a medical emergency and if untreated can progress to Non-ST Elevation
Myocardial Infarction (NSTEMI)

Diagnostic Criteria
Presents as chest pain or discomfort like stable angina but with the following additional
characteristics:
• Angina at rest or minimal effort, occurring for the first time, particularly at rest and prolonged
>10minutes, not relieved by sublingual nitrates.
• The pattern of angina accelerates and gets worse.
• The chest pain may be associated with ST segment depression or T wave inversion or
normal ECG without rise in cardiac enzymes (biomarkers ie. Total Createnine, Creatine -
MB and Troponin).

20.4.2 Non-ST Elevation Myocardial Infarction (NSTEMI)


Non-ST Elevation Myocardial Infarction is a medical emergency characterized with chest pain that is
increasing in frequency and/or severity or occurring at rest, associated with elevated cardiac
enzymes and ST segment depression or T wave inversion or normal ECG.

Diagnostic Criteria
Presents with typical chest pain with the following additional characteristics.
• Electrocardiogram (ECG) may show ST segment depression or transient ST segment
elevation, or normal ECG does not exclude the diagnosis (serial ECG is important).
• Raised Cardiac Biomakers – Total Creatine Kinase (Total-CK), Creatine Kinase - MB (CK-
MB) and standard/high sensitive Troponin I or T.

Non-pharmacological Treatment
Both UA and NSTEMI are medical emergencies with the same pathophysiological progressive
instability of CAD, which share similar management approach.

Supportive Therapy
• Admit patient into high dependent ward/ICU/CCU for haemodynamic monitoring, bed rest
in Fowler’s position and reassurance.
• Oxygen via nasal blog cannula or face mask if saturation < 92%.
• Establish Peripheral Intravenous line for intravenous fluid or drug administration.
• Haemodynamics blood pressure, heart rate and electrocardiogram rhythm monitor.

Pharmacological Treatment
Adjunctive therapy
Control cardiac pain
C: glyceryl trinitrate (Nitroglycerin) sub–lingual/ spray 0.5mg (make sure patient has not
taken phosphodiesterase–5 inhibitor).

For persistent pain and if oral therapy is insufficient.


S: glyceryl Trinitrate (Nitroglycerin) (IV), 1–2µg/kg/min titrated with chest pain over 8–
24hours.
OR
C: morphine (IV)1–2mg/minute dilute 10mg up to 10mL with sodium chloride solution 0.9%.
Total maximum dose10 mg, repeat after 4hours if necessary

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Note
• If pain is not responsive to this dose, it is suggestive for ongoing unresolved ischaemia. This
requires immediate referral to high level of care where resources available to manage Acute
Coronary Syndrome or to exclude differential diagnosis.

Antiplatelet Therapy
A: acetylsalicylic acid (PO) 300mg stat then followed by 75mg/100mg 24hourly
AND
D: clopidogrel (PO) 300mg /600mg start then followed by 75mg 24hourly
OR
S: ticagrelor (PO) 180mg stat.
For first year following ACS event: 90 mg 12hourly.
After 1year of maintenance: 60mg 12hourly.

Statin high dose


B: atorvastatin (PO) 80mg stat then 40mg 24hourly
OR
S: rosuvastatin (PO) 10mg-40mg 24hourly

Anticoagulant
B: heparin UFH (IV) 70–100U/Kg body weight a 24hourly
OR
S: low molecular weight heparin (SC) 1mg/kg body weight 12hourly

Beta blocker (ß –blockers)


In case of LV dysfunction
C: carvedilol initial dose (PO) 6.25mg 12hourly preferred, titrate the dose upward. Max.
Dose 25mg 12hourly
OR
In the settings of normal LV systolic function
B: atenolol 25–50mg (PO) 24hourly,
OR
S: metoprolol tartrate 5mg (IV) 2min for maximum of 3 doses, then (PO) 50-100mg
12hourly
OR
C: metoprolol succinate (SR) (PO) 25 – 200mg 24hourly.
OR
S: bisoprolol (PO) 2.5mg – 10mg 24hourly

Angiotensin Converting Enzyme Inhibitors (ACEIs)


B: captopril (PO) 6.25mg–25mg 8hourly
OR
C: enalapril (PO) 10mg 12 hourly
OR
C: lisinopril (PO) 5mg /10mg 24hourly

Referral
High suspicion index of acute coronary syndrome immediate consider referral to high level of care
where resources are available to manage. In acute settings before referral from low to high level of
care if available consider giving the following urgently:
• glyceryl trinitrate (Nitroglycerin) sub-lingual 0.5mg spray prn for intolerable chest pain
• acetylsalicylic acid (PO)300mg stat (chew)
• clopidogrel (PO) 300mg/600mg stat
• High dose statin simvastatin (PO) 80mg stat OR atorvastatin (PO) 80mg stat

20.4.3 ST Elevation Myocardial Infarction (STEMI)


STEMI is a medical emergency caused by the complete or partial occlusion of a coronary artery and
requires prompt hospitalization and intensive care intervention management.

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Clinical Presentation
Severe chest pain with the following characteristics
• Site: retrosternal or epigastric, quality: crushing, constricting, or burning pain or discomfort.
• Radiation to the neck and/or down the inner part of the left arm.
• Duration: at least 20 minutes and often not responding to sublingual nitrates.
• Occurrence: at rest. May be associated with pulmonary oedema sweating, hypotension or
hypertension, arrhythmias.

Diagnostic Criteria
Simple recognition triage: Two out of three points most likely point to STEMI diagnosis
• Symptoms - typical/atypical chest pain
• ECG – ST elevation in in two contiguous leads ≥0.1mV
• Raised cardiac biomakers– Total Creatine Kinase (Total-CK), Creatine Kinase -MB (CK-MB)
and Standard/Highly Sensitive Troponin I or T

Non-pharmacological Treatment:
Supportive therapy
• Consider cardio-pulmonary resuscitation if necessary, before transfer (cardiac arrest–
cardiopulmonary resuscitation).
• Oxygen 40% via facemask, if saturation < 92% or if in distress
• See section 20.4.2 above on supportive therapy for NSTEMI

Adjunctive therapy
Control cardiac pain
C: glyceryl trinitrate sub-lingual/ spray 0.5mg (make sure patient hasn’t taken
phosphodiesterase-5 inhibitor).

For persistent pain and if oral therapy is insufficient


S: glyceryl Trinitrate (IV) 1–2 µg/kg/min titrated with chest pain over 8–24 hours.
OR
C: morphine (IV) 1–2 mg/minute dilute 10 mg up to 10 mL with sodium chloride solution
0.9%. Total maximum dose: 10 mg, repeat after 4 hours if necessary.

Anti-platelets therapy
A: acetylsalicylic (PO) 300mg stat then followed by 75mg/100mg (PO) 24hourly
AND
D: clopidogrel (PO) 300mg/600mg stat then followed by 75mg 24hourly
OR
S: prasugrel (PO) 60mg stat, given after defining coronary anatomy prior to onset of PCI,
then 10mg as maintenance dosage.

Statin high dose


B: atorvastatin (PO) 80mg start then 40mg 24hourly
OR
S: rosuvastatin (PO) 10mg-40mg 24hourly

Anticoagulant
B: heparin UFH (IV) 70–100U/Kg 24hourly
OR
S: low molecular weight heparin (SC) 1mg/kg 12hourly, Reduce dose in renal failure patient
to 0.5mg/kg

Beta blocker (ß –blockers)


In case of LV dysfunction
C: carvedilol (PO) initial dose 6.25mg 12hourly daily preferred, titrate dose upward to
maximum dose 25mg hourly daily

In the settings of normal systolic function


B: atenolol (PO) 12.5mg or 25mg or 50mg 24hourly
OR
S: metoprolol tartrate (IV) 5mg 2min for max 3doses, then (PO) 50-100 mg 12hourly
OR

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C: metoprolol succinate (SR) (PO) 25 – 200mg 24hourly
OR
S: bisoprolol (PO) 2.5mg – 10mg 24hourly
OR
S: verapamil SR (PO) 240 mg – 480 mg daily in 1-2 divided doses

Note
Verapamil SR should be initiated from 7 days’ post myocardial infarction; any single dose should
not exceed 240mg as secondary prevention of myocardial infarction.

Angiotensin-Converting Enzyme Inhibitors (ACEIs)


B: captopril (PO) 6.25mg or 12.5mg 8hourly
OR
C: enalapril (PO) 10mg 12hourly
OR
C: lisinopril (PO) 5mg-10mg 24hourly

Definitive management of STEMI – Reperfusion therapy (Myocardial reperfusion)


Myocardial reperfusion with rapid recanalization of infarct related artery is the key to success in the
management of ST Elevation Myocardial Infarction (STEMI). Timely reperfusion is crucial for
minimization of infarct size and thereby for preservation of left ventricular function and reduction in
mortality in STEMI patients. The two main reperfusion strategies for STEMI patients are;
• Thrombolytic/Fibrinolytic therapy (preferably chest pain duration less 12 hrs)
• Primary percutaneous coronary intervention (PPCI) (preferably less than 90 mins of Door to
Needle Time)

Thrombolytic agents
S: streptokinase (IV) 1.5 million units diluted in 100 mL sodium chloride 0.9%, infused over
30–60minutes
OR
S: alteplase (TPA) (IV) 15mg as bolus, 0.75mg/kg over 30min, then 0.5mg/kg over 60min

Absolute contraindication for Thrombolytics


• Previous allergy to streptokinase or used within the last year for streptokinase only.
• Stroke CVA within the last 3 months
• History of recent major trauma
• Bleeding within the last month
• Aneurysms
• Brain or spinal surgery or head injury within the preceding month
• Active bleeding or known bleeding disorder.

Relative contraindication for Thrombolytics


• Refractory hypertension • Pregnancy
• TIA in the preceding 6 months, • Traumatic resuscitation
• Subclavian central venous catheter • Recent retinal laser treatment
• Warfarin therapy

Referral is urgent for all suspected or diagnosed cases to high level care equipped with cardiac
catheterization laboratory for Coronary angiogram (CAG) followed by Percutenous Coronary
Intervention (PCI).
20.5 Hypertension
Hypertension is elevation of Blood Pressure SBP ≥ 140 mmHg and DBP ≥90 mmHg measured
atleast three separate occasions. Hypertension is a major independent risk factor for the
development of CAD, stroke, and renal failure.

Diagnostic Criteria
Blood Pressure should be measured on three separate occasions, a minimum of 2 days apart and/or
taken over period of two months. Minimum of 3 blood pressure readings must be taken at the first
visit to confirm hypertension.
Ambulatory Blood Pressure monitoring should be done to exclude Masked or white coat hypertension
and monitoring of Blood Presure response to anti-hypetensives.

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Table 20.3: Classification of Hypertension
Class of SBP DBP Confirm diagnosis
hypertension mmHG mmHg
Grade 1 140-159 90-99 After 3 months of life style modification
Grade 2 160-179 100-109 Same visit
Grade 3 >180 >110 Same visit

Consider secondary hypertension with identifiable cause in young patients < 40 years or elderly
patient > 60 years presenting for first time with hypertension.

Note
• Recommend an alternative contraceptive method for women using oestrogen containing oral
contraceptive.
• Evidence of end organ damage, i.e. cardiomegaly, proteinuria or uraemia, retinopathy or
evidence of stroke, dictates immediate treatment.

Treatment goal of Hypertension


• In patients aged 18 - 59 years without major comorbidities, and in patients 60 years or older
who have diabetes, chronic kidney disease (CKD), or both conditions, the blood pressure goal
level should be <140/90 mm Hg.
• In patients aged 60 years or older who do not have diabetes or chronic kidney disease, the
blood pressure goal level should be <150/90 mm Hg.

Non-pharmacological Treatment
Lifestyle modification:
• Lifestyle modification (refer to table 20.2)
Assess or stratify according to risk factors and target organ damage see figure 20.1 below.

Figure 20.1:Non-Pharmacological Management flow diagram of hypertension

Pharmacological Therapy
First-line treatment without compelling indications, Thiazide diuretics should be initiated.
Combination therapy may be considered if SBP >20mmHg or DBP> 10mmHg above target.

Refer Figure 20.2, Algorithm II and Table 20.4 below show choice of anti-hypertensives.

449
Figure 20.2: Approach of Pharmacological Treatment of hypertension in Primary Healthcare
Facility.

450
Figure 20.3: Approach of Pharmacological Treatment in Hypertensive Emergency and
Hypertensive Urgency.

451
Table 20.4: Compelling Indications and Anti-Hypertensive Drug Combination
Compelling indications Drug class
Angina • ß–blocker or Long-acting calcium channel blocker
Prior or Post–myocardial • ß–blocker and ACEI or ARB if patient sensitive to ACEIs
infarct •If ß–blocker contraindicated: Long-acting calcium channel blocker
eg Verapamil Sustained Release / Diltiazem Extended Release.
Heart failure • ACE inhibitor and ß–blocker eg carvedilol
Volume overload • Diuretics–Loop diuretics eg furosemide and/or spironolactone
*(exclude Renal Failure before adding spironolactone)
Left ventricular hypertrophy ACE inhibitor or ARB if patient sensitive to ACEIs
(confirmed by ECG or
Echocardiography)
Stroke: secondary Hydrochlorothiazide or Indapimide and ACE inhibitor
prevention
Diabetic mellitus ACE inhibitor or ARB, usually in combination with diuretic
Chronic kidney disease ACE inhibitor, usually in combination with diuretic
Isolated systolic Hydrochlorothiazide or Long-acting calcium channel
hypertension Blocker
Pregnancy Labetalol, Nifedipine, Methyldopa or Hydralazine (Avoid ACEI/ARB
due to teratogenic effect)
Prostatism alpha–blockers
Elderly Calcium channel blocker CCB

Anti-hypertension therapy:
Thiazide diuretics: Refer Figure 20.2, Step2 above

Loop diuretics
B: furosemide initial dose (PO) 40mg 12hourly
OR
S: torsemide (PO) 2.5mg /5mg/10mg 24hourly
Dose can be up scaled depending on congestive status to maximum dose

Mineralocorticoid (Aldosterone) Receptor antagonist


C: spironolactone (PO) 25mg 24hourly
OR
S: eplerenone (PO) 25mg 24hourly

Angiotensin Converting Enzyme Inhibitor (ACEI)


B: captopril (PO) 6.125mg, 12.5mg or 25mg 8hourly
OR
C: enalapril (PO) 10mg 12hourly

Angiotensin Receptor Blocker–ARB (*Do not combine with ACEI, indicated in patient sensitive to
ACEIs)
C: losartan (PO) 25mg/50mg 24hourly
OR
S: candesartan (PO) 8mg/16mg 24hourly
OR
S: telmisartan (PO) 40mg / 80mg 24hourly
OR
S: irbesartan (PO) 150mg / 300mg 24hourly

Note
The prescription of ARBs should depend on patient’s presenting conditions

Beta blocker (Beta 1 selective Beta Blocker)


B: atenolol (PO) 25mg /50mg/ 100mg 24hourly
OR
C: metoprolol succinate (SR) (PO) 50- 200mg 24hourly
OR
S: metoprolol injection (IV) 1mg/ml in 5ml stat
OR
S: bisoprolol (PO) 2.5mg – 10mg 24hourly

452
Beta blocker (Non-selective Beta)
A: propranolol (PO) 40mg 24hourly
OR
C: carvedilol (PO) 6.25mg/12.5mg 24hourly
OR
C: labetalol (PO) 100mg 24hourly
OR
C: labetalol injection (IV) 5mg/ml in 2ml or 10mg/ml

Calcium Channel Blocker


Dihydropyridines:
B: nifedipine (PO) 10mg/20mg 24hourly
OR
B: nifedipine (Slow Release/Long Acting) (PO) 20mg/30mg/ 60mg/90mg/daily
OR
C: amlodipine (PO) 5mg or 10mg 24hourly
OR
S: nimodipine (PO) 30mg 24 hourly (indicated in subarachnoid hemorrage, less
anti-hypertensive effect)
Non–dihydropyridine
S: verapamil (PO) 30mg 8-12hourly for 24hours
OR
S: verapamil (Sustained Release) (PO) 120mg 24hourly (Initial daily dose),
Maximum dose: 120mg 12hourly (single dose should not exceed 240mg)
OR
D: diltiazem (Extended Release) (PO) 60mg / 120mg 24hourly
OR
D: diltiazem (PO) 30mg 8-12hourly for 24hours

Alpha-2 adrenergic agonists


A: methyldopa (PO) 250mg 24hourly
OR
S: clonidine (PO) 50mcg/100mcg 24hourly
Alpha-1 adrenergic blockers
S: doxazocin (PO) 1mg / 2mg 24hourly
OR
D: tamsulosin (PO) 0.4mg24hourly

Vasodilators
B: hydralazine (PO) 25mg 8hourly
OR
C: hydralazine (IV) 20mg/ml in 1ml injection
OR
S: nitroglyceride/glyceryl trinitrate Injection (IV) 50mg/ml in 10ml

Fixed Dose Combination (Poly Pills) - FDCs


C: losartan + hydrochlorothiazide (FDC) (PO) 50mg/12.5mg
OR
S: candersatan+hydrochlorothiazide (FDC) (PO) 16/12.5 mg
OR
S: telmisartan + hydrochlorothiazide (FDC) (PO) 40/12.5mg, 80/12.5mg
OR
S: irbersatan + hydrochlorthiazide (FDC) (PO) 150/12.5mg

Referral indicated when:


• Resistant (Refractory) hypertension suspected,
• Secondary hypertension is suspected
• Complicated hypertensive urgency/emergencies,
• Hypertension with Heart failure.
• When patients are young (<30 years).
• Blood pressure is severe or refractory to treatment.

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20.6 Resistant (Refractory) Hypertension
Hypertension that remains >140/90mmHg despite the use of 3 antihypertensive drugs in a rational
combination at full doses and including a diuretic i.e. thiazide. Consider all correctable causes of
refractory hypertension before you refer.

20.7 Hypertensive Urgency


Symptomatic severe hypertension SBP 180mmHg and/or DBP >110 mmHgwithout evidence of
target organ damage, such as pulmonary edema, cardiac ischemia, neurologic deficits, or acute renal
failure.

Note
All patients with hypertensive urgency should be treated in hospital

Pharmacological Treatment
The goal is to lower DBP to 100mmHg slowly over 48–72hours. This can be achieved with two or
more oral agents preferably, Refer to Figure 20.3.

20.8 Hypertensive Emergency


A marked elevated systolic blood pressure SBP≥180mmHg and/or a diastolic DBP≥130mmHg
associated with life threatening situations (target end organ damage) one or more of the following:
• Unstable angina/myocardial infarction
• Hypertensive encephalopathy e.g. severe headache, visual disturbances, confusion, coma,
or seizures which may result in cerebral haemorrhage
• Acute left ventricular failure with severe pulmonary oedema (extreme breathlessness at
rest)
• Excessive circulating catecholamine: e.g. pheochromocytoma – rare cause of emergency;
food or drug interaction with monoamine oxidase inhibitors
• Rapidly progressive renal failure
• Acute aortic dissection
• Eclampsia and severe pre-eclampsia

Pharmacological Treatment
C: labetolol (IV) 20–80mg bolus every 10 minutes or 0.5–2mg/min infusion stat 20 mg, then
20–80 mg every10 min as needed, or stat with 0.5 mg/min infusion, then 1–2 mg/min (may be
up to 4 mg/min) IV infusion up to 300 mg/d max.
Onset: 5–10 min; duration: 3–6 hours
AND / OR
S: nitroglycerin (glyceryl trinitrate; highly effective in setting of coronary ischemia, acute
coronary syndromes. Dose is (IV) 5–100µg/min as infusion
S: nitroglycerin (IV) initially 5–10 ug/min then may be up to >200 ug/min as needed
Onset: immediate; Duration: 1–5 minutes
AND / OR
C: hydralazine (IV) 5mg slow push over 1–2 minutes, repeat 5–10mg as needed
20.9 Heart Failure
Heart Failure is a clinical syndrome characterized by typical symptoms (e.g. breathlessness, ankle
swelling and fatigue) that may be accompanied by signs (e.g. elevated jugular venous pressure,
pulmonary crackles and peripheral oedema) caused by a structural and/or functional cardiac
abnormality, resulting in a reduced cardiac output and/or elevated intracardiac pressures at rest or
during stress.

Heart Failure in Pregnancy


Symptoms and signs of heart failure in a pregnant woman are an indication for urgent assessment to
establish a diagnosis and appropriate management. This is best accomplished through a
multidisciplinary approach in which both cardiologists and obstetricians need to participate in order to
provide expert counselling and care in pursuit of safe motherhood, as well as to exclude underlying
cause of heart failure.

454
Acute Heart Failure (AHF) or Decompensated Acute Heart Failure (ADHF)
AHF is defined as rapid or gradual onset of signs and symptoms of heart failure that results in urgent
unplanned hospitalization or Emergency Medicine Department visits. The clinical signs and
symptoms are significantly life threatening if the above features occur in patients with established
diagnosis with structurally heart disease categorized as Acute Decompensated Heart Failure
(ADHF). The cause and immediate precipitating factor(s) of the AHF must be identified and treated to
prevent further damage to the heart.

Non-pharmacological Treatment:
Oxygen therapy and/or ventilatory support.
• Non-invasive positive pressure ventilation includes both CPAP and bi–level positive
pressure ventilation (PPV)
• Mechanical ventilation

Note
In AHF, oxygen should not be used routinely in non–hypoxaemic patients, as it causes
vasoconstriction and a reduction in cardiac output

Pharmacological treatment
Recommendations for the management of patients with acute heart failure:

Diuretics: Diuretics are a cornerstone in the treatment of patients with AHF. In patients with new-
onset AHF or those with chronic, decompensated HF not receiving oral diuretics the initial
recommended dose should be 20–40 mg intravenous furosemide (or equivalent); for those on
chronic diuretic therapy, initial intravenous dose should be at least equivalent to oral dose.
Diuretics should either be given as intermittent boluses or as a continuous infusion, and the dose and
duration should be adjusted according to patients’ symptoms and clinical status. Combination of loop
diuretic with either thiazide-type diuretic or spironolactone may be considered
Loop diuretic
B: furosemide (IV) 20–120mg 24hourly
OR
S: torsemide (PO) 5–20mg 24hourly
AND
Mineralocorticoid (Aldosterone) Receptor Antagonists:
C: spironolactone (PO) 25–50mg 24hourly
OR
S: eplerenone (PO) 25–50mg 24hourly

Vasodilators: theseare the cornerstone of treatment of AHF and have dual benefit by decreasing
venous tone (to optimize preload) and arterial tone (decrease afterload). Consequently, they increase
stroke volume
Intravenous vasodilators should be considered for symptomatic relief in AHF with SBP >90 mmHg
(and without symptomatic hypotension). Symptoms and blood pressure should be monitored
frequently during administration of intravenous vasodilators. In patients with hypertensive AHF,
intravenous vasodilators should be considered as initial therapy to improve symptoms and reduce
congestion. Intravenous vasodilators for treating AHF are described in table 20.4.

Note
Vasodilators should be used with caution in patients with significant mitral or aortic stenosis.

Consider oral vasodilators in case intravenous vasodilator not available or unavailability of intensive
care or high dependent unit care.
C: isosorbide dinitrate (PO) 10–20mg 12hourly
OR
B: hydralazine (PO) 25mg 6–8hourly. Maximum dose: 200 mg 24hourly

Inotropes (Inotropic agents): Indicated in patients with hypotension (SBP <90 mmHg or mean
arterial BP < 60mmHg) and peripheral hypoperfusion. Dosage see table 20.5 below.

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Vasopressor (norepinephrine preferably):Indicated in patients with cardiogenic shock, despite
treatment with another inotrope, to increase blood pressure and vital organ perfusion. Dosage see
table 20.5 below

Indication: Patients with cardiogenic shock, despite treatment with another inotrope, to increase
blood pressure and vital organ perfusion.

Table 20.5: Positive inotropes and/or vasopressors for treat acute heart failure.
Inotropes / Bolus Infusion rate
Vasopressors
Dobutamine No 2–20µg/kg/min(beta+)
Dopamine No 3–5 µg/kg/min; inotropic(beta+)
>5 µg/kg/min:(beta+), vasopressor(alpha+)
Norepinephrine No 0.2–1.0µg/kg/min
Epinephrine Bolus:1mg can be given iv during 0.05–0.5µg/kg/min
resuscitation,
Repeated every3–5 min

Other Inotropes & inodilators:


D: digoxin injection (IV) 0.25 mg/mlin 2 ml injection
OR
D: digoxin (PO) 0.125mg / 0.25mg

Special pharmacological treatment consideration:


Add ACEI
B: captopril (PO) 6.25–25mg 8hourly
OR
C: enalapril (PO) 5–20mg 12hourly
OR
C: lisinopril (PO) 5mg – 10mg 24hourly (When patient is out of congestive state)
Add Beta-blocker
C: carvedilol (PO) 6.25–25mg 12hourly a day especially in heart failure with reduced
systolic function

Thrombo–embolism prophylaxis
In Thrombo–embolism prophylaxis, Low Molecular Weight Heparin (LMWH) is recommended in
patients not already anticoagulated and with no contra indication to anticoagulation, to reduce the risk
of deep venous thrombosis and pulmonary embolism.
B: unfractionated heparin (SC) 5,000IU 12hourly
OR
S: Low molecular weight heparin (SC) 40mg–80mg 12hourly
OR
S: Rivaroxaban (PO) 15mg/20mg 24hourly

Note
All patients with AHF should be treated at centre/hospital where at least can perform
Echocardiographic assessment and Intensive Care Units (ICU) or High care dependent Units
(HDUs) are available.

20.10 Chronic Heart Failure


Patients who have had HF as defined above for some time are often said to have ‘Chronic Heart
Failure’. A treated patient with symptoms and signs that have remained generally unchanged for at
least 1 month is said to be ‘Stable chronic heart failure’

Diagnostic Criteria
The diagnosis of chronic heart failure requires the following features:
• Symptoms of heart failure, typically breathlessness or fatigue, at rest or during exertion
• Objective evidence of cardiac dysfunction preferably by Echocardiography (Systolic and/or
Diastolic)
• A clinical response to treatment is supportive but not sufficient for diagnosis.

456
Hence diagnosis and management of CHF should be sought at referral centres where at least
echocardiography assessment can be performed.

Treatment of Systolic Heart Failure (LVEF< 45–50%)


Goals of treatment
• Prevention of disease leading to cardiac dysfunction and heart failure eg hypertension,
coronary artery disease, valve disease etc.
• To achieve maintenance or improvement in quality of life and improve survival

Non-pharmacological Treatment
• Avoid excessive fluid intake in severe HF Limit fluid intake to 1–1.5 L/day if fluid overloaded
despite diuretic therapy.
• Regular exercise within limits of symptoms and other lifestyle modification (refer to table
20.2).

Note
Sexual counselling regarding the risk of pregnancy and the use of oral contraceptives and
phosphodiesterase-5 inhibitors (e.g sildenafil) are not recommended in advanced HF, if used
nitrates should be avoided <24–48hours of nitrate intakes.

Medicines to avoid or to be used with caution.


• NSAIDs & COXIBS
• Class I anti–arrhythmic
• Calcium antagonists
• Lithium
• Tricyclic antidepressants
• Corticosteroid

Pharmacological Treatment (Approach combination therapy)


Diuretics
B: furosemide (PO) 40–80mg 12hourly
OR
S: torsemide (PO) 5–20mg 24hourly
AND
Mineralocorticoid (Aldosterone) Receptor Antagonists:
C: spironolactone (PO) 25–50mg 24hourly
OR
S: eplerenone (PO) 25–50mg 24hourly
Thiazide
D: hydrochlorothiazide (PO) 12.5–25mg 24hourly
OR
S: metolazone (PO) 0.1–10mg 12hourly
Angiotensin Receptor Inhibitors ACEI or Angiotensin Receptor Blockers (ARB)
B: captopril (PO) 6.25–25mg 8hourly
OR
C: enalapril (PO) 5–20mg12hourly
Angiotensin Receptor Blocker–ARB (*Do not combine with ACEI, Indicated in patient sensitive to
ACEIs)
C: losartan (PO) 50mg 24hourly
OR
S: candesartan (PO) 4–16mg 24hourly
Beta blocker (Carvedilol–improve Morbidity & Mortality in CHF).
C: carvedilol (PO) 6.25–25mg twice a day especially in heart failure with reduced systolic
function

Note
Beta Blockers is contraindication to patients with Bronchial Asthma or Severe Pulmonary Disease
Symptomatic bradycardia or hypotension

457
Heart failure in Type 2 Diabetes Mellitus and Non-DM:
S: empagliflozin (PO) 10mg/ 25mg 24hourly

Add on therapy in patient in NYHA class III/IV.


Vasodilator agents: The combination of hydralazine/nitrate
C: isosorbide dinitrate (PO) 10–20mg 12hourly
AND
B: hydralazine (PO) 25 mg 6–8hourly. Maximum dose: 200 mg/day

Cardiac Glycosides–Digoxin, give with caution as has narrow therapeutic index see below under
section of Cardiac Glycosides
D: digoxin (PO) 0.125mg–0.25mg 24hourly

Note
Patients at high risk of digoxin toxicity are: Elderly, patients with poor renal function,
hypokalaemia and low body weight

Anti–thrombotic agents.
Heparin &/or warfarin – firmly indicated on congestive heart hailure with atrial fibrillation, previous
thromboembolic events or a mobile LV thrombus Heparin for DVT prophylaxis for patients admitted to
hospital, unless contraindicated:
B: unfractionated heparin (SC) 5000 units 8hourly
OR
S: low molecular weight heparin (IV) 40-60mg/ml 24hourly
OR
C: warfarin (PO) 5 mg 24hourly (Monitor INR to therapeutic range (2.0–2.5)
OR
S: rivaroxaban (PO) 15-20mg 24hourly

Antidote for heparin


B: protamine (IV) 10ml/ml in 5mls Ampoule/vial.
1mg of protamine sulphate neutralizes approximately 100units of heparin.
Thiamine Supplement: Consider in all unexplained heart failure

Note
• Ideally all patients with CHF should be managed in dedicated HF clinics/units with devoted HF
expert staffs (nurses & doctors) for further evaluation and Device therapy including CRT, CRT-
D and ICD. The following category of patients should be referred for specialized care
o Severe HF class III/IV
o HF of unknown origin
• Relative contraindication: asymptomatic bradycardia, low blood pressure, Intolerance to low
doses, Previous use of ß –blockers and discontinuation because of symptoms, Bronchial
asthma, or severe pulmonary disease.

20.11 Pulmonary Oedema


Diagnostic Criteria
Common cause of pulmonary oedema is cardiac/fluid overload, and the common causes
• Systolic heart failure complicating fluid overload
• Renal failure complicating fluid overload
• Iatrogenic fluid overload
Other Cause of pulmonary oedema
• Increased capillary permeability Acute Respiratory Distress Syndrome (ARDS); many causes
include Systemic sepsis–gram negative infection, pancreatitis, head injury, aspiration of gastric
contents, amniotic embolus.

Non-pharmacological Treatment
Initial management
• Maintain airway, bed rest in Fowler`s position except if hypotensive or comatose.
• Administer oxygen to keep PO2> 60 mmHg (O2 saturation > 90%)

457
• Correct base–acid & electrolyte disorders, determine and correct arrhythmias,

Pharmacological Treatment
Cardiac failure
B: furosemide (IV) 20mg–80mg may be repeated in 10–15 minutes, If symptoms persist,
C: morphine (IV) 1–3mg diluted form,
• Inotropic support if hypotensive SBP <90mmHg,
S: dobutamine (IV) 2–20 µg/kg/min
• Intravenous vasodilator nitroglyceride if SBP > 100mmHg

Non–cardiac (ARDS)
• Treat the underlying conditions
• Ventilate with PEEP – if RF
• Inotropic support if SBP<90mmHg
• Dialysis if renal failure

Note
• All patients suspected with pulmonary oedema should be referred to high level of
care where hospital resourced with high care dependent unit or intensive care unit.
• Patient should be stabilized first at low level of care before referral to the high level
of care.

20.12 Infective Endocarditis (IE)


The infective process of endocardial layer of the heart can involve native or prosthetic valve and
congenital defects/shunts. Alpha–haemolytic streptococci are the most common causes of native
valve endocarditis but Staphylococcus aureus is more likely if the disease is rapidly progressive with
high fever or is related to a prosthetic valve (Staphylococcus epidermidis).

Diagnostic Criteria
Use Modified Dukes Criteria below and consult microbiologist where possible. Three sets of blood
cultures should be taken before starting treatment.

Modified Dukes Criteria


Major Criteria
• Positive blood cultures of typical organism for IE from at least two separate blood cultures
• Evidence of endocardial involvement by echocardiogram (Trans–thoracic Echo/Trans–
oesophageal Echo)
Minor Criteria
• Fever > 38ºC
• Presence of Rheumatic heart disease, congenital heart disease
• Vascular phenomena; Major arterial emboli, septic pulmonary infarcts, mycotic aneurysm,
intracranial haemorrhage, conjuctival hemorrhage, Janeway lesions
• Immunological phenomena; glomerulonephritis, Osler`s nodes, Roth`s spots,
• Rheumatoid factor.
• Serologic evidence of active infective endocarditis or blood culture not meeting major
criterion.

Definition of infective endocarditis according to the modified Duke criteria:


Definitive diagnosis of IE
Pathological criteria
• Microorganisms demonstrated by culture or on histological examination of a vegetation, a
vegetation that has embolized, or an intracardiac abscess specimen
OR
• Pathological lesions: vegetation or intracardiac abscess confirmed by histological
examination showing active endocarditis.

Clinical criteria
• Two major criteria OR
• One major and three minor criteria OR
• Five minor criteria

458
Possible Diagnosis of IE
• One major and one minor OR
• Three minor criteria

Rejected IE
Firm alternate diagnosis.
• Resolution of symptoms suggesting IE with antibiotic therapy for ≤4 days; or
• No pathological evidence of IE at surgery or autopsy, with antibiotic therapy for ≤4 days;
OR
• Does not meet criteria for possible IE, as above.

Note
• Positive blood cultures remain the cornerstone of diagnosis and provide live bacteria for both
identification and susceptibility testing.
• To improve yield of culturing bacteria at least three blood sample sets are taken at 30
minutes apart each containing 10mL of blood and should be incubated in both aerobic and
anaerobic atmospheres.
• Sampling should be obtained from a peripheral vein using a meticulous sterile technique.

Pharmacological Treatment
Empirical Treatment
Consider for negative blood culture or if risk delaying treatment for blood culture outweigh the befit of
starting treatment early

Treatment for native valves:


A: benzyl penicillin G (IV) 18–24milllion Units/24hours 4hourly in equally divided dose 4–
6weeks
OR
B: ceftriaxone (IV) 2g 24hourly 4–6weeks
AND
B: cloxacillin (IV) 2g 6hourly 4–6 weeks
AND
A: gentamicin (IV) 1–1.5mg/kg 8 hourly for at least 2weeks
OR
If methicillin–resistant staphylococci anaerobes (MRSA)
S: vancomycin (IV) 30mg/kg 24 hourly in two equally divided dose, not to exceed 2gm in
24hours unless serum levels are monitored 4–6weeks.

Note
It is important to assay serum gentamicin levels every 3–4days. One–hour peak concentration
should not exceed 10mg/l and trough concentration (2–hour pre– dose) should be less than 2mg/l.

Prosthetic valve empirical treatment


A: benzyl penicillin G (X–Pen) (IV) 18 –24 milllion Units 4 hourly for 24hours in equally
divided dose 6 – 8 weeks
OR
B: ceftriaxone (IV) 2g 24hourly >6 weeks
AND
B: cloxacillin (IV) 2g 6 hourly >6 weeks
AND
A: rifampicin 300 –600mg (IV) 8hourly >6 weeks
AND
A: gentamicin 1mg/kg (IV) 8hourly 2 weeks.
Note
• It is important to assay serum gentamicin levels every 3–4days. One–hour peak concentration
should not exceed 10mg/l and trough concentration (2–hour pre– dose) should be less than
2mg/L.
• Gentamycin in renal failure should be given based on CrCl.
• Patients with complicated IE should be evaluated and managed in high level of care or centre,
with immediate surgical facilities and the presence of a multidisciplinary including an Infectious
Disease specialist, a microbiologist, cardiologist, imaging specialists, and cardiac surgeons

459
Infective Endocarditis Prophylaxis
• Antibiotic prophylaxis should be considered for patients at highest risk for IE:
• Patients with any prosthetic valve, including a trans catheter valve, or those in whom any
prosthetic material was used for cardiac valve repair.
• Patients with a previous episode of IE.
• Patients with Congenital Heart Disease (CHD):
I. Any type of cyanotic CHD.
II. Any type of CHD repaired with a prosthetic material, whether place surgically or by
percutaneous techniques, up to 6 months after the procedure or lifelong if residual
shunt or valvular regurgitation remains.

Note
Antibiotic prophylaxis is not recommended in other forms of valvular or CHD.
Prophylaxis of Endocarditis Infective
• To reduce the risk of bacterial endocarditis, antibiotic prophylaxis should be given to patients
undergoing dental procedures requiring manipulation of the gingival or periapical region of the
teeth or perforation of the oral mucosa.

Antibiotic prophylaxis is not recommended for,


• Respiratory tract procedures including bronchoscopy or laryngoscopy, or trans nasal or
endotracheal intubation
• Gastrointestinal or urogenital procedures or Trans–oesophageal Echocardiogram, gastroscopy,
colonoscopy, cystoscopy, vaginal or caesarean delivery.
• Skin and soft tissue procedures

Table 20.6: Recommended prophylaxis for high–risk dental procedures in high-risk patient
Single–dose 30–60 minutes before procedure
Situation Antibiotic
Adults Children
No allergy to penicillin or amoxicillin or 2g (PO/IV) 50 mg/kg (PO/IV)
ampicillin ampicillin*
Allergy to penicillin or ampicillin clindamycin 600 mg (PO/IV) 20 mg/kg (PO/IV)

*Alternatively, B: ceftriaxone (IV) 1g for adults or 50 mg/kg for children. Cephalosporins should not be
used in patients with anaphylaxis, angio–oedema, or urticaria after intake of penicillin or ampicillin
due to cross–sensitivity.
20.13 Acute Rheumatic Fever
It is a non–suppurative sequela of a group A ß haemolytic streptococcal (GABHS) pharyngeal
infection.

Diagnostic Criteria Jones See table 20.7 below


Definitive Diagnosis
• Two major criteria or
• One major criterion with two minor criteria, with evidence of antecedent streptococcal
infection

Table 20.7: Criteria for Acute Rheumatic Fever Diagnosis


Major Criteria Minor Criteria
1. Carditis 1. Clinical
2. Migratory polyarthritis • Fever
3. Sydenham’s chorea • Arthralgia
4. Erythema Marginatum 2. Laboratory
• Elevated Acute Phase Reactants eg CRP
• Prolonged PR interval
Plus
Supporting evidence of recent group, A streptococcal infection e.g. positive throat culture or antigen
detection and/or elevated streptococcal antibody tests*
*anti –streptolysin O, anti –deoxyribonuclease B

460
Non–pharmacological Treatment
Acute stage:
• Bed rest and supportive care until all evidence of active carditis has resolved
• Patient education.
• Intensive health education for prevention of sore throats.

Pharmacological Treatment
Treatment of acute attack for eradication of streptococci in throat: Regardless of the presence or
absence of pharyngitis at the time of diagnosis.
A: benzathine penicillin (IM) 1.2MU stat
Paediatric> 5 years 0.3MU, 5–10 years 0.6 MU > 10 years 1.2 MU stat
OR
A: penicillin V (PO) 500mg 8-12 hourly 24 hourly for 10days
Children > 10years 500mg, 5–10 years 250mg, < 5years 125mg (PO) 8-12 hourly for 10
days

Patients allergic to penicillin


A: erythromycin (PO) 500mg or 40mg/kg 6hourly for 10days.

Treatment of Acute Arthritis and Carditis:


A: acetylsalicyclic acid (PO) 25mg/kg 6hourly 24hourly as required.
Acetylsalicyclic acid should be continued until fever, all signs of joint inflammation and
the ESR have returned to normal and then tapered gradually over 2 weeks. If symptoms
recur, full doses should be restarted. *dose should be reduced if tinnitus or other toxic
symptoms develop

In severe carditis with development of increasing heart failure or failure of response to aspirin, Add

A: prednisolone (PO) 1–2mg/kg 24hourly for 3–4weeks

Then review and gradual reduction and discontinuation of prednisolone may be started after 3–4
weeks when there has been a substantial reduction in clinical disease.

Heart failure should be managed in the usual way (see Heart Failure Section 20.9).

Treatment of Sydenham’s chorea:


B: haloperidol(PO) 1.5–3mg 8hourly for 24 hours as required (Adult).
Paediatrics 50µg/kg for 24 hours in 2 divided doses.

Referral: Ideally all patients should be referred to high level of care a specialized hospital care,
where surgery is contemplated

Antibiotic prophylaxis after rheumatic fever


Prophylaxis should be given to all patients with a history of acute rheumatic fever and to those with
rheumatic heart valve lesions. The optimum duration of prophylaxis should be up to at least 21years
of age.

Note
Specific situations requiring prophylaxis for longer periods (up to 30years as a guide):
• definitive carditis in previous attacks
• high risk of exposure to streptococcal infection at home or work (crowded conditions,
high exposure to children)

Medicine of choice
A: benzathine penicillin (IM) 2.4MU monthly or every three weeks*
Paediatrics <12yrs 1.2MU every 4 weeks or 3 weeks* up to 21–30yrs
OR
A: phenoxymethylpenicillin (PO) 250mg 12hourly Adult
Paediatric<12yr 125–250mg 12hourly for 24hours up to 21–30years
OR
A: erythromycin (PO) 250mg 12hourly for 24hours Adult

461
Paediatric <12yr 125–250mg 12hourlyfor 24hours up to 21–30yrs*every 3week regimen is
more effective
Valvular Heart Disease and Congenital Structural Heart Disease
Valvular Heart Disease are chronic acquired sequelae of Acute Rheumatic Fever or Acute Sequelae
of Infective Endorcaditis or Ischaemic Heart Disease, consisting of valvular damage, usually left heart
valves, with varied progression of severity and complications.
Congenital Heart Disease is a congenital chamber defects or vessel wall anomalies
Valvular Heart Disease and Congenital Structural Heart Disease may be complicated by:
• Heart failure
• Infective endocarditis
• Atrial fibrillation
• Systemic embolism eg Stroke

General measures
• Advise all patients with a heart murmur regarding the need for prophylaxis treatment prior
to undergoing certain medical and dental procedures.
• Advise patients to inform health care providers of the presence of the heart murmur when
reporting for medical or dental treatment

Referral: Should be considered from low level of care to high level of care where specialized
(physician`s care) or super–specialized care (Cardiologist`s care) can be offered
20.14 Pulmonary Embolism
20.14.1 Acute Pulmonary Embolism
Clinical Spectrum less than two weeks
• Sudden onset of dyspnoea often with unexplained anxiety (most common)
• Pleuritic chest pain and haemoptysis
• Massive embolism: pleuritic chest pain, cyanosis, right heart failure and shock. Minor
emboli or pulmonary infarction may herald massive embolism and must be treated
vigorously
• About 90% of emboli are from proximal leg deep vein thromboses (DVTs) or pelvic vein
thromboses. DVTs are at risk for dislodging and migrating to the lung circulation. Thus,
termed as venous thromboembolism (VTE).

Diagnostic Criteria
Determination pre-test probability of PE
Use validated scoring system: Wells Score
• Score > 6.0–High clinical probability proceeds with imaging test to confirm PE and treat,
• Score 2.0 to 6.0–Moderate clinical probability; negative D–dimer, PE is excluded and D–
dimer positive, obtain imaging tests to confirm based on result treat.
• Score < 2.0–Low clinical probability negative D–dimer, PE is excluded. Positive D–dimer
obtain imaging tests to confirm or rule out and based on result treat

Alternatively
• Score > 4–PE likely, d–dimer positive proceeds with diagnostic imaging to confirm and treat
PE.
• Score 4 or less–PE unlikely, consider d–dimer to rule out PE.

Table 20.8: Wells Score


Variable Score
Clinically suspected DVT 3.0 points
alternative diagnosis is less likely than PE 3.0 points
Tachycardia (heart rate > 100) 1.5 points
Immobilization (≥ 3d)/surgery in previous four weeks 1.5 points
History of DVT or PE 1.5 points
Hemoptysis 1.0 points
Malignancy (with treatment within six months) or palliative 1.0 points

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• ECG – Not reliable test for diagnosis may be normal. However,
• Sinus tachycardia most common feature, acute right ventricular strain – i.e. right axis shift,
S1Q3T3 occurs in small percentage of cases, may develop acute bundle branch block –
right or left, may simulate right ventricular infarction, may develop arrhythmias – eg atrial
fibrillation
• Arterial blood gases; not diagnostic, the pO2 decreased <60mmHg due ventilation/perfusion
mismatch. pCO2 decreased due to hyperventilation, pH increased but may decrease in
shocked patient
• D–dimer test – very sensitive blood test, but not specific. A negative test d–dimer test
excludes an embolus in majority of cases (best exclusive test to rule out PE when is
negative)
• Chest X–ray – Not very reliable usually normal, diaphragm may be raised on affected area,
atelectasis may occur, peripheral wedge–shaped shadow & plural effusion
• Cardiac Echocardiography: Useful in diagnosis, features suggestive or support
• evidence of massive embolus acute right ventricular strain
• Computer Tomography Pulmonary Angiogram Scan (CTPA); Useful can demonstrate the
presence and extent of proximal pulmonary emboli
• Ventilation/Perfusion Scan; Useful in stable patient to confirm the diagnosis. The presence
of a perfusion defect with normal ventilation not corresponding to an x–ray abnormality is
characteristic
• Pulmonary Angiography: Still gold standard investigation, may be necessary to establish
• Diagnosis and catheter-based embolectomy in the catheterization lab.

Non-pharmacological Treatment
• Administer O2 – maintain pO2 > 60mmHg,
• Treat shock
• Correct electrolyte & acid base abnormalities and arrhythmias
• Ventilate if patient in respiratory failure

Pharmacological Treatment
Anticoagulation
B: unfractionated heparin (UFH) (IV) 10,000units then maintenance infusion starts with
6,000U over 6 hours to keep PTT or clotting time 2–3times above baseline. PTT should
be performed 12hourly per lab instruction.
OR
S: low molecular weight heparin (SC) 1mg/kg 12hourly for 24hours

Start warfarin after 24hours of heparin and continue post discharge for long–term. If the aetiology
unknown may be for life, if aetiology is established at least for six months. Maintain INR 2.0–3.0

Thrombolytic (Fibrinolysis)
Indicated in proximal massive pulmonary emboli and haemodynamically unstable if no
contraindication exists
S: streptokinase (IV)250,000IU over 30minutes, then 100,000IU per hour for 24hours
OR
S: alteplase (rtPA) (IV) 100mg over 2hours

Referral: All cases suspected of pulmonary embolus should be referred to a high level of care –
specialized hospital care with HCDU/ICU

20.14.2 Chronic Pulmonary Embolism


Chronic pulmonary embolism is mainly a consequence of incomplete resolution of acute pulmonary
thromboembolism. Clinically symptoms and signs may be preceded by Acute Pulmonary Embolism
for more than 2weeks.

Pharmacological Treatment
Long-term oral anticoagulation
C:warfarin(PO) 2–10mg 24hourly
OR
S: rivaroxaban (PO) 15-20mg 24hourly

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Maintain INR 2.0–3.0 for warfarin use individuals.

Referral: All cases suspected of pulmonary embolism should be referred to a high level of care
20.15 Cardiac Arrhythmias/ Dysrhythmias
Always exclude underlying structural cardiac disease in all patients with cardiac dysrhythmias as well
as performing Holter ECG monitoring aiding at detecting type of arrhythmia.

20.15.1 Tachyarrythmias
20.15.1.1 Narrow QRS Complex Tachyarrythmias (SVTs)
Definition Sustained (> 30 seconds) or non–sustained narrow QRS (≤ 0.1 seconds) tachycardias.

Atrial Fibrillation
Acute onset (< 48 hours)
• Assess clinically, e.g. heart failure, mitral stenosis, thyrotoxicosis, hypertension, age and
other medical conditions.
• Consider anticoagulation with heparin or warfarin.
• Synchronized DC cardioversion is occasionally necessary in emergency especially
haemodynamic instability or consider if is the first episode.

Non-acute/chronic (> 48 hours)


• As above, but not immediate DC cardioversion is indicated, unless in hypotensive
emergency cases. Anticoagulation with oral warfarin 2-5mg orally once a day for at least a
month, then perform elective cardioversion at specialized hospital.

Atrial flutter
• P waves visible before QRS, commonly occurs, usually 2:1. (150 per minute). P waves,
usually negative in Lead II precede QRS, blocked P in ST segment or hidden by QRS.
• Vagal stimulation with ECG may reveal blocked P waves.

AV Junctional Re-Entry Tachycardias


Usually paroxysmal, often young with normal heart.
• AV nodal re-entry or WPW syndrome. P waves usually not visible (hidden by QRS).

Non-pharmacological Treatment
Electrical Cardioversion.
Synchronized DC cardioversion, 200 J, after sedation with:
A: diazepam (IV)10–20 mg stat
If flutter has been present longer than 48hours, defer cardioversion for 4weeks after anticoagulation
with warfarin, unless severe symptoms or heart failure requires urgent cardioversion.

Pharmacological Treatment
None is nearly as effective as DC cardioversion.
Consider anticoagulants if Atrial flutter sustained.
Long term treatment: Recurrent atrial flutter is an indication for referral. Many can be cured by
radiofrequency catheter ablation.
Atrial tachycardias
• Rare, often incessant P before QRS (often long PR) or hidden in T
• May cause heart failure (tachycardia cardiomyopathy).

Atrial fibrillation
I. With fast ventricular response without abberant conduction.

Pharmacological Treatment, Initial:


Anticoagulation with warfarin
OR
S: rivaroxaban (PO)15-20mg 24hourly (in Non-valvular AF)
Rate control (Control the ventricular rate with one of the following):
D: digoxin (IV) Initial dose: 0.25-0.5mg; then 0.25mg 4-6hourly to maximum of 1mg;
Maintenance dose: 0.125-0.25mg 24hourly (IV) or (PO) (Digoxin0.25mg (PO) daily; use
only in heart failure).

464
OR
B: atenolol (PO) 50–100mg 24hourly (contraindicated in asthmatics).
OR
D: diltiazem (IV) initial dose: 15-20mg over 2minutes; may repeat in 15 minutes,
Maintenance dose: 5-15mg hourly by continuous IV infusion
OR
S: verapamil (IV) 5 to 10 mg over 2minutes; may repeat in 30minutes

DC cardioversion in selected cases, after 4weeks of anticoagulation

Digoxin only controls rate at rest and is insufficient on its own. If used for long-term, combine with β –
blocker:
D: digoxin (PO) 0.125-0.25mg 24hourly

In the elderly and patients with renal impairment: Adjust dosages according to trough levels within the
therapeutic range. Do levels only if the patient has been on the drug for at least 10 days.
AND / OR
B: atenolol (PO) 50–100 mg 24hourly
OR
S: bisoprolol (PO) 2.5mg – 10mg 24hourly
OR
C: metoprolol (PO) 25mg -50mg 24hourly
OR
S: sotalol (PO) 80mg – 160mg 12hourly

Note
Avoid use of Digoxin in patients with Accessory pathway.

II. With fast ventricular response with Aberrant conduction (eg: Wolff-Parkinson-White
syndrome, WPW)
Catheter ablation of the accessory pathway in symptomatic patients with preexcited AF, especially if
the accessory pathway has a short refractory period that allows rapid antegrade conduction.
Long – term
• Continue warfarin anticoagulation long-term, unless contraindicated:
C:warfarin (PO) 5mg 24hourly
OR
S: rivaroxaban (PO) maintance dose; 15mg / 20mg 24hourly
OR
Left atrial appendage occlusion (LAAO).

Note
• INR monitoring in patients on warfarin. Maintain therapeutic Range INR 2–3: Stable patients
check 3 monthly. If INR < 1.5 or > 3.5: do monthly monitoring.
• Left atrial appendage occlusion (LAAO) is indicated in Atrial Fibrillation patients who can not
tolerate long-term Anticoagulantion or contraindicated to OACs (Oral anticoagulants) and
have thrombo-embolic risk (CHA2DS2-VASc score ≥2), increased risk of bleeding (HASBLED
score ≥ 3) and thrombo-embolic events despite adequate OAC after excluding other
plausible causes (eg carotid disease).

20.15.2 AV Junctional Re-Entry Tachycardias


Non-pharmacological Treatment
Vagal manoeuvres: Valsalva or carotid sinus massage. The patient should be supine and as relaxed
as possible, to avoid competing sympathetic reflex

Pharmacological Treatment
If vagal manoeuvres fail:
S:adenosine (IV) 6mg over 1-3 seconds (maybe given IO) followed by rapid flush with
20mL NS, if no conversion within 1-2minutes give 12mg, repeat a second time if necessary
(30mg total)
If none of the above is effective, and patient is hypotensive, consider DC shock

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Prevention of recurrent paroxysmal atrial fibrillation
Only in patients with severe symptoms despite the above measures:
S: amiodarone (PO) 200mg 8hourly for 1week, followed by 200mg 12hourly for one
week and thereafter 200mg 24hourly. Specialist initiated.

Precautions:
• Halve dosage of warfarin and monitor INR closely if patient on warfarin, until stable
• Avoid concomitant digoxin use.

Note
Verapamil and digoxin are contraindicated in WPW syndrome.

Long-term treatment: Teach the patient to perform vagal manoeuvres, Valsalva is the most
effective. For infrequent, non–incapacitating symptoms:

ß –Blockers
B: atenolol (PO) 50–100mg 24hourly (If asthmatic)
OR
S: verapamil (PO) 80–120mg 8hourly for 24hours (Normal heart)

Referral: Refer to Cardiac specialized center for Mapping and Radiofrequency Ablation (RFA)

20.15.3 Wide QRS (Ventricular) Tachyarrhythmias (VTs)


Sustained (> 30 seconds) or non-sustained wide QRS (> 0.12 seconds) tachycardias

Regular Wide QRS Tachycardias


These are ventricular tachycardias until proved otherwise. Regular wide QRS supraventricular
tachycardias are uncommon.

Non-pharmacological Treatment
Refer all cases after resuscitation and stabilization. Emergency DC cardioversion is mandatory with a
full protocol of Cardiopulmonary Resuscitation (CPR)
• If no cardiac arrest: DC cardioversion, 200J, after sedation with: Diazepam, I.V, 10–20mg If
200J fails, use 360J.
• If cardiac arrest: Defibrillate (not synchronized).

Pharmacological Treatment
DC cardioversion is first line therapy for regular wide QRS tachycardias.
Medicines are needed if VT recurs after cardioversion or if spontaneous termination/recurrence.
S: amiodarone (IV) 5mg/kg (150-300mg) infused over 30minutes then continue with
maintenance dose to total dose of 1200mg/24hours
OR
S: amiodarone (PO)800 mg 24hourly for 7days, 600mg/day for 3days followed by a
maintenance dose of 200–400mg/day

Amiodarone may cause serious long-term side effects due to long half-life. Therefore, patients
require regular monitoring by specialist.
A: lidocaine (IV) 50–100mg (1–2mg/kg) initially and at 5minute intervals if required to a total
of 200–300mg,
Thereafter, for recurrent ventricular tachycardia only
A: lidocaine (IV)1–3mg/minute for 24–30hours. lidocaine will only terminate ± 30% of
sustained ventricular tachycardias, and may cause hypotension, heart block or convulsions.

Note
• Never give verapamil IV to patients with a wide QRS tachycardia.
• For emergency treatment of ventricular tachycardia, DC cardioversion is first–line therapy,
even if stable.

Sustained (> 30 Sec) Irregular Wide QRS Tachycardias


They are usually due to atrial fibrillation with bundle branch block, or pre-excitation (WPW syndrome).

466
Non-pharmacological/Pharmacological Treatment
• If the QRS complexes have a pattern of typical right or left bundle branch block, with a rate
< less than 170/minute, treat as for atrial fibrillation. See the section on atrial fibrillation.
• If the rate is > 170 per minute, and/or the complexes are atypical or variable, the likely
diagnosis is WPW syndrome with atrial fibrillation, conducting via the bypass tract, DC
conversion.

Referral: Refer patient to high care centre for further management including arrhythmia mapping and
RFA

Non-Sustained (< 30 Sec) Irregular Wide QRS Tachycardias


They are usually ventricular, commonly in acute myocardial infarction. In acute myocardial infarction,
only treat non–sustained ventricular tachycardia if causes significant haemodynamic compromise.
Ensure the serum potassium level is above 4 mmol/L.

Pharmacological Treatment
Medicines are needed if VT recurs after cardioversion or if spontaneous termination/recurrence.
S: amiodarone (IV) 5 mg/kg (150-300mg) over 30minutes then continue with maintenance
dose to total dose of 1200mg for24hours
OR
S: amiodarone (PO) 800mg 24hourly for 7days, followed by 600mg 24hourly for 3 days
then a maintenance dose of 200–400mg 24hourly

Only in a haemodynamically stable patient:


A: lidocaine (IV) 50–100mg (1–2mg/kg) initially and at 5minute intervals if required to a total
of 200–300mg
Thereafter, for recurrent ventricular tachycardia only:
A: lidocaine (IV) 1–3mg/minute for 24–30hours
In the absence of acute ischaemia or infarction, consider torsade’s de pointes.

Torsade’s De Pointes Ventricular Tachycardia (VT)


• Has a twisting pattern to the QRS complexes and a prolonged QT interval in sinus rhythm,
it is usually due to a QT–prolonging drug, ± hypokalaemia.

Non-pharmacological Treatment
• Cardioversion/defibrillation, as necessary.
• Torsade’s complicating bradycardia: temporary pacing

Pharmacological Treatment
Stop all QT-prolonging drugs. Correct serum potassium.
A: magnesium sulphate (IV) 2g over 5–10minutes
If recurrent episodes after initial dose of magnesium sulphate:
A: magnesium sulphate (IV) 2g over 24hours
Torsade’s complicating bradycardia: temporary pacing.
A: adrenaline infusion to raise heart rate to >100 per minute
(if temporary pacing unavailable).
Referral: Refer all cases of wide QRS tachycardia, after resuscitation and stabilization for possible
arrhythmia mapping and RFA.

20.16 Heart Block (Second and Third Degree)


Most cases occur in patients over 60 years and is idiopathic. Acute, reversible AV block commonly
complicated by inferior myocardial infarction, here temporary Pacemaker used as bridge therapy.
The condition may also be induced by medicines, metabolic and electrolyte derrangments.

Non-pharmacological Treatment
• Emergency cardio-pulmonary resuscitation.
• External pacemaker should be available in all secondary hospitals and must be preceded
by appropriate analgesia.

Pharmacological Treatment
Analgesia if external pacemaker:

467
C: morphine (IM)10–15mg 3–6hourly

For Temporary treatment of complete AV block before referral for pacemaker:


A: atropine (IV) bolus 0.6–1.2mg every 3 – 5min (max 3mg) may be repeated until a
temporary or permanent pacemaker is inserted.
(Use in an Inferior Infarct patients, hypotension, and second-degree AV block).
For resuscitation of asystole:
A: adrenaline (IV) 1:10000, slow 5mL (0.5mg)

Referral
• All cases with a heart rate below 40 beats/minute after resuscitation and stabilization to
high level of care where permanent pacemaker implantation can be performed.
• All cases of second or third-degree AV block, whether myocardial infarct or other reversible
cause is suspected, and whether the patient is thought to be symptomatic.

Note
Complete Heart Block Is a Medical Emergency Refer Urgently

20.17 Sinus Bradycardia & Sinus Arrest


This rhythm does not require treatment, unless they are causing symptoms, i.e. syncope, dizziness,
tiredness, and poor effort tolerance. Sinus bradycardia <50/minute or sinus arrest with slow escape
rhythm, accompanied by hypotension, strongly suggests a treatable underlying cause:
• Acute inferior myocardial infarct
• Hyperkalaemia, especially if wide QRS and/or peaked T waves
• Drugs, especially combination of verapamil and ß –blocker or digoxin
• Hypothermia
• Hypoxia
Treat the cause. Consider atropine if inferior infarct.

Note
• Refer the patient After stabilization to the Cardiac Specialized centre for thorough
evaluation and Pacemaker Implantation [Temporary/Permanent Pacemaker
Implantation (single or Dual chamber) depending on the underlying cause], prepare
Vancomycin injection for sterilization of Permanent Pacemaker pouch.

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CHAPTER TWENTY-ONE
KIDNEY AND UROLOGICAL DISORDERS

These are disorders resulting from structural malformation or function of the genitourinary system that
may lead to kidney impairment. These disorders include diseases originating from the kidney and
systemic diseases, which result in complications affecting the kidney. Hypertension and diabetes
mellitus are the commonest conditions causing complications in the kidney, therefore all patients with
hypertension and diabetes mellitus should be regularly screened for kidney complications.

21.1 Chronic Kidney Diseases (CKD)


It is structural or functional kidney damage present for >3months, with or without a decreased
glomerular filtration rate (GFR). Early screening in high-risk groups [hypertension, Diabetes and
glomerular diseases] is crucial in improving outcome of CKD. Once cause and plan for care has been
established, adults with early CKD stages 0-3 can be managed at primary care level.

Clinical Presentation
Clinical features depend on the stage of kidney disease. In advance stage includes:
• Anorexia • Vomiting
• Malaise • Oliguria/anuria

Investigations
• Kidney function tests (serum creatinine and urea) - at diagnosis check every month for
3months. If active sediment/proteinuria, provider may check more frequently
• FBC (HB)
• Urinalysis (Protein, red blood cells and cast cells) then quantify the amount of protein in
urine by Esbach test or Urine albumin-creatinine ration or Urine protein-creatinine ratio
• Kidney-Ureter-Bladder (KUB) ultrasound
• CXR
• ECG
• Serum electrolytes Potassium, Calcium Phosphate and Sodium [CKD stage 3-5: Check
monthly]
• Serum albumin (for corrected calcium)
• Serum bicarbonate levels (venous) [CKD stage 3-5: Check monthly]
• Parathyroid hormone levels, Serum Phosphate and Alkaline phosphatase (ALP) [CKD
stage 5 on dialysis]

Note
Cause of CKD should be determined and addressed. Especially when thinking of kidney
transplantation
The general management of the patient with chronic kidney disease involves the following issues
• Treatment of reversible causes of kidney dysfunction
• Preventing or slowing the progression of kidney disease
• Treatment of the complications of kidney dysfunction
• Identification and adequate preparation of the patient in whom kidney replacement therapy
will be required

Table 21.1: Staging of kidney disease for adequate management of CKD stage/glomerular
filtration rate (GFR*) (ml/minute/1.73)

Stage Description Action Includes actions from preceding


stages
Stage 0 or GFR Increased risks for CKD e.g. Screening for advanced CKD and CVD
>90 • Diabetes mellitus disease
• Hypertension CKD risk reduction i.e. treat hypertension,
• Glomerular disease diabetes and HIV
• HIV • Check creatinine/BUN every month for 3
months then yearly if stable

469
• Hepatitis B/C

Stage 1 or GFR Kidney damage with normal GFR Diagnose and treat comorbid conditions See
>90 for Stage 0
Stage 2 or GFR 60- Kidney damage with mild GFR Refer to determine cause and develop care
89 reduction plan
While on the care plan, monitor the GFR in
these patients and make sure kidney
function is not worsening rapidly and watch
for stage 3
Stage 3 or GFR 30- Moderate GFR reduction Refer to physician/nephrologist
59 Monitor and manage complication
Check creatinine/BUN every 3months
Stage 4 or GFR 15- Severe GFR reduction Refer to nephrologist
9 Prepare for kidney replacement therapy
Stage 5 or GFR Kidney failure requiring kidney Refer to nephrologist
<15 replacement therapy End stage kidney
disease
* Use CKD-EPI formula without the ethnicity factor. This calculator is available freely online.
Laboratories in Tanzania should report as eGFR.(Delanaye and Mariat, 2013)[1, 2]

Non-pharmacological Treatment
• Reduce salt intake.
• Low protein diet (not exceed 1g/kg per day) is indicated in the presence of CKD stage 4
and 5. (Evidence)
• Reduce cardiovascular disease risk factors – See section: Prevention of ischaemic heart
disease and atherosclerosis.
• Treat underlying conditions.
• Decrease significant proteinuria, if present.

Significant proteinuria = more than +2 protein on urinalysis OR spot urine protein creatinine ratio of >
0.1 g/mmol OR ACR (albumin-creatinine ratio) > 100 g/mol, confirm as positive if raised on at least 2
of 3 occasions, in the absence of infection, cardiac failure and menstruation.

Proteinuria
• In established chronic kidney disease, decrease proteinuria, irrespective of presence or
absence of systemic hypertension.
• Monitor kidney function and potassium especially with impaired kidney function.
• If volume depleted, first rehydrate before commencing ACE-inhibitor.
• ACE-inhibitor are contraindicated in:
ü Hyperkalaemia
ü known allergy to ACE-inhibitor
Begin with low dosage of ACE-inhibitor and titrate up ensuring blood pressure remains in normal
range and no side effects are present, up to the maximum dose or until the proteinuria disappears –
whichever comes first.

Pharmacological Treatment
Adults
C: enalapril (PO) 10–20mg 12hourly
OR
C: lisinopril (PO) 5-10mg 24hourly (titrate max 40mg 24hourly)
Also see other ACEI in hypertension treatment (Cardiovascular Chapter)

Hyperlipidaemia
If hyperlipidaemia is a co-existent risk factor manage according to section

21.1.1Diabetic Kidney Disease


This is a clinical diagnosis based on the presence of albuminuria, decreased estimated glomerular
filtration rate (eGFR) or both in diabetes. This diagnosis includes diabetic nephropathy which has

470
microalbuminuria (30-300mg/g) and retinopathy in its defining characteristics. In diabetics, optimise
control according to section 9.6: Diabetes mellitus type 2, in adults.

Investigations
• Urinalysis (Dipstick biochemistry + microscopy)
• Kidney biopsy with the following indications – if cause not apparent
o Albuminuria >300mg/g within 5years of DMt1 onset
o RBC cell cast, dysmorphic RBC or WBC casts in urine sediment
o Presence of other systemic illness eg SLE
o Rapid decline (per year) of eGFR>5mL/min/1.73m2
• Ultrasonography kidney ureter and bladder (KUB)

Table 21.2: Pharmacological Treatment of CKD patients with Diabetes mellitus


[3-5, 20-25) (Saisho, no date; Wanner et al., 2016; V. Perkovic et al., 2019; Vlado Perkovic et al.,
2019; Zou et al., 2019)]
Non-dialysis CKD Adults (Titrate carefully)
eGFR Medication Considerations

>90 As in treatment of non-CKD Diabetes: see Strong consideration of including


Stage 1 Diabetes Mellitus Chapter SGLT2-Inhibitors
For type-2 DM with high cardiovascular risk (an
89-60 add on)
Stage 2 S: empagliflozin (PO) 10mg 24hourly
OR
S: stagliptin (PO) 50mg 24hourly
59-30 A: gliclazide (PO) 40–80mg 12hourly if not Caution on Metformin and long
Stage 3 available use acting sulphonyl urea
OR
C: glimepiride (PO) 1-8mg 24hourly +/- Titrate carefully
S: empagliflozin (PO) 10 mg 24hourly
29-15 C: gliclazide (PO) 40 – 80mg 12hourly If on insulin, dose reduction is
Stage 4 OR needed
C: glimepiride (PO) 1-8mg 24hourly +/-
S: sitagliptin 25mg 24hourly
< 15 Insulin preferred. Reduce dosage with decreasing fluid control
Stage 5 eGFR
OR D: pioglitazone (PO)15-30mg 24hourly
On dialysis

21.1.2 Hypertension and CKD


Treat if present. See Cardiovascular chapter
The target blood pressure for CKD patients without proteinuria should be <140/90 and
for those with proteinuria should be <130/80.

Investigation
• Ambulatory blood pressure monitoring
• As for CKD section
• R/o secondary causes and control

Non-pharmacological Treatment
• Salt restriction (low sodium diet)
• Cardiovascular risk reduction as per Hypertension/CVD section

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Table 21.3: Pharmacological Treatment of Hypertension and CKD

eGFR Medication Considerations


STAGE *At least one medication be taken at bedtime
>90 With Proteinuria >500mg/day Check K+ level
Stage1 C: enalapril (PO) 10–20mg 12hourly
OR Consider repeat creatinine
And C:lisinopril) 5-10mg 24hourly (titrate after 5-7days of starting
max 40mg 24hourly) ACE-Inhibitor
89-60 OR
Stage2 S: irbesartan (PO) 150-300mg 24hourly
If not available, use another ARB as in
Hypertension treatment
If poorly response + oedema
Diuretics as in section on fluid overload
+/-
D: diltiazem (PO) 60-120mg 12hourly
OR
S: verapamil (PO) 40–80mg 8hourly
With no Proteinuria <500mg/day
If has oedema
Diuretics See section on fluid overload
PLUS
ACE-Inhibitors/ARB as above
ADD if not controlled
D: diltiazem (PO) 60-120mg 12hourly
OR
S: verapamil (PO) 40–80mg 8hourly

Other medications If above fails


C: spironolactone
OR
S: eplerenone as in Hypertension
treatment/Portal hypertension +/-
B: hydralazine (PO)12.5 mg – 50 mg +/-
B: nifedipine (PO) 20-40mg 12hourly
OR
C: amlodipine 5-10mg 24hourly +/-
B: atenolol (PO)25–00mg 24hourly

If not available or intolerable use below


C: carvedilol (PO)6.25mg-25mg
12hourly
OR
S: bisoprolol (PO) 2.5-5 mg 24hourly +/-
S: doxazosin (PO) 1mg 24hourly (titrate
max 16mg)
OR
A: methyldopa (PO)250-1000mg
8hourly
59-30 As above Monitor potassium more
Stage 3 Dose adjustment frequency
C: lisinopril (PO) 5-10mg 24hourly

29-15 DO NOT USE ACE inhibitor OR angiotensin Fluid control may be more
Stage 4 receptor blocker. Treatment as above important

< 15 Dose reduction for *Diuretics


Stage 5 S: bisoprolol (PO)2.5mg 24hourly *Salt restriction
OR A: methyldopa (PO)250mg – 1 g 24hourly *Ultrafiltration volume in
On dialysis S: doxazosin (PO) 1mg 24hourly (titrate max dialysis
16mg 24hourly

472
Fluid overload
Treat fluid overload if present and refer. Exclude other causes of oedema as part of management.

Adults
B: furosemide (slow I.V, PO) 40–80mg 12hourly.
OR
D: torsemide (PO) 10-20mg 24hourly (titrate max 200mg/day)
If poor response, repeat after 1hour.

If diuresis is inadequate and there is no hypokalemia a combination therapy with thiazide or thiazide-
like diuretics could be used
B: furosemide (maximal 600mg/day) slow infusion rather than boluses +/-
D: hydrochlorothiazide (PO) 25-50mg 12hourly
OR
S: metolazone (PO) 2.5–20mg 24hourly

Note
Do not give I.V fluids – use heparin lock or similar I.V access.

Referral to nephrologist
• All cases of suspected chronic kidney disease stages 3–5 for assessment and planning
• All children
• All cases of CKD with:
o haematuria,
o proteinuria
o raised blood urea or creatinine initially for assessment and planning
• Uncontrolled hypertension/fluid overload
• CKD associated with hyperlipidaemia
• No resolution of proteinuria with ACE-I therapy

Note
Patients who might qualify for dialysis and transplantation or who have complications should be
referred early to ensure improved outcome and survival on dialysis, i.e. as soon as GFR drops
below 30 mL/min/1.73m2, or as soon as diagnosis is made/suspected

21.1.3 Dialysis
Refer to the National guidelines for Dialysis services from the MOHCDGEC for the detailed
indications, procedures and management of patients on dialysis (Haemodialys or Peritoneal dialysis)

21.1.4 CKD Associated Metabolic Acidosis


(serum bicarbonate below 22mmol/l)
S: sodium bicarbonate (PO) 650mg 12hourly. Titrate to serum bicarbonate levels 23-
29mmol/l
OR
S: calcium carbonate (PO) 500mg 12hourly.

21.1.5. Hyperkalaemia
Refers to an elevation in potassium concentration ≥5.5 mmol/l. Kidney failure and use of
medications use are common causes. Severity of hyperkalaemia may be mild (5.5-6), moderate 6.1-
6.5 and Severe >6.5. Severity grading increases once there is ECG changes.

Clinical Presentation
• Muscle weakness (ascending) • Cardiac conduction abnormalities
• Muscle fasciculation • Cardiac arrhythmias
• Paralysis

Investigation
• Serum potassium – frequent • Serum bicarbonate
reassessment 0hr, 1hr, 3hr • Full blood picture
• ECG (decreased size of p waves, T • Serum creatinine
wave changes, prolonged PR and
widening QRS)
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• Lipid levels – Total cholesterol and • Blood glucose
LDL
• Uric acid

Non-pharmacological Treatment
• Avoid foods rich in potassium; which include potatoes, bananas, green vegetables
• Stop offending medication Renin-angiotensin-aldosterone system inhibitors. NSAIDS and
potassium sparing diuretics

Pharmacological Treatment
Cellular membrane stabilization – All patients with potassium >6.5mmol/l or with ECG changes

Adults
A: calcium gluconate (IV) 10% 10-30mls stat

Reserve for ICU through a central line.


D: 10% calcium chloride (IV) 10mls stat
-may repeat again if ECG abnormal within 5-10minutes
-do not give together with sodium bicarbonate

Potassium shift to the intracellular compartment (repeated dosing of insulin may be


necessary)
Adults
A: insulin short acting 5-10IU +50mls of 50% Glucose iv injection. Only give glucose if
RBG is <11
• Monitor RBG for hypoglycaemia
• Repeat insulin short acting /glucose every 4-6 hours
Children
A: insulin short acting 0.1IU/kg + dextrose 0.5g/kg for 30min

AND
Adults
C: salbutamol nebulized 2.5-10mg every 4-6hours
OR

If has metabolic acidosis and not overloaded

Adults and Children


C: sodium bicarbonate (IV) 1mEg/kg over 15minutes

Removal of Potassium from the body


D: calcium (or sodium) polystyrene sulphonate 15-30g 8hourly for 3days. (Caution: Bowel
perforation risk). Can be given 3time a week chronically
AND
B: furosemide (PO/slow I.V) 40–80mg 12hourly +/- haemodialysis

If above is not available


C: lactulose (PO)10-30ml hourly until rapid laxation then 30mls 8hourly per 24hours

21.1.6 CKD Associated Anaemia


Patients with CKD present with anaemia, which may be contributed by several factors including
inability to produce erythropoietin, frequent, blood loss (form gastritis, dialysis therapy and poor
appetite. [Refer to the national guidelines for dialysis]

Investigations for anaemia for patients with CKD stage 3-5


• Peripheral smear
• Reticulocyte count
• Full blood count
• Iron studies; serum iron, transferrin saturation and serum ferritin
• Stool for occult blood

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Patients with CKD stage 3 and below with anaemia should be given erythrocyte stimulating agents
(ESA) when Haemoglobin is < 10 g/dL and interrupt or reduce once Haemoglobin level reaches
11g/dL.

S: erythropoietin alfa (IV) 50-100 units/kg 3times a week as approximate starting dose,
May be given with IV iron supplimentation

Patients with CKD stage 3 and below with iron deficiency indicated by transferrin saturation <30% or
serum ferritin <500ng/ml should be given iron supplementation;

D: Iron sucrose (IV) 100mg with each dialysis for 10doses

Note
IV Iron is preferred to oral iron and can be given with ESA among patients on dialysis.

21.1.7 Mineral Bone Disease (MBD)


Mineral bone diseases are common among patients with CKD including those undergoing
maintenance haemodialysis and these diseases contribute cardiovascular complication and
mortality. Clinical features of these disorders include Bone pain, Convulsions, Tetany, Tissue
calcification, Fractures. The following investigations should be carried out to identify these disorders
among patients with CKD stage 3 and below;
• Serum calcium,
• Albumin (for correction of calcium)
• Phosphate
• Parathyroid hormone (intact)
• Vitamin D Levels
• Lumbar-X-ray (lateral)
• DEXA scan (those suspected)

Non-pharmacological Treatment
• Nutritional consultation: Low phosphate diet and high calcium diet

Pharmacological Treatment
Hyperphosphataemia treatment
S: calcium carbonate (PO) 500-1500mg 8hourly with meals [For patients with
hypocalcaemia]

21.1.8 Haemodialysis (HD) Catheter Related Blood Stream Infection


A common life-threatening complication which needs prompt recognition and response in the
dialysis unit.

Clinical Presentation
• Chills and/or fever ≥ 37.8 oC
• Tunnel or exit site purulence
• Rigors

Investigations
• Blood culture
• FBP
• Investigate for metastatic infection when indicated

Non-pharmacological Treatment
• Refer to management of sepsis if in shock
• Removal of catheter if there is non-response to therapy, exit site infection, tunnel infection,
metastatic infection or hemodynamic instability

Pharmacological Treatment
Usual 14-21days of treatment
• Empirical (while waiting for microbiological results)
Children
C: flucloxacillin (IV) 25-50mg/kg/day in 3 divided doses
AND
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D: ceftazidime (IV) 50mg/kg/dose every 48hourly, give after dialysis or on dialysis days
Adults
C: flucloxacillin (IV) 1-6g/d in 3 divided doses
AND
D: ceftazidime (IV) 1gstat immediately after HD and 1g after subsequent HD session
OR
Adult
S: vancomycin (IV)20mg/kg loading over last 1 hour then 1g during the last hour of
subsequent HD sessions
AND
D: ceftazidime (IV) 1gm STAT immediately after HD and 1g after subsequent HD session

Children
S: vancomycin (IV) 10mg/kg/dose (consider checking serum levels)
AND
D: ceftazidime 50mg/kg/dose 48hourly, give after dialysis or on dialysis days

• Tailored
o According to bacteriological results
o If negative continue with empirical treatment showing clinical improvement
Note
In case all above mentioned antibiotics are not available, patients should be treated empirically with
antibiotics favouring both gram negatives and gram positives.

Catheter lock (during treatment)


D: gentamicin lock
D: vancomycin lock

21.2 Acute Kidney Disease


Acute kidney disease is a sudden decline in the glomerular filtration rate (GFR) resulting elevation of
serum blood urea, creatinine and other waste products. Practically AKI is recognized when there is
urine output of less than 0.5ml/kg/hour for >6 hours. Causes of AKI are classified as pre-renal, renal
and post-renal causes and usually result in reversible kidney failure, these causes include;

Table 21.4: Causes of acute kidney injury

Category Examples Intervention


Pre-renal: loss of effective Low blood volume Restore blood volume
blood flow to the kidneys • Diarrhea, burn, • IV fluids
acute blood loss Low blood pressure
Heart failure • Use of inotropes
Hepatic failure
Renal: caused by intrinsic -Glomerulonephritis Treatment of specific
kidney insult -Nephrotoxic medications Glomerular disorders
-Rhabdomyolysis Omit offending nephrotoxic drugs
-Tumor lysis syndrome

Post renal: occurs as a -BPH Relief of obstruction


consequence of -Urinary stones -Urinary catheterization
urinary obstruction -Obstructed urinary catheters -Nephrostomy
-Bladder stones

Clinical Presentation
• Oedema
• Oluguria/anuria
• Convulsions in children

Investigation
Early disease
• Creatinine [increase of ≥ 26micromol/l within 48hrs or ≥ 50% increase within 7 days
defines AKI]
• Urea
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• Ultrasound KUB
• Urinalysis (Dipstick and microscopy)

Advanced disease defined by urine output of less than 0.5ml/kg/hour for >12 hours.
• Serum electrolytes [potassium, chloride, bicarbonate, Sodium phosphate and calcium]
• Arterial Blood Gases
• Uric acid
• Urine electrolytes – Fractional excretion of Sodium
• Chest X-ray
• ECG
• Kidney biopsy if cause not obvious clinically
• Creatine kinase if Rhabdomyolysis is suspected

Non-pharmacological Treatment
• Give oxygen, and nurse in semi-Fowlers’ position if patient has respiratory distress.
• Stop intake of all salt and potassium containing foods and fluids
• Restrict fluid intake to 10 mL/kg/day daily plus visible fluid losses
• Remove nephrotoxic medications
• Adequate nutritional support: sufficient amounts of energy and adequate protein. Consider
enteric/parenteral nutrition

Pharmacological Treatment
Treat underlying cause

Adults
If dehydrated,
A: 0.9% sodium chloride (PO/IV) while monitoring urine output
If diastolic blood pressure is greater than 100 mmHg or systolic blood pressure is above 150
mmHg:
C: amlodipine (PO) 5 mg
If there is respiratory distress (rapid respiration, orthopnoea) and is fluid overloaded [chest crackles
and raised JVP]:
B: furosemide (IV bolus) 80mg. (higher doses may be tried once)
If there is respiratory distress (laboured breathing with low serum bicarbonate=metabolic acidosis)
C: sodium bicarbonate (IV) 150mEq in 1L of 5%Dextrose
Consider Proton pump inhibitors to reduce risk of gastrointestinal bleeding
C: pantoprazole (IV/PO) 40mg 24hourly
Treat Hyperkalaemia as in CKD
Haemodialysis or Peritoneal dialysis when indicated

Note
• Indications for dialysis include pulmonary oedema, Hyperkalaemia, metabolic acidosis
not responding to medical therapy and uremic encephalopathy or pericarditis. Acute
poisoning with a dialysable substance is another indication.
• Patients with AKD will be followed regularly to monitor and prevent CKD. A weekly
kidney assessment (creatinine and/or urinalysis) for one month and then monthly for 2
months and then 6-monthly thereafter is a suggested regime when there is no CKD.
• Do not put up a drip and do not give a fluid infusion if the patient is fluid overloaded or
urine does not increase with iv. fluids

Referral
All cases where adequate laboratory and clinical resources exists, management according to the
hospital level guidelines may be instituted. Referral to the nephrologist should occur in the
following:-
• Glomerulonephritis is a strong possibility – haematuria and proteinuria.
• Worsening despite initial treatment.

21.3 Glomerular Diseases (GD)


Glomerular diseases include a broad array of clinicopathological syndromes which progress to
glomerulosclerosis and eventually end stage kidney disease. Glomerular disease may be a result of
a primary condition of the kidney or may be secondary to a systemic disorder.

477
Clinical Presentation
• Proteinuria • Hypertension
• Reduced GFR (and its effects) • Oedema.
• Haematuria
21.3.1 Glomerular disease - Nephritic syndrome
A non-infectious inflammatory process that involves the nephron. History and examination should
exclude secondary causes.

Clinical Presentation:
• Painless macroscopic turbid, bloody or brownish urine
• Peripheral and facial oedema
• Difficulty in breathing
• Hypertension encephalopathy with impaired level of consciousness or convulsions
• Little or no urine excretion

Investigations
• Serum Creatinine
• Blood urea nitrogen/Urea
• Urinalysis (Dipstick + microscopy)
• confirm proteinuria by Urine albumin-creatinine ratio (UACR) or Urine protein-creatinine
ratio (UPCR)
• Urine culture
• Complete blood count
• Kidney biopsy and histology
• Others on tertiary hospital e.g. ANA, dsDNA, RF, , complements, Syphillis tests (VDRL or
RPR)

Non-pharmacological Treatment
• Give oxygen, and nurse in semi-Fowlers position if patient has respiratory distress.
• Restrict intake of all salt
• Restrict potassium containing foods and fluids
• Restrict fluid intake to 10 mL/kg/day daily plus visible fluid losses

Pharmacological Treatment
Adults
Fluid overload
B: furosemide (IV bolus) 80mg
If hypertension
If diastolic blood pressure is greater than 100mmHg or systolic blood pressure is above 150mmHg:
C: amlodipine (PO) 5mg stat before referral to higher facility
Continue with other medications as in hypertension section (caution contraindications)

Note
The definitive treatment of nephritis depends on the cause – an assumption of acute post
streptococcal nephritis or any other disease cannot be made without specific investigation, which
may include kidney biopsy.
21.3.2 Nephrotic syndrome
It is a kidney disorder characterized by urinary protein loss leading to generalized body swelling. It
is severe proteinuria defined as: Adults: 3.5 g/day,

Clinical Presentation
• Oedema
• Hypoalbuminaemia
• Hyperlipidaemia

Note
• Diagnosis of nephrotic syndrome requires a kidney biopsy, however in children (1year-18
years) biopsy is indicated for children with steroid resistant nephrotic syndrome
• Children (1-18 years) should be given treatment with steroid, they should be referred for
renal biopsy if there is no response.

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Non-pharmacological Treatment
Adequate calories and adequate protein 1g/kg/d
No added salt to limit fluid overload

Pharmacological Treatment
The management of glomerular disease depends on the type/cause of the disease and is
individualized guided by a specialist according to the histology results obtained after renal biopsy.
Note
Referral to nephrologist may include treatment using immunosuppressant such as prednisolone,
mycophenolate mofetil, cyclophosphamide, angiotensin blockade etc

Table 21.5 Histology based treatment of Glomerular diseases


S/N Histological Treatment Regime Special considerations
Pattern
Minimal Children In children biopsy is
1 change Steroid Sensitive indicated for
disease Initial: A: prednisolone 60mg/m2/d] or 2mg/kg/d
[max 60mg/d] for 6 weeks [complete 6weeks of 1. Children with
initial treatment if remission is attained at steroid
4weeks) resistant NS
Continue: A: prednisolone 40mg/m2 or 2. Late failure to
1.5mg/kg for 6weeks, if the patient has attained respond
remission by 4weeks of initial treatment, after following initial
6weeks of alternate days’ therapy taper and response
stop within 6weeks (taper by 5-10mg a week) 3. Decreasing
kidney
Relapsing Steroid Sensitive 0.9% sodium function
chloride
A: prednisolone 60mg/m2 or 2mg/kg [max
60mg/d] until in complete remission for 3 days,
THEN
A: prednisolone single dose on alternate days
(40mg/m2 per dose or 1.5mg/kg per dose:
maximum 40 mg on alternate days) for at least 4
weeks.

S: levamisole (PO) 2.5mg/kg on alternate days Monitor calcineurin


for 12months inhibitor toxicity/levels

Frequent relapse steroid dependent


S: cyclophosphamide 2mg/kg/d 10-12 weeks
[max 168mg/kg cumulative dose] OR
S: cyclosporine 4-5mg/kg/d (starting dose) OR
S: tacrolimus 0.1mg/kg/d (starting dose) OR
S: everolimus 0.5-2mg 12hourly OR
S: sirolimus 1-3mg 12hourly OR
S: mycophenolate mofetil 1200mg/m2/d in two
divided doses
S: rituximab 375-1000mg/m2

Steroid resistant Nephrotic syndrome


S: mycophenolate mofetil 1200mg/m2/d in two
divided doses OR
S: mycophenolate sodium AND
A: prednisolone high dose
Adults
D: prednisolone (PO) 1mg/kg 24hourly Slow taper after
(maximum 80 mg) OR remission over 6 months

alternate-day single dose of 2 mg/kg (maximum Check HBA1c monthly


120 mg – 4-week if remission, continue to 16 Screen osteoporosis
weeks if complete remission not achieved
Frequent relapse/steroid dependent/resistant

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Focal for idiopathic only Exclude secondary
2 segmental
glomerulos D: prednisolone (PO) 1mg/kg [max 80mg] daily Slow taper after
clerosis or alternate day dose 2mg/kg [max 120mg] 4- remission over 6months
16weeks
OR
Intolerance for steroids or steroid resistant
Monitor levels
S: cyclosporine 3.5-5mg/kg/d in 2divided doses
OR
S: tacrolimus 0.1mg/kg/day in 2 divided doses
(then titrate)

Membrano For idiopathic membranous nephropathy only Exclude secondary


3 us
nephropath Children Monitor for 6 months
y Alternating monthly treatment with Methyl before initiation unless
prednisolone + Prednisolone (month 1, 3 & 5) life threatening
and oral Cyclophosphamide (month 2, 4 & 6) symptoms OR
D: methylprednisolone 10mg/kg for 3days, Raising creatinine
prednisolone 0.5mg/kg for 27 days -Do not use serum
S: cyclophosphamide 2mg/kg for 30 days creatinine >309
micromol/l [CKD patient]
Alternative regimes
S: cyclosporine 3.5-5mg/kg in two divided doses Kidney biopsy might be
with prednisolone 0.15 mg/kg/day for 6 months repeated
S: tacrolimus 0.2mg/kg in two divided doses
without prednisolone

Adults
S: cyclophosphamide
A: prednisolone 1mg/kg/day
D: methylprednisolone IV monthly

Alternative regimes
S: tacrolimus 0.1mg/kg/day in 2 divided doses
for 6 months OR
S: cyclosporine 3.5-5mg/kg/d in 2 divided doses

If albumin is less than 25g/l + thrombosis risk


C: warfarin 5mg PO [refer to DVT
anticoagulation]
Membrano S: cyclophosphamide OR
4 proliferative S: mycophenolate mofetil 1200mg/m2/d in two
divided doses
OR
S: mycophenolate sodium
AND
A: prednisolone
Immunoglo Initial supportive care for 3-6 month Note
5 bin A C: enalapril (PO)10-20mg 24hourly OR Other registered ACEI
Nephropath C: lisinopril (PO)2.5-10mg 24hourly or ARBs may be used
y as in Hypertension
For those persistent proteinuria 1g/d for 6 section
months

Adults and children


A: prednisolone (PO) 1mg/day for 6 months
Lupus All patients
6 nephritis S: hydroxychloroquine (PO) 6mg/kg/day
Adult maintenance

Class II with proteinuria >3g/day


Treat as in Minimal change disease above

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Class III and class IV
Initial 6 months
D: methylprednisolone (IV slow) 250mg-1000mg
30min 3days monthly
AND Oral prednisolone less
S: cyclophosphamide (IV) 500-1000mg/m2 effective 60mg/day may
monthly be given
OR
S: mycophenolate mofetil (PO) 0.5-1g 12hourly Open to use a shorter
titrating (PO) 1.5g 12hourly if tolerated OR more frequent regime
S: mycophenolate sodium EURO lupus
Cyclophosphamide
Maintenance 500mg every two weeks
S: azathioprine (PO) 1.5-2.5mg/kg/d x 6doses
OR
S: mycophenolate mofetil (PO) 0.5-1g 12hourly
OR
S: mycophenolate sodium OR
S: cyclosporine 4-5mg/kg/d (starting dose) 6
months OR
S: tacrolimus 0.1mg/kg/d (starting dose)

Class V + persistent nephrotic range proteinuria


As clas II and IV
Pauci- Initial S: Haemodialysis
7 Immune S: cyclophosphamide (IV) 15mg/kg every 2 S: Plasmapheresis
focal and weeks x3 doses then every three weeks for 3-6
segmental months OR In special indications
necrotizing S: cyclophosphamide oral 1.5-2mg/kg daily 3-6
glomerulon months
ephritis AND
D: methylprednisolone (IV) 250mg-1000mg slow
30min 3days as induction then
Prednisolone 1mg/kg then taper to 30mg in one
week then taper down to 5mg by 4-6months

Severe disease
S: rituximab 1g followed by 14 days later
another 1g
OR
S: rituximab 375 mg/m2 per week for 4 weeks
AND
D: methylprednisolone (IV) 250-1000mg slow
30min 3days as induction then
A: prednisolone 1mg/kg then taper to 30mg in
one week then taper down to 5mg by 4-6months

Maintenance therapy
S: azathioprine (PO) 1-2mg/kg/d 18months
OR
S: mycophenolate mofetil 1g 12hourly OR
S: mycophenolate sodium

21.4 Kidney Transplantation


Kidney transplantation is one of the kidney replacement therapies with good outcomes in morbidity
and mortality. A Kidney Transplant recipient (KTR) is a fully rehabilitated individual who is capable of
contributing to the society.

21.4.1: Transplant Donor Evaluation


General principles of preparing a live Kidney Transplant Donor will be outline in this subsection. Risk
assessment and communication to ensure the donor candidate is able to decide without undue
pressure is one of the early steps in evaluation. The transplant program policies of concerned centre

481
should be the basis for decision. Post decision for both accepted or excluded, follow up care should
be formulated.
Clinical presentation
A complete history and physical examination should be documented.

Investigations
Investigations will be based on the following :-
Adults aged 18years and above should be considered for live related donation. Pre-donation
evaluation should include
• Psychosocial assessment
• Surgical assessment for suitability
o Obesity
o Anticoagulation
o Vascular anatomy and native kidneys in polycystic kidney disease
o Urology
• Diabetes screening
• Cancer screening this should proceed even after transplantation.
o Imaging, cystoscopy even colonoscopy for candidates with specific increased
risks
o Do not exclude patients with cured malignancy. Waiting time will depend on
malignancy
• Pulmonary disease assessment
• Cardiovascular disease assessment
o ECG and ECHO
o Stress ECG
o Dobutamine ECHO if above 40 years/ has risk of myocardial arterial disease.
• Peripheral arterial disease
o All candidates by history and physical examination. Imaging may be necessary.
Consult vascular surgeon prior to transplantation.
• Neurological disease screening
o Wait for 6 months after a stroke or TIA
o Screen for intracranial aneurysms in high risk autosomal dominant polycystic
kidney disease
• Gastrointestinal and Liver disease
o History and physical examination to exclude active PUD, Diverticulitis,
Pancreatitis Cholelithiasis Inflammatory bowel disease and liver disease
§ Specific investigations may be necessary
• Haematological
o Screen for thrombophilia and antiphospholipid antibodies in high risk individuals
o Need for anticoagulation is not a contraindication for transplantation
• Immunological assessment
o Document and communicate all sensitizing events (blood transfusion &
miscarriage)
o Perform HLA antibody testing at transplant evaluation
• Infection screening
o Hepatitis B/C
o HIV
o CMV
• Compatibility testing
o ABO blood typing
o Human leukocyte typing for MHC and Class I, II in both donor and recepients
o Donor specific anti-HLA antibodies in recipients
• Pre-donation Kidney function
o Serial Serum creatinine, eGFR
o Measured creatinine clearance
o OR measured GFR
o In special situations single kidney GFR (using radio labelled agents eg TC-DTPA
- technetium 99mTc-diethylenetriamine pentaacetic acid (DTPA)

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21.4.2: Transplant Candidate
All patients with CKD stage 4-5 should be informed of, educated about and considered for kidney
transplantation regardless of socioeconomic status, sex, or ethnicity. Pre-emptive transplantation
referral should be 6-12 months before anticipated RRT initiation. Active diseases should be
controlled first before transplantation.
The following are not recommended for kidney alone transplant
• Multiple myeloma and AL amyloidosis
• Decompensated cirrhosis
• Severe irreversible obstructive or restrictive lung disease
• Severe uncorrectable and symptomatic cardiac disease
• Progressive central neurodegenerative disease

Transplant candidate assessment should include the following


• Psychosocial assessment, Adherence to therapy and Tobacco use avoidance
• Surgical assessment for suitability
o Obesity
o Anticoagulation
o Vascular anatomy and native kidneys in polycystic kidney disease
o Urology
• Diabetes screening
• Cancer screening this should proceed even after transplantation.
o Imaging, cystoscopy even colonoscopy for candidates with specific increased
risks
o Do not exclude patients with cured malignancy. Waiting time will depend on
malignancy
• Pulmonary disease assessment
• Cardiovascular disease assessment
o ECG and ECHO
o Stress ECHO
o Dobutamine ECHO if above 40 years/ has risk of myocardial arterial disease.
• Peripheral arterial disease
o All candidates by history and physical examination. Imaging may be necessary.
Consult vascular surgeon prior to transplantation.
• Neurological disease screening
o Wait for 6 months after a stroke or TIA
o Screen for intracranial aneurysms in high risk autosomal dominant polycystic
kidney disease
• Gastrointestinal and Liver disease
o History and physical examination to exclude active PUD, Diverticulitis,
Pancreatitis Cholelithiasis Inflammatory bowel disease and liver disease
§ Specific investigations may be necessary
• Haematological
o Screen for thrombophilia and antiphospholipid antibodies in high risk individuals
o Need for anticoagulation is not a contraindication for transplantation
• Immunological assessment
o Document and communicate all sensitizing events (blood transfusion &
miscarriage)
o Perform HLA antibody testing at transplant evaluation
• Infection screening
o Hepatitis b/c
o HIV
o CMV

21.4.3 Transplant Recipient


This section will cover the management of kidney transplant recipients (KTRs). It includes initial and
maintenance immunosuppression, monitoring and management of special conditions. Enhanced
investigations and treatment in this group is paramount to ensure kidney graft survival.

483
21.4.4.1 Induction Therapy
There is a choice of Interlukin 2 receptor blockers and lymphocyte depleting agents. Patients with
high immunologic risk for acute graft rejection should receive lymphocyte-depleting agents instead
of IL2-RA. The following factors favor using lymphocyte-depleting agents.

• One or more human leukocyte antigen (HLA) mismatches


• Younger recipient and older donor age
• Panel reactive antibody (PRA) greater than 0 percent
• Presence of a donor-specific antibody (DSA)
• Blood group incompatibility
• Delayed onset of graft function
• Cold ischemia time greater than 24 hours

For low risk patients


Adults
S: basiliximab 20mg (IV) stat within 2hours before transplant and (IV) 20mg stat on day 4

OR (high risk patients)

S: rabbit anti-thymocyte globulin 1.5 mg/kg/day for 4 to 7 days; the first dose prior to
transplant (Intra OP)

OR
S: Antithymocyte globulin ATG (horse)

Children

For children above 35kg use same dose as adults.

Below 35kg use below


S: basiliximab (IV) 10mg stat within 2hours before transplant and 10mg IV stat on
day 4
OR (high risk patients)
S: horset anti-thymocyte globulin 1.5mg/kg/day for 4 to 7days; the first dose prior
to transplant
21.4.4.2 Maintenance Immunosuppressive Medication
A combination of immunosuppressive medication which include a calcineurin inhibitor (CNI) and an
antiproliferative agent with or without corticosteroids is recommended at this stage. Except for when
mammalian target of rapamycin inhibitors (mTORi) is used, it is recommended to start
immunosuppression before or during transplantation without waiting for graft function establishment.
Monthly investigations

• Serum creatinine and Blood urea nitrogen


• Urinalysis
• Urine biochemistry (Urine dipstick)
• Serum Tacrolimus (12-h trough) or cyclosporin (12-h trough or 2-h post dose) levels
according to patient’s regime

Pharmacological Treatment
Adults

S: tacrolimus initial 0.1-0.2mg/kg/day in 2divided doses titrate to planned serum levels


(immediate release)
OR
If tacrolimus is not available

Adults and Children

S: cyclosporin (modified) 7-12mg/kg/day in 2divided doses (titrate to serum levels)

484
In special indications (eg. with Kaposi Sarcoma) or mostly low risk KTRs
Adults
S: sirolimus loading dose: 15mg loading dose on day 1. Maintenance: 5mg/day (trough
concentration 5-7ng/mL
AND
S: mycophenolate mofetil (PO) 1-1.5g 12hourly

OR
S: mycophenolate sodium 360-1080mg 12hourly

OR
S: azathioprine Initial following transplant IV/PO 2-5mg/kg stat. Maintenance (PO) 1-
3mg/kg 24hourly

AND
Glucocorticoids as part of triple-agent immunosuppressive regime

Initial

D: methylprednisolone 7mg/kg (maximum of 500mg) IV stat intra (OP) –operation


OR

A: prednisolone 1mg/kg/day (max 80mg) for first 3 days’ post-transplant


Maintenance
A: prednisolone 20mg/day 7 days then taper by 5mg weekly maintain at 5mg/kg

After 4months post transplantation efforts to decrease dose of immunosuppression if there has been
no acute rejection. Do not stop steroids or CNIs

Note
• Use of a non-dihydropyridine CCB to minimize CNI dosage may be economical.
• Assessment for medication adherence is crucial. So education for all KTRs and family
members is important.

21.4. 4. 3 Monitoring schedule for the Kidney Transplant Recipients (Routine)


Kidney transplant recipients have high risk of getting complications including surgical complications
(first 3 months), frequent infections (first six months) and complication related to immunosuppressive
medications including diabetic mellitus. Some of the immunosuppressive medications have a narrow
therapeutic window and have toxic effects including nephrotoxicity. Therefor these patients need
regular and frequent follow up as indicated in the table below.

Table 21.6: Monitoring schedule for the Kidney Transplant Recipients (Routine

Test Screening intervals by time after transplantation


1week 1month 2-3months 4-6months 7- >12months
12month
s
Creatinine + Daily 2-3 per week Weekly Every 2 Monthly Every 2-3
eGFR weeks mo
Urine protein Once Every 3 months Annually
(UACR/UPCR
)
Complete Daily 2-3/week Weekly Monthly Annually
blood count

485
Diabetes Weekly Every 3 months Annually
Lipid profile - - Once - - Annually
BKV Nucleic monthly Every 3 months -
acid testing
EBV Nucleic Once Monthly Every 3 months -
acid testing
BP/pulse/weig Each clinic visit
ht/height

21.4.5. Acute Kidney Graft Rejection


An acute rejection is clinically suspected in patients with increased serum creatinine, after the
exclusion of other causes of graft dysfunction. Other causes are generally excluded with a biopsy.
Acute rejection should be treated after kidney biopsy unless this will substantially delay treatment.
Clinical presentation

• Occur within the first six months • Oliguria


after transplantation • Graft pain and/or tenderness
• Fever • Worsening hypertension
• Malaise

Investigations

• Kidney biopsy which may be • Nuclear medicine renal scans


repeated if there is failure of • Urinalysis – urine biochemistry and
treatment microscopy
• Serum creatinine and Blood Urea • BK polyomavirus
nitrogen • CMV
• Kidney Ultrasound and dopper US
of the kidney

Acute cellular rejection (Use Banff classification in treatment)


D: methylprednisolone (IV) 300-500mg 24hourly for 3-5days followed by prednisolone
taper.
If corticosteroids have failed

OR/AND
S: rabbit Anti-thymocyte globulin 1.5 mg/kg/day for 4 to 7days
OR

S: anti-thymocyte globulin (ATGam) Children and Adolescents: IV: 10 to 15mg/kg/dose


once daily for 14days, then if needed, may administer every other day up to a total of 21
doses in 28 days

Antibody-mediated acute rejection (Histology of injury + vascular endothelium c4d staining +


serologic evidence)
D: methylprednisolone (IV) 300-500mg daily for 3-5days
AND
S: plasma exchange 24hourly or alt. day until serum creatinine within 30% of previous
(max 5sessions)
OR
S: rituximab 200 to 375 mg/m2 after completion of plasmapheresis and IVIG
OR
S: rabbit Anti-thymocyte globulin 1.5 mg/kg/day for 4-7days
OR
S: anti-thymocyte globulin (ATGam) Children and Adolescents: IV: 10 to 15 mg/kg/dose
24hourly for 14days, (up to 21 doses in alternate days sometimes)

486
21.4. 6 Other Conditions in Transplantation and their Managements
Table: 21.6 Other Common Conditions That Are Encountered Among Transplant Recipients
and Their Management
Diagnosis/Conditions Evaluation Treatment
Recurrent Kidney Disease Urine protein +/- Plasmapheresis
Serum creatinine +/- Cyclophosphamide and corticosteroids
Kidney biopsy
+/- ANCA -/+ ACE-Inhibitor or ARBs
+/- Anti-GBM antibodies
CBC, LDH
Vaccinations Check Hepatitis B surface All inactivated vaccines (unless not approved) are okay
antibodies 12weeks after HBV vaccination before transplant
completing vaccination Avoid vaccinations in the first 6/12
Influenza vaccine may be given in the first 6months.
AVOID live vaccines
Pneumococcus
Viral diseases

BK polyoma virus (BKV) Kidney biopsy Reduce immunosuppression


BKV Nucleic acid testing
Cytomegalovirus CMV serologies pre- Prophylaxis for 3 months
transplant both donor and S: valganciclovir (PO) 900mg 24hourly
recipient
For treatment of life-threatening disease
CMV plasma Nucleic acid S: ganciclovir (IV) 6mg/kg 12hourly until clinical response
testing is used for diagnosis Then continue with
and montoring treatment S: valganciclovir (PO) 900mg bid until symptom resolution
Epstein-Barr Virus and Post- EBV by nucleic acid testing Reduce immunosuppressive medication with patients who
Transplant have raising EBV loads
Lymphoproliferative disease
EBV disease and post-transplant lymphoproliferative
disease
Herpes simplex virus 1,2 Superficial disease
and varicella zoster virus Oral acyclovir /valacyclovir until lesions have resolved

Systemic disease
1. Reduce immunosuppressive medication
2. Iv. Acyclovir
Frequent attacks
Give prophylactic antivirals
Pneumocystis jirovecii Diagnosis by bronchial -Prophylaxis for 3-6 months with
pneumonia alveolar lavage and/or lung A: trimethoprim+sulfamethoxazole
biopsy -After treatment for acute rejection (6 weeks)
-Add corticosteroids for moderate to severe disease

Candida Prophylaxis with oral clotrimazole lozenges, nystatin or


fluconazole
Cardiovascular diseases
CVD
New onset diabetes after Fasting plasma glucose Adult
transplantation (NODAT) and/or A: acetylsalicylic acid 75mg PO (Balance risk/benefit)-
HbA1c and/or maintenance
Glucose tolerance testing Oral – check section on DM management in CKD patients.

See above schedule or after


starting or changing
medication

Atherosclerotic CVD A: acetylsalicylic acid (PO)75mg per 24hours maintenance


Malignancy
All malignancies Education on self- See relevant chapter on management
examination and Health care
directed screening
Kaposi Sarcoma Change to mTOR Inhibitors

487
21.5 Cystic Kidney Disease
Acquired or hereditary disorders of the kidneys. Autosomal dominant polycystic kidney disease is a
common cause of end stage kidney disease. It is progressive and incurable condition.
Clinical presentation

• Kidney
o Nocturia, polyuria and frequency due to concentration defect
o Hypertension
o Pain syndrome (infection, bleeding, stones, rupture or compression)
o Uremic manifestations

• Extra-kidney manifestations
o Polycystic liver disease
o Intracranial aneurysms
o Cardiac – valvular heart disease
Diagnostic ultrasonographic criteria

15-39 -years ≥3 cysts, unilateral or bilateral

40-59 years ≥2 cysts in each kidney

≥60 years ≥4 cysts in each kidney


Investigations

• Ultrasonography – KUB
• Serum creatinine
• Urinalysis – biochemistry and microscopy
• Genetic testing for those who want.to be donor (family history)
• CT scan – contrast enhanced has better sensitivity
• ALT, AST and bilirubin if using Tolvaptan

Non-pharmacological Treatment

• Increase fluid intake >3 L if has no fluid retention (eGFR <30mL/min/1.73m2)


• Kidney transplantation when indicated
o Might need pretransplant native nephrectomy

Pharmacological Treatment

S: tolvaptan (PO) 45mg in the morning and 15mg 8hours later (titrate to 90mg am and
30mg pm)

o pm dose should be taken before 4pm


21.6 Renal artery stenosis
Renal artery stenosis is narrowing of the one or both renal arteries. Atherosclerosis or fibromuscular
dysplasia are the commonest causes. Progression to chronic kidney disease and end-stage disease
may be prevented or slowed.
Clinical presentation

• Hypertension, which is resistant, refractory to therapy with three or more drugs.


• Young onset hypertension with no family history
• An acute rise in serum creatinine >30% after ACE-inhibitor or ARB use
• Episodes of flash pulmonary oedema
• Asymmetrical kidneys.
• Unexplained hypokalaemia

488

Investigations

• Serum creatinine/BUN • Computer tomography angiography


• Urine protein creatinine ratio • Magnetic resonance angiography
• Urinalysis • ACE-inhibitor Scintigraphy
• Duplex Doppler ultrasonography • Conventional arteriography

Non-pharmacological Treatment
Revascularization (when >80% stenosis)

Pharmacological
A: acetyl salicylic acid (PO) 75mg 24hourly

ACE-Inhibitors or ARBs as in the section of Hypertension


A pathological description characterized by thrombocytopenia, microangiopathic hemolytic anemia
and organ injury. AKI is a common manifestation in the kidney due to the glomerular circulation
damage and occlusion. Early recognition is important.
Clinical presentation

• Haemolysis
• Ischemic organ dysfunction
• AKI
• Extrarenal manifestations include
o Pancreatitis and Hepatitis
o Seizures
o Diarrhoea/vomiting and abdominal pain
o Digital gangrene

Investigations

• ADAMTS13 activity (>10% excludes TTP)


• Bacterial culture/serology
o HIV serology
• ANA, anti-ds DNA, anti-phospholipids, anti Scl70
• Kidney biopsy

Pharmacological Treatment

Identify and treat the underlying cause. Primary thrombotic microangiopathies includes complement
mediated aHUS and Thrombotic thrombocytopenic purpura with decreased ADAMTS13.

S: plasma exchange (until ADAMTS13 to exclude TTP) +/- immunosuppression

21.8 Reflux nephropathy


A type of chronic interstitial nephritis associated with vesico-ureteric reflux (VUR) in early life with the
appearance of scars in the kidney as demonstrated by various imaging modalities. May be
associated with renal dysplasia and other congenital abnormalities of the urinary tract. Including
urethral valves.
Clinical presentation

• Usually asymptomatic • Dysuria


• Hypertension • Aching lumbar pain
• Frequency of micturition • Urinalysis shows leucocytes

Investigations

• Ultrasonography – KUB • Serial imaging by Magnetic


• Radionuclide DMSA scans Resonance Imaging – MRI
• Renal biopsy

489

• MCUG- micturating • Serum creatinine


cystourethrography • Urine culture
• Urine analysis –
dipstick/biochemistry/microscopy

Non-pharmacological Treatment
• If recurrent pyelonephritis occurs in an abnormal kidney with minimal function –
Nephrectomy
• Hypertension may be cured by removal of a diseased kidney
• Severe reflux may be managed by ureteric reimplantation or sub trigonal injection of
Teflon/polysaccharide

Pharmacological Treatment
Treat UTI as in section with Urinary tract infection.

21.9 Contrast Induced Nephropathy (CIN)


Contrast induced nephropathy (CIN), which is also known as Contrast Induced Acute Kidney Injury
may occur after administration of iodinated contrast material, which is called contrast-induced
nephropathy. Common contrast based studies resulting in CIN include CT scan, MRI and coronary
angiography. Contrast induced acute kidney injury is usually characterized by rapid recovery of renal
function.

Clinical features
Major clinical manifestations of CIN include
• Early mild increase in serum creatinine that is generally observed within 24-48 hours after
the iodinated contrast exposure and that is usually mild. Serum creatinine starts to decline
within 3-7days of exposure
• Nonoliguria, patients with CIN are passing urine normally and if it occurs develop
immediately.
o Oliguria and more severe elevation of creatinine may develop in patients with
moderate to severe CKD.
• Urinalysis may show sediments consistent with acute tubular necrosis.
• Other manifestations of reduced GFR including hyperkalaemia, acidosis and
hyperphosphataemia

Investigations
• All patients scheduled for contrast studies should have serum creatinine performed before
the study and 24-48hours after contrast study
• For patients with raised creatinine
o Serial creatinine should be performed until 7 days
o Potassium, sodium, phosphorus, calcium and urinalysis
o Kidney ureters and bladder ultrasound

Treatment and prevention of CIN


Non-pharmacologic Treatment

• Identify all at risk patients; diabetic mellitus, heart failure, patients with CKD
• Stop NSAID 24-48 hours prior to contrast study
• Encourage adequate hydration prior to study
• Use lower possible dose of contrast (<125 ml)
• Use low osmolar (iohexol, ioversol) or iso-osmolar (iodixanol) contrast media

Pharmacologic Treatment

• Fluid administration should be used if there are no contra-indications. Normal saline should
be administered before and continued for few hours after the study
o Outpatients: 3mL/kg over one-hour pre-procedure and 1-1.5mL/kg/hour during
and for four to six hours’ post-procedure, with administration of at least 6mL/kg
post-procedure

490

o Inpatients; 1mL/kg/hour for 6-12hours pre-procedure, intra-procedure, and for 6-


12hours post-procedure
Note
Patient with severe CIN may need to undergo haemodialysis if there is no improvement within
7days.

21.10 Urinary Tract Infection (UTI)


Urinary tract infections may involve the upper or lower urinary tract. Infections may be complicated
or uncomplicated. Uncomplicated cystitis is a lower UTI in a non-pregnant woman of reproductive
age and who has a normal urinary tract. All other UTIs should be regarded as complicated. The
commonest causative pathogens for UTIs irrespective of the group of patients involved in Tanzania
are Escherichia coli, Klebsiella pneumonia, Proteus spp. and Staphlococcus aureus.

Note
• Differentiation of upper from lower urinary tract infection in young children is not possible
on clinical grounds
• Upper UTI is a more serious condition and requires longer and sometimes intravenous
antimicrobial treatment.
• Special considerations should be given in the following groups of patients: children,
pregnant women, elderly (>60 years) and other individuals with functional or structural
abnormalities in the urinary tract.

Clinical presentations of lower UTI (cystitis)


• Suprapubic pain/tenderness, dysuria, frequency, and urgency
• Pyuria and occasionally haematuria
• Temperature 380C or higher

Clinical presentations of upper UTI (pyelonephritis)


• Flank pain/tenderness • Temperature 380C or higher
• Pyuria and occasionally haematuria • Vomiting

Clinical presentations of catheter associated UTI (CAUTI)


• Presence of symptoms and signs of UTIs (as stated in cystitis or pyelonephritis above)
occurring in a person whose urinary tract is currently catheterized or has had a catheter in
place within the past 48 hours.

Clinical presentations of urosepsis


• Any of the above features of cystitis or pyelonephritis plus two or more of the following: (1)
Temperature >38° C or <36° C; (2) tachycardia >90 beats per minute; (3) tachypnoea
>20/minute, (3) WBC count>12,000/mm3 or <4000/mm3; confusion, hypotension or any
other evidence of organ dysfunction as a sequelae of UTI complications.

Investigations
• Quantitative or semi-quantitative urinalysis (high protein, low sugar, nitrites positive,
leucocyte esterase positive, and low pH) and Urine microscopy (>8–10 WBC/HPF) may be
suggestive of UTIs.
• Quantitative urine culture (growth of at least 104 or 105 colony forming units of bacteria/ml
of urine) and antimicrobial sensitivity testing. Concomitant urine and blood cultures are
indicated in case of urosepsis.
• Urinary LAMM – in patients with suspected to have genitourinary TB
• Ultrasound (kidney and pelvis) to exclude stones or structural abnormalities in patients with
recurrent UTI

Note
Positive WBC counts on urinalysis or urine microscopy + compatible 2 or more clinical presentations
supported by urine culture in centers where this test is available.

Non-pharmacological Treatment,
• Ensure adequate hydration

491

• Voiding of urine whenever an urge to micturate occurs; or after sexual intercourse in


adults.
• Removal of indwelling bladder catheter (where indicated)

Pharmacological Treatment
Analgesics in severe dysuria and flank pain
Adult:
A: paracetamol (PO) 500-100mg every 6-8hours.
Children:
A: paracetamol (PO) 15 mg/kg/dose 4–6hourly when required to a maximum of 4doses
per 24hours;

Uncomplicated cystitis

Adults:
A: nitrofurantoin (PO) 100mg 12hourly for 5days
OR
B: flucloxacillin + amoxicillin (FDC) (PO) 500mg 8hourly for 5days

Complicated cystitis
Adults:
A: ciprofloxacin (PO) 500mg 12hourly for 7days
OR
B: amoxicillin+ clavulanic acid (FDC) (PO) 625mg 12hourly for 7days

For pregnant women and adolescents


A: nitrofurantoin (PO) 100mg 12hourly for 5days
OR
B: amoxicillin + clavulanic acid (FDC) (PO) 625mg 12hourly for 7days

For children
A: nitrofurantoin (PO) 50mg 12hourly for 5days (Do not give Nitrofurantoin if the child has
G6PG deficiency or porphyria)
OR
B: amoxicillin + clavulanic acid (FDC) (PO) 40mg/kg/day of amoxicillin in 3divided doses
(maximum 2000 mg amoxicillin) for 7days

Acute Pyelonephritis
Outpatient therapy is only indicated for women of reproductive age, who do not have any of the
danger signs – see referral criteria. All other patients should be referred.
A: ciprofloxacin (PO) 500mg 12hourly for 10days
OR
B: ceftriaxone (IV) 1g [For a child ceftriaxone (80 mg/kg I.V or I.M)] 24hourly for 5days

Catheter associated UTI (CAUTI)


Patients with indwelling or suprapubic catheters and nephrostomy tubes invariably become carriers
of potential bacterial pathogens and routine antimicrobial treatment is not indicated. However,
judicious evidence from clinical and laboratory evidence is critical to warranty antimicrobial
therapies.
A: ciprofloxacin (PO) 500mg 12hourly for 7days

Urosepsis
A: gentamicin (I.V/I.M) 120mg [For children 7.5mg/kg] 24hourly for 5days (completion of
10days treatment to be guided by culture results)
AND
D: ceftriaxone + sulbactam (FDC) (IV) 1g [For children 80 mg/kg I.V or I.M] 24hourly for
5days

Alternatively;
A: gentamicin (I.V/I.M) 120mg [For children 7.5mg/kg] 24hourly for 5days (completion of
10 days’ treatment to be guided by culture results)
AND
S: piperacillin + tazobactam (FDC)(IV) 4.5g 6-8hourly for 5–7days
492

OR
S: Meropenem (IV) 250–500mg 8hry for 5–7days

Once results for urine and blood cultures are available change the antibiotic treatment options
accordingly.

Referral
Refer the patient urgently to the next facility with adequate expertise and facilities if: -

Acute pyelonephritis with:


o Vomiting
o Features of suggestive of urosepsis
o Diabetes mellitus
Acute pyelonephritis in:
o Pregnant women
o Women beyond reproductive age
o Men

21.10 Urology Disorders


Are diseases that affect urinary system including urinary incontinence, urolithiasis, benign prostatic
hyperplasia, prostate cancer.

21.10.1 Prostatitis
It is an inflammation of the prostate usually secondary to bacterial infection caused by urinary or STI
pathogens.

Clinical Presentation
• Perineal, sacral or suprapubic pain • Varying degrees of obstructive
• Dysuria and frequency symptoms which may lead to
urinary retention
• Sometimes fever

Investigations
• Urine analysis
• Urine culture

Pharmacological Treatment
Acute bacterial prostatitis
In men < 35 years or if there are features of associated urethritis (STI regimen):
S: cefixime (PO) 400mg as a single dose

Followed by:
A: doxycycline (PO) 100mg 12hourly for 7days

In men > 35 years or if there is associated cystitis:


A: ciprofloxacin (PO) 500 mg 12hourly for 14days

Referral to Urologist if
• No response to treatment
• Urinary retention
• High fever
• Chronic/relapsing prostatitis

21.10. 2 Benign Prostatic Hyperplasia (BPH)


Benign prostatic hyperplasia is a noncancerous (benign) growth of the prostate gland. Management
of BPH depends on severity of symptoms according to International Prostate Symptom Score (IPSS)

Clinical Presentation
• Obstructive symptoms: weak, intermittent stream and urinary hesitancy
• Irritative (frequency, nocturia and urgency) voiding symptoms.
• Digital Rectal Examination reveals a uniform enlargement of the prostate with smooth
surface and firm in consistence. The median sulcus is also palpable

493

• Urinary retention with a distended bladder may be present in the absence of severe
symptoms, therefore it is important to palpate for an enlarged bladder during examination.
• Pelvic or transrectal USS confirms the prostate enlargement
• Prostatic specific antigen levels are within normal range
• Symptoms should be graded by the IPSS – international prostate symptom score into mild,
moderate and severe

Non-pharmacological Treatment
• Patients with mild symptoms should be put under watchful waiting (change of lifestyle and
regular follow up)
o Reduce fluid intake especially in the evening, avoid caffeinated drinks
• Patients with severe symptoms should undergo surgery, transurethral resection of the
prostate for prostate weighing up to 75g and those weighing more than 75g should
undergo open prostatectomy
• For patients presenting with urinary retention, insert a urethral catheter as a temporary
measure while patient is transferred to hospital
• Remove drugs that prevent urinary outflow e.g. tricyclics and neuroleptics.

Pharmacological Treatment
Patients with moderate symptoms according to IPSS should be put under medical therapy unless
opt for surgery.
Medical treatment of BPH includes alpha-adrenergic blocker or 5 alpha- reductase inhibitor or a
combination of both

Adrenergic Alpha Blockers:


D: tamsulosin (PO) 0.4mg 24hourly
OR
D: alfuzosin (PO) 10mg 24hourly

5-alpha Reductase Inhibitors


D: finasteride (PO) 5mg 24hourly
OR
S: dutasteride (PO) 0.5mg 24hourly
Anticholinergics
S: oxybutynin (PO) 5mg 8hourly for patients with persistent urgency despite above
medications

Note
All patients with BPH and associated complications like recurrent UTI, Haematuria, Kidney
insufficiency, hernia and urinary stones need surgery and should be referred to centres where
specialized care can be offered.

21.10. 3 Prostate Cancer


Usually occurs in men over 50years and is most often asymptomatic. Systemic symptoms, i.e.
weight loss, bone pain, etc. occurs in 20% of patients. Obstructive voiding symptoms and urinary
retention are uncommon in the early stages of the disease.

Clinical Presentation
• The prostate gland is hard and may be nodular with obliterated median sulcus on digital
rectal examination and/or PSA elevation
• Verification of prostate cancer is by prostate core biopsy
• As the axial skeleton is the most common site of metastases, patients may present with
back pain or pathological fractures.
• Lymph node metastases can lead to lower limb lymphoedema.
• Serum prostate specific antigen (PSA) is generally elevated and may be markedly so in
metastatic disease.

Note
Interpretation of PSA should be interpreted careful, PSA has a low sensitivity therefore some
patients may have low PSA value (<4.0ng/mL) and have prostate cancer. There false positivity
where PSA is raised in the absence of prostatic cancer

494

Non-pharmacological Treatment
• Watchful waiting- low risk patients with short life expectancy
• Active surveillance-lowest risk of cancer progression and more than 10years life
expectancy
• Radical prostatectomy- patients with localized cancer and life expectancy more than
10years
• Surgical Androgen deprivation therapy (bilateral orchidectomy) for advanced prostate
cancer

Pharmacological Treatment
Medical androgen Deprivation Therapy is offered in patients with advanced disease, PSA levels
more than 50ng/ml, poorly differentiated tumour and in those who cannot receive any form of local
treatment.

For early disease


• Watchful waiting – low risk patients with short life expectancy
• Active surveillance – lowest risk for cancer progression and more than 10 years life
expectancy
• Radical prostatectomy – patients with localized cancer and life expectancy more than 10
years

Late disease
Luitenising hormone releasing hormone (LHRH) Agonists
S: goserelin (subcutaneous) 3.6mg every week or 10.8mg every 12weeks
OR
S: bicalutamide (PO) 50–150mg 24hourly
OR
S: Both LHRH and bicalutamide 50mg 24hourly if above options fail
OR
Castrate resistant prostate cancer
S: docetaxel 75mg/m2 every 3weeks

Referral for oncologist: All patients with suspected cancer (For more detail refer to the Malignant
diseases section)

21.10.4 Urolithiasis
Stones formed in the urinary tract are a result of urine, which is supersaturated with respect to a
stone-forming salt. Kidney stones have been associated with an increased risk for chronic kidney
disease, end-stage kidney failure, and cardiovascular diseases.

Clinical Presentation
• Sudden onset of acute colic, localized to the flank, causing the patient to move constantly.
• Sweating, pallor, nausea and vomiting and blood in urine
• Referred pain to the scrotum or labium (L1) on the same side as the stone moves down
the ureter
• Urinalysis with features of infection or microscopic haematuria
• Ultrasound with an acoustic shadow with features of obstructive uropathy eg. Hudroureter
or hydronephrosis
• Plain x-ray can pick up to 90% of calculi as they are radio-opaque
• Conventional intravenous urogram or CT urography confirms upper urinary tract lithiasis.

Investigations
• Plain abdominal X-ray
• Non-contrast CT-Scan of the Kidney Ureter and Bladder (CTKUB) – GOLD STANDARD
• Ultrasonography – Kidney Ureter and Bladder (KUB)
• Chemical composition of the stone – most valuable test
• Urinalysis – Dipstick biochemistry +Microscopy

For First Stone


• Serum Calcium, magnesium, phosphate, uric acid, urea, K, Na, Cl, HCO3

495

Recurrent Stone
• Parathyroid hormone
• Urine dipstick – biochemistry
• 24-HR Urea, creatinine clearance, sodium, calcium, oxalate and uric acid

Table 21.7: Non-Pharmacological Treatment

Type of stone Prevention strategy


All stones Increase water intake to have at least 2L of urine/day
Hyperoxaluria Low oxalate diet + increase dietary calcium intake
Limit vitamin C supplementation
Calcium stones Reduce salt intake, Restriction of animal protein (less meat, fish
and poultry)
Increase intake of fruits and vegetables
Calcium oxalate, cystine and Diet high in fruits and vegetables, Prescription citrate,
uric acid
Uric acid Control gout
Calcium phosphate and struvite Acidify urine

• Surgical intervention is indicated (uteroscopy, percutaneous nephrolithotomy and


extracorporeal shockwave lithotripsy) for
o obstructive uropathy
o infection,
o urgent intervention (surgical or otherwise) if a patient has a solitary kidney
emergency decompression is indicated by percutaneous nephrostomy placement
or ureteric DJ Stenting
• Stone fragmentation with ureteroscopy stone fragmentation/ ultrasonic
disaggregate/extracorporeal shock wave lithotripsy

Pharmacological Treatment
Analgesia for pain, if needed:
A: ibuprofen (PO) 400mg 8hourly for 3 days
OR
A: diclofenac (IM) 75mg stat then continue (PO) 50mg 8hourly
OR
B: tramadol (IV) 100mg stat then continue with (PO) 50mg 8hourly
OR
B: pethidine (IM) 100mg stat
Other management e.g. antiemetic for vomiting may be needed or IV fluids

For distal ureteric calculi less than 7mm


D: tamsulosin (PO) 0.4mg 24hourly for a month may be prescribed for spontaneous stone
expulsion.
OR
B: nifedipine (PO)10mg 24hourly for 30days (monitor blood pressure)

For prevention of stone


Thiazide diuretics for calcium stones ANY of the following
A: bendrofluazide (PO) 5mg 24hourly
OR
D: hydrochlorothiazide (PO) 12.5-50mg 24hourly

For low uric acid levels


AND
B: allopurinol (PO) 50-100mg 24hourly

21.10.5 Obstructive uropathy


Obstructive uropathy contribute to the burden of CKD, obstruction may occur anywhere along the
urinary tract. Causes of obstruction vary based on the location of obstruction
• Obstruction within the kidney causing dilatation of individual calyces

496

• Obstruction at or distal to the renal pelvis causes diffuse caliectasis of hydronephrosis.


Ureteral obstruction may result from stones, tumors, enlarged lymph nodes and
retroperitoneal fibrosis
• Bladder tumors can obstruct one or both ureters or ureteric orifices

Clinical Presentation
Generally, patients present one or more of the following symptoms
• Pain
• Change in urine output
• Hypertension
• Hematuria
• Increased serum creatinine

Investigations
• Urinalysis
• Full blood count
• Serum creatinine
• KUB ultrasound
• Intravenous pyelography
• CT IVU
• MRI
• Examination under anaesthesia

Non-pharmacological treatment
Measures to reduce recurrence risk
• Taking adequate fluids 2L/day for patients with renal stones

Pharmacological Treatment
• Relief of pain
C: diclofenac (PO) 100mg as initial dose followed by 50mg 6-8hourly
OR
C: morphine (IV/SC) 1-4mg 1-4hourly (may increase up to 10mg 4hourly as needed for
acute pain)

Referral of the patients


• The patient should be referred to the urologist for definitive treatment of the cause of
obstruction
• Patient may need long term follow up if there is impaired renal function

21.11 Sexual Dysfunction


21.11.1 Female Sexual Dysfunction
Sexual dysfunction in women refers to sexual problems associated with personal distress and may
take different forms including lack of sexual drive, impaired arousal, failure to achieve orgasm or
dyspareunia. Diagnostic criteria are reached when a sexual problem is recurrent/ persistent and
result in personal distress.

The causes of sexual dysfunction are multifactorial and may include psychological problem
(depression or anxiety), relationship conflicts, fatigue, stress, prior physical or sexual abuse,
medications or physical problems that make sexual activity uncomfortable (endometriosis,
genitourinary symptoms of menopause).

497

Non-pharmacological Treatment
Correction of contributing factor (genital lesion, systemic or hormonal factors and drugs e.g. SSRIs)
Psychological therapies
Use of antidepressants

21.11.2 Male sexual dysfunction


It is inability to attain and maintain an erect penis with sufficient rigidity for vaginal penetration and
ability to ejaculate. Organic causes include neurogenic, vasculogenic, endocrinological as well as
many systemic diseases and medications.

Non Pharmacological Treatment


• Education counselling
• Consider the removal of drugs that may be associated with the problem.
• A change in lifestyle or medications may resolve the problem, e.g. advise cessation of
smoking and alcohol abuse.

Pharmacological Treatment
• Treat the underlying condition.
• If persist refer the patient

Note
The use of medication like sildenafil may result to serious problem.

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CHAPTER TWENTY-TWO
MALIGNANT DISEASE CONDITIONS

22.1 Cancer Prevention, Screening and Early Detection


Cancer represents a unique public health opportunity, unlike other Non-Communicable disease, it is
possible to prevent most of cancers prevails in Sub-Saharan Countries including Tanzania by
intervening at both Primary and secondary levels of the natural history of the disease.

Primary prevention is mainly based on educating the public to modify their life styles to avoid risk
factors for cancer as well as ensure the availability and affordability of prophylactic vaccines, the
secondary prevention focus on the availability of effective screening programs that allow for
reducing incidence and downstage cancer.

Early detection detects (or diagnoses) the disease at an early stage, when it has a high potential for
cure (e.g. cervical or breast cancer) reduce morbidity, improve quality of life as well as increase
survival due to good outcome following treatment.

Key interventions in Cancer Prevention Primary Prevention


This is the most efficient and cost-effective form of cancer control it involves prevention interventions
that keeps a cancerous process from developing which can be through behavior change by health
counseling, education and environmental controls or through a biological mechanism, such as
Vaccination.

Among the most important modifiable risk factors for cancer are: tobacco use; overweight, and
obesity; harmful alcohol use; sexually transmitted human papilloma virus (HPV) infection, HIV/AIDS;
air pollution, both outdoor and indoor; and occupational carcinogens.

Public health education and promotion: Public Awareness raising on risk factors for cancer and
providing education on ways of avoiding as well as reducing exposure through behavior change is
essential. However, this is a long term intervention and may be difficult to quantify. Community
education should also focus raise awareness and knowledge on the benefits of early diagnosis,
ways of detection and screening. These preventive measures should be highly promoted by also
raise awareness of warning symptoms and signs of cancer and taking prompt action, by the general
public as well as physicians, nurses and other health care providers, can have a great impact on the
disease through early diagnosis and hence more effective management.

Vaccination
Human papillomaviruses (HPVs) is among the most important infections associated with cancers,
which can cause most cervical and anal cancers as well as a fraction of oral cancers; hepatitis B
virus (HBV) and hepatitis C virus (HCV), which can cause liver cancer; and Helicobacter pylori,
which is a bacterium that can cause cancer of the stomach.

Highly effective vaccines against HBV have been available for several decades and most countries
include HBV vaccination in their childhood immunization programs; vaccination is also highly
effective in preventing infection with the HPV types that cause the majority of cervical cancers.

Hepatitis Vaccination is recommended to general population and the high risk group such as health
care workers, and can be done at all levels. The Vaccine is given in 3 doses in 6 months. Second
dose should be given after 1 month after 1st dose and 3rd dose 6 months after the first dose.

HPV vaccination is recommended to girls between the age of 9 to 14 years. HPV vaccine is given in
two doses at 6 months apart.

Secondary Prevention: Early detection and Cancer Screening


The main aim of cancer screening is to prevent death from cancer. Screening can also make it
possible to use less severe treatment methods if the cancer is detected early enough. Cervical,
breast, skin, Prostate and bowel cancer, screening can actually prevent the cancer from developing.
However only cervical cancer screening is offered as part of an organized program with adequate
resources for high quality.

`499

Breast Cancer: Screening for breast cancer includes breast self-examination (BSE), clinical breast
examination (CBE) and breast imaging (mammogram and/or ultrasound scanning). BSE is
recommended at day 10 of the menstrual cycle. For post-menopausal women, a monthly BSE
schedule should be established.

All patients with clinical suspicious lesions should have imaging as part of early detection.
Mammogram is recommended for women over 40 years, while ultrasound is the imaging of choice
for younger women. MRI may be used where possible for screening and early detection in patients
at high risk of breast cancer such as those with BRCA1 & 2 gene mutations.

For prevention and early detection, all women aged 25 years and above should be taught on breast
self–examination and should be advised to have regular physical check with a heath provider and
have a regular annual Mammography. They should also be encouraged on physical excise and
proper diet.
Skin Cancer: Prevention or early detection is through frequent self–health check–up or screening
exercise and prompt treatment of early skin lesions. For light skinned people–avoid UV light
especially people with Albinism.

Colon: colorectal cancers are usually asymptomatic until advanced stage hence regular screening
with annual digital rectal examination, stool for occult blood + colonoscopy and are recommended
starting at 50 years of age.
Prostate: Routine screening not recommended, but when done should begin with PSA and digital
rectal examination at age 50 if life expectancy is >10 years. It is recommended that screening of
high risk group should take place starting at age 45.

22.2 Gynecological Malignancies


22.2.1 Cancer of the Uterine Cervix
It is caused by persistent infection with human papilloma Virus (HPV). Risk factors include early
coitus and childbirth, multiple sexual partners, smoking and HIV infection. It is preventable through
avoiding risk factors, screening and vaccination. When detected early, it is curable by surgery or
radiotherapy hence regular screening is required for all women.

Diagnostic Criteria
• Asymptomatic in early stages of the disease.
• Majority present with abnormal vaginal bleeding (post coital, inter-menstrual or
postmenopausal vaginal bleeding).
• Foul smelling discharge, pain and incontinence (VVF or RVF) are symptoms of late
disease

Investigations
• FBC, LFT, RFT and HIV test.
• CXR.
• Abdomen and Pelvis USS.
• Pelvic MRI, CT Scan of the abdomen and pelvis.
• PET/CT
• Bimanual Examination under Anesthesia (EUA) and Biospy.

Table 22.1 Management of Cervical cancer by disease stage.


Stage Management
Stage IA1: Simple hysterectomy or if patient desires fertility consider conization
Stage IA2–IB2 Consider Wertheim Hysterectomy plus bilateral pelvic lymph node
dissection. RT may be given post operation or alone. No benefit of
adjuvant chemotherapy
Stage IB2; IIA and IIB 2.0Gy/Per Fraction to 50Gy external beam + 8.0 Gy x 3 Fractions HDR
+/– Chemotherapy depending on renal function
Stage IIIA and IIIB If stage by CT or MRI and no distant metastasis and good renal function:
2.0Gy to 50 Gy external beam + 8.0 Gy x 3 Fractions HDR
Stage lll A and lll B 2.5 Gy to 50 Gy external beam only no HDR nor chemotherapy if poor
renal function
Stage lV A + good general Can be given curative dose of 50 Gy external beam

`500

condition, no VVF or RVF: + Brachytherapy or palliative dose of 20Gy/5 Fractions or 30 Gy/10


Fractions or 10Gy Single Fraction monthly X 2 Fractions
Stage lll B advanced/stage Palliative care / supportive care
lV B with bad general
condition

Pharmacological Treatment
Chemotherapy is given as a radiotherapy sensitizer or on palliative intent.
S: cisplatin (IV) 40 mg/m2 to max of 70 mg is given weekly during radiation therapy.
• If patient is HIV positive or has mild renal impairment consider 30 mg/m2 to max of 60 mg
weekly.
• Available and preferred palliative chemotherapy drugs for metastatic, recurrent or
persistent cancer after RT, given in single or combination regimen include: cisplatin,
paclitaxel, bevacizumab, carboplatin, docetaxel and gemcitabine.
• Do FBC, urea and creatinine before each cycle of chemotherapy.

Follow up:
First visit at 4–6 weeks post treatment then 3–6 months in the first 2 years, there after yearly.

*This follow-up schedule applies to all malignancies with few exceptions*


Note
• All patients suspected or confirmed to have cervical cancer should be
referred to cancer specialized centers for definitive management.
• All women aged 25 years and above are advised to have regular cervical
screening with VIA and VILI or Pap smear

22.2.2 Endometrial Cancer


This is predominantly a disease of old women. Adenocarcinoma is the commonest histological type.
Risk factors for endometrial carcinoma include obesity, diabetes, high fat diet, early age at
menarche, nulliparity and late age at menopause, old age and use of tamoxifen.
Diagnostic Criteria
• Abnormal Uterine Bleeding for women in the post-menopausal period.
• For Pre-menopausal women; may present with irregular bleeding, intramenstrual bleeding,
vaginal discharge, pain during intercourse and unexpected weight loss.
Investigations
• FBC, LFT, Urea, Creatinine
• Cancer Antigen 125 (CA 125)
• CXR
• Abdomen and Pelvis USS
• Abdomen and Pelvic CT scan and/or Pelvic MRI
• Endometrial biopsy to confirm the diagnosis
• PET/CT

Staging: FIGO and TNM

Table 22.2 Management of Endometrial cancer by Stage


Stage Management
All Patients Medically operable patients should undergo Surgery.
Perform TAH and BSO or radical hysterectomy if cervical stromal involvement
and obtain peritoneal cytology. Consider selective pelvic and paraaortic LN
dissection for myometrial invasion or if grade 2–3, and include nodes from
paraaortic, common iliac, external iliac, internal iliac, and obturator chains.

Stage 1A/1B Grade 1 - Observation; Grade 2-3 or presence of other adverse features: Offer
Vaginal Brachytherapy (VBT) 7Gy x 3 fractions
Stage IA, IB, II Offer Adjuvant Chemotherapy + Vaginal Brachytherapy 7Gy x 3 fractions Or
clear cell or Pelvic External Beam Radiation Therapy alone (46Gy)
serous

`501

carcinoma, IB
High Grade
Stage III Adjuvant Chemotherapy + Radiotherapy (High Risk Disease: EBRT (46Gy) +
VBT 7Gy x 3 fractions )
Stage IV Chemotherapy

Note
• For inoperable disease stage llb – lVA, radiotherapy and or chemotherapy can be offered
as neo-adjuvant prior to surgery

Pharmacological Treatment
Cytotoxic therapy for inoperable, metastatic or recurrent disease is given with palliative intent.
Recommended regimens are;
S: doxorubicin (IV) 60 mg/m2 over 30 minutes AND cisplatin (IV) 50 mg/m2 1 hour(IV)
infusion on day 1; repeat every 21days for 4 – 6 cycles
OR
S: cisplatin (IV) 50 mg/m21-hour infusion on day 1 AND doxorubicin(IV) 45 mg/m2 over 20
minutes on day 2 AND paclitaxel (IV) 160 mg/m2 over 3hours on day 2 AND filgrastim
(SC) 5 µg/kg on days 3–12; repeat every 21days for 4-6 cycles
OR
S: carboplatin (IV) AUC 5–6 1-hour infusion day 1 AND paclitaxel (IV) 175 mg/m2 over
3hours on day 1 repeat every 21 days for 4-6 cycles
Note
• All patients should be referred to a gynecologist for evaluation and surgical management
• All surgical specimens should be sent for histopathology diagnosis and staging.
• After surgery and histopathology report, all patients should be referred to cancer
specialized center for management and follow up.

22.2.3 Cancer of the Vulva


Vulva cancer is predominantly a disease of older women. Squamous cell carcinoma is the
commonest histological type, usually arising from premalignant lesions–vulva intraepithelial
neoplasia (VIN). Risk factors contributing to development of VIN and later vulva cancer include HPV
infection, infection with HIV, and cigarette smoking.

Diagnostic Criteria
• A lump or vulva mass
• Presence of leukoplakia and other dystrophic changes on the vulva
• Itching is a common manifestation and may become ulcerative (“non-healing ulcers”)

Investigations
• FBC, LFT, Urea, Creatinine, HIV test
• CXR
• Ultrasonography or CT scan of Abdomen and Pelvis
• Colposcopy to determine presence of other lesions in the vagina and cervix
• Biopsy from the vulvar lesion to confirm the diagnosis
• PET/CT

Staging: FIGO and TNM.


Management:
Treatment is individualized, taking into considerations of histological type, disease stage and patient
factors

Primary treatment is surgery. Wide Local Excision (Radical Vulvectomy) plus Groin Lymphnode
dissection.

Radiotherapy is indicated in the following conditions:


• As primary therapy for patient with small primary tumors particularly young patients in
whom surgical resection would have significant psychological consequences.
• For patients with locally advanced disease where resection is not possible.

`502

• After surgery to treat the pelvic and groin nodes.


• After surgery in patients with positive surgical margins.
• In palliation (Pain, Bleeding etc)

Pharmacological Treatment: As for cervical cancer

22.2.4. Gestational Trophoblastic Disease


22.2.4.1 Hydatidiform mole
Two types; complete and partial hydatidiform mole. Treatment is suction curettage or hysterectomy.
Careful risk assessment is needed to determine patients who require chemotherapy after surgery.
Patient with high risk hydatidiform mole will have to reserve single agent chemotherapy;
methotrexate or actinomycin D
Note: Patient should be followed up with weekly serum β–hCG after surgery until it is undetectable.
22.2.4.2 Choriocarcinoma
Choriocarcinoma is extremely chemo sensitive; cure is possible even in metastatic disease. All
patients with choriocarcinoma should undergo a careful pre-treatment evaluation for proper staging
and risk stratification.

Investigations:
• Serum β-hCG level
• LFT, RFT, TSH, T3, T3
• CXR and or CT Scan chest
• Abdomen and Pelvis USS or CT Scan
• Brain MRI
• Tissue sample for histology
• CSF hCG level
• PET/CT
Clinical presentation:
• Persistently raising or plateau BhCG postmolar pregnancy.

Staging: FIGO Staging

Stage I – Persistently elevated human chorionic gonadotropin (hCG) levels; tumor confined to the
uterine corpus
Stage II – Tumors extending to the adnexa or to the vagina, but limited to the genital structures
Stage III – Pulmonary metastases on chest radiograph, with or without uterine,pelvic, or vaginal
involvement
Stage IV – Metastatic disease outside of the lungs and pelvis and/or vagina

Table 22.3 Prognostic Factors required for Stage grouping and Risk score
Risk Score
Prognotic Factor 0 1 2 4 Factor
score
Age (years) <40 >40
Antecedent pregnancy Hydratidiform Abortion Term
mole pregnancy
Interval months from index <4 4-6 7-12 >12
Pregnancy
Pretreatment hCG (IU/mL) <103 103 to 104 to 105 >105
<104
Largest tumor size, <3 3-5 >5
including uterus (cm)
Site of metastasis Lung Spleen, Gastrointestinal Brain,
kidney tract liver
Number of metastasis 1-4 5-8 >8
identified
Previous failed Single Two or
chemotherapy medicine more
medicines
Total Risk Score

`503

Table 22.4 Risk Stratification (FIGO) and Treatment recommendation


Stage / Score Recommendation
Low risk: Stage I – III with Single agent: methotrexate (IV) or actinomycin D (IV)
WHO risk score below VI
High risk: Stage IV or II Combination therapy:
and III with WHO risk 1. EMACO (etoposide, methotrexate, actinomycin D,
score above VI cyclophosphamide, vincristine) (IV)
2. APE ( actinomycin D, cisplatin, etoposide) (IV)
Brain metastasis methotrexate, dexamethasone and prophylactic anti epileptic to
control seizures Or High dose EMACO plus intrathecal
methotrexate and leucovorin.
Concomitant whole brain radiation: 20-30 Gy in 2Gy daily fraction
concurrently with high dose chemotherapy(MTX)

Note
Do serial measurement of BhCG at start of treatment and weekly during therapy.

Table 22.5 Recommended Chemotherapy regimens for Single agent


Single Agent
1 S: actinomycin D (IV) 12µg/Kg daily for 5 days
With response: Repeat same dose
Without response: add 2µg/Kg to the initial dose or switch to methotrexate protocol
2 S: methotrexate (IV) or (IM) 0.4mg/Kg daily for 5 days
With response: Repeat same dose
Without response: add 0.6mg/Kg to the initial dose or switch to actinomycin D protocol
Note:
• Do serial measurement of BhCG at start of treatment and weekly during therapy.

• Do FBC, Platelet count, LFT daily.

• If no response to single agent , give combination drugs.

Table 22.6 Recommended Chemotherapy regimens for Combination therapy


Combination Therapy (EMACO – Regimen)
Course Day 1 S: VP – 16 (etoposide) (IV) 100mg/m2 infusion over 30 minutes AND actinomycin
1 D (IV) 0.5mg bolus AND methotrexate (IV) 100mg/m2 bolus, followed by a
200mg/m2 IV infusion over 12 hours
(EMA)
Day 2 S: VP – 16 (etoposide) (IV) 100mg/m2 infusion in 200ml of saline over 30 minutes
AND actinomycin D (IV) 0.5mg bolus
folinic acid (IM) 15mg OR orally every 12 hours for 4 doses beginning 24 hours
after start of methotrexate (IV)

Course Day 8 S: vincristine (IV) 1mg/m2 (IV) bolus AND cyclophosphamide 600mg/m2 1 hour
2 (IV) infusion.
(CO)
Note
• Cycles are repeated after every 14 days until β–hCG is normal

`504

Follow-up
• Weekly measurement of hcg level until they are normal for 3 consecutive weeks
• Monthly hcg levels until levels are normal for 12 consecutive months
• Effective contraception during the entire period of hormonal follow–up

22.2.5 Cancer of the Ovary


Epithelial tumours comprise 90% of all ovarian malignancies. Due to anatomical location, most
patients present with advanced disease.

Diagnostic Criteria
• Minimal or no symptoms in early stage
• Abdominal distension with palpable mass, pain and ascites are all late signs

Investigations:
• Inspection and bimanual examination under anesthesia (EUA) recto–vagina are mandatory
to exclude primary disease or extension from other sites such as cancer of the cervix
• FBC, RFT, LFT, CA 125 & CEA
• CXR
• Abdomen and Pelvis CT Scan or USS
• Histology of Oophorectomy specimen or biopsy obtained at laparotomy
• Ascitic fluid/peritoneal and pelvic washing cytology

Staging: Is based on surgical diagnosis (laparotomy): FIGO: IA, IB, IC, IIA, IIB, IIC, IIIA, IIIB, IIIC,
IVA and IVB.

Table 22.7: Management: Surgery


Stage 1 and 2 Total hysterectomy with Bilateral Salpingo –Oophorectomy (TAH+BSO) and
omentectomy should be performed in resectable tumor.

If total tumor removal is not possible, then maximum debulking (Cyto –


reductive) surgery is done. This is followed by adjuvant Chemotherapy.
Unilateral salpingo-oophorectomy is only justified for stage IA tumour with
favourable histology.
Stage 3 Neoadjuvant chemotherapy followed by Surgery and then Adjuvant
Chemotherapy.
Stage 4 As stage 3 +/- Palliative care.

Pharmacological Treatment
Adjuvant chemotherapy
Indicated in all patients at high risk i.e. stage IC or II, high grade or clear cell cancers of any stage.
Recommended regimens is;
S: carboplatin (IV) AUC 6 1 hour infusion Day 1 AND paclitaxel (IV) 175 mg/m2 over 3
hours day1; repeat every 21days for 6 cycles.

For recurrent disease: give same regimen if tumor is platinum sensitive (recurrence after 6 months
since last chemotherapy cycle)
For platinum resistant disease give gemcitabine or bevacizumab as single agent or in combination
with taxanes. When available, liposomal doxorubicin is active and indicated in recurrent disease.

S: gemcitabine (IV) 1000 mg/m2 30 minutes infusion Day 1, Day 8 and Day 15;
Repeat every 4 weeks for 6 Courses
S: bevacuzimab (IV) 15 mg/kg 1-hour infusion Day1, every 3 weeks until
disease progression

Endocrine therapy is indicated in selected cases with recurrent disease.


S: tamoxifen (PO) 20mg every 12 hourly,daily AND goserelin (SC) 3.6 mg
every 4 weeks or 10.8mg every 12 weeks

Note
All patients must be referred to a gynecologist and cancer specialized center for evaluation and
proper management

`505

22.3 Breast Cancer


The etiology of breast cancer is so far unknown, however, age, nulliparity, not breastfeeding, first
pregnancy age 35years, previous radiation exposure, family history of breast cancer, smoking and
alcohol consumption, are the risks associated with breast cancer.

Screening for breast cancer includes breast self-examination (BSE), clinical breast examination
(CBE) and breast imaging (mammogram and/or ultrasound scanning and or MRI Breast). All
patients with clinical suspicious lesions should have imaging as part of early detection.

Diagnostic criteria
A solitary hard lumps or mass in the breast that may be associated with
• Changes of breast skin appearance or ulceration
• Nipple retraction
• Presence of axillary lymphadenopathy or elsewhere
• Attachment/fixed to chest wall muscles

Other symptoms and signs include cough, bone pain/fracture, or neurological symptoms depending
on site of metastasis

Investigations
• FBC, LFT, Urea, Creatinine
• ECHO Mammogram/MUGA (Baseline Ejection Fraction and follow up)
• Bilateral Mammography, Breast Ultrasound as necessary
• CXR
• Abdominen and Pelvic USS
• Bone scan
• CT scan and or PET/ CT where indicated
• Open biopsy for histopathology and Immunohistochemistry (IHC)
• A core needle biopsy done manually, or preferably by ultrasound or stereotactic guidance
is recommended.
• Immuniohistochemistry (IHC) – ER, PR and Her 2
• FISH/CISH for Equivocal Her 2 for Confirmation of Her 2 OverExpression
• Breast MRI may be of value in select group of women who have had equivocal
mammogram/ ultrasound.

Staging: TNM
Management: Includes surgery, chemotherapy, radiotherapy, hormonal therapy and targeted
therapy

Surgery
Optimal management includes multidisplinary evaluation by clinical oncologist and breast surgeon.

Options for surgical management include:


• Breast conserving surgery with lumpectomy/quadrantectomy
• Modified radical mastectomy
• Toilet Mastectomy

As described above, all surgical approaches should include surgical axillary staging with axillary
lymph node dissection to level 1 and 2 nodes (>10 lymph nodes dissected).

Surgical approaches aimed at breast conservation should only take place in cases that allow for
multi-disciplinary management with access to radiotherapy. If radiotherapy access is limited,
mainstay of surgical care should be modified radical mastectomy.

Radiotherapy is strongly indicated in the following conditions:


• After BCS
• T3–4 tumor
• Positive surgical margin
• If ≥ 4 sampled lymphnodes are positive
• Palliation for fungating and bleeding tumor, mets to bones, brain etc.

`506

Radiotherapy dose: 50Gy/25 Fractions given in 5 weeks or Hypofractionation 40.05Gy/15


Fractions. For palliative intent usually 30Gy/10 Fractions in 2 weeks

Pharmacological Treatment
Chemotherapy is indicated for almost all patients as neo-adjuvant, adjuvant or palliative. Patients,
who are planned for surgery and have ≥ T3 tumors, should receive neo-adjuvant chemotherapy
before operation.

Table 22.8 Recommended chemotherapy regimens for Breast cancer


Dosing schedules for combinations for HER 2 negative disease:

1 Dose-dense doxorubicin (IV) AND cyclophosphamide(IV) followed by weekly paclitaxel (IV)

S: doxorubicin (IV) 60 mg/m2 over 30 minutes’ day 1 AND cyclophosphamide (IV) 600 mg/m21-hour
infusion day 1 given every 14 days for 4 cycles

Followed by

S: paclitaxel (IV) 80 mg/m2 by 1-hour infusion weekly for 12 weeks.

2 Dose-dense adriamycin AND cyclophosphamide followed by 3 weekly taxanes

S: doxorubicin 60 mg/m2 (IV) over 30 minutes on day 1 PLUS cyclophosphamide 600 mg/m2 1 hour
(IV) infusion day 1 given every 21 days for 4 cycles then

Followed by

S: paclitaxel (IV) 175 mg/m2 3 hours infusion day 1, given every 21days for 4 cycles
OR
S: docetaxel (IV) 100 mg/m2 3 hours infusion day 1 given every 21days for 4 cycles.

3 TAC (IV) chemotherapy regimen

S: docetaxel (IV) 75 mg/m2 3 hours’ infusion day 1 AND doxorubicin (IV) 50 mg/m2 30 minutes’ day
1 AND cyclophosphamide (IV) 500 mg/m2 1-hour infusion day 1 given every 21 days for 6 cycles.

Dosing schedule for combinations for HER2-Positive disease:

1 S: doxorubicin (IV) 60 mg/m2 30 minutes’ day 1 AND cyclophosphamide (IV) 600 mg/m2 1-hour
infusion day 1 given every 21 days for 4 cycles followed by paclitaxel (IV) 80 mg/m2 1-hour infusion
weekly for 12 weeks
AND
S: trastuzumab (IV) 4 mg/kg with first dose of paclitaxel (IV) followed by trastuzumab (IV) 2 mg/kg
weekly to complete 1 year of treatment.

2 As an alternative, trastuzumab (IV) 6 mg/kg (IV) every 21 days may be used following the
completion of paclitaxel (IV) and given to complete 1 year of trastuzumab (IV) treatment.

Note
• All cycles are with myeloid growth factor support.
• FBC, RFT, LFT before each cycle.
• Cardiac monitoring at baseline, 3, 6, and 9 months.

Other Regimens are:


S: CAF (cyclophosphamide, adriamycin and 5-flourouracil)/
S: CEF (cyclophosphamide, epirubicin and 5-fluorouracil) and
S: CMF (cyclophosphamide, methotrexate and 5-fluorouracil) (for elderly patients>65 yrs
with poor cardiac function)

`507

For Metastatic Breast Cancer (Stage 4):


Chemotherapy regimens for either combinations ie
S: CAF, CEF, gemcitabine/paclitaxel,
S: trastuzumab+paclitaxel/carboplatin or trastuzumab+paclitaxel or trastuzumab +
docetaxel or trastuzumab+capecitabine; or single agent
S: trastuzumab, taxane or capecitabine or gemcitabine.

Endocrine therapy
Premenopausal ER/PR Positive
S: tamoxifen (PO) 20 mg daily for 5 years

Post-menopausal ER/ PR Positive


S: anastrazole (PO) 1 mg daily for 5 years
OR
S: tamoxifen (PO) 20 mg daily for 2 years followed anastrazole (PO) 1 mg daily for 3
years.

Note
● All patients must be referred to a specialized oncology center for proper management

22.4 Cancer of The Skin


Skin cancers are classified into non melanoma and malignant melanoma.
22.4.1 Non-melanoma Skin Cancers
Basal cell carcinoma (BCC) and squamous cell (SCC) are the most common non melanoma skin
cancers. SCC is more aggressive than BCC and has the potential to metastasis. The main cause of
these skin cancers is overexposure to Ultraviolet radiation. Risk factors include light-coloured skin
(e.g albinism), previous burn and immunosuppression eg after transplant or HIV infection

Prevention or early detection; is through frequent self–health check–up or screening exercise and
prompt treatment of early skin lesions. For light skinned people–avoid UV light especially people
with Albinism.

Diagnostic Criteria
The most common warning sign of skin cancer is a change in the appearance on exposed areas of
the skin, such as a new growth or a sore that will not heal. Occasionally, such changes may appear
on an old burn area.

Investigations
• None if lesion is small
• Local X-ray if bone involvement is suspected
• CXR
• Biopsy – preferably excisional biopsy where possible for histology
• CT or MRI for suspected Nodal and bone involvement.
• PET/CT when indicated

Management
Surgery is the primary treatment. Wide local excision that achieves negative surgical margins is
adequate. Skin grafting may be required after surgery. Amputation sometimes is done for palliation.
Locally destructive methods such as curetting or cryotherapy may be employed
Radiotherapy
Indication: Positive margin, high grade disease or inoperable tumour.
Dose: 60-66Gy/ in 30-33 Fractions EBRT for Radical Treatment, 30Gy in 10 Fractions for palliative
treatment

Pharmacological Treatment
S: 5-fluorouracil topical cream apply every after 12 -24 hours, for very superficial lesions or
carcinoma in situ
Systemic chemotherapy is given for palliation in advanced stage or as radio sensitizer.

`508

22.4.2 Malignant Melanoma


Diagnostic criteria
History of a pre-existing naves which has changed recently –itching, colour change, increase in size,
satellite lesions, elevated surface, ulceration and/or oozing.

Investigations
• CXR
• Abdomen and Pelvic CT Scan or USS
• PET CT
• Excisional biopsy of suspicious lesion for histopathology

Staging: Clark’s or Breslow classifications are used. Tumour size closely correlates with prognosis.
Detection/ prevention: Frequent self –check up or screening exercise and prompt treatment of naves

Management: Surgery is the primary treatment.


• Wide local excision and graft
• Amputation sometimes for advanced useless limb

Pharmacological Treatment

S: cisplatin (IV) 20mg/m2/day 30 minutes’ infusion day 1-4 AND vinblastine (IV)
1.6mg/m2/day bolus day 1-5 AND dacarbazine (IV) 800mg/m2 30minutes infusion day 1
repeat every 21 days for 6 cycles
OR
S: dacarbazine (IV) 250mg/m2 30 minutes’ infusion Day1–Day 5 every 21 days
for 4 cycles
OR
S: temozolomide (PO) 200mg/m2 Day 1–Day 5 every 28 days

Radiotherapy used for palliation if:


• Lesion is inoperable. May use large fractions: 30Gy/6Fractions/1 week
• Excision margins are involved or very close
• Palliative intent 30Gy in 10 Fractions/ 20Gy in 5 Fractions (brain mets, fungation or profuse
bleeding, bone pain etc)

22.4.3 Kaposi’s sarcoma (KS)


It is a malignant tumour of angio–formative cells usually starting from the skin but occasionally
involving many other organs of the body. Kaposi sarcoma can be primarily categorized into four
types: epidemic of AIDS–related, immunocompromised, classic or sporadic, and endemic (African).
Here we have Non AIDS related (endemic) KS and AIDS related (epidemic) KS where the late is
more common 80–85%.
Diagnostic criteria
• KS presents as a firm, dark brown nodules or plaque in the skin. Usually more on the limbs
• In young children and those with immunodeficiency it presents as wide spread
lymphadenopathy with or without skin lesions.
• Presence of B symptoms (fever, sweating and weight loss) is commonly associated with
epidemic type.

Investigations
• FBC, LFT, Urea & Creatinine, HIV test (if positive CD4 count and viral load)
• CXR
• Abdomen and Pelvis ultrasound or CT scan
• Chest Scan CT
• Bronchoscopy and Endoscopy
• Skin biopsy for histological confirmation

Staging of KS: Epidemic Kaposi sarcoma use AIDS clinical trials group (ACTG) system and for
endemic/classical Kaposi sarcoma use Mitsuyasu classification system.

`509

Management:
• Treatment is palliative irrespective of type and stage hence careful assessment and
decision is required to choose the best palliative treatment.
• ARVs should be initiated in epidemic KS patients who have not started the treatment.
• Choice of palliation depends on clinical presentation and patient general condition.

Radiotherapy: Is the best palliative treatment in symptomatic patient with local or extensive
disease.
• 8Gy single fraction for disease on limbs or lower half body
• 6Gy single fraction for upper half body
• Dose of 9Gy/3Fractions or 22Gy/11 Fractions can be prescribed for lesions elsewhere.

Pharmacological Treatment
Palliative chemotherapy is usually given in patient with generalized disease.

Recommended regimens are:

S: doxorubicin (IV) 25 mg/m2 over 30 minutes day1 AND bleomycin (IV) 10 IU/m2 over 10
minutes’ day 1 PLUS vincristine (IV) 1.4mg/m2 over 10 minutes (max.2mg) day1 given
every 21 days for 6 –8 cycles
OR
S: paclitaxel (IV) 100mg/m2 day 1 every 14days
OR
S: docetaxel (IV) 75mg/m2 day 1 every 21days is given for persistent or recurrent after
ABV.

22.5 Head and Neck Cancers


Cancer of the head and neck include the following: The oral cavity, pharynx, larynx, nasal cavity,
para nasal sinuses, salivary glands, and thyroid.

These tumours may present with a neck mass due to lymph node metastases, with or without
findings from the primary disease site. Important etiological factors are smoking, excessive alcohol,
viral infections (eg HPV and EBV), genetic predisposition, previous exposure to radiation and
industrial chemicals. Squamous cell carcinoma is the commonest histological type for the
malignancies but salivary gland tumors are mostly adenocarcinoma.

22.5.1 Nasopharyngeal Cancer


Nasopharyngeal carcinoma is the predominant tumor type arising in the epithelium of the
nasopharynx.

Diagnostic Criteria
• Neck mass, unilateral hearing loss, tinnitus, nasal obstruction, epistaxis, and cranial nerve
palsies

Investigations:
• FBC, RFT, LFT and HIV
• CXR
• Abdominal ultrasound
• CT scan and/or MRI of the nasopharynx, skull base, and neck
• Nasopharyngoscopy
• Endoscopic guided biopsy of the primary tumor for histology
• PET CT
• Immunohistochemistry to further confirm the diagnosis

Staging: TNM staging system

Management
Due to deep location of nasopharynx, and anatomic proximity to critical structures, radical surgery is
typically not used. Role of surgery is initially for biopsy for histological confirmation. It may also be
used for management of the neck for persistently enlarged lymph node.

`510

Nasopharyngeal cancer is mainly treated by radiotherapy either alone or in combination with


chemotherapy.

Table 22.9 Management of Nasopharyngeal cancer by Stage


Stage Management
Stage I Radiotherapy alone to primary disease and neck
Stage II–IVB Concurrent chemotherapy and radiation to the primary disease and neck
Stage IVC palliative care (which may include chemotherapy and radiotherapy)
Induction chemotherapy If delays are anticipated in initiation of concurrent chemotherapy and
can be considered for radiation.
stage III–IVB
Local recurrence Chemotherapy, surgery or re-irradiation

22.5.2 Laryngeal Cancer


Laryngeal cancer is one of the most common cancers of head and neck. It is predominantly found in
men and mostly in those with history of tobacco smoking and alcohol intake. It is divided into three
major anatomic regions; supraglottis, glottis and subglottic.

Diagnostic Criteria
• Hoarseness, stridor, difficulty in breathing, neck mass, odynophagia, cough.

Investigations:
• FBC, RFT and LFT
• CXR
• CT scan and/or MRI of the Head and Neck
• Laryngoscopy
• Pathology: Definitive diagnosis is confirmed by laryngoscopy-guided biopsy of the primary
tumor

Staging: TNM Staging system


Table: 22.10 Management of Laryngeal Cancer by Stage
Stage Management
Stage I and II Primary site: Partial or Total laryngectomy OR Radiotherapy alone.
Stage III–IVB Concurrent Chemoradiation or Total Laryngectomy and neck dissection
followed by Adjuvant Radiotherapy or Chemo radiotherapy
Stage IVC Palliative care

22.5.3 Hypopharyngeal Cancers:


Hypopharyngeal cancer includes tumors arising from the pyriform sinus, posterior pharyngeal wall,
postcricoid region. It is associated with tobacco use, alcohol consumption, and Plummer–Vinson
syndrome.

Diagnostic Criteria:
• Dysphagia, odynophagia, change in speech (dysarthria), neck mass, referred otalgia,
throat pain, weight loss, sensation of mass in throat and hoarseness of voice.

Investigations
• FBC, RFT and LFT
• Hypopharyngoscopy and biopsy for histopathology
• CXR
• CT scan and/or MRI of the Head and Neck

Staging: TNM staging system.

Management
Radiation therapy is the mainstay of first-line local treatment for early stage hypopharyngeal
carcinoma. For more advanced disease, concurrent chemoradiation reduces the rate of distant
metastasis, and improves local control.

`511

22.5.4 Salivary Gland Cancer


Salivary gland cancers arise from major or minor salivary glands in the head and neck region. The
most common malignant salivary gland tumors are mucoepidermoid carcinoma and
adenocarcinoma

Presentation: Depends on primary site involved.


• Mass, pain, nerve palsies, neck mass

Investigations:
• FBC, LFT, and RFT
• CXR
• CT scan and/or MRI of Head and Neck
• Biopsy of the primary tumor for histology.

Staging: TNM staging system:


Treatment:
• Complete surgical resection with adjuvant radiotherapy if adverse features are present
• If disease is not resectable, definitive radiotherapy or concurrent chemoradiotherapy is
indicated
• Neck dissection is indicated for high-grade tumors or clinically positive neck disease

22.5.5 Nasal Cavity and Paranasal Sinus Cancer


These are tumors arising from nasal cavity and the four paired paranasal sinuses (frontal, ethmoid,
maxillary, and sphenoid).

Diagnostic Criteria:
Nasal obstruction, epistaxis, proptosis, double vision, cheek mass, loss of sensation of the cheek
and loosening or pain of the teeth

Investigations:
• FBC, RFT and LFT
• CXR
• Abdominal Ultrasound
• CT scan and/or MRI of the Para nasal sinuses and neck
• Direct fibre-optic endoscopy
• Endoscopic guided biopsy of the primary tumor for histopathology

Staging: TNM Staging system


Treatment:
• Treatment is by surgery and or radiotherapy with or without chemotherapy.
• Surgical resection of the primary tumor and neck dissection followed by radiotherapy can
be done in early disease stages. It may also be used for management persistently
enlarged lymph nodes, persistent or recurrent disease after radiotherapy.
• Stage I–IINO: Complete surgical resection followed by radiotherapy alternatively definitive
radiotherapy.
• Radiotherapy can be given as an alternative definitive treatment, either alone or in
combination with chemotherapy. It is used in palliative care for advanced diseases
• Chemotherapy is used in induction, concurrent or adjuvant therapy.

22.5.6 Oral Cavity Cancer


Oral cavity consists of the upper and lower lips, gingivobuccal sulcus, buccal mucosa, upper and
lower gingiva, retromolar trigone, hard palate, floor of mouth, and anterior two–third of the tongue.
Risk factors include smoking, excessive consumption of alcohol, poor oral hygiene, prolonged focal
denture irritation, betel nut chewing, and syphilis.

Diagnostic Criteria:
• Non-healing ulcer, speech difficulty, hypersalivation, neck mass, dysphagia and otalgia

`512

Investigations:
• FBC, LFT, RFT and HIV
• CXR
• CT Scan and/or MRI of the Head and Neck
• Mirror and fibre-optic endoscopic examination
• Biopsy for histologic confirmation

Management:

Surgery is the mainstay treatment modality for cancer of the oral cavity. Single modality treatment
with surgery or radiation therapy is preferred for early-stage oral cavity cancer.

Definitive radiation with concurrent chemotherapy is the current standard for unresectable locally
advanced disease. Radiotherapy can be given as palliative treatment to primary or metastatic area.
Chemotherapy may also be given as palliative care in a very advanced disease.

22.5.7 Oropharyngeal Cancer


Oropharynx is located between the soft palate superiorly and the hyoid bone inferiorly. The
oropharynx has four walls; soft palate, tonsillar region, base of tongue, and pharyngeal wall. It is
associated with tobacco use and alcohol consumption and HPV. Tonsillar and pharyngeal tongue
tumors frequently are initially recognized by nodal metastases.

Clinical Presentation
• Sore throat, non-healing oropharyngeal ulcers, dysphagia, referred otalgia, hoarseness
(with larynx invasion), odynophagia, hot potato voice and impaired tongue movement,
including protrusion.

Investigations:
• FBC, LFT, RFT and HIV
• CXR
• CT Scan and/or MRI of the Head and Neck
• Mirror and fibre-optic endoscopic examination
• Biopsy for histologic confirmation

Management:
Oropharyngeal cancers are mainly treated by Radiotherapy in combination with chemotherapy.
Surgery can be used in selected cases.

Table 22.11 Recommended Radiotherapy and Chemotherapy treatment for Head and Neck
tumours
Curative radiotherapy Radiotherapy dose for head and neck cancers is 66–70Gy given at
conventional fraction of 1.8–2Gy/fractions.
Concurrent Chemotherapy S: cisplatin (IV) 40mg/m2 1hour infusion weekly during Radiotherapy
OR
S: cisplatin (IV) 75mg/m2 1 hour infusion day 1 repeat every 21 days
during radiotherapy.
Induction Chemotherapy For patients with Advanced Head and Neck Cancers - PF or TPF (taxane,
platinum and 5 FU) for 3 – 6 cycles.
S: carboplatin (IV) AUC 5 1hour infusion day 1 AND 5-flourouracil (IV)
400mg/m2 bolus day 1 AND paclitaxel (IV) 175mg/m2 3 hour infusion day
1 repeat every 21 days for 3-6 cycles.
Adjuvant Chemotherapy: In curative intent concurrent chemoradiotherapy is indicated with
cisplatin/5FU (IV) If induction chemotherapy was not given then adjuvant
chemotherapy is recommended. Alone or in combination with cetuximab.
S: carboplatin (IV) AUC 5 1hour infusion day 1AND 5-flourouracil (IV)
400mg/m2 bolus day 1 AND Cetuximab (IV) 400mg/m2 2 hours infusion
day 1 (to be administered 1 hour before cisplatin/5-Fu) (IV) every 21 days
for 3-6 cycles.
Treatment of Recurrent or Combination therapy cisplatin or carboplatin/docetaxel or paclitaxel.
Metastatic disease paclitaxel/ cisplatin/ 5-FU cisplatin/ gemcitabine, gemcitabine/ vinorelbine,
carboplatin, cetuximab (IV).
Single agents cisplatin, carboplatin, paclitaxel, docetaxel, 5-FU,
methotrexate, gemcitabine and capecitabine (IV)

`513

Note
• Head and neck tumour patients must be referred to cancer specialized centers for
evaluation and definitive management. Follow up visits: 1st visit at 4–6weeks then after
each 3–4 months in the 1st year, 6 monthly in the 2nd year thereafter yearly.

22.5.8 Thyroid Carcinoma


Thyroid cancer is a commonest endocrine malignancy in Tanzania. It accounts approximately 0.8-
1% of all malignancies seen at Ocean Road cancer institute annually. Histological types are
medullary, anaplastic and well differentiated thyroid cancer.

Majority of these cases are differentiated thyroid cancer, the commonest being follicular subtype
followed by papillary subtype and rare ones being Hurthle cell, follicular variant of papillary thyroid
carcinoma, tall cell, columnar, solid and clear cell. Female are mostly affected, the male to female
ratio being 3:1

Diagnostic Criteria
• Thyroid mass (Anterior neck mass), Obstructive symptoms (Stridor, hoarseness), laryngeal
nerve palsy, dysphagia
• Metastatic symptoms such as weight loss, difficulty in breathing, bone pain/pathological
fractures

Investigations:
• Thyroid function tests (T3, T4, TSH), FBC, LFTs, Urea & Creatinine, Serum calcitonin,
Serum thyroglobulin levels
• Thyroid Scan
• CXR
• Isotope bone scan
• CT Scan of the neck
• Biopsy or Fine needle aspiration cytology (FNAC) of a thyroid lesion

Staging: TNM Staging system


Treatment:
Surgery is the mainstay of treatment; lobectomy, total or near total thyroidectomy. Radiotherapy is
indicated in all cases of anaplastic carcinoma.

Pharmacological Treatment
• Radioactive iodine I-131 sodiumor potassium iodide ablation is indicated in all patients with
well differentiated thyroid cancer after surgery.
• Post ablation; Thyroid-stimulating hormone (TSH) suppression therapy (levothyroxine) is
indicated in all patients post ablation and post-lobectomy. Aim is to keep TSH <0.1mU/L.
• Tumor recurrence or metastasis: Local reccurence should be managed surgically. Local
reccurence or distant metastases not suitable for surgery that are iodine avid are treated
with I-131.
• Palliative chemotherapy is indicated for patients with visceral metastatic diseases not
responding to I-131. Recommended regimen is:

S: pacliataxel (IV) 175mg/m2 3 hours infusion day 1 AND doxorubicin (IV)


60mg/m2 bolus day1 every 3 weeks up to 6 cycles.

• Radiotherapy is indicated for Adjuvant treastment to the thyroid bed post surgery with
macro/microspopic residual disease, in unresectable and local reccurence that does not
take up I-131 and palliation of bone and brain metastasis. Palliative dose: 30Gy in 10
Fractions.
• For anaplastic carcinoma radiation is indicated and dose recommended 50-60Gy in 20-30
Fractions.
• Medullary Thyroid Tumor (MTC) is primarily managed by surgery, Radiotherapy
• Anaplastic Thyroid Cancer (ATC) is aggressive disease. A Total thyroidectomy followed by
adjuvant radiotherapy is indicated to resectable disease. If unresectable ATC palliative
radiotherapy and combination chemotherapy is indicated. The recommended
chemotherapy regimen is as above in metastatic disease.

Note: All patients must be referred to a cancer specialized center for proper management.

`514

22.6 Gastrointestinal Malignancies


22.6.1 Esophageal Cancer
Histologically there are two types; SCC and adenocarcinoma. Tobacco and alcohol abuse are major
risk factors for SCC whereas obesity, gastroesophageal reflux disease (GERD) and Barrett’s
esophagus are the major risk factors for adenocarcinoma.

Diagnostic Criteria
• Difficult in swallowing (dysphagia) is the commonest symptom which is associated with
weight loss and poor performance status.

Investigation
• FBC, LFT, Urea, Creatinine
• Barium swallow and meal
• Chest and Abdominal CT scan
• Abdominal USS
• Rigid oesophagoscopy or oesophagoduodenoscopy (OGD) and biopsy for histology

Staging: TNM Staging system


Management: Surgery and radiotherapy
Surgery is a major component of treatment for resectable disease. Surgery and or radiotherapy may
be curative in early diseases. However, most patients present in late stages, hence the goal of
treatment is to prolong survival and relieve symptoms. Radiation (alone or in combination with
chemotherapy) is given as a definitive, preoperative, postoperative therapy or palliative setting.

Chemotherapy

Table 22.12 Recommended chemotherapy regimens for neo-adjuvant, adjuvant or palliative


for Esophageal cancer
2
Neoadjuvant Chemotherapy S: paclitaxel (IV) 175 mg/m 3hours’ infusion day 1 AND cisplatin (IV)
2
75 mg/m 1-hour infusion day 1 OR carboplatin (IV) AUC 5 1-hour
infusion day 1 given every 21 days for 6 cycles
OR
2
S: docetaxel (IV) 75mg/m 3hours’ infusion day 1 AND cisplatin (IV)
2
75mg/m 1-hour infusion day 1 every 3 21 days for 6 cycles
2
Adjuvant Chemotherapy S: 5–FU (IV) 1000 mg/m (IV) bolus day 1–day 5 AND cisplatin (IV)
2
75 mg/m 1 hour infusion day1 given every 21 days for 6 cycles
2
Palliative Chemotherapy S: capecitabine (PO) 1000mg/m 12 hourly on day 1–14, cycled every
21 days for 6 cycles or until disease progression or intolerable toxicity

Note
• All patients should be referred to cancer specialized centers for proper management
Stenting, gastrostomy tube and parenteral nutrition are employed to provide feeding
when there is total dysphagia.

22.6.2 Gastric Cancer


Gastric cancer is often diagnosed at an advanced stage. Among the risk factors include age,
gender, genetic factors, smoking, smoke or salt preserved food, diet less of fruits and vegetables,
infection with H. Pylori and Epstein Barr Virus. About 90–95% of the tumors are adenocarcinoma.

Diagnostic Criteria:
• Epigastric pain worsened by food intake, early satiety
• Distal tumours may present with obstructive symptoms
• Occult of manifest bleeding may be a feature
• Other symptoms include epigastric mass, pallor, weight loss, supraclavicular nodes,
hepatomegaly, periumbilical nodes

`515

Investigations:
• FBC, LFT, RFT
• Stool for occult blood
• Carcinoembryonic antigen (CEA)_
• IHC – Her 2 Status
• CXR
• Barium meal (double contrast)
• Abdomen and pelvis CT scan or USS
• Endoscopy and biopsy for histology

Staging: TNM staging system


Management:
Surgery is the primary treatment for early stage gastric cancer. Total or partial gastrectomy is
performed together with lymph node dissection. By pass surgery is done to relieve obstructive
symptoms. Surgery is usually preceeded by Chemotherapy (Perioperative) or adjuvant
chemoradiotherapy.

Pharmacological Treatment
Table 22.13 Recommended chemotherapy regimens for Gastric cancer
Perioperative S: 5-fluorouracil (IV) 500mg/m2 bolus day 1 AND epirubicin (IV) 50mg/m2 30
chemotherapy minutes’ infusion day 1 AND cisplatin (IV) 60mg/m2 1-hour infusion day 1, cycled
every 21 days for 6 cycles.
OR
S: capecitabine (PO) 625mg/m2 12 hourly daily for 21 days AND epirubicin (IV)
50mg/m2 30 minutes’ infusion day 1 AND cisplatin (IV) 60mg/m2 1-hour infusion day
1, cycled every 21 days for 6
cycles.
OR
S: 5-fluorouracil (IV) 200mg/m2/day Continous infusion day 1-4 AND epirubicin (IV)
50mg/m2 30 minutes’ infusion day 1 AND cisplatin (IV) 60mg/m2 1-hour infusion day
1, cycled every 21 days for 6 cycles.
23
locally advanced S: paclitaxel (IV) 175mg/m hours’ infusion AND carboplatin (IV) AUC 5 1-hour
and metastatic infusion on day 1, cycled every 21 days for 6 cycles AND/OR trastuzumab (IV)
gastric 6mg/m2 2hours loading dose day1, and then 4mg/m2 every 14 days (For Her 2 +
adenocarcinoma. Patients).
OR
2 21
S: docetaxel (IV) 60mg/m 2 hours’ infusion day 1 AND cisplatin (IV) 60mg/m 1
2
hourday1 + 5–FU (IV) 750mg/m continuous infusion over 24 hours on day1–4,
cycled every 21 days for 6 cycles AND/OR trastuzumab (IV) 6mg/m2 2hours’
infusion loading dose day1, and then 4mg/m2 every 14 days (For Her 2 + Patients).
2
Palliative setting S: capecitabine (PO) 1000mg/m 12 hourly on day 1–14, cycled every 3 weeks, 6
cycles or until disease progression or intolerable toxicity.

Note
• Concurrent Chemo radiotherapy with 3DCRT may be used as adjuvant post surgery.
• Radiotherapy can also be used in palliative setting to control bleeding and pain.
• Gastric (MALT) lymphoma are associated with Chronic H. pylori inflammation. They are
managed by H. pylori eradication and Chemoradiotherapy (see details in Lymphoma
section).
• Patients with CD 117 positive gastro intestinal stromal tumor (GIST) respond well to
imatinib.

22.6.3 Hepatocellular Carcinoma


Associated with chronic Hepatitis B/C infection

Diagnostic criteria
• An arterial bruit and ascites may be present
• Right upper abdominal swelling and pain often associated with weight loss, fever, jaundice

`516

Investigation
• FBC, LFT, RFT, Biochemistry, Serum alpha feto protein, HBsAg, HBcore antibody, partial
thromboplastin time (PTT)
• CXR
• Abdomen and Pelvis USS
• 3 Phase Liver Protocol CT/MRI Scan with IV Contrast
• PET/CT
• Biopsy or FNAC of the liver

Staging: TNM staging system

Table 22.14 Child Pugh Score


Parameter Points for increasing abnormality
I II III
Encephalopathy None 1-2 3-4
(grade)
Ascites None Slight Moderate
Albumin >3.5 2.8-3.5 <2.8
Prothrombin time (s) 1-4 4-6 >6
Bilirubin (mg/dl) For 1-2 2-3 >3
primary biliary 1-4 4-10 >10
cirrhosis

Management
Table 22.15 Treatment Recommendations
Presentation Recommended treatment
Resectable Partial hepatectomy
Unresectable, Liver transplant
medically
operable
Unresectable, Conformal Radiotherapy +/- Chemotherapy
medically Systemic therapy alone
inoperable Supportive care
Palliative Radiotherapy for Bone and Brain metastases

Flow Chart 22.1 Management of Hepatocellular cancer by Stage and Child Pugh Score

Pharmacological Treatment
Recommended systemic regimen used for palliation

S: doxorubicin (IV) 60 mg/m2 over 30 minutes day1 given every 3 weeks for 4–6 cycles.
S: sorafenib (PO) 400mg daily until disease progression or unacceptable
toxicity.

`517

Prevention: Vaccination for Hepatitis B/C

22.6.4 Rectal Cancer


Risk factors include: inherited genetic syndromes, diet high in red and processed meat, smoking and
alcohol abuse, having inflammatory bowel disease, type ll diabetes and obesity. Histology;
commonest is adenocarcinoma 95%.

Diagnostic Criteria:
• Change in bowel habit eg constipation or diarrhea, sense of incomplete bowel emptying.
• Rectal bleeding or blood in stool.
• Abdominal mass with or without obstructive symptoms
• Unexplained weight loss and other symptoms of advanced disease.

Investigations:
• FBC, RFT, LFT, CEA
• Stool for occult blood
• CXR
• Barium enema (double contrast)
• Abdomen and Pelvis USS
• Digital rectal examination
• Sigmoidoscopy or Colonoscopy with Biopsy of the lession
• Abdomen and Pelvis CT Scan

Staging: TNM staging system


Management
Surgery is the primary treatment for early disease. Hemicolectomy with lymphnode dissection is
commonly performed in colon cancer. Give preoperative chemotherapy for locally advanced disease
to shrink the tumor. Radiotherapy plays a role in rectal tumor as neo–adjuvant, adjuvant or palliative.

Pharmacological management:
Management of locally advanced and metastatic colorectal cancer involves various active
chemotherapy drugs, either in combination or as single agents: 5–FU, leucovorin, capecitabine,
oxaliplatine, irinotectecan and bevacizumab are available for various combination regimens and
schedules.

Table 22.16 Recommended Chemotherapy regimens for Rectal cancer


2
Neo-adjuvant chemo radiotherapy S: 5–FU (IV) 350 mg/m over 30 minutes AND leucovorin (IV) 20
2 st th
mg/m infusion over 30 minutes’ day 1–day 5 given on 1 and 5
weeks of RT, concurrent with RT: 45 Gy/25#/5weeks followed by
surgery in 4–10 weeks.

3–10 weeks after surgery continue with chemo as below:


2
S: 5–FU (IV) 50 mg/m over 30 min day 1–day 5 PLUS leucovorin
2
(IV) 20 mg/m 30 minutes infusion day1–day5 every 21 days for 4
cycles

Adjuvant chemo Radiotherapy 3–10 weeks after surgery


2
S: 5–FU (IV) 500 mg/m over 30 minutes’ day 1–5 & day 29–33,
concurrent with RT:45 Gy/25#/5 weeks.
Four weeks after completion of chemo radiation; continue with
2
chemo: 5–FU (IV) 450 mg/m bolus day 1–day 5, Every 4 weeks for
2 cycles
OR
S: capecitabine (PO) 825mg/m2 12 hourly during Radiotherapy.

Management of Metastatic disease


As colon

`518

22.6.5 Colon Cancer


Investigations
• FBC, RFT, LFT, CEA
• Stool for occult blood
• CXR
• Barium enema (double contrast)
• Abdomen and Pelvis USS.
• Digital rectal examination
• Sigmoidoscopy or Colonoscopy with Biopsy of the lession
• Abdomen and Pelvis CT Scan

Staging: TNM staging system


Management
• Management of Non-metastatic disease: Surgery then Adjuvant Post Op
Chemotherapy.
• Management of Metastatic disease: Single or Combination Chemotherapy.

Table 22.17 Recommended Chemotherapy regimens for Colon cancer


Adjuvant Chemotherapy S: oxaliplatin (IV) 85mg/m2 2 hours’ infusion day 1 AND leucovorin(IV)
400mg/m2 over 20 minutes day1 AND 5-fluorouracil (IV) 400mg/m2
bolus day1, then 1200mg/m2/day X 2 days (IV) Continous infusion (USE
INFUSION PUMP) repeat after every 14 days for 6-12 cycles.
OR
S: oxaliplatin (IV) 130mg/m2 2hours’ infusion AND capecitabine (PO)
1000mg/m2 12 hourly for 14 days, 21 days’ cycles for 4-8 cycles.
OR
S: capecitabine (PO) 1000mg/m2 12 hourly daily for 14 days, 21 days
cycle for 6 cycles.

Metastatic disease S: oxaliplatin (IV) 85mg/m2 2 hours infusion day 1 AND leucovorin (IV)
400mg/m2 infusion over 20 minutes day1 AND 5- fluorouracil (IV)
400mg/m2 bolus day1, then 1200mg/m2/day X 2 days (IV) Continous
infusion (USE INFUSION PUMP) repeat after every 14 days for 6-12
cycles. With/without bevacizumab (IV) 5mg/kd 1 hour infusion day 1 or
cetuximab (IV) 500mg/m2 infusion over 2 hours day 1
OR
S: oxaliplatin (IV) 130mg/m2 2hours’ infusion AND capecitabine (PO)
1000mg/m2 12 hourly daily for 14 days, 21 days’ cycles for 4-8 cycles.
With/without bevacizumab (IV) 5mg/kg 1-hourinfusion day 1
OR
S: capecitabine (PO) 1000mg/m2 12 hourly daily for 14 days, 21 days
cycle for 6 cycles.

Note
• Colorectal cancers are usually asymptomatic until advanced stage hence regular
• Screening with annual digital rectal examination, stool for occult blood + colonoscopy
and is recommended starting at 50 years of age.

22.6.6 Anal Cancer


Investigations
• FBC, RFT, LFT, HIV/CD4
• CXR
• Abdomen and Pelvis USS.
• Digital rectal examination
• Sigmoidoscopy or Colonoscopy with Biopsy of the lession
• Abdomen and Pelvis CT scan

Staging: TNM Staging system

`519

Management
• For resectable Good Performance status: Surgery (APR) then Adjuvant
Chemoradiotherapy (45Gy-50Gy)
• For Unresectable Good Performance status: Neoadjuvant Chemoradiotherapy (45Gy-
50Gy) then Surgery (APR)
• For Inoperable and Poor Performance statu: Palliative Radiotherapy

Pharmacological Management
Concurrent Chemoradiotherapy:

S: mitomycin C (IV) 10mg/m2 bolus day 1 and 29 AND 5-flourouracil (IV) 1000mg/m2
Continous infusion day 1-4 and 29-32. (USE INFUSION PUMP).
OR
S: capecitabine (PO) 825mg/m2 12 hourly a day during radiotherapy (5 days a week)
AND 5- fluorouracil (IV) 1000mg/m2 Continous infusion day 1-4 and 29-32. (USE
INFUSION PUMP).

Metastatic disease
As Rectum
22.7 Lung Cancer
Worldwide lung cancer is the leading cause of cancer-related death. Approximately 85 %–90% of
lung cancer cases are caused by cigarette smoking. There are 2 main types of lung cancer; Non-
small cell lung cancer (NSCLC) and small cell lung cancer (SCLC). These 2 types have different
prognosis and management approach.

22.7.1 Non-small cell lung Cancer


Accounts for approximately 85% of all lung cancer cases

Diagnostic Criteria
• Chronic chest symptoms in a smoker
• Haemoptysis
• May present with superior vena cava obstruction (SVCO) syndrome
• Cough in patient exposed to asbestos
• Findings of chest symptoms, weight loss, poor karnofsky performance scale (KPS)

Investigations:
• FBC, LFT, Urea, Creatinine
• CXR PA & lateral views
• CT Scan of Thorax and Abdomen
• Abdominal USS
• Bronchoscopy and Biopsy for histopathology
• Cytology of sputum or bronchial aspirate examination

Staging: TNM staging system


Management: Surgery (pneumonectomy or lobectomy) is curative for stage I and some stage II
disease.

Pharmacological Treatment:
Recommended Chemotherapy regimens for adjuvant, unresectable or recurrent and metastatic
disease are;

S: carboplatin (IV) AUC 1-hour infusion 6 day1 AND paclitaxel (IV) 175 mg/m2 3 hours’
infusion day 1 every 21 days for 6 cycles

Radiotherapy
With advanced radiotherapy machine and treatment technic, RT may be given for neo–adjuvant or
adjuvant to surgery. Palliative Radiotherapy is frequently used in metastatic disease to bone, spinal
cord compression, brain, liver and in case of superior vena cava obstruction (SVCO), atelectasis,
obstructive pneumonitis and fungating masses. Dose of 30GY/10 Fractions/2weeks gives good
symptom relief.

`520

22.7.2 Small cell lung cancer


SCLC is characterized by early development of widespread of metastases. It is highly sensitive to
initial chemotherapy and radiotherapy; however, most patients eventually die of recurrent disease.

Diagnostic criteria and investigations: As in non – small cell lung cancer (NSCLC) however brain
scan and bone marrow aspirate are necessary

Staging: Limited disease versus extensive disease

Pharmacological Treatment
Aim is for local control and palliation. Cure rate is low

Platinum + Etoposide are the major drugs for which the tumor is sensitive.

S: cisplatin (IV) 60 mg/m2 1-hour infusion Day 1 AND etoposide (IV) 100 mg/m2 over 30
minutes Day1–3, Every 21 days for 4 –6 cycles
OR
S: carboplatin (IV) AUC 5 1-hour infusion Day 1 AND etoposide 100 mg/m2 30 minutes (IV)
infusion Day1–3, every 21 days for 4–6 cycles

Other recommended chemotherapeutic drugs are irinotecan and gemcitabine

Radiotherapy:
Consolidation to primary site and mediastinum: 50Gy/25Fractions/5weeeks
• Prophylactic brain irradiation in complete responders
• Palliative treatment for symptoms relief in respiratory, bone or CNS symptoms:
30Gy/10Fractions/2wks

22.8 Genitourinary Malignancies


22.8.1 Carcinoma of the Prostate
The most common type of prostate cancer is adenocarcinoma (95 %). Tumours are stratified by T
stage, Gleason score (GS), and PSA into three prognostic groups of low, intermediate and high risk.
• Low risk: T1–T2a and PSA < 10 ng/ml and GS ≤ 6
• Intermediate risk: T2b or PSA 10 – 20 ng/ml or GS 7
• High risk: T2c–T4 or PSA > 20ng/ml or GS 8–10

Patient can be offered appropriate treatment options according to stage of disease, prognostic risk
group and estimated survival taking into account performance status and comorbidity.

Diagnostic Criteria
• May be asymptomatic in early stages of the disease
• May present incidentally following examination for benign prostatic hypertrophy or elevated
serum prostatic specific antigen (PSA)
• Prostatic symptoms are associated with advanced stages of the disease, which include:
reduced potency, urinary frequency and nocturnal, poor stream, hesitancy and terminal
dribbling
• Very often patients may present with bone pain including backache or pathological fracture
• Digital Rectal Examination (DRE) typically reveals a hard, irregular prostate. TURP is
carried out to both confirm the diagnosis and also as part of the treatment (to relieve
obstruction).

Screening for prostate cancer


Routine screening not recommended, but when done should begin with PSA and digital rectal
examination at age 50 if life expectancy is >10 years. It is recommended that screening of high risk
group should take place starting at age 45 .

Investigations
• FBC, LFT, Urea, Creatinine, Serum PSA, ALP, Testosterone
• X-rays of the painful bone or spine
• CXR

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• Abdomen and Pelvis USS and or CT Scan


• Pelvic MRI in early-stage disease
• PET/CT
• Bone scan
• Biopsy for histopathology

Staging: TNM staging system

Treatment:
Treatment depends on disease profile (Risk stratification) and patient factors as noted above.
Options include:
• Watchful waiting
• Active surveillance
• Surgery (curative or palliative)
• Radiotherapy (curative or palliative)
• Hormonal therapy (chemical vs surgical castration)
• Chemotherapy

Surgery
Early stages (Low and Interediate risk groups) can be treated with either radical prostatectomy or
radical Radiotherapy with cure intent. However, surgery may cause postoperative impotence and
impaired urinary control. TURP is carried out to both confirm the diagnosis and also as part of
relieving obstruction.

Radiotherapy
Radical Radiotherapy for Adjuvant and definitive, EBRT up to 74 Gy/37 Fractions can be given using
3DCRT or IMRT Techniques. Palliative radiotherapy is valuable to bone metastases, massive
hematuria, spinal cord compression and brain mets,

Hormonal Therapy
Hormonal manipulation is by surgical or medical castration. It is carried out in patients with locally
advanced or metastatic disease. Bilateral orchydectomy is a surgical hormonal manipulation and
should not be regarded curative surgery.

Pharmacological Treatment:
S: goserelin (SC) 3.6 mg every 4 weeks or 10.8mg every 12 weeks with/ without oral
bicalutamide (PO) 50mg once daily

Note
• Goserelin is not required after orchydectomy but patient may receive Bicalutamide.
• Treatment with goserelin and bicalutamide may be given up to 2 years depending on
patient condition and Prostate Specific Antigen (PSA) levels

Chemotherapy
Recommended chemotherapy regimens for hormonal refractory prostate cancer are:

S: doctetaxel (IV) 75mg/m2 2 hours’ infusion day 1 given every 21 days for 6 cycles. It is
mainly reserved in hormonal refractory prostate cancer.

For Bone metastases/osteolytic/tumour induced hypercalcemia are:

S: zolendronic acid (IV) 4mg over 15min given 4 Weekly

Metastatic disease
Life long ADT ± palliative RT ± bisphosphonates for hormone refractory disease. docetaxel and
prednisone for androgen independent disease can add Carboplatin if docetaxel not working to
Castrate resistant prostate cancer patients.

Evaluation every 3 months (Check PSA level) Castrate resistant patients with rising PSA zoledronic
acid should be given monthly. These are given together with Ca2+ and Vitamin D supplements.

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In Castrate resistant patients which did not respond to Docetaxel plus carboplatin and
prednisolone, patients Abberaterone acetate with prednisolone is an option (500mg OD taken with
food is highly recommended)

S: abberaterone acetate (PO) 500mg one a day (Taken with food)


OR
S: enzalutamide (PO) 160mg daily

22.8.2 Urinary Bladder Cancer


Urinary bladder cancers are malignant tumors that commonly arise from the inner lining of the
bladder or its connective tissue. Common pathologies include transition cell carcinoma, squamous
cell carcinoma, adenocarcinoma, sarcomas and secondary deposits.

Risk factors for bladder cancer include chronic irritation (schistosomiasis, irradiation, and
catheterization), chemicals (aromatic amines, aniline dyes, tobacco, analgesics) and genetic
predisposition. Symptoms include blood in the urine, dysuria, Lower urinary tract symptoms (LUTS),
and low back pain.

Diagnostic Criteria
• Symptoms include blood in the urine, pain with urination, and low back pain.

Investigations
• FBC, RFT, LFT, Alkaline phosphatase
• Urinalysis, Urine culture and sensitivity, Urine for cytology
• CXR and /or CT chest
• Bone scan
• Abdomimen and Pelvis USS or CT scan
• PET/CT
• Cystoscopy with bladder mapping & Biopsy
• EUA
• Bimanual examination
• TURBT with random biopsies of normal appearing mucosa to exclude CIS. (If trigone
involved, biopsy prostatic urethra)

Staging: TNM staging system


Management
Treatment of Urinary bladder cancer depends on how deeply the tumor invades into the bladder
wall.

Surgery: Several modalities that may extend from bladder preserving surgery–TURB; to radical
cystectomy with urine diversion depending bladder muscle invasion. Post operation patient may
receive adjuvant chemo and/or radiotherapy

Chemotherapy: chemotherapy in bladder cancer may be offered before surgery or after surgery. It
may also be given concurrent with radiotherapy or as palliative in inoperative tumor.

Recommended chemotherapy regimens for locally advanced and meatasatic disease are;

S: gemcitabine (IV) 1000mg/m2 infusion over 30minutes day 1, 8 & 15 AND cisplatin (IV)
70mg/m2 infusionAND over 30mins day 2 given every 28 days for 6 cycles
OR
MVAC regimen
S: methotrexate (IV) 30mg/m2 over 5 minutes day1, 15 & 22
AND
S: vinblastine (IV) 3mg/m2 over 10 minutes day2, 15 & 22
AND
S: doxorubicin (IV) 30mg/m2 over 15 minutes day2
AND
S: cisplatin (IV) 70mg/m2 over 30mins day2

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Radiotherapy
Radiotherapy may be given after bladder preserving surgery or alone in small lesions with a dose up
to 66Gy/33Fractions concurrent with cisplatin. It is also commonly used as palliative therapy to
control bleeding and or pain locally advanced and metastatic disease. Palliative dose
30Gy/10Fractions or 20Gy/5Fractions

22.9 Haematological Malignancies


22.9.1 Lymphomas
World Health Organization broadly classifies lymphomas into Hodgkin lymphoma (HL) and non-
Hodgkin lymphoma (NHL).

22.9.1.1 Non-Hodgkin’s lymphoma


NHLs are a heterogeneous group of diseases which are mainly linked by their origin within the
lymphoid system and its different cellular components. They are sub classified based on the stage of
maturation (immature vs. mature) and cell of origin [B cell, T cell, or natural killer cell (NK) cell].

Diagnostic Criteria
• Peripheral Lymph node enlargement (commonest site-neck)
• Hepatomegally and/or splenomegally in advanced stages
• B-symptoms: Unexplained weight loss, fever, drenching night sweats
• Coughing, trouble breathing, or chest pain in case of Superior vena cava obstruction
(SVCO)

Investigations:
• CXR
• Chest and abdominopelvic CT Scan
• PET/CT
• FBC, differential and film
• Bone marrow aspirate and trephine
• Immunohistochemistry (IHC)
• LDH, Urea and Electrolyte, Creatinine, Albumin, Aspartate transaminase (AST), Bilirubin,
Alkaline phosphatase, Serum calcium, Uric acid
• Pregnancy test in females of child–bearing age
• Hepatitis B and C
• HIV status
• Tissue Biopsy for histopathology
• MUGA scan/ ECHO

Note: Lumbar puncture and CSF cytology if there is CNS involvement of in NHL associated with a
high risk of CNS relapse eg. Testicular, paranasal sinuses, extradural/paraspinal mass.

Staging: Ann Arbor classification.

Management:
NHL diseases are sensitive to both chemotherapy and radiotherapy

Indolent lymphoma
They include Indolent B-cell lymphomas such as Follicular lymphoma, MALT lymphoma, nodal
marginal zone lymphoma, splenic marginal zone lymphoma and small lymphocytic lymphoma,
and Indolent T-cell lymphomas such as mycosis fungoides.

Treatment
Stage 1 and 2 can be treated with involved node radiotherapy or R_CHOP / R-CVP followed by
radiotherapy.

R-CHOP regimen:
S: rituximab (IV) 375 mg/m2 3 hours’ infusion day 1 AND cyclophosphamide day1 750
mg/m2 1-hour infusion AND doxorubicin (IV) 50 mg/m2 15 minutes’infusion day 1 AND
vincristine (IV) 1.4 mg/m2 over 10 minutes (maximum 2mg) day1 AND prednisolone
(PO) 100mg once a day, day 1–5, every 21 days for 6–8 cycles.

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Aggressive lymphoma with CD 20 positive


These include Diffuse Large B-cell lymphoma (DLBCL), primary CNS lymphoma, adult Burkitt
lymphoma, mantle cell lymphoma and aggressive T-cell lymphomas.

Treatment: R–CHOP
S: rituximab (IV) 375 mg/m2 3 hours’ infusion day1 AND cyclophosphamide (IV) day1
750 mg/m2 1-hour infusion AND doxorubicin (IV) 50 mg/m2 15 minutes’ infusion day 1
AND vincristine (IV) 1.4 mg/m2 over 10 minutes (maximum 2mg) day1 AND
prednisolone (PO) 100mg once a day, day 1–5, every 21 days for 6–8 cycles.

Radiotherapy
• Radiotherapy is directed to genuinely stage IA and IIA Disease
• Mantle or inverted Y: 40Gy/20 Fractions/4weeks with shielding of the critical organs.
• Involved field RT (IFRT): 46Gy/23 Fractions/4.5weeks

Primary CNS Lymphoma


Standard chemotherapy regimens like CHOP are not effective possibly due to poor penetration of
the blood-brain-barrier (BBB).

S: methotrexate (IV) 8mg/m2/day twice a week until remission is achieved

Burkitt Lymphoma (BL)


Recommended chemotherapy regimens are:
S: CODOX-M AND IVAC (Magrath regimen- cyclophosphamide, vincristine, doxorubicin,
methotrexate/ifosfamide, etoposide, cytarabine) (IV)
OR
S: CALGB 9251 (cyclophosphamide, prednisolone, ifosfamide, mesna, methotrexate,
leucovorin, vincristine, cytarabine, etoposide, dexamethasone and doxorubicin) (IV)
OR
S: Hyper CVAD (cyclophosphamide, vincristine, doxorubicin and dexamethasone,
methotrexate, cytarabine, leucovorin, methylprednisolone and 6-mercaptopurine) (IV)
OR
S: Dose-adjusted CHOP+Etoposide (IV)

Aggressive T-cell lymphomas


Rare and more aggressive than DLBCL. First line therapy is usually
S: CHOP with Etoposide (CHEOP) (IV)
OR
S: cyclophosphamide (IV) day1 750 mg/m2 1-hour infusion AND doxorubicin (IV) 50
mg/m 15 minutes’ infusion day 1 AND vincristine (IV) 1.4 mg/m2 over 10 minutes
2

(maximum 2mg) day1 AND prednisolone (PO) 100mg once a day, day 1–5 AND etoposide
100mg/m2 (IV) day 1-day 3; repeat every 21 days for 6–8 cycles.

Note
• For MALT lymphoma, eradication of Helicobacter pylori is essential.Splenectomy is
recommended in splenic marginal zone lymphoma.
• Topical corticosteroids are indicated for localized or generalized skin involvement in
mycosis fungoides. Systemic therapy indicated for non responders and Sezary
syndrome.

These include S: retinoids, interferons and low dose methotrexate.

S: fludarabine AND Cyclophosphamide (FC) regimen is used as a second-line therapy for


indolent B-cell lymphoma.

Hodgkin’s disease (HD)


Hodgkin Lymphoma comprises about 30% of all lymphomas. The disease is characterized by
scattered large multinucleated Reed-Sternberg or mononuclear Hodgkin’s cells in an inflammatory
background of a lymph node biopsy section.

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Classified into two main types:


• Nodular lymphocyte predominant Hodgkin lymphoma–NLPHL
• Classical Hodgkin lymphoma–CHL, which is sub–divided into:
o Nodular sclerosis classical Hodgkin lymphoma–NSHL
o Mixed cellularity classical Hodgkin lymphoma–MCHL
o Lymphocyte–rich classical Hodgkin lymphoma–LRCHL
o Lymphocyte–depleted classical Hodgkin lymphoma–LDHL

Diagnostic Criteria
• Enlarged painless lymph nodes in the neck or elsewhere
• B symptoms (weight loss, night sweats, and fever), pruritus, alcohol induced pain, general
condition, throat, lymph nodes (site, number, size, consistency, mobility, matting),
respiratory system, abdomen (liver, spleen, other masses), bone tenderness

Investigations:
• CXR
• CT Scan of neck, chest, abdomen and pelvis
• PET/CT
• FBC, LFT, RFT, ESR, LDH, HIV Test
• Bone marrow aspirate and biopsy (Not required in Stage I or II A)
• Biopsy for histological diagnosis
• MUGA scan / ECHO

Management:
As it is for NHL, HL diseases are sensitive to both chemotherapy and radiotherapy.

Pharmacological Treatment
Chemotherapy aims at cure for any stage of the disease. It is indicated in Stages II–IV.

Recommended chemotherapy regimen is ABVD which include combination of the following drugs:

S: doxorubicin (IV) 25 mg/m2 over 30 minutes AND bleomycin (IV) 10 IU/m2 over 10
minutes AND vinblastine (IV) 6 mg/m2 over 10 minutes AND dacarbazine (IV) 375 mg/m2
infusion over 30 minutes all given on day 1 & 15, every 28 days for 4–8 cycles.

Other recommended chemotherapy regimens that can be used as salvage regimens are DHAP,
DHAC, IGEC, ICE and MINE-ESHAP.

Radiotherapy: can either be; involved field RT or mantle or inverted Y depending on site of disease:
1.8–2Gy/Fraction for 30–40Gy total dose.

22.9.2 Leukemia
The symptoms and signs are caused by: (i) bone marrow failure (e.g. anaemia, neutropenia,
thrombocytopenia); and (ii) infiltration of organs (e.g. liver, spleen, lymph nodes, meninges, brain,
skin or testes).

Investigations:
• FBC, LFT, RFT, Coagulation indices
• Peripheral blood film
• Bone marrow aspiration and trephine biopsy
• Flow cytometry analysis, immunophenotyping, cytogenetic and molecular evaluation.
• ECHO/ECG for Cardiac function evaluation.

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22.9.2.1 Acute Myeoid Leukemia (AML)


Classification: WHO classification
Table 22.18 Treatment recommendations for AML
Induction phase 7+3 (cytarabine + daunorubicin) regimen;
2
S: cytarabine (IV) 100mg/m 24 hourly for 7days AND daunorubicin (IV)
2
60mg/m 24hourly for 3 days

Consolidation phase If in remission ie blast cells < 2% in bone marrow,

S: high dose cytarabine (HiDAC) (IV) regimen is used.

Transplant S: Allogeneic hSCT is considered in some patients (high risk patients)

Relapsed AML (FLAG-IDA) regimen is used in relapsed cases. This is followed by allogeneic
hSCT if remission is achieved.
2 2
S: fludarabine (IV) 30mg/m for 4 days, ANDhigh dose cytarabine (IV) 2g/m
2
for 4 days AND Filgastrim (SC) 300mcg/m for 5days, AND idarubicin (IV)
2
10mg/m for 3 days.

Palliative single-dose S: Low- dose cytarabine (SC) 20mg 12 hourly for 10 days. OR azacitidine
2
regimen (SC) 75mg/m /day for 7 days. Repeat after every 4-6 weeks.

Management of acute promyelocytic leukemia (APL)


It is a medical emergency. Treatment should be initiated as soon as diagnosis is suspected based
on cytologic criteria, before definitive genetic, cytogenetic or immunostaining confirmation is made.

All -trans - retinoic acid (ATRA) is added in all three phases of APL treatment. There is a high risk of
developing DIC and differentiation syndrome. Differentiation syndrome is treated with;

S: dexamethasone (IV) 10mg twice a day for 3 days or until symptoms resolve. Consider
cessation of ATRA if symptoms are severe.

Table 22.19 Treatment recommendations for APL


2
Induction phase S: ATRA (IV) 45mg/m /day AND Arsenic trioxide (ATO) (IV)
0.15mg/kg/day daily until bone marrow remission. OR ATRA (IV)
2 2
45mg/m /day AND daunorubicin (IV) 50mg/ m for 4days PLUS/MINUS
2
cytarabine (IV) 200mg/ m for 7days
cytarabine (IV) is added in patients with high risk of relapse.

Consolidation phase S: ATRA AND ATO, OR ATRA AND daunorubicin OR ATO AND
daunorubicin OR daunorubicin AND cytarabine
2
Maintanance phase ATRA alone OR ATRA (IV) 45mg/m /day orally for 15 days after every
2
3months PLUS 6-mecaptopurine (IV) 60mg/ m orally once a day PLUS
2
methotrexate (IV) 20mg/ m orally once weekly. All given for 2 years.

22.9.2.2 Acute Lymphoblastic Leukemia (ALL)


Treatment: The treatment of ALL is complex. The recommended regimens are;

S: HYPER-CVAD/MTX-ARA-C Regimen (cyclophosphamide/mesna/vincristine/


doxorubicin/dexamethasone/methotrexate/cytarabine/leucovorin) (IV)

22.9.2.3 Chronic Myeloid Leukemia (CML)


Investigations: similar to other leukemia, plus BCR-ABL1 analysis by PCR or FISH for Ph
chromosome analysis

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Treatment
For BCR-ABL1 positive, first line treatment is Tyrosine kinase inhibitors (TKI)

Chronic phase: Characterized by blast cells < 10%.

S: imatinib (PO) 400mg once a day every day.

Accelerated phase: blasts 10 – 19%.

S: imatinib (PO) 600-800mg/day in 2 divided doses until chronic phase is reachived.


Thereafter continue with 400mg once a day daily.

Blast crisis: Blast cells > 20%. If the patient was not on TKIs, treat as in accelerated phase.
If patient was on TKIs, treat as acute leukemia.
S: Second line TKIs include nilotinib, dasatinib, bosutinib and ponatinib (PO)

If BCR-ABL1 negative
S: hydroxyurea (PO) 40mg/kg daily. The dose ranges between 1mg and 3mg based on the
WBC count.

Note
• Adequate hydration should be maintained.Blood transfusion is indicated based on the
degree of anaemia

D: allopurinol (PO) 300mg 24hourly daily to prevent hyperuricemia.

22.9.2.4 Chronic Lymphoid Leukemia (CLL)


Staging: Rai and Binet staging systems.
Treatment
S: chlorambucil (PO) 0.1mg/kg 24hourly for 2weeks, then rest for 2 weeks, repeat until
remission is achieved.
OR
S: Combination of Fludarabine, Cyclophosphamide and Rituximab (FCR) regimen (IV)

B: prednisolone (PO) 1mg/kg 24 once a day for 2 weeks is added if there is evidence of
autoimmunity (autoimmune hemolytic anaemia or autoimmune thrombocytopenia)

22.9.3 Multiple myeloma


Clinical features – CRAB: Features of hypercalcemia, renal impairment, features of anaemia, bone
pain, reccurent infections due to impaired antibody production, and bleeding tendencies and
hyperviscosity syndrome in rare cases.

Investigations:
• FBC, RFT, LFT, Serum electrolytes
• Peripheral smear
• Bone marrow aspiration and trephine biopsy
• Serum protein electrophoresis, urine for Bence Jones protein
• Skeletal survey by X-ray, CT Scan or MRI
• Serum β2 microglobulin
Staging: Revised International Staging System (RISS) Adopted by the International Myeloma
Working Group

Treatment: Radiotherapy is used for pain control of lytic lesions that are refractory to systemic
therapy, treatment of spinal cord compression from plasmacytoma and primary treatment of solitary
plasmacytoma.Supportive treatment with blood transfusion, antibiotic, hydration and analgesia when
indicated.

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Bisphosphonate therapy
S: zoledronic acid (IV) 4mg once monthly for 2 years

Recommended chemotherapy regimens include the following drugs in various combinations:


Melphalan, Thalidomide, Lenalidomide, Bortezomib, Cyclophosphamide, Prednisolone and
Dexamethasone.

S: thalidomide (PO) 200mg 24hourly for 28days


OR
S: lenalidomide (PO) 25mg 24hourly for 21days,
AND
S: dexamethasone (PO) 40mg 24hourly on day 1, 8, 15, 22, repeats after every 4 weeks.
OR

S: bortezomib (IV) 1.3mg/m2 24hourly AND dexamethasone (PO) 40mg 24 hourly


WITH/WITHOUT cyclophosphamide (PO) 300mg/m2 all on day 1,8,15,22. Repeat every 4
weeks

22.10 Central Nervous System Maligancies


22.10.1 Meningiomas
Meningiomas are the second commonest tumors of the brain and constitute 20% of all intracranial
tumors. Commonest sites are cerebral convexity, parasagittal and sphenoid
ridge.

Clinical presentation
• Chronic headache
• Adult onset seizures
• Loss of vision
• Focal neurological deficits

Investigations
• FBP
• Serum electrolytes
• CT / Brain
• CT/MR angiography
• Histopathology studies

Pharmacological management
• Seizures: Give anticonvulsants.
• Brain edema: Give Dexamethasone
Non-pharmacological management
Surgical management
• Intracranial meningiomas are best managed with total excision following the principle of
maximum safe excision (Refer to Simpson grading for intracranial meningiomas)
• Subtotal resection is associated with inferior outcome and higher regrowth rates.

Radiotherapy
• Radiotherapy is indicated in unresectable tumors, postoperative incomplete resection for
WHO grade 1, and all grade 2/3 tumors.
• Meticulous attention to operative notes is required, as well as to postoperative CT/MRI.

Follow up
• Follow up CT Scan/ MRI every 6 months for 1 year, then annually.
• In older patients and small tumors managed conservatively, consider CT/MRI scan yearly.

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22.10.2 Pituitary Tumors


Pituitary tumors constitute 10% of intracranial tumors. Morbidity is often due to mass effect and
endocrine consequencs including hyper or hyposecretion of pituitary hormones.

Clinical presentation
• Chronic headache
• Loss of vision
• Focal neurological deficits

Investigations
• FBP, Serum electrolytes,
• Anterior pituitary hormones
• CT / MRI Brain
• CT/MR angiography
• Visual fields assessment
• Histopathology studies

Pharmacological management of functional tumors

Prolactinomas
These should be treated initially with dopamine receptor agonist:
Give:
D: bromocriptine (PO) 2.5mg 8 hourly
OR
S: cabergoline (PO) 0.25mg once/twice a week (Titrate with prolactin levels checked 2
weekly, aim is to maintain PRL < 30ng/ml)

Cushing’s disease
Surgical management is recommended. Consider medicines that inhibit adrenocortical function only
when surgery is not possible: S: metyrapone 250mg once a day (can be escalated based on
response)

Acromegaly
Somatostatin analogues may be used to treat acromegaly. Give S: octreotide SR
Efficacy is measured using clinical response defined as basal GH levels < 2.5 ng/ml, glucose-
suppressed levels <1.5 ng/ml and normalization of serum IGF-1 levels.

Surgical management of pituitary tumors


• This is the primary treatment for most pituitary tumors, except for prolactinomas which may
be managed medically.
• Trans-sphenoidal approach (endoscopic or microsurgical) is preferred as it is safer and
better tolerated.
• Frequently subtotal especially in large tumors or tumors invading into
cavernous sinuses. Hypopituitarism occurs post-operative in about 12% of patients.

Radiotherapy
Indicated post subtotal tumor resection, recurrent tumors, persistently elevated circulating hormone
levels, and inoperable patients.

Follow up MRI 3 months after surgery to assess residual tumor.

Radiotherapy is very effective for control of growth of pituitary tumors (>95%), but less effective for
decreasing circulating hormone levels in functional tumors.

Common complications
Diabetes Insipidus: is characterized by excessive urine output due to lack of ADH, usually
immediate post-operative. Consider
D: desmopressin (PO) 0.05mg 12 hourly daily (titrate based on response.

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SIADH is characterized by decreased urine output and hyponatremia due to excessive ADH
secretion, usually immediate post-operative. Manage hyponatremia and consider

B: furosemide (PO) 40mg

CSW: characterized by excessive urine sodium secretion and hyponatremia, usually immediate
post-operative. Manage hyponatremia with Hypertonic 3% saline. Consider
D: fludrocortisone (PO) 0.05-0.1mg 12hourly daily.
Follow up
• There is significant risk of pituitary hypofunction after surgery or irradiation and this risk
may occur up to 15 years later – the patients should be warned of the symptoms and be
tested regularly.
• Patients treated with standard radiotherapy are unlikely to show an early response and
would therefore be assessed at 12 monthly intervals in terms of hormone levels and
pituitary function.

22.10.3 Gliomas
Gliomas constitute the most common tumors of the brain affecting all age groups, with predilection
to the adult population.

22.10.3.1 Low grade Gliomas (LGGs)


Clinical presentation
• Seizures are common
• progressive neurologic symptoms depending on site of tumor

Imaging
• CT or MRI should be done in diagnosis of Gliomas.
• MR spectroscopy
• Diffusion tensor tractography (DTI)

Pharmacological management
Seizures:
Surgical management
Long term survival approaches 100% with complete removal. After partial
resection, survival rates range from 80-90% at 5 years to 70-80% at 10 years
and 50-60 % at 20 years.

Repeat the scans at 6, 12, 24 months to check for growth. If this is surgically resectable then repeat
surgery should be attempted.

Radiotherapy
• Dose for low grade gliomas: 1.8 Gy X 28 Fractions = 50.4 Gy (5 times per
week). Concurrent and adjuvant use of Temozolomide is indicated if available,

S: temozolomide (PO) 75mg/m2 daily during RT and 150-200mg/m2 day 1-5


Monthly for 6 months.

• If the hypothalamus /pituitary are in the RT field, then endocrine function should also be
evaluated annually by T4 & TSH, testosterone or FSH/LH.

Follow up
• CT scan immediate postoperative to assess resection.
• MRI recommended at 3months and then annually unless other clinical indications
emergency.

22.10.3.2 High Grade Gliomas (HGGs)


Anaplastic Astrocytoma (AA) and Glioblastoma Multiforme (GBM)

Clinical presentation
seizures, progressive neurologic symptoms depending on site of tumor features of mass effect, or
focal signs depending on location.

`531

Investigations
• FBP, Serum electrolytes,
• Histopathology studies
• Immunohistochemistry studies: IDH, 1p/19q codeletion, ATRX mutations.

Imaging
• CT brain scan
• MRI preferred investigation
• MR spectroscopy
• CT/MR angiography
• Functional MRI (fMRI)

Pharmacological management
Seizures: Treat as per guidelines

Surgical management
• Complete excision of the tumor is essential for improved survival. Preoperative and
intraoperative techniques to improve extent of resection in a safe manner (maximum safe
resection) including brain mapping, use of intraoperative fluorescein guidance to expand
resection magins and neuromonitoring techniques are advocated.
• Extent of resection is best assessed on post-op CT/MRI scans.

Radiotherapy
• Patients should be CT-planned, with contrast administration. 3mm to 5mm slices cuts from
Vertex to Base of skull. Large volume PTV = should completely encompass enhancing
lesion seen on pre-op T2/FLAIR scan, plus small (2cm) margin.
• Dose to LARGE VOLUME = 2.00 Gy X 23 Fractions = 46.00 Gy (5 times per week).
• Small volume PTV (PTV2) is based on Gd-enhanced T1 weighted image=
enhancing lesion on pre-op scans +1- 2 cm margin.
• Dose to SMALL VOLUME = 2.00 Gy X 7 Fractions = 14.00 Gy
• Total dose 60Gy in 30 fractions.
• Other alternative radiotherapy fractionations can be used in elderly, more
than 65 years of age are Hypo fractionation; 40Gy/ 15 Fractions and 5Gy X 5
Fractions

Note
• Imaging techniques such as MR Spectroscopy may be indicated during follow up to
distinguish tumor recurrence from post RT changes.

Chemotherapy
Concurrent chemotherapy + RT:
S: temozolomide (PO) 75 mg/m2 daily during RT, Then 150-200mg/m2 given D1-D5 of a 28
day cycle for 6 cycles after RT
Oral steroid/ Ondansetron should be taken half an hour prior to chemotherapy tablet on each
day. Tablets must be taken 1st thing in the morning on an empty stomach.
Prophylaxis for PCP pneumonia with co-trimoxazole (one tablet twice daily) should be given
during daily temozolomide treatment.

Recurrent disease
• Surgery plays an important role in selected patients- relieves symptoms,
improves PS and QOL and reduces steroid requirement.
• Repeat radiotherapy can be considered, depending on size of lesion and
previous dose.
• Palliation Chemotherapy may be only modality available- active regimens are BCNU, PCV,
Temozolomide and more recently, Irinotecan and Bevacizumab.

Follow up
• A baseline scan should be done at 4 months’ post RT as a reference.
• Thereafter scans are usually done at 6 months and annually, or if clinically indicated.
• High index of suspicion and testing if indicated for pituitary function.

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22.11 Oncological Emergencies


Important oncological emergencies include Hypercalcemia, Superior venous cava obstruction,
Spinal cord compression and Neutropenic sepsis.

22.11.1 Superior Vena Cava Syndrome (SVCS)


Superior vena cava syndrome (SVCS) is the clinical expression for obstruction of blood flow through
the SVC. Malignancy (90%) is the most frequent cause of SVC obstruction. SVC obstruction is a
strong predictor of poor prognosis in patients with non–small cell lung cancer. SVC obstruction in
cancer patients can result from
• Extrinsic compression of SVC
o Lung Cancer (65%)
o Lymphomas (15%)
o Other cancers (10%)
• Intrinsic compression

Diagnostic Criteria
Common symptoms and physical findings of SVCS are:
• Dyspnea
• Headache
• Oedema and change in colour in the areas drained by SVC (examples–face and upper
limb)
• Venous distension of neck, upper chest and arms
• Cough
• Pemberton’s sign (development of facial flushing, distended neck and head superficial
veins, inspiratory stridor and elevation of the jugular venous pressure (JVP) upon raising
both of the patient's arms above his/her head simultaneously, as high as possible
(Pemberton's maneuver)

Investigations:
• CXR
• CT scan Chest Abdomen and Pelvis
• PET/CT
• Tissue diagnosis for appropriate treatment modality
• Bronchoscopy
• Needle aspiration of a peripheral lymph node, or mediastinoscopy
• Sputum cytology
• Thoracentesis.

Non-pharmacological treatment: Treatment of SVC syndrome is divided into supportive and


definitive therapy
Supportive measures
• Head elevation–To decrease the hydrostatic pressure and thereby the edema. There are
no data documenting the effectiveness of this manoeuvre, but it is simple and without risk.
• Glucocorticoid therapy (dexamethasone, 4 mg every 6 hours) to relieve inflammation and
oedema (to be avoided before biopsy if lymphoma is suspected as steroid induced tissue
necrosis might obscure the diagnosis)
• Loop diuretics (furosemide) are also commonly used, but it is unclear whether venous
pressure distal to the obstruction is affected by small changes in right atrial pressure.

Definitive Therapy
• Radiation treatment to the malignant mass.
• Chemotherapy–in chemo sensitive cancers like lymphoma, germ cell tumours or small cell
lung cancer
• SVC Stent–can be useful in cases of thrombosis and for patients not responding to cancer
treatment
• Removal of central venous device.

Note
• It is advisable to avoid placement of intravenous lines in the arms so that fluid is not
injected into the already compressed SVC.

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22.11.2 Hypercalcaemia
Hypercalcaemia refers to elevated calcium level in blood (normal range 2.2–2.6 mmol/L) that occurs
in 10–20% patients with advanced cancers (most commonly in cancer of the breast, kidney, lung,
prostate, head and neck and multiple myeloma)

Diagnostic Criteria
• Symptoms of hypercalcaemia include nausea, vomiting, constipation, polyuria and
disorientation
• Psychiatric overtones (depression 30–40%, anxiety, cognitive dysfunction, insomnia,
coma)
• Clinical evidence of volume contraction secondary to progressive dehydration may be
apparent. Severe hypercalcaemia (above 3.75–4.0 mmol/L) is a medical emergency and a
poor prognostic sign

Investigations include
• Specific biochemistry like PTH,
• ECG to detect arrhythmias and
• Imaging with Bone Scan or PET–CT scan to identify metastatic bone disease.

Pharmacological Treatment
Treat the hypercalcaemia first and the cause later:
• Hydration & dieresis: 1–2 litres of isotonic saline (NS) over 2 hours with 30–40 mg of
furosemide expands intravascular volume and enhances calcium excretion.
o In elderly and cardiac patients, rate of hydration needs to be slower.
• Bisphosphonates–via a complex mechanism inhibit osteoclast and in turn both normal and
pathological bone resorption. Commonly used bisphosphonates are:
S: zolendronic acid (IV) infused as 4mg (IV) in 100 mls of NS over 15 mins.
Normalisation of serum calcium occurs in 4–10 days and lasts 4–6 weeks. Therefore,
if re–treatment is required, dose is repeated after 7 days
OR
S: ibandronate (IV) 6 mg over 2 hours infusion

Note
• Bisphosphonates and denosumab cause increasing risk of osteonecrosis of jaw
following extraction of teeth or oral surgical procedures. Therefore, a dental review may
be necessary to make sure the necessary dental procedures are completed prior to
commencing therapy
• Calcitonin – a thyroid hormone given 4–8 IU/kg IM or SC every 6–8 hours can bring
about a rapid decline in calcium levels, however tachyphylaxis limits its utility.

22.11.3 Spinal–cord Compression


Spinal cord compression threatens mobility, independence and longevity in patients with metastatic
cancer and may be the first presentation of curable malignancy in others. It most commonly occurs
due to an enlarging vertebral metastasis encroaching on the epidural space or due to pathologic
fracture of a vertebra infiltrated by malignancy.

Management
• Immobilising the patient and obtaining urgent MRI/CT whole spine should be priorities.
• Corticosteroids should be initiated on suspicion of cord compression.

B: dexamethasone (IV) 16 mg immediately followed by 16 mg daily in divided doses.


• Bladder catheterisation is appropriate.
• Once spinal cord compression is confirmed, urgent neurosurgical opinion should be
sought. There are potential improvements in outcomes for patients treated with surgery
upfront, though appropriateness for this will depend upon spinal stability, patient and
malignancy related factors.
• Radiotherapy: for patients who are not candidates for upfront surgery.
• Palliative dose: 8Gy Single fraction or 20Gy/5Fractions or 30Gy/10 Fractions.

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Note
• All patients suspicious for spinal cord compression should be referred to
neurosurgeon and radiation oncologist as soon as possible.

22.11.4 Tumor Lysis Syndrome


The syndrome is mostly observed in cancers with a rapid proliferation index such as Burkitt’s
lymphoma, acute lymphocytic leukemia, acute non-lymphocytic leukemia, and less frequently, solid
tumors of small-cell type, breast cancer, and medulloblastoma.

Clinical Presentation
Clinically, the syndrome is characterized metabolically by the presence of hyperuricemia,
hyperkalemia, hyperphosphatemia, hypocalcemia and acute renal failure.
• Work Up
• FBP, RFT, LFT, LDH
• Serum electrolytes phosphates and calcium
• Urine pH and output
• ECG.
• CXR
• CT-Scan.
• Abdomen and Pelvis USS

Treatment
• Frequent monitoring of electrolytes such as blood-urea-nitrogen (BUN), creatinine, uric
acid, potassium, sodium, phosphate, calcium levels and Lactate dehydrogenase (LDH) at
least three times per day
• Also Alkalization of urine by Sodium bicarbonate added to IV fluids at 100 mEq/L this
should continue for 48-72 hours after start of chemotherapy.
• Hydration in high risk patients must start 12-48 hours’ prior the start of chemotherapy and
continue 48- 72 hours post chemotherapy; continuous infusion should exceed 3 L/m² daily,
resulting in urine volumes of at least 3L/Day.
• IV Allopurinol 300 mg/day daily
• Patients with high potassium levels must be evaluated and monitored constantly for
cardiac rhythm disorders, do administer calcium and exchange resins, those with
continuously low levels calcium a calcitriol must be given.
• Empiric antibiotics can be administered for opportunistic infections, consider also
perenteral nutrition (TPN) and GCF (neupogen) if indicated.

20.11.5 Febrile Neutropenia


Appllied only to the management of patients with:
• Fever and neutropenia as a result of a known or suspected malignancy or the use of
chemotherapy
• Fever and neutropenia as a result of a bone marrow failure syndrome.
• Fever (or evidence of infection) who are receiving chemotherapy or who have completed
cancer therapy within 6 months even though they are not neutropenic.

Work up

• FBP, LFT, RFT


• Malaria screen
• Urine analysis Urine / blood / stool culture Serum Electrolytes Throat Swab

Treatment
• Antibiotic administration
• Anti pyretics and analgesics

`535

Initial (first-line) and subsequent (second-line – deteriorating patients) empiric antibiotic selection.
Patients with no significant betalactam reactions:
D: piperacillin+tazobactam (FDC) (IV) 4 g piperacillin / 0.5 g tazobactam given every IV 6
hourly PLUS Gentamicin 3-6mg/kg once daily. Deteriorating patients on first line treatment
with no history of anaphylaxis to Beta Lactams (i.e. if history of rash only, can still use
meropenem
OR
D: meropenem (IV) 500mg 8 hourly AND amikacin (IV) 15mg/kg/dose in 2-3 devided dose
(or ciprofloxacin 200– 400 mg IV 12 hourly) AND vancomycin 15 - 20mg/kg/dose 8 - 12
hourly
Patients with history of definite anaphylaxis to Beta Lactams
D: ciprofloxacin (IV) as above AND metronidazole (IV) 500mg – 750mg dose 8 hourly AND
amikacin dose as above AND vancomycin dose as above
Culture Negative Patients
First 48 hours

• Patient had a single spike of fever (i.e. patient’s temperature returns to normal within 4
hours of the initial fever), antibiotics may be discontinued.
• Patient had more than a single spike of fever, antibiotics must be continued for a minimum
of 7 afebrile days. Also consider the following.
• If patient develops oral herpes or severe mucositis, commence IV Aciclovir.
• Obvious fungal infection – suspect candida – add fluconazole IV; suspect other fungal
infection – add Amphoteracin B IV.
• Diarrhoea and vomiting – culture stool and commence ciprofloxacin and metronidazole
• Signs of skin infection – add vancomycin
• No clinical focus but deteriorating rapidly or extremely unwell – consider adding
vancomycin

If by day 5-7 patient remains febrile, neutropenic, consider performing a fungal work-up, prior to
commencing empiric appropriate antifungal treatment.

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CHAPTER TWENTY-THREE
MENTAL HEALTH CONDITIONS
23.1. Patients with Aggressive and Disruptive Behaviours
These are agitated and acutely disturbed patients, who may or may not have a mental disorder.
Many acute medical conditions, trauma, toxicological conditions and substance related disorders
(especially substance induced disorders) can also present with agitation.

Clinical Presentation
• Agitation
• Aggressive behaviours

Non-Pharmacological Treatment
• Ensure the safety of the patient and those caring for them.
• Caution is needed with elderly and frail patients as they are vulnerable to falls and
further injury if sedated.
• The use of physical restraint should only be employed when there is a need to protect
the patient and surrounding people in an acute setting and it should be for as short
time as possible with a constant monitoring of patients’ safety
• Assess for sign of delirium.

De-escalation Techniques should be attempted first:


• Calm the patient
• Manage in a safe environment
• Ensure the safety of all staff members

Pharmacological Treatments
For cooperative patients
A: promethazine (PO) 25-50mg stat
OR
C: diazepam (PO)10 mg stat
OR
C: lorazepam PO)4 mg stat

Uncooperative and severely agitated patients


If oral treatment fails after 30–60 minutes, OR If there is significant risk to the patient and others,
give
Parenteral treatment as follows:

B: haloperidol (IM) 2.5-5mg stat, repeat in 30-60minutes, if required. (Maximum dose:


20mg, within 24hours)
AND
A: diazepam (IV/IM) 10mg stat. Repeat after 30–60minutes if needed. (maximum dose:
60mg per 24hours)
OR
A: promethazine (deep IM) 25–50mg Repeat after 30–60minutes if needed
OR
C: lorazepam (IM) 1-4mg stat. Repeat after 30–60minutes if needed to a maximum dose of
12mg in 24hours
OR
D: midazolam (IV/IM) 2-10mg stat

If haloperidol is unavailable,
A: chlorpromazine (deep IM) 25–50mg may be repeated as necessary 4 times in 24hours
(Maximum dose: 2000mg per 24hours).

If patient is known to suffer from schizophrenia and is not neuroleptic naïve give:
S: zuclopenthixol acetate IM) 50–150 mg (Repeat after 2–3 days, if necessary.Give a
maximum of 3 repeat injections and should not be used for longer than 2 weeks. The
maximum administered dose should not exceed 400mg.
If patient develops acute dystonia give:

`537

A: promethazine (deep IM) 25–50 mg. In the elderly 25 mg.


OR
A: atropine (IM) 0.5 -2 mg when required

Note
• Repeated doses of high potency antipsychotics may lead to the development of the life-
threatening neuroleptic malignant syndrome. If suspected, stop antipsychotic, and institute
supportive care.
• Elderly patients are at increased risk of respiratory depression and delirium from
benzodiazepines, so they should be avoided as far as possible.
• Always monitor vital signs of sedated patients

23.2. Delirium
Delirium or acute confusion state is a condition characterized by altered level of consciousness,
disorientation to time, place and sometimes to person.

Clinical presentation
• Reduced awareness of the environment
o Inability to stay focused on a topic or to switch topics
o Getting stuck on an idea rather than responding to questions or
conversation
o Being easily distracted by unimportant things
o Being withdrawn, with little or no activity or little response to the environment
• Poor thinking skills (cognitive impairment)
o Poor memory, particularly of recent events
o Disorientation — for example, not knowing where you are or who you are
o Difficulty speaking or recalling words
o Rambling or nonsense speech
o Trouble understanding speech
o Difficulty reading or writing
• Behavioral changes
o Seeing things that don't exist (hallucinations)
o Restlessness, agitation or combative behavior
o Calling out, moaning or making other sounds
o Being quiet and withdrawn — especially in older adults
o Slowed movement or lethargy
o Disturbed sleep habits
o Reversal of night-day sleep-wake cycle
• Emotional disturbances
o Anxiety, fear or paranoia
o Depression
o Irritability or anger
o A sense of feeling elated (euphoria)
o Apathy
o Rapid and unpredictable mood shifts
o Personality changes

Non-Pharmacological Treatment
• Control the acute disturbance.
• Perform proper physical assessment as well as investigations in order to rule out or
ascertain the underlying medical condition and treat accordingly

Pharmacological Treatment
Treat the underlying medical condition, if present. And any other presentations, symptomatically

Acute Management
B: haloperidol (IM) 5mg stat repeated in 30-60 minutes when required (Maximum dose:
20mg within 24 hours)

`538

• Monitor vital signs and beware of acute dystonia and neuroleptic malignant syndrome
• Dosing may vary according to clinical circumstances

AND/OR
A: diazepam (IV) 10mg.
OR
C: lorazepam (IM) 1-4mg.
Switch to oral route once containment is achieved.

Note
• Benzodiazepines, especially diazepam IV, can cause respiratory depression. Monitor
patients closely
• In the frail and elderly patient or where respiratory depression is a concern, reduce the
dose by half
• The safest route of administration is oral followed by IM with the IV route having the
highest risk of respiratory depression and arrest. Use the safest route wherever
possible.
• Monitor vital signs closely during and after administration
• Use haloperidol instead of benzodiazepines in patients with respiratory insufficiency
• To avoid benzodiazepines toxicity, allow at least 15-30 minutes before repeating the
IM dose

23. 3. Dementia
It is a condition which involves progressive and cognitive deficits. Dementia usually affects memory
first, with subsequent progression to cause dysphasia, agnosia, apraxia, diminished ability with
executive function and eventually personality disintegration.

DSM-5 diagnostic criteria


To diagnose Dementia, the following criteria need to be met:
• There must be significant cognitive decline from a previous level of performance in one or
more of the following cognitive domains - attention, executive function, learning and
memory, language, perceptual motor and social cognition.
• These deficits affect independence in performing everyday activities.

Non-pharmacological Treatment
• Psychoeducation about the disorder, to the patient and family
• Mini Mental Status Examination, functional and behavioural assessment should be
performed every 6 months.

Pharmacological Treatment
Mild to moderate:
S: donepezil (PO) 5mg initially, may increase to 10mg/24hours after 4-6weeks
Moderate to severe:
S: donepezil (PO) 5mg initially, may increase to 10mg /24hours after 4-6weeks; may
further increase to 23 mg/day after 3 months
23.4. Schizophrenia
It is a chronic mental disorder, characterized by disturbances in thought, emotions, drive, behaviour
and withdrawal from reality. Symptoms vary from patient to patient and from time to time.

DSM-5 Diagnostic Criteria


To diagnose Schizophrenia, the following criteria need to be met;
• Presence of 2 or more of the following symptoms over a 1-month period:
a. Delusions
b. Hallucinations
c. Disorganized speech
d. Disorganized behavior
e. Negative symptoms
(at least 1 of which must be a, b or c)
• Individual’s premorbid level of functioning is affected in several major domains of life.

`539

• There must be continuous impairment over a period of at least 6 months, during which the
individual might experience either active or residual symptoms.
• These symptoms must not be due to the effects of substance usage or an underlying
medical condition

Non-Pharmacological Treatment
• Family counselling and psycho-education
• Cognitive Behavioural Therapy (CBT) for stabilized patients
• Supportive group therapy for patients with schizophrenia
• Rehabilitation may be enhanced by assertive community programs, work assessment,
occupational therapy and bridging programs prior return to the community

Pharmacological Treatment
In acute attacks:
Treat like under section: patients with aggressive and disruptive behaviours.

For maintenance:
B: haloperidol (PO) 3-4.5mg 12hourly,
OR
A: chlorpromazine (PO) 100–600mg 24hourly in divided doses
OR
S: olanzapine (PO) 5–10mg titrate to maximum dose 20mg/24hours
OR
S: risperidone (PO) 1mg 12hourly then increase by 1mg every 2–3 days to 2–3mg 12
hourly. Maximum dose 16mg/day

Note:
• Titrate to maximum dose while monitoring dose-response to target symptoms against
adverse effect
• The above medicines should not be given in combination
• The atypical antipsychotics have been shown to be comparatively more effective in
treatment of negative symptoms

For patients who have poor compliance to oral medications and patient preference, give
depot antipsychotics
C: fluphenazine decanoate (IM) 6.25-50mg 2-4weekly, and monitor dose-response to
target symptomsagainst adverse effect, if necessary, dose may be tapered
OR
S: zuclopenthixol decanoate (IM) 100-600mg 2-4weekly, and monitor dose-response to
target symptomsagainst adverse effect, if necessary, dose may be tapered
OR
S: flupenthixol decanoate (IM) 20–40 mg every 4weeks, and monitor dose-response to
target symptomsagainst adverse effect, if necessary, dose may be tapered

Note
• . Give a test dose first. This is in view of the fact that depots are known to be long acting
• Giving a test dose helps to determine whether the patient is sensitive to the medication
(either via development of EPSE or any adverse reactions to the oil base)
• Commence treatment with the lowest therapeutic dose
• Administer the depot at the longest possible duration
• adjustment of dosages should be conducted after an adequate period of assessment

Adjunct Treatment
Antiparkinsonian medicines should only be used if extrapyramidal side effects(except tardive
dyskinesia) occur, or at higher doses of antipsychotics likely to cause extrapyramidal side effects.
Any of the following can be used:

A: promethazine (PO) 25-50mg 24hourly, until symptoms/signs subside


OR
A: benzhexol (PO) 5mg 24hourly to12hourly, last dose before 1400 hourstoavoidinsomnia

`540

Referral
Refer to the next level in the following situations:
• First psychotic episode • Pregnant and lactating women
• High suicidal risk or risk of • No response to treatment
harm to others • Intolerance to medications
• Children and adolescents • Concurrent medical conditions
• Elders or other mental disorders
23.5. Catatonia
Causes of catatonia: schizophrenia, severe depressive disorder, bipolar disorder, organic disorders
e.g. CNS infections, CNS tumour, cerebrovascular accident, severe intoxication of recreational
drugs and lethal catatonia.
Clinical features: Ambitendency, automatic obedience, waxy flexibility / catalepsy, negativism,
stereotypy, mannerism, echolalia and echopraxia.
Investigations: FBP, RFT, LFT, TFT, blood glucose, CK, urine drug screen, ECG, CT, MRI, EEG,
urine and blood culture, syphilis screen, HIV, heavy metal screen, auto-antibody screen and lumbar
puncture.
Non-pharmacological treatment
Hydration, early mobilization, close monitoring, transferal to ICU if patient deteriorates.

Pharmacological treatment

A: diazepam (IV/IM) 10-20mg 24hourly


OR
C: lorazepam (IM) 1-4mg 24hourly

Note
• If benzodiazepine does not work and symptoms are severe, ECT is an option
23.6. Schizoaffective Disorder
DSM-5 Diagnostic criteria

For an individual to fulfill the diagnostic criteria, there must be the presence of solely hallucinations
or delusions for at least 2 weeks in the absence of an affective episode, throughout the whole
duration of the psychiatric illness. There must also have an uninterrupted period where there are
prominent affective symptoms concurrent with symptoms of schizophrenia. Individuals should have
symptoms fulfilling the diagnosis of an affective disorder for most of the duration of the illness.
DSM-5 has specified 2 subtypes of schizoaffective disorder, which are:

• Bipolar type - Whereby a manic episode is part of the entire course of the illness
• Depressive type - Whereby a major depressive episode is part of the entire course of the
illness

Non-Pharmacological Treatment
• Family counselling and psycho-education
• Cognitive Behavioural Therapy (CBT) for stabilized patients
• Supportive group therapy for patients
• Rehabilitation may be enhanced by assertive community programs, work assessment,
occupational therapy and bridging programmes prior return to the community

Pharmacological Treatment
For Psychotic symptoms:
A: chlorpromazine (PO) 100-1000mg in divided doses*, per day (max. dose 1000mg, per
24hours)
OR
B: haloperidol, (PO) 1.5-6mg in divided doses*, per day (max. dose 20mg)

`541

For Manic subtype:


A: carbamazepine (PO) 200-1000mg 24hourly, in divided dose*
OR
C: sodium Valproate (PO) 500-1000mg 24hourly, in divided dose*

For Depressive subtype:


A: amitriptyline (PO) 12.5-75 mg nocte
OR
S: fluoxetine (PO) 10-20 mg nocte

Note
• Symptoms should be monitored and medication can be tapered* divided doses: in acute
phase 8hourly or 12hourly while in maintenance phase titrate to 12hourly or preferably
24hourly

23.7. Brief or Acute/Transient Psychotic Disorder


DSM-5 Diagnostic criteria
For an individual to fulfill this diagnosis;
• He/she must have, for a duration of between 1 day to 1 month the following symptoms:
o Delusions
o Hallucinations
o Disorganized speech
o Grossly disorganized or catatonic behaviour
• Exclude differentials like major depression or bipolar depression with psychotic features,
schizophrenia and exclude the possibility of the symptoms being due to underlying
substance use or medical conditions.

Non-pharmacological Treatment
Manage as Schizophrenia

Pharmacological Treatment
Manage as Schizophrenia
23.8. Bipolar Mood Disorders
These are lifelong mental disorders, which may have an episodic, variable courses. The presenting
episodes may be manic, hypo manic, depressive or mixed. By definition, a diagnosis of bipolar
disorders requires either a current or previous episode of mania or hypomania.

Bipolar I Disorder Diagnostic Criteria


DSM-5 specified that an individual need to have at least 1 manic episode in order to fulfill the
diagnostic criteria of Bipolar I disorder.

Manic Episode
A manic episode is characterized by a period of time, of at least 1 week, during which the individual
has persistent elevated (extreme happiness) or irritable mood and present for most of the days.
In addition, the individual needs to have at least 3 (4 if mood is only irritable) of the following
symptoms:
• Increased self-confidence(Grandiose and/or religious delusions)
• Reduction in the need for sleep
• Chattier than usual, with increased pressure to talk
• Racing thoughts
• Easily distractible
• Increase in number of activities engaged
• Involvement in activities that might have a potential for serious consequences

There must be marked impairments in terms of functioning with the onset of the above
symptomatology.

`542

Non-Pharmacological Treatment
• Hospitalization may be required during acute mania
• Psychotherapy, usually after the manic episode has been controlled with medication
• Family therapy and psycho-education of patient and family to increase compliance and
knowledge of the condition
• In severe cases, electroconvulsive therapy may be required.

Pharmacological Treatment
For Manic or Mixed Episodes
For agitated and acutely disturbed patient: See section on patients with aggressive and disruptive
behaviours.

Maintenance therapy
A: carbamazepine (PO) 600mg 24hourly in 2-3 divided doses, increase by 200mg at three-
day interval up to a maximum of 2000mg
OR
C: sodium valproate (PO) 20 mg/kg/day in 2–3 divided doses (maximum of 2000 mg, per
day)
OR
S: lamotrigine (PO) 600mg once a day, increase by 200mg at three-day interval up to a
maximum of 2000mg

Note
• The option of combining two mood stabilizers at S: level should be allowed i.e. sodium
valproate and Lithium carbonate

Treatment for Severe Depressive Episodes in Bipolar Patients


Give antidepressant in combination with mood stabilizer and antipsychotic if there is psychosis:

A: amitriptyline (PO) 12.5 to 50mg nocte


OR
S: fluoxetine (PO) 10-20mg nocte,
AND
A: carbamazepine (PO) 200-400mg 12hourly, maximum 2000mg/per day
OR
C: sodium valproate (PO) 500-2000mg 24hourly
AND
A: chlorpromazine (PO) 100-1000mg 24hourly in divided doses, (max. dose 1000mg, per
day)
OR
B: haloperidol (PO) 1.5mg –10mg 12hourly (if there is psychosis) and symptoms should be
monitored, and medication to be tapered

Note
Do not use monotherapy antidepressants in bipolar patients.

Referral
Refer to the next level in the following situations:
• Mixed or rapid cycling bipolar disorder
• Depressive episodes in bipolar patients not responding to treatment
• Manic episodes not responding to treatment
23.9. Major Depressive Disorder
It is a mood disorder characterized by at least 2 weeks of depressed mood and/or diminished
interest and pleasure in activities. It is associated with impairment in level of functioning in different
areas including social and occupational.

Diagnostic Criteria • Guilt


Psychological symptoms • Diminished concentration
• Depressed mood • Thoughts of death and suicide
• Feeling of worthlessness

`543

Somatic symptoms
• Change in appetite • Retardation
• Sleep disturbances • Loss of energy
• Agitation

Non-Pharmacological Treatment
Effective psychotherapies include: • Marital and family issues
• Cognitive Behavioural Therapy • Sleep hygiene advice
• Interpersonal psychotherapy
• Stress management / coping skills

Pharmacological Treatment
A: amitriptyline (PO) 12.5–75mg 24hourly at night, increase gradually to a maximum of
150mg 24hourly. {Elderly: Initially 12.5–50 mg. Max. 75mg)
OR
D: citalopram (PO) 10-60mg 24hourly
OR
S: fluoxetine (PO) 20-60mg 24hourly (morning)
Note
• Efficacy of the treatment is gauged by amelioration of symptoms and the dose should be
titrated according to clinical response.
• Monitor all patients recently started on antidepressants closely for increased agitation and
suicidal behaviour, especially young patients (younger than 25 years).
• Some symptoms, such as sleep and appetite, may improve more quickly.
• If partial response or non-response, increase the dose or switch to another antidepressant.
The first line is an alternative SSRI. The second line is an antidepressant from a different
class.

Referral
Refer to the next level in the following situations:
• Suicidal ideation
• Major depression with psychotic features
• Failure to respond to available antidepressants
• Patients with concomitant medical illness, e.g. heart disease, epilepsy
• Poor social support systems
• Pregnancy and lactation
23.10. Suicide
Suicide is the act of intentionally causing one's own death. Mental disorders—
including depression, bipolar disorder, autism spectrum disorders, schizophrenia, personality
disorders, anxiety disorders, physical disorders such as chronic fatigue syndrome, and substance
abuse—including alcoholism and the use of and withdrawal from benzodiazepines—are risk
factors.Some suicides are impulsive acts due to stress (such as from financial or academic
difficulties), relationship problems (such as breakups or deaths of close ones), or
harassment/bullying. Those who have previously attempted suicide are at a higher risk for future
attempts.

Effective suicide prevention efforts include;


• Limiting access to methods of suicide—such as hanging, firearms, drugs, and poisons
• Treating mental disorders and substance misuse
• Careful media reporting about suicide
• Improving economic conditions.

23.11. Generalized Anxiety Disorder


Generalized anxiety disorder is characterized by excessive, exaggerated anxiety and worry about
everyday life events with no obvious reasons for worry.

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Diagnostic Criteria
Symptoms include
• Persistent worry • Mood disturbances
• Disturbances in sleep • Muscle tension
• Poor concentration • Tremors

Non-pharmacological Treatment
• Psychotherapy
• Most patients can be treated as outpatients

Pharmacological Treatment
Indicated where symptoms are interfering with normal functions of daily living. Where there is
concomitant drug/alcohol dependence or co-morbid major depressive episode, an antidepressant
may be more appropriate.

Acute management
For an acute episode or intense prolonged anxiety:
A: diazepam (PO) 2–5 mg stat repeat 12hourly when required
o Duration of therapy: up to 2weeks, taper off to zero within 6weeks

Maintenance Therapy
A: amitriptyline (PO) 25–75mg nocte (Medication should be titrated according to symptoms
resolution)
OR
D: citalopram (PO) 10–40mg 24hourly (Medication should be titrated according to
symptoms resolution)
OR
D: clonazepam (PO) 0.5 – 4 mg 24hourly (Medication should be titrated according to
symptoms resolution)
OR
S: fluoxetine (PO) 20–40mg 24hourly (Medication should be titrated according to
symptoms resolution)

Note:
• Prolonged treatment with benzodiazepines often leads to tolerance and withdrawal
symptoms if the medicine is discontinued abruptly
• Avoid combining more than one benzodiazepine.

Referral
Refer to the next level if there is lack of improvement with treatment.
23.12. Panic Disorder
Panic disorder is an anxiety disorder characterized by recurrent unexpected panic attacks. A panic
attack is characterized by an acute onset of intense anxiety accompanied by a sense of
dread/impending threat, usually for no apparent reason.

Diagnostic Criteria
The patient will experience significant fear and emotional discomfort, typically peaking within 10
minutes and resolving within 30 minutes. There will usually be accompanying physical symptoms
including:
• Rapid pulse/palpitations
• Shortness of breath
• Dizziness
• Sweating

Non-Pharmacological Management
• Psycho-education and reassurance
• Psychotherapy, e.g. cognitive-behaviour therapy
• Exclude an underlying medical condition, e.g. thyrotoxicosis

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Pharmacological Treatment
Panic attack
Acute management
The initial aim is to control the panic symptoms and exclude an underlying medical cause.
A: diazepam (PO) 5-10mg 12hourly (Medication should be titrated according to symptoms
resolution)
OR
C: lorazepam (PO) 2-4mg 12hourly (Medication should be titrated according to symptoms
resolution)
OR
D: clonazepam (PO) 0.5-3mg 12hourly (Medication should be titrated according to
symptoms resolution)

Panic disorder
A: amitriptyline 25–75mg (PO) nocte (Medication should be titrated according to symptoms
resolution)
OR
D: citalopram 10–40mg (PO) 24hourly (Medication should be titrated according to
symptoms resolution)
OR
S: fluoxetine 20–40mg (PO) 24hourly (Medication should be titrated according to
symptoms resolution)

Note
• Initiate at low dose and gradually titrate to therapeutic dosages according to tolerability.
• Duration of therapy: variable, initially 6 months–1 year.
• Long term medicine treatment may be necessary.
• Relapses may occur when treatment is discontinued.
• Consider short term co-administration of a benzodiazepine, due to the slow onset of action
and the potential for increased anxiety during the initial phase of treatment with
antidepressants.

Referral
Refer to the next level in the following situations; Treatment resistance or need for benzodiazepine
treatment beyond 6 weeks
23.13. Obsessive-Compulsive Disorder
This condition is characterized by the presence of persistent intrusive thoughts or concerns, and is
usually associated with compulsions, which are mental acts or behaviours which an individual
engages in to attempt to get rid of the obsessions and/or decrease his or her distress i.e. excessive
hand washing. Obsessive thoughts and compulsions may interfere with daily functioning. The
features are usually distressing to the patient.

Diagnostic Criteria
• A pattern of repetitive behaviours
• Anxiety symptoms

Non-pharmacological Treatment
• Psycho-education
• Psychotherapy
• Behaviour therapy

Pharmacological Treatment
D: citalopram, Initial dose: (PO) 20mg. If there is no or partial response after 4-8weeks,
increase to 40mg, if well tolerated.
OR
S: fluoxetine, Initial dose: (PO) 20mg. If there is no or partial response after 4-8weeks,
increase to 40mg, if well tolerated.

Referral
Refer to the next level in the following situations: Inadequate response to treatment

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23.14. Acute Stress Disorder and Post-Traumatic Stress Disorder


Acute stress and post-traumatic stress disorder arise in response to stressful events. The patient
should have experienced the event as life threatening or as a physical threat to themselves or
others, at which time they felt fear and helplessness.

Diagnostic Criteria
Symptoms associated with both of these conditions include:
• Re-experiencing of the event, e.g. flashbacks, dreams
• Avoidance of situations associated with the event
• Features of anxiety or increased arousal, e.g. hyper vigilance, heightened startle
response and insomnia

The conditions are symptomatically similar but differ with regard to the duration and time of onset of
symptoms. The symptoms of acute stress disorder arise within 4 weeks of the event and last up to 4
weeks, whereas the symptoms post-traumatic stress disorder last longer than 4 weeks, and may
arise more than 4 weeks after the traumatic incident.

Non-pharmacological Treatment
• Reassurance and support of patient and family
• Psychotherapy, supportive/cognitive-behavioural therapy

Pharmacological Treatment

Acute stress disorder:


For acute anxiety or agitation give:
D: clonazepam (PO) 0.5–2 mg 24hourly to 12hourly for 2weeks
Not for longer than 2 weeks and taper to a stop in the course of 26 weeks. The maintenance
treatment needs antidepressants

Note
• Prolonged use of benzodiazepines > 1 week may be detrimental to adaptation,
leading to higher rates of post-traumatic stress disorder

Post-traumatic stress-disorder:
A: amitriptyline (PO) 50–150mg nocte Elderly: 25- 75mg. (PO) for 4-8weeks
OR
D: citalopram 20-40mg (PO) 24hourly for 4–8weeks
OR
S: fluoxetine (PO) 20-40 mg 24hourly morning for 4–8weeks

Note
An adequate antidepressant trial of treatment is 8–12 weeks, before an alternative treatment should
be considered.

Referral
Refer to the next level in the following situations:
• Inadequate response to treatment
• Co-morbid conditions

23.15. Substance Related Disorder



23.15. 1. Substance Use Disorder
23.15.1.1. Alcohol Use Disorder
DSM-5 diagnostic criteria
There must be a problematic usage of alcohol that has led to significant impairments
occurring over a total of 12 months’ duration. The problematic usage of alcohol is manifested by at
least 2 of the following:
• Increasing usage of alcohol, or over a longer period than originally intended
• Repeated unsuccessful efforts to cut down or control usage, despite the desire to do so.

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• Large amount of time is spent on activities to obtain alcohol, use alcohol, or recover from
the effects of alcohol.
• Presence of a strong desire or urge to use alcohol
• Repeated alcohol usage resulting in a significant failure to fulfill major roles
• Persistent usage of alcohol despite having recurrent social or interpersonal problems due
to the usage of alcohol.
• Important activities are given up due to the usage of alcohol
• Repeated usage despite significant impairments in physical health
• Continued use despite knowing that there have been physical or psychological problems
arising from the usage of alcohol
• Tolerance as defined by either (1) Need for increasing amounts of alcohol to achieve the
same or desired effects or (2)
• Reduced effects with continued use of the same amount of alcohol
• Withdrawal as defined by either (1) Characteristic withdrawal symptoms or (2) Alcohol is
being used to prevent or avoid withdrawal symptoms

Non-pharmacological Treatment
• Cognitive Psychotherapy – Involves assessment of the patient’s readiness for behavioural
change using the stage of change model and also make use of motivation interviewing to
enable patients to be empowered to change
• Alcoholic Anonymous groups
• A self-help group, with the sole purpose of enabling patients to quit their drinking habits.
Their program is based on 12 core principles.

23.15.1.2. Opioid Use Disorder


DSM-5 diagnostic criteria
It states that there must be problematic usage of opioid that has led to significant impairments in
terms of functioning over a 12-month period. The rest of the criteria are similar to that of alcohol use
disorder
Non-pharmacological Treatment

• Motivational interviewing
• Therapeutic group therapy in a structured environment is helpful for helping individuals
with their addiction.
• Psycho-education with regards to their possibility of HIV transmission when using shared
needles would be helpful

Pharmacological Treatment
Opioid substitutes
C: methadone (PO) 10-30mg stat based on clinical assessment and UDS test then
increase by 5-10mg every 3-5days to achieve optimal dose when opioid withdrawal
features are well controlled.Once stability is reached, the client should be planned to
remain on treatment for a minimum of two years. For more detail refer to national
guidelines for comprehensive management of opioid use disorder

OR
S: buprenorphine 8-32mg (PO) 8hourly (Medication should be titrated according to
symptoms resolution)

23.15.1.3. Nicotine Use Disorder


For an individual with nicotine use disorder, abstinence from nicotine usually leads to withdrawal
symptoms. Nicotine detoxification requires the use of medication to prevent the symptoms which
could become severe and potentially lead to mortality.

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Diagnostic Criteria
Withdrawal symptoms include:
• Restlessness • Anxiety
• Tremors • Loss of appetite
• Difficult in getting/maintaining
sleep

Non-Pharmacological Treatment
• Support group that encourage abstinence
• Inpatient rehabilitation programme where necessary

23.15.2 Substance Induced Disorder


23.15.2.1. Substance Intoxication
Alcohol Intoxication
DSM-5 diagnostic criteria

It specifies that there must be recent usage of alcohol and that clinically significant behavioral or
psychological changes have arisen during or shortly after the usage.

This is characterized by at least one of the following signs or symptoms:


• Slurred speech • Nystagmus
• Incoordination • Impairments in attention or memory
• Unsteady gait • Stupor or coma

Treatment
Symptomatically, depending on how patient presents
Opioid Intoxication
DSM-5 Diagnostic criteria

• It states that there must be recent usage of opioid, with the presence of pupillary
constriction (or pupillary dilation due to anoxia from severe overdose) and at least 1 of the
following signs and symptoms:
• Feeling drowsy or losing consciousness
• Slurring of speech
• Impairments in attention or memory
There must also be significant problematic behavioral or psychological changes that have arisen
during or shortly after the usage.

Pharmacological Treatment
B: naloxone (IM/IV) 0.04-15mg mg; if there is no response, the dose should be increased
every 2 minutes
Stimulant Intoxication
DSM-5 diagnostic criteria
It specifies that there must be recent usage of amphetamine-type substance, cocaine or other
stimulant that has led to significant impairments in functioning, shortly after usage. This is
manifested by at least 2 of the following signs and symptoms:

• Increase or decrease in heart rate • Psychomotor agitation or


• Pupillary dilation retardation
• Elevated or lowered blood pressure • Muscular weakness, respiratory
• Perspiration or chills depression, chest pain or cardiac
• Nausea or vomiting arrhythmias
• Evidence of weight lost • Confusion, seizures and coma

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Pharmacological treatment of cocaine intoxication:


If patient presents with agitation, refer to treatment of patient with aggressive and disruptive
behaviors
If patient presents with psychosis, give
A: chlorpromazine (PO) 100-1000mg in divided doses, per day (max. dose 1000mg, per
day)
OR
B: haloperidol (PO) 1.5-6mg in divided doses, per day (max. dose 20mg)

Note
Treatment rendered largely targets the symptoms that individuals are experiencing

Pharmacological treatment of Amphetamines intoxication:

If patient presents with agitation, refer to treatment of patient with aggressive and disruptive
behaviors
If patient presents with depressive symptoms after detoxication, refer to pharmacological treatment
with depressive symptoms

Pharmacological treatment of Cannabis intoxication:


A: chlorpromazine (PO) 100-1000mg in divided doses, per day (max. dose 1000mg, per
day)
OR
A: haloperidol (PO) 1.5-6mg in divided doses, per day (max. dose 20mg)

23.15.2.2. Substance Withdrawal


Alcohol Withdrawal
For an individual with alcohol use disorder, abstinence from alcohol usually leads to withdraw
symptoms. Alcohol detoxification requires the use of medication to prevent the symptoms which
could become severe and potentially lead to mortality.

Diagnosis features
Withdrawal symptoms include:
• Insomnia
• Tremors
• Chills
• Anxiety

Non-Pharmacological Treatment
• Support group that encourages abstinence
• Inpatient rehabilitation program where necessary

Pharmacological Treatment
C: thiamine (IM) 300mg 24 hourly
For the CNS symptoms
C: diazepam (PO) 10 mg every 4–6 hours on the first 24 and reduce by 20% over 5 days
(only in inpatient care)
OR
C: Lorazepam (PO)

Relapse prevention following detoxification


S: naltrexone (PO) 50mg 24hourly, and should be titrated, according to response
Alcohol Withdrawal Delirium (Delirium Tremens)
It is an acute episode of delirium that is usually caused by withdrawal from alcohol. Although the
typical delirium occurs 2–3 days following cessation of prolonged alcohol intake, reaching a peak at
around 5 days, some withdrawal symptoms such as tremor may start within 12 hours.

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Diagnosis Criteria
• Visual hallucinations • A low-grade fever may be
• Disorientation present
• Fluctuating level of • Withdrawal tonic-clonic
consciousness seizures may occur between
• Agitation 24 and 48 hours following
• Tachycardia cessation of alcohol intake
• Hypertension

Note
It is important to consider alternative causes, when making the diagnosis. This is especially true
for cases with an atypical presentation.

EmergencyCare
• Secure airway
• Ensure breathing
• Circulation
• Give IV fluid (Dextrose Normal Saline) to prevent hypoglycaemia and hypotension
• Monitor for respiratory depression

Pharmacological Treatment
A: diazepam (IV)10mg for immediate sedative or hypnotic action. If no response gives a
second dose.
OR
C: lorazepam (IM/IV) 2mg for immediate sedative or hypnotic action. If no response gives
a second dose.
OR
S: chlordiazepoxide (IV) 20–60mg taper over one month
AND
C: thiamine (IM) 100-300mg 24hourly
OR
A: vitamin B Complex (IV) 1ampoule in 500ml 5% Dextrose

Note:
• Do not administer at a rate over 5 mg/minute
• Switch to oral once containment is achieved

Heroin Withdrawal
Heroin addiction, is a chronic, relapsing brain disease that is characterized by compulsive substance
seeking and use, despite harmful consequences. When your body has become dependent on
heroin, a number of unpleasant withdrawal symptoms will arise when the drug hasn’t been used for
a certain amount of time.

Diagnostic features include:


Myalgia, gooseflesh, diarrhea, rhinorrhea, lacrimation, agitation, anxiety, Insomnia, sweating,
yawning, abdominal cramping, dilated pupils, nausea and vomiting
Pharmacological Treatment
To prevent repeating using of the heroin, give;

S: methadone (PO) 30-120mg 24hourly for a minimum of 1 year


OR
S: buprenorphine (PO) 2-8mg 24hourly for a minimum of 1 year
OR
S: naltrexone (PO) 25-50mg 24hourly for 6 months.

Symptomatic Treatment
For difficult to get sleep, give:
A: diazepam (PO) 5–20 mg 24hourly to a minimum of 7days
OR

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A: promethazine (PO) 50mg 24hourly at bed time (medication should be titrated according
resolution)
OR
A: Chlorpromazine (PO) 50–100mg 24hourly at bed time (medication should be titrated
according resolution)

For abdominal cramps, give:


A: hyoscine butyl bromide (PO) 20mg 8-24 hourly (medication should be titrated according
resolution)
OR
A: diclofenac (PO) 50mg 8hourly (medication should be titrated according resolution)

For diarrhoea give


B: loperamide 4 mg (PO) stat, then 2mg after each loose stool (medication should be
titrated according resolution)

Cocaine Withdrawal

Non-Pharmacological Treatment
These patients usually do not require admission, however beware of depression and assess suicide
risk

Pharmacological Treatment
No substitute drug available for detoxification

C: diazepam (PO) 5–10mg 8hourlyfor 5–7 days (medication should be titrated according
resolution)

Referral
Refer patients to specialized clinic

23.16. Psychiatric Disorders Associated with Epilepsy


Epilepsy is a disorder of the brain characterized by an enduring predisposition to generate epileptic
seizures and by the biologic, cognitive, psychological, and social consequences of this condition.
This association may reflect the anatomical and neurobiological source of both epileptic seizures
and the behavioral manifestations.

Antiepileptic drugs (AEDs) can play a role in the genesis of psychiatric symptoms; on the other
hand, some psychotropic medications can lower the seizure threshold and provoke epileptic
seizures.

The following are common psychiatric disorders in patients with epilepsy;


• Major depressive disorder • Psychoses
• Bipolar mood disorder • Suicidality
• Anxiety disorder

Treatment of Psychotic Disorders in patients with epilepsy;

Non-pharmacological Treatment
• Psychoeducation to the patient and the family
• Family therapy
• Supportive group therapy
• Occupational therapy

Pharmacological Treatment
A: carbamazepine (PO) 200-1000mg, in divided doses, per day (symptoms should be
monitored and medication titrated accordingly)
OR
A: phenobarbitone (PO) 30-200mg, in divided doses, per day (symptoms should be
monitored and medication titrated accordingly)
OR

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C: sodium valproate (PO) 500-2000mg in divided doses, per day (symptoms should be
monitored and medication titrated accordingly)

If psychosis persists, give


B: haloperidol (PO) 0.75-4.5mg 12hourly. Maximum dose 20mg/day
OR
S: olanzapine (PO) 5-10mg in divided doses, per day. Maximum dose 20mg/day
(symptoms should be monitored and medication titrated accordingly)
OR
S: risperidone (PO) 0.5mg 12hourly then increase by 1mg every 2-3days to 2-3mg
12hourly. Maximum dose 16mg/day

Note
• Postictal psychosis remits spontaneously even without treatment but that the use of
effective neuroleptics may shorten the duration.
• Interictal psychosis is treated with antipsychotic drugs. Medications that lower the seizure
threshold should be avoided.
• Atypical antipsychotic medications may have better profiles than typical antipsychotic
medications.
• Medications that lower the seizure threshold should be avoided.
• The doses should be as minimal as possible

Treatment of Depressive symptoms/signs in patients with epilepsy;

Non-pharmacological Treatment
• Psychoeducation to the patient and the family
• Family therapy
• Supportive group therapy
• Occupational therapy

Pharmacological treatment
A: carbamazepine (PO) 200-1000mg, in divided doses, per day (symptoms should be
monitored and medication titrated accordingly)
OR
A: phenobarbitone (PO) 30-200mg, in divided doses, per day (symptoms should be
monitored and medication titrated accordingly)
OR
C: sodium valproate (PO) 500-2000mg in divided doses, per day (symptoms should be
monitored and medication titrated accordingly)
AND
A: amitriptyline 12.5-75mg (PO), nocte (symptoms should be monitored and medication
titrated accordingly)
OR
S: fluoxetine 1 (PO) 0-20mg in divided doses, per day (symptoms should be monitored and
medication titrated accordingly)

Note
• In the treatment of epilepsy-related depression, priority should be given to optimizing
seizure control, since improved psychosocial functioning tends to accompany seizure
remission
• Some anticonvulsant therapies, including sodium valproate, gabapentin, carbamazepine,
and lamotrigine, also have antidepressant effects and may prove effective in treating
depression in patients with epilepsy.
Phenobarbital is known to produce depression.

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Treatment of Mania/hypomania in patients with epilepsy;


Non-Pharmacological Treatment
• Psychoeducation to the patient and the family
• Family therapy
• Supportive group therapy
• Occupational therapy

Pharmacological Treatment
A: carbamazepine (PO) 200-1000mg, in divided doses, per day
OR
A: phenobarbitone (PO) 30-200mg, in divided doses, per day
OR
A: sodium valproate (PO) 500-2000mg in divided doses, per day

Note
Symptoms should be monitored and medication titrated accordingly

23.17. Psychiatric Disorders in Pregnancy


In some women, pregnancy and motherhood increase their vulnerability to psychiatric conditions
such as depression, anxiety disorders, eating disorders,panic disorder, bipolar illness, and
psychoses. These conditions are often underdiagnosed because they are attributed to pregnancy-
related changes in maternal temperament or physiology. In addition, such conditions are often
undertreated because of concerns about potential harmful effects of medication.

23.17.1 Depression
Several risk factors and psychosocial correlates have been identified as contributing to depression
during pregnancy, like;
• Previous history of depression, discontinuation of medication(s) by a woman who has a
history of depression, a previous history of postpartum depression, and a family history of
depression

Several key psychosocial correlates may also contribute to depression during pregnancy: a negative
attitude toward the pregnancy, a lack of social support, maternal stress associated with negative life
events, and a partner or family member who is unhappy about the pregnancy. The relationship
between maternal depression and early childhood problems may be part of a sequence that starts
with depressive symptoms during pregnancy.

Non-pharmacological Treatment
• Psychotherapies
o Cognitive behavioral therapy
o Interpersonal psychotherapy
o Education and support are also important, particularly as pregnancy is a unique
experience for women, some of whom may not know what to expect.

Pharmacological Treatment
A: amitriptyline (PO) 12.5–75 mg 24hourly at night, increase gradually to a maximum of
150 mg daily. {Elderly: Initially 12.5–50 mg. Max. 75mg)
OR
D: citalopram 10-60mg (PO) 24hourly morning or evening and symptoms should be
monitored, and medication to be tapered
OR
S: fluoxetine 20-60mg (PO) 24hourly (morning)

Note
• Full disclosure of both the risk and benefits of various antidepressant medications should
be made to the patient and, if possible, her partner prior to starting any pharmacological
treatment.
• Low doses of antidepressants should be considered when initiating medication.

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12.17.2 Panic Disorder


Some women may experience first-onset panic disorder during pregnancy. Women presenting with
panic attacks for the first time should be screened for thyroid disorder. The correlation between
plasma levels of cortisol in the mother and in the fetus may have implications for the developing fetal
brain.

Non-pharmacological Treatment
• Cognitive behavioral therapy
• Supportive psychotherapy
• Relaxation techniques
• Sleep hygiene
• Dietary counseling

Pharmacological Treatment
Refer panic disorders

Note
• Full disclosure of both the risk and benefits of various antidepressant medications
should be made to the patient and, if possible, her partner prior to starting any
pharmacological treatment.
• Low doses of antidepressants should be considered when initiating medication

12.17.3 Obsessive-Compulsive Disorder


Obsessive-compulsive disorder (OCD) is characterized by thoughts that cannot be controlled
(obsessions) and repetitive behaviors or rituals that cannot be controlled (compulsions) in response
to these thoughts.

Non-pharmacological Treatment
• Cognitive behavioral therapy
• Supportive psychotherapy
• Relaxation techniques
• Sleep hygiene
• Dietary counseling

Pharmacological Treatment
Refer to the specific section above

Note
Treatments for GAD in pregnancy are the same as those in non-pregnant adults.

12.17.4 Bipolar Mood Disorder


Non-pharmacological Treatment
• Cognitive behavioral therapy
• Supportive psychotherapy
• Relaxation techniques
• Sleep hygiene
• Dietary counseling

Pharmacological Treatment
Refer to the specific section above
Note
• Decision whether to use mood stabilizers must be made following an assessment of risks
and benefits.
• Low doses of mood stabilizers should be as low as possible
• Factors to consider include number and severity of previous episodes, level of insight,
family supports, and the wishes of the woman
• Careful monitoring of psychological symptoms throughout the pregnancy is of paramount
importance

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12.17.5 Schizophrenia
Non-pharmacological Treatment
• Cognitive behavioral therapy
• Supportive psychotherapy
• Relaxation techniques
• Sleep hygiene
• Dietary counseling

Pharmacological Treatment
Treat as in the treatment of schizophrenia in non-pregnant woman

Note
• Women with a history of psychosis require close monitoring during pregnancy
• Psychosis during pregnancy can have devastating consequences for both the mother and
her fetus, including failure to obtain proper prenatal care, negative pregnancy outcomes
such as low birth weight and prematurity, and neonaticide or suicide
• Treatment of acute psychosis in pregnancy is mandatory and includes mobilization of
supports, pharmacotherapy, and hospitalization
• Electroconvulsive therapy may be used for psychotic depression

23.18. Autism Spectrum Disorder


DSM-5 Diagnostic criteria
It states that an individual diagnosed with Autism spectrum disorder would have marked difficulties
in terms of communication and engagement with others across multiple social situations. These
difficulties include:
• Difficulties with demonstrating appropriate behaviours in social contexts
• Difficulties associated with non-verbal communications used for social interactions
• Difficulties associated with failure to initiate or adapt to social interactions

In addition, the DSM-5 also requires the individuals to have characteristic repetitive behavioural
patterns, such as
• Repeated stereotypical movements or
• Highly ritualized behavioural patterns. DSM-5 criteria specified that these behaviours must
have started since the early developmental period and has resulted in marked
impairments in terms of functioning.

Non-pharmacological Treatment
For children
• Every pre-school child diagnosed with autism should have an individualised intervention
plan that sets out the goals, type(s), frequency and intensity of intervention, in order to
address particular developmental and educational needs
• An individualised intervention plan should consist of a variety of quality programs and
activities. This includes attendance in comprehensive early intervention programmes,
programmes targeting specific needs and also positive engagement with parents and/or
caregivers
• Alternative-augmentative communication systems may be recommended for pre-school
children with autism because the expanded (spoken or written) communication may
stimulate speech acquisition in non-verbal children and enhance expression in verbal
children.
• Visual strategies are useful interventions for children with autism because they offer
visual support to communication, increase spontaneous imitation and socially
communicative behaviour.
• Social skills programmes depend on the functioning level of the preschool child with
autism and may include:
o Assessment and teaching of social skills interaction in natural settings.
o Provision of structure, visual cues and predictability.
o Making abstract concepts more “concrete”.
o Activities that enable purposeful and appropriate interaction with typically
developing peers.
o Goals focusing on fostering self-appreciation and self-esteem.

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For the parents
• Parents and caregivers should be encouraged to discuss the need for practical emotional
support. This enables
information to be provided, referrals made and support services made available
• Parents and caregivers are recommended to consult appropriate professionals when
considering educational placement for their child with autism

Pharmacological Treatment
A: haloperidol (PO)1.5-3mg 24hourly (medications should be titrated according to
symptoms resolution)
OR
A: methylphenidate (PO) 18- 54 mg 24hourly(medications should be titrated
according to symptoms resolution

23.19. Attention Deficit / Hyperactivity Disorder (ADHD)


DSM-5 Diagnostic criteria
It states that an individual diagnosed with attention-deficit and hyperactivity disorder would have
difficulties in terms of functioning, mainly due to (a) inattention and/or (b) hyperactivity and
impulsivity.

The DSM-5 states that these inattentive and/or hyperactivity and impulsivity symptoms must be
present before the age of 12 years old. In addition, these symptoms must have resulted in impaired
functioning in at least 2 different social situations.
The DSM-5 requires the individual to fulfill at least 6 of the following signs and symptoms of
inattention:
• Failing to pay close attention to details
• Concentration difficulties
• Difficulties with sustaining attention at tasks
• Daydreaming and does not seem to be able to follow normal conversations
• Difficulties with organization of tasks
• Reluctance to participate in tasks that involve much attention
• Frequently loses important objects
• Easily distractible
• Forgetfulness about daily activities.

The DSM-5 also specified that only 5 of the above signs and symptoms of inattention
need to be fulfilled if individuals are 17 years of age and above.

DSM-5 also requires the individual to fulfil at least 6 of the following signs and symptoms of
hyperactivity and
impulsivity:
• Moving about and unable to sit still
• Leaves seat even when required to remain seated
• Climbs or runs about in inappropriate situations
• Always having excessive energy and always on the move
• Chats excessively
• Impulsive and gives answers even before being asked to
• Having difficulties waiting for his/her turn
• Unable to carry out normal conversation due to frequent interruptions

Non-pharmacological Treatment
a) Parent-training/ education programmes
Refer parents to educational programmes to learn about ADHD, its management and coping
strategy.
• For parents, the programme should include individual or group-based parent-training/education
programmes.
• For children and youth with ADHD, the programme should include CBT or social skill training.
• Offer training to the teachers on behavioural interventions in the classroom to help the child to
cope with ADHD

b) Behaviour therapy
• Positive reinforcement of positive behaviour including reward system and praises. The
parents can consider using

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a star chart to promote positive behaviour at home.
• Environmental modifications aim at improving attention e.g. placing the child in the front
row of class,
minimising distractions etc.
• Combination of behaviour therapy and medication is better than medication alone.

23.20. Enuresis
DSM-5 Diagnostic criteria
• Repeated voiding of urine into bed or clothes (whether involuntary or intentional)
• Behavior must be clinically significant as manifested by either a frequency of twice a week
for at least three consecutive months or the presence of clinically significant distress or
impairment in social, academic (occupational), or other important areas of functioning.
• Chronological age is at least 5 years of age (or equivalent developmental level).
• The behavior is not due exclusively to the direct physiological effect of a substance (such
as a diuretic) or a general medical condition (such as diabetes, spina bifida, a seizure
disorder, etc.).

Non-pharmacological Treatment
• Fluid restriction at night especially 1 hour before the desmopressin dose until the next
morning, or at least 8 hours after the dose. If child wakes up during the night, limit the
amount that he or she drinks.
• Star chart: effective in one-third of cases
• Alarm: Child must wake up and urinate.

Pharmacological Treatment
A: amitriptyline (PO) 25mg nocte (medications should be titrated according to symptoms
resolution)
OR
C: imipramine (PO) 100mg nocte (medications should be titrated according to symptoms
resolution)

23.21. Neuroleptic Malignant Syndrome (NMS)


Mostly is caused by the use of high dose of antipsychotics; potent antipsychotics (e.g. haloperidol)
and antipsychotics that are given via the intravenous or intramuscular routes.

Diagnostic Signs and symptoms


• Muscle rigidity • Labile blood pressure
• Fever • Tremor
• Altered consciousness • Incontinence
• Mutism • Leukocytosis
• Dysphagia • Laboratory evidence of muscle
• Diaphoresis injury: increase in creatinine kinase
• Tachycardia levels.

Pharmacological Treatment
A: diazepam10 mg (IV)
OR
C: lorazepam (IM/IV) 2 mg for immediate sedative or hypnotic action. If no response gives a second
dose
OR
C: bromocriptine (PO) 2.5 mg 8hourly
Note
• NMS is a clinical emergency, It needs ICU care
• It is important to stop the antipsychotics immediately
• Supportive measures such as bed rest and controlling the hyperthermia by rapid cooling
with the help of tepid water spray and via direct fluid replacement should be started
immediately
• Consideration of ventilator support or intubation would be necessary if the patient has
severe breathing difficulties

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23.22. Somatic Symptom Disorder


DSM-5 diagnostic criteria
• One or more somatic symptoms that are distressing or result in significant disruption of
daily life.
• Excessive thoughts, feelings, or behaviors related to the somatic symptoms or associated
health concerns as manifested by at least one of the following:
o Disproportionate and persistent thoughts about the seriousness of one’s symptoms.
o Persistently high level of anxiety about health or symptoms.
o Excessive time and energy devoted to these symptoms or health concerns
DSM-5 specified time duration of at least 6 months of the presentations.
Non-pharmacological Treatment
• Regular appointments: Patients diagnosed with somatic symptom disorder should have a
fixed, regular physician whom they can seek help from and be seen on a regular basis.
• Avoid unnecessary investigation but physical examination should be performed if new
complaints arise.
• Offer empathy to the sufferings experienced by the patient.
• Psychotherapy:
o Self-help techniques
o Supportive psychotherapy
o Cognitive behaviour therapy (e.g. challenge cognitive distortions, activity scheduling
to enhance physical activities).
• Increase in social and occupational functioning

Pharmacological Treatment
A: amitriptyline (PO) 25-50mg 24hourly (medications should be titrated according to
symptoms resolution)
OR
C: imipramine (PO) 100mg 24hourly (medications should be titrated according to
symptoms resolution)
OR
S: fluoxetine (PO) 10-20mg 24hourly (medications should be titrated according to
symptoms resolution)

23.24. Conversion Disorder


DSM-5 Diagnostic criteria
• One or more symptoms of altered voluntary motor or sensory function.
• Clinical findings provide evidence of incompatibility between the symptom and recognized
neurological or medical conditions.
• The symptom or deficit is not better explained by another medical or mental disorder.
• The symptom or deficit causes clinically significant distress or impairment in social,
occupational, or other important areas of functioning or warrants medical evaluation

Non-pharmacological Treatment
• Psycho-education
• Cognitive-psychotherapy

Pharmacological Treatment
A: amitriptyline (PO) 25-50mg 24hourly (medications should be titrated according to
symptoms resolution)
OR
C: imipramine100mg (PO) once a day (medications should be titrated according to
symptoms resolution)
OR
S: fluoxetine (PO)10-20mg 24hourly (medications should be titrated according to
symptoms resolution).

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CHAPTER TWENTY-FOUR
NUTRITION DISORDERS
Nutrition disorders can be caused an insufficient intake of food or certain nutrients, or by inability of
the body to absorb and use nutrients, or by over consumption of certain foods.

24.1 Iodine Deficiency Disorders (IDD)


Clinical presentation
• Goitre enlarged thyroid gland from over activity.
• Hypothyroidism - dry skin, weight gain, puffy face, frequent constipation, and lethargy from
under-active thyroid
• Hyperthyroidism - exophthalmia, rapid pulse, and weight loss from over-active thyroid
• Cretinism

Table 24.1: Criteria for Assessing Iodine Deficiency Using Urinary Iodine Concentration.

Micronutrient indicators Urinary iodine concentration


for determining iodine status
in the population
Median urinary iodine (µg/l) Iodine intake Iodine status
Pregnant women
< 150 Insufficient Severe iodine deficiency
150 – 249 Adequate Adequate iodine nutrition
250 – 499 Above requirements May pose slight risk of more than
adequate iodine intake
> 500 Excessive Risk of adverse health
consequences
Lactating womenand children < 2 years

< 100 Insufficient Severe iodine deficiency


> 100 Adequate Adequate iodine nutrition
c
School age children (6 years or older)

<20 Insufficient Severe iodine deficiency


20 – 49 Insufficient Moderate iodine deficiency
50 – 99 Insufficient Mild iodine deficiency
100 – 199 Adequate Adequate iodine nutrition
200 – 299 Above requirement May pose slight risk of more than
adequate iodine intake
> 300 Excessive Risk of adverse health
consequences

Table 24.2: Epidemiologic criteria for assessing iodine nutrition based on median urinary
iodine concentrations in different target groups

MUIC (ug/L)
Population group Insufficient Adequate Above requirement
and excessive
School aged children <100 100-299a > 300a
Adults (women reproductive <100 100-299a > 300a
age)
Pregnant women <150 150-249 > 250
Lactating women <100 > 100
Children < 2 years <100 > 100
a
adjusted based on best available scientific evidence to date
Non Pharmacological Treatment
• Use of iodated salt (strategy for control of iodine deficiency worldwide)
• Use of iodine rich foods like: drinking water (reflecting amount of I2 present in the soil),
Fish, Sea weeds (Sea weeds are rich in iodine but are a rare component of the diet).

560

Pharmacological Treatment
A: iodized oil (PO) 400mg repeated after one to two years
AND
B: potassium iodide solution (PO) 21mg stat

24.2 Vitamin A Deficiency (VAD)


Clinical presentation
• Night blindness or inability to see in the dark
• White foamy patches on the eye (Bitot’s spot) or conjunctival and corneal dryness
• Keratomalacia or wrinkling and cloudiness of cornea
• Corneal ulceration or the cornea becomes soft and bulges

Diagnosis
Common indicators of VAD used for population surveys/assessments
• Clinical eye signs (Exophthalmia)
• Serum Retinol Concentration

Table 24.3 Serum Retinol Concentration


Public Health Importance Serum or plasma retinol: <0.70 µmol/l in preschool-age
children or pregnant women
Mild > 2% - < 10%
Moderate > 10% - < 20%
Severe > 20%

Non-pharmacological Measures
Dietary consumption of vitamin-A rich foods

Pharmacological Treatment
Prophylaxis
A: vitamin A (retinol)(PO) 4-6monthly up to the age of 5years.

Table 24. 4: Administration of Vitamin A


Age range Dose units Frequency Route of Administration

Infants 6–11 months 100,000 IU (30 mg RE) Stat Oral liquid, oil-based
(including HIV +ve) vitamin A3 preparation of retinol
Children 12 months– 200,000 IU (60 mg RE) 4-6 monthly palmitate or retinol
59months (including vitamin A acetate
HIV +ve)

Treatment
For children 6- 59months and children refer to table 24.4
For adults (except women of reproductive age)
A: vitamin A (retinol) (PO) 200,000 IU stat.

In case of Exophthalmia and Measles:


For infants < 6 months’ give
A: vitamin A (retinol)(PO) 50,000IU immediately on diagnosis repeat next day and on day 14
For infants 6-11months
A: vitamin A (retinol)(PO) 100,000IU immediately on diagnosis repeat next day and on day 14
For children 12-59 months
A: vitamin A (retinol)(PO) 200,000IU immediately on diagnosis repeat next day and on day 14
For all adults except women of reproductive age
A: vitamin A (retinol)(PO) 200,000IU immediately on diagnosis repeat next day and on day 14
For exophthalmia or Bitot’s sport for women of reproductive age
A: vitamin A (retinol)(PO) 10,000IU 24hourly for 4weeks

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Note
Children who received a prophylactic dose within the previous month should not receive the
treatment dose of vitamin A.

Referral: All complicated cases

24.3 Vitamin B Deficiencies


24.3.1 Vitamin B1/Thiamine Deficiency (Wernicke Encephalopathy and Beriberi)
Clinical features
• confusion
• short term memory loss
• confusion
• paralysis of one or more of the ocular muscles or ophthalmoplegia
• nystagmus
• ataxia
• peripheral neuropathy
• cardiac failure

Non-pharmacological Treatment
• Lifestyle adjustment including discouraging of alcohol abuse.
• Increase intake of thiamine rich foods

Pharmacological Treatment
For Peripheral neuropathy and cardiac failure
C: thiamine (PO) 100mg 24hourly

24.3.2 Vitamin B3/Nicotinic Acid Deficiency (Pellagra)


Pellagra is a condition associated with nicotinic acid deficiency. It is usually accompanied by other
vitamin deficiencies.

Clinical features
• diarrhea
• dementia
• dermatitis with darkening of sun-exposed skin

Non-pharmacological Measures
• Lifestyle adjustment including discouraging of alcohol abuse.
• Increase intake of vitamin nicotinic acid rich foods

Pharmacological Treatment
For severe deficiency
Children:
C: nicotinamide (PO) 50mg 8hourly for 7days
Adults
C: nicotinamide (PO) 100mg 8hourly for 7days

For mild deficiency


Children
C: nicotinamide (PO) 50mg 24hourly for 7days
Adults
C: nicotinamide (PO) 100mg 24hourly for 7days.

Referral: On failure to respond on above treatment.

24.3.3 Vitamin B6/Pyridoxine Deficiency


Pyridoxine deficiency is related to malnutrition and alcoholism.

Clinical featurestingling sensation


• burning pain or numbness of the feet
• Isoniazid or combination TB therapy

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Non-pharmacological measures
• Increase intake of pyridoxine rich foods.
• Minimize alcohol consumptions

Pharmacological Treatment
For deficiency
Children:
B: pyridoxine (PO) 12.5mg 24hourly for 3weeks.
Adults:
B: pyridoxine (PO) 25 mg 24hourly for 3weeks.

For medicine-induced neuropathy


Children
B: pyridoxine (PO) 50mg 24hourly for 3weeks.
Adults
B: pyridoxine (PO) 200mg 24hourly for 3weeks.
Then followed by:
B: pyridoxine (PO) 25mg daily as maintenance dose (for patients on TB therapy/isoniazid)

Referral
• Failure to respond.
• Children.

24.3.4 Vitamin B12 (Cobalamin) Deficiency


Refer Haematological Disease Conditions chapter

24.4 Malnutrition
Classes of malnutrition are moderate acute malnutrition (MAM) and severe acute malnutrition
(SAM)
MAM is identified by moderate wasting WfH<-2 z-score for children 0–59 months (or for children 6 -
59months MUAC <125mm and ≥115mm)
SAM is defined by severe wasting WfH<-3 z-score for children 0–59 months (or for children 6-
59months, MUAC<155mm) or the presence of bilateral pitting oedema.

Clinical Features
Marasmus Kwashiorkor
• Severe weight loss and wasting • Bilateral pitting oedema, beginning in the
• Ribs prominent lower legs and feet; can become more
• Limbs very thin generalized (trunk, face “moon”, hands,
• Muscle wasting old man’s’ arms).
appearance • Reduced fat and muscle tissue which may
• Extremely emaciated be masked by oedema.
• Frequent infection with minimal • Skin cracked and peeling off.
signs • Fragile skin prone to ulceration and infection.
• Electrolyte imbalance • Pale appearance.
• Alert and irritable • Hair changes: blond (yellow, red, sparse,
dry, thin). Can be pulled out easily and
without pain (atrophy of the hair roots). Bald
patches.
• Frequent infections, e.g. URT, otitis media,
URI
• Frequent association with dehydration which
may be masked by oedema
• Generally apathetic lethargic and miserable
when left alone. Irritable when handled.
• High risk of death

Diagnostic criteria
Infants less than 6 months
• Weight for Length less than <-3SD
• Bilateral pitting oedema of feet

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• Infant is too weak to suck effectively


• The infant does not gain weight or lose more than 10% of the initial weight.

Table 24.5 Summary of medical complications and danger signs


Appetite No appetite or unable to eat
Vomiting Persistent/severe
Temperature Hypothermia (Axillary Temperature <35.5°C, Rectal Temperature
<36.5 °C) High fever (≥38.5 °C)
Respiratory symptoms Cough and fast breathing (as per IMCI guidelines)
and signs Lower chest in-drawing
Anaemia Severe palmar pallor and jaundice
Dehydration Severe dehydration based on recent history of fluid loss (watery
diarrhoea/vomiting) with weight loss
Alertness Extremely weak and lethargic, unconscious, fitting/convulsions
Infections Open skin lesions, extensive infection

Note
• All children with complicated SAM are at risk of complications or death.
• Stabilize before referral.
• Refer urgently.

24.4.1 Management of Severe Acute Malnutrition (SAM)


General guidelines for management of SAM:
Refer to IMAM guidelines

Non Pharmacological Treatment


The therapeutic diet for malnourished children consists of two formulas,
A: F-75 initial phase of treatment
THEN
A: F-100
OR
A: Ready to use Therapeutic Food (RUTF).

Note
• F–100 and Ready Therapeutic food is used when appetite has returned
• For children 6–59 months start with 2hourly feeds (12feeds per day), and gradually
decrease the frequency of feeding and increase the volume of each feed until the patient
is getting 3hourly feeds (8feeds per day)

If the child is conscious and has hypoglycaemia give:


Medicine Child Dose Frequency Duration
C: 10% glucose 50ml bolus stat
solution
OR
C: 10% sucrose
solution
THEN F-75 3ml/kg/Feed Every 3minutes 2hours

11ml/kg/Feed 2hourly 2days

Treatment of dehydration in Severe Malnourished Children: Refer to IMCI guidelines

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Pharmacological Treatment
Table 24.5 vitamin and mineral therapy supplementation in severe acutemalnutrition:
Medicine Paed age Dose Frequency Duration
A: vitamin A (PO) <6mnths 50,000iu 24hourly 2days
6–12mths 100,000iu
1-5yr 200,000iu
AND 24hourly 14days
A: ferrous sulphate (PO) 4-<6kg 6mg Fe

6 - <10kg 12mg
1-3yrs 18mg
3-5yrs 24mg
AND <6kg 2.5mg 24hourly 14days
A: folic acid (PO)
>6kg 5mg
AND ≥2 years 400 mg stat On discharge from
A: albendazole (PO) SC/ direct
admission to OTP

Children with SAM and signs of shock or severe dehydration, and who cannot be rehydrated orally
or by nasogastric tube should be treated with intravenous fluids, either:
A: compound sodium lactate
OR
A: 0.45% saline
AND
A: Dextrose 5%

Table 24.6 Inpatient Therapeutic Feeding Recommendations Phase 1


Phase 1 (Stabilization care) Phase 2 (Transition and Rehabilitation)
Age Group Product and Prescription
• Give Diluted F-100 at 130ml/kg of • Give twice the volume offered during
body weight per day. phase I
Children <6 • Breastfed children should always
Months be offered breast milk before the
therapeutic milk, and always on
demand
• Give F-75 at 130ml/kg of body • Replace F75 with F-100 at 150ml/kg
weight per day until the patient re- of body weight per day.
gains appetite. • Gradually introduce RUTF in small
• Start with 2hourly feeds (12 feeds amounts until the child can consume
Children 6-59
per day), and gradually decrease ¾ Sachet per day
Months
the frequency of feeding and • When accepted, provide RUTF at
increase the volume of each feed 130kcal per kg of body weight per
until the patient is getting 3hourly day
feeds (8 feeds per day)

Note
If the child is able to swallow:
• If breastfed: ask the mother to breastfeed the child, or give expressed breastmilk.
• If not breastfed: give a breastmilk substitute (F-75). Give 30–50mL before the child is
referred.
• If no breastmilk substitute, and IVs available, give 30–50mL of sugar water.
If the child is not able to swallow:
• Insert a nasogastric tube and check the position of the tube.
• Give 50mL of milk or sugar water by nasogastric tube (as above).
If blood sugar <3mmol/L treat with 10% Glucose:
• Nasogastric tube: 10mL/kg.
• Intravenous line: 2mL/kg.

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Table 24.7 Time frame for the inpatient management of severe acute malnutrition in children
Stabilization/Transition* Rehabilitation
Day 1-2 Day 3-7 Week 2-6
1. Treat/prevent hypoglycaemia
2. Treat/prevent hypothermia
3. Treat/prevent dehydration
4. Correct electrolyte imbalance
5. Treat/prevent infection
6. Correct micronutrient deficiencies No iron No iron Give iron
7. Start cautious feeding F-75 F-100 RUTF
8. Achieve catch-up growth
9. Provide sensory stimulation and emotional
support
10. Prepare for discharge and follow-up after
recovery

Note
• In case of shock with lethargy or unconsciousness, intravenous rehydration should begin
immediately, using 15mL/kg/h of one of the recommended fluids.
• Blood transfusion should be done if a child with severe acute malnutrition presenting with
shock does not improve after 1h of intravenous therapy, a blood transfusion (10mL/kg
slowly over at least 3h) or presents with severe anaemia, i.e. Hb <4g/dL or <6g/dL if with
signs of respiratory distress;
• It is important that the child is carefully monitored every 5–10min for signs of over
hydration and signs of congestive heart failure.
• Treat other medical conditions as per Integrated Management of Acute Malnutrition
(IMAM) guideline 2018
• All cases require careful assessment for possible TB or HIV

24.5 Growth Faltering/Failure to Thrive


Children and infants who have either:
• Unsatisfactory weight gain (growth curve flattening or weight loss) on the Road to Health
chart/ booklet.
OR
• Low weight for age, i.e. WHZ < –2 but > –3
Note
• Babies who were premature and are growing parallel to or better than the Z-score line,
should not be classified as having failure to thrive or not growing well.

Table 24.8 Feeding recommendations for all children


Age Frequency (Per Amount of food per Texture Variety
(month) day) serving (in addition (thickness/
to breast milk) consistency)
At 6 start 2 to 3 tablespoons Thick porridge/ Breast milk + Animal
months complementary Start with ‘tastes’ pap foods (local examples) +
foods 2 to 3 meals Legumes (local
plus frequent examples) + Staples
breastfeeds (porridge, other local
From 6 up 2 to 3 meals plus 2 to 3 table spoonful Thick porridge/ examples) + Fruits/
to 9 frequent per feed Increase pap Mashed/ Vegetables (local
months breastfeeds 1 to 2 gradually to half (½) pureed family examples) +
snacks may be 250 ml cup/bowl foods Micronutrient Powder
offered (country specific
From 9 up 3 to 4 meals plus Half (½) 250 ml Finely chopped

566

to 12 breastfeeds 1 to 2 cup/bowl family foods


months snacks may be Finger foods
offered Sliced foods
From 12 3 to 4 meals plus Three-quarters (¾) to Sliced foods,
up to 24 breastfeeds 1 to 2 1 250 ml cup/ bowl Family foods
months snacks may be
offered
From 24- Give 3 family Staples (local examples)
59 Months meals a day. Give Animal foods (local
snacks in examples) Legumes
between meals. (local examples) Fruits
(local examples)
Vegetables (local
examples)
Note: If a Add 1-2 extra Same as above Same as above Same as above, plus 1
baby is not times food and according to age according to age to 2 cups of milk per day
breastfed snacks group group + 2 to 3 cups of extra
fluid especially in hot
climates
Responsive /Active feeding Be patient and actively encourage the baby to eat
Hygiene • Feed the baby using clean cup and spoon, DO NOT use a bottle
as this is difficult to clean and may cause the baby to get diarrhoea
• Wash hands with soap and water before preparing food, before
eating and before feeding young children.

24.6 Obesity and Overweight


Management of Obesity and Overweight
Aim of nutritional management is to:
• Achieve and maintain ideal body weight by bringing about gradual weight loss
• Correct fault food habits
Management
• Control total energy intake based on individual assessment by limiting energy intake from
total fat and simple sugars.
• Put the client on a weight reduction diet regime of 30-25kcal/kg /day.
• High fiber, restricted fat diets based on individual assessment is recommended
• Offer nutrition education and counseling to the clients with emphasis on weight
management, fat diets and other unhealthy practices in weight control
• Recommend suitable exercise program and encourage physical activity for gradual weight
loss
• Recommend support systems for the clients who need behavior modification.

Note
• A maximum reduction of 1000kcal daily is required to lose about 1kg a week and a
reduction. Drastic reduction of calorie intake is however not advisable.
• Diet adjustments should be gradual as such people experience excessive appetite. Use of
appetite suppressants is not recommended

Dietary considerations in the management of obesity and overweight


Proteins
Give slightly higher than normal as it gives a feeling of satiety and helps to maintain a good
nutritional status yet excess is deaminated. Provide approximately 20% of total energy from
proteins. This should include good quality proteins, lean and whole pulses.
Fats
Provide 20% or less of total energy from fats. Emphasize on the use of unsaturated fats to reduce
the risk of heart problems. Restrict or avoid fried foods
Carbohydrates

567


Provide the rest of energy 60% from carbohydrates which should be mainly in complex form;
starches and dietary fiber. Limit simple forms like sugars

Minerals and Vitamins


Provide adequate amount of essential nutrients like minerals and vitamins to maintain a good
nutrition status
Generally, increase intake of the following food:
• Vegetables such as broccoli, mushroom, zucchini, cabbage, lettuce, cucumber
• Fruits such as pineapple, cherimoya, peach, grapefruit
• Tubers such as sweet potatoes
• Low fat milk
• Diuretic foods such as celery, apples, watermelon (diuretic drugs are not
recommended)
24.7 Nutritional Management in TB, HIV and AIDS
• Maintain and improve nutrition status of a person living with HIV/ AIDS thus delay the
progression from HIV to AIDS related diseases.
• Ensure adequate intake of all nutrients thus preventing development of nutritional
deficiencies.
• Preservation of lean body mass.
• Maintain body weight and fitness.
• Improve performance of immune system.
• Replenishment of nutrient losses incurred during infection.
• Minimizing symptoms of malabsorption.
• Regeneration of glycogen stores.
• Maintain laboratory values within normal limits.

Note
Control side effects due to medication and monitor drug – nutrient interaction

Table 24.9: Side Effects related to TB drugs and food intake recommendations to minimize
them.
Drug name Food recommendation Avoid Possible side effects
Rifampicin To be taken 1 hour before or 2 after Alcohol Nausea, vomiting,
food. appetite loss
I hour before antacids
Isoniazid Taken 1 hour before or 2 hours after Alcohol Interferes with
food. Give 10mg B6 daily
Ethambutol May be taken with food Avoid alcohol
Streptomycin Increase fluid intake Taste changes, taste of
food, nausea
Pyrazinamide May be taken with food
Ethionamide Take with or after meals(Supplement Alcohol Abdominal
with Vit B6) discomforts,
nausea
Ofloxacin Take 2hours before or after food Antacids, milk
products
Kanamycin Can be taken without regard to food
Capreomycin Increase fluid and foods intake rich in
in potassium(bananas, avocados)
Para- Take with or immediately after food. Alcohol
aminosalicylic Increase fluid intake
acid(PAS)
Cycloserine Supplement with vitamin B6 Alcohol

568

24.7.1 Nutrient Requirements and Dietary Management in TB, HIV and AIDS
Patients
Energy
Most patients with chronic tuberculosis, HIV and AIDS are malnourished, energy needs are
increased in order to minimize weight loss and achieve a desirable weight. An additional 300- 500
kcal (35 -40 kcal per ideal body weight) is recommended. This will help in protein sparing.

Protein
An intake of 1.2- 1.5 g of protein per kg body weight is required to generate serum albumin levels
per day, due to tissue wasting and repair of worn out tissues.

Fats/ oils
These should provide 25-30% or less of the total energy requirements of an individual.

Vitamins and minerals


The body should be provided with liberal amounts of vitamins and minerals. In TB conversion of
beta carotene to retinol is affected in the intestinal mucosa. The client should be supplemented with
vitamin A (as per the National Vitamin A supplementation schedule) and encouraged to eat vitamin
A rich food. Patients on isoniazid should ideally be supplemented with 10mg of pyridoxine B6 daily
since the drug inhibits its absorption. Additional amounts of vitamin C is recommended in the diet to
facilitate healing of lesions. Other antioxidants (Vit A, C, and E, folic acid, zinc and selenium)
neutralize free radicals and prevent the production of peroxides from lipids.

Water
At least 8 glasses or more of safe drinking water per day
24.8 Dumping Syndrome.
It is a rapid gastric emptying occurs when food especially sugar moves from stomach into small
bowel too quickly.

Nutritional implications
• Loss of nutrients
• Weight loss

Aims of nutrition management


• Provide adequate calories and nutrients to support tissue healing
• Prevent weight loss
• Correct hypoglycaemia in the short term

Dietary Management
After surgery the following should be done:
• All fluids and foods by mouth should be withheld for 3 to 5 days and the patient fed by
nasogastric tube
• Ice chips should be held in mouth or small, infrequent sips of water should be given.
Some people tolerate warm water better than ice chips or cold water
• Low carbohydrates, clear liquids such as soups, or diluted unsweetened fruit juices should
be given and limited to ½ to 1 cup servings, however, at least 6 cups of fluids should be
consumed daily to replace losses resulting from diarrhoea. Carbonated beverages and
milk are not recommended in the initial stages of the diet
• The post-gastrotomy diet then begins with gradual progression to a general diet as
tolerated. Bland foods should be started first, but a more important priority is offering the
patient foods he/she likes and can tolerate. By the 5th to 7th day most patients can
tolerate solid foods
• For persons near desirable body weight about 1.5g to 2g protein should be given (35Kcal
to 45Kcal/kg)

569

• Pectin, a dietary fibre found in fruits and vegetables maybe helpful in treating dumping
syndrome. Pectin delays gastric emptying, slow carbohydrate absorption and reduces
glycemic response, though small dry meals are of more benefit
• Vitamin and mineral supplementation maybe necessary depending on the extent of
surgery and whether the symptoms of dumping syndrome persist
• Generally, liquids are served between meals rather than with meals to slow the passage
of the food mass. Limit simple carbohydrates
• Lie down immediately after eating to help slow the transit of food to the intestines. Clients
who experience reflux should not lie down after eating. Beware that lactose intolerance
may develop and produce discomfort in relation to milk and milk products.

24.9 Dietary Management in Diabetes Mellitus


There are two main types of diabetes mellitus; Type I and Type II
Type I
Usually under 30 years but can present at any age, present acutely, with weight loss and ketonuria:
treated with diet and insulin.
Type II
Usually over 30 years, insidious onset, frequently obese: treated with diet and oral anti-diabetic
agents. 40% will eventually require
insulin treatment.
Dietary control and weight loss plays an important part in the management of diabetes mellitus.
Many Type II diabetics are overweight. Reducing body weight through careful control of energy
intake and physical activity like walking helps to control the symptoms.
General eating guidance when on Insulin:
• In Type I diabetes, when initiating treatment, the starting dose of insulin is 0.5-1.0units
/kg/day. Doses should be given about 30 minutes before meals.
• Ideally a “basal/bolus” regimen should be used where basal (intermediate acting) insulin
is taken at bedtime and 6-8u of soluble insulin (bolus) taken 3 times a day before meals.
This regimen allows more flexibility with meals as the soluble insulin dose can be varied
according to what is to be eaten and can be given at different times.
• Self-monitoring of blood glucose is recommended (range 5-7mmol/litre), and the patient
can be taught to adjust doses appropriately based on results.
• Insulin treatment often leads to weight gain; hence patients need to follow a healthy diet and
it is recommended that patients should not change dietary and medicine regimens
simultaneously.
• Select an insulin schedule best suited to the individual patient’s eating pattern, physical
activity and general lifestyle.
Diabetic Diet
Dietician should calculate dietary requirements for individual patients in order to reduce the
blood sugar to normal and to maintain a constant blood sugar level.
§ 45-50% of energy intake should be in the form of complex carbohydrates than simple sugars
with adequate intake of fibers.
§ Carbohydrates and calories should be taken in equal portions through the day with addition of
snacks between meals.
§ Alcohol is NOT RECOMMENDED in Diabetics as it can induce low blood sugars.
§ Avoid intake of sugar and sugar-containing food/drinks with the exception of patient feels faint
or is ill and cannot eat normally.
§ Encouraged exercise and a snack should be taken before and after playing sport.
§ Encourage take of other balanced group of foods at right proportion as per individual patients’
dosage regimen.
§ Encourage change of life style and regular general body check-up such eyes and oral dental
care

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24.10 Nutrition Care and Support in the Intensive Care


The goal of nutrition management is to preserve lean body mass

Oral Nutrition Supplement


Oral nutritional supplements (ONS) should be used whenever possible to meet patient’s needs,
when dietary counseling and food fortification are not sufficient to increase dietary intake and reach
nutritional goals.

Enteral and Parenteral Nutrition


Where nutritional requirements cannot be met orally or, expected to be impossible >3 days or
expected to be below half of energy requirements for >1 week, enteral nutrition (EN) should be
administered.
This should be assessed on a case-by-case basis and the long-term impact of nutrition deficit
considered.

Parenteral nutrition (PN)


Parenteral nutrition (PN) should be considered when EN is not indicated or unable to reachtargets
over 3-7 days despite use of appropriate management strategies, and calorie and protein delivery is
consistently <50% of prescribed targets.
Supplemental PN should be considered after other measures to improve EN have been attempted
or insertion of a post-pyloric enteral feeding tube is deemed unsafe and calorie and protein intake
remain significantly less than prescribed targets (i.e. <50% over a 3-7day period)

Table 24.10 Oral Nutrition Supplements

Drinks
Name Amount Calorie Protein Indication Contraindications
s
Fresubin 200mls 400kcal 20g • Inadequat • Not suitable for
drink e intake of children <3yrs
2kcal meals • Use with caution in
• Chronic children < 6yrs
wasting • Not suitable in
• Liver patients with
disease galactosemia

Supporta 200mls 300kcal 20g • Oncology • Not suitable for


n drink • Cachexia children <3yrs
• Acute or • Use with caution in
chronic children < 6yrs
respiratory • Not suitable I
conditions patients with
• Immuno galactosemia
compromi
sed
Diben 200mls 300kcal 20g For diabetic patients • Not suitable for children
drink -Hyperglycemia <3yrs
- insulin resistance • Use with caution in
- Impared glucose children < 6yrs
tolerance Not suitable in patients with
galactosemia
Powder formular
Lifegain 30g 120 15g For building and • Not suitable for children
nutrition regaining strength <12yrs
suppleme Note: To be used • Not suitable for patients
nt with caution to with soy or milk protein
(sachet) diabetic patients allergy

Maxvida 30g 122 4 Adults •

571

Groviva 30g Children 2yrs and •


above
Vidavance 30g Diabetic •

Table 24.11 Enteral feeds


Type of Calories Protein Indicatons Contraindications
enteral / 100mls /
feeds 100mls
Supportan 150 kcal 10g • Cancer • Not suitable for children <
• Cachexia 1yrs
• Chronic wasting diseases • Use with caution in
• Immuno-compromised children < 6yrs
• Ventilated patients • Not suitable in patients
• Electrolyte abnormalities with galactosemia
• Fluid restricions

Survimed 133 kcal 6.7g • Malabsorption, • Not suitable for


OPD HN • Pre-operative children <3yrs
preparation of • Use with caution in
patients who are children < 6yrs
undernourished, • Not suitable in
• Patients with proven patients with
inflammatory bowel galactosemia
disease,
• Following total
gastrectomy,
• Haemodialysis,
• Disease related
malnutrition.
• After long term
parenteral nutrition
Diben 105 kcal 4.5g • Impaired glucose tolerance • Not suitable for children
• Insulin resistance <3yrs
• Diabetes mellitus • Use with caution in
• Hyperglycaemia children < 6yrs
• Not suitable in patients
with galactosemia
Fresubin 100kcal 3.8g • Anorexia • Not suitable for children
Original • Convalescence <3yrs
• Low residue tube feed • Use with caution in
• Jejunostomy children < 6yrs
• Not suitable in patients
with galactosemia
Fresubin 100 kcal 3.8g • Long term tube • Not suitable for
Original feeding children <3yrs
Fibre
• Anorexia • Use with caution in
• Convalescence children < 6yrs
• Not suitable in
patients with
galactosemia

572

CHAPTER TWENTY-FIVE
POISONING
Poison is any substance (liquid, solid, gas), that is harmful to the body, when ingested, inhaled,
injected or absorbed through the skin. There is a variability of the clinical presentation and
poisonings vary by nature of poison, victims’ age group, intention, geographic region, and level of
economic development. Poisons can be classified according to whether the chemical is metallic
versus nonmetallic, organic versus inorganic, or acidic versus alkaline.

25.1 Common Poisons


The common poisoning in our setting are:
• Household agents:
o Organophosphate e.g malathion (insecticide)
o Pesticides - nuvan top, rat poison, hydrocarbons e.g kerosene
o Disinfectants and bleach
• Medicines – Acetylsalicylic Acid, Paracetamol, Anticonvulsants (carbamazepine),
Hematinic (Iron and Vitamins),
• Major tranquilizers and herbal products
• Foods-eg Mushroom, infected foods

25.2 General Principles of Management of Poisoning


In managing a patient who has been exposed to toxins holistic approach should be considered.
These include.

Resuscitation and stabilization


• Airway, breathing and circulation should be reassessed and treated accordingly as a
priority. Refer Approach to patient with Emergency conditions chapter.

Note
• A low respiratory rate with decreased oxygen saturations may indicate hypoventilation. A
normal saturation does not exclude hypercarbia or indeed hypoxia in carbon monoxide
poisoning. If in any doubt, arterial blood gases should be measured. Tachypnoea can be
seen with metabolic acidosis (e.g. tricyclics, methanol), anxiety, and stimulant drug
overdose and as an early feature of salicylate poisoning (respiratory alkalosis).
• Supplementary oxygen via facemask should be given to all patients initially, taking
account of pulse oximetry (noting the limitations described above).
• Many drugs exhibit cardiovascular toxicity hypotension and or cardiac arrhythmias in
overdose (e.g. tricyclics, b-blockers, digoxin, lithium). ECG should be recorded,
intravenous access established and initial fluid resuscitation given as appropriate
• General examination may give corroborating evidence of significant ingestions or clues
in unknown overdoses (SSRIs, tricyclics, phenothiazines) have serotonergic or
anticholinergic effects with pupil dilatation, and extrapyramidal movements, whilst opioid
type drugs will cause sedation and pin point pupils.
• Temperature, blood glucose (low in b-blocker, ethanol poisoning)
• Weight is important in identifying a toxic dose against the weight and may guide
treatment, for example in paracetamol overdose.
• Examination for injury (intentional or un-intentional self-harm) suggest appropriate
methods for treatment, or the presence of other substances such as alcohol.
• If clinical condition allows, an assessment of the patient’s mental state should be made.

Use the tabulated Toxidromes to identify toxins and apply the antidotes

573


Table 25.1 Common Toxidromes to help identification of toxins.
Toxidrome Mental status Pupils Vitals Other Examples of toxic
s manifest agents
ations
Sympathomi• Hyper alert, Mydriasis Hyperthermia,• Diaphore• Cocaine,
metic agitation, tachycardia, sis, amphetamines,
hallucination, hypertension, tremors, ephedrine,
paranoia, widened pulse hyperrefle theophylline, caffeine,
Anxiety / pressure xia, phencyclidine (PCP),
Delirium seizures, Lysergic acid (LSD)
Hyperpyr Withdrawal from
exia narcotics,
benzodiazepine,
alcohol, long term
beta-blocker therapy
Cholinergic Confusion, Miosis, Bradycardia, • Salivation Organophosphate and
drowsiness, Hypotension carbamate
• Urinary
Comma, tachypnea, incontine insecticides, nerve
Headache, hypotension, agents, nicotine,
nce
Insomnia, bradypnea physostigmine,
Giddiness, Hypothemia, • Defaecati edrophonium
on
• Gastric
cramping,
hypermoti
lity
Emesis,
Diaphore
sis,
lacrimatio
n, GI
cramps,
bronchoc
onstrictio
n, muscle
fasciculati
ons and
weakness
, seizures
Anticholiner Agitation, Mydriasis Hyperthermia, Dry flush Antihistamines, TCA,
gic hallucinations, tachycardia, skin, dry antiparkinsonism
delirium, coma hypertension, mucous agents, atropine,
tachypnea membran antispasmodics
es,
decrease
d bowel
sounds,
urinary
retention,
myoclonu
s
Hallucinoge Hallucinations, Mydriasis Hyperthermia, Nystagmu Phencyclidine, MDMA,
nic perceptual (usually) tachycardia, s MDEA
distortions, hypertension,
depersonalizati tachypnea
on, agitation
Opioid CNS Miosis Bradypnea, Hyporefle Heroin, morphine,
depression, apnea xia, methadone,
coma pulmonar diphenoxylate
y edema,
needle
marks

574

Sedative- CNS Variable Often normal; Hyporefle Benzodiazepines,


hypnotic depression, hypothermia, xia barbiturates, alcohols,
confusion, bradycardia, zolpidem
stupor, coma hypotension,
bradypnea,
apnea
Serotonin Confusion, Mydriasis Hyperthermi, Tremors, MAOIs, SSRIs,
syndrome agitation, coma tachycardia, myoclonu meperidine,
hypertension, s, dextromethorphan,
tachypnea hyperrefle TCA
xia,
clonus,
diaphores
is,
flushing,
trismus,
rigidity,
diarrhea
Note:PCP, Phencyclidine; LSD Lysergic acid; TCA, tricyclic antidepressant; MDMA, 3,4-methylenedioxymethamphetamine; MDEA,
methylenedioxymethamphetamine; CNS, central nervous system; GI, gastrointestinal; MAOI, monoamine oxidase inhibitor; SSRI, selective
serotonin reuptake inhibitor,

Table 25.2 Toxins causing Dysrhythmias


Heart rate Narrow QRS Wide QRS
Tachycardia Amphetamines Antihistamines
Anticholinergic agents Cocaine
Theophylline Propoxyphene,
Sodium channel blockers and
Tricyclic antidepressants
Bradycardia α-Adrenergic lytic agents β-Adrenergic blocking agents
β-Adrenergic blocking agents, Calcium channel antagonists
Calcium channel antagonists,
Cardiac glycosides,
Class Ia antiarrhythmics
And Sodium channel blockers

Note
• For patients presenting with cardiac problems, consider reading ECG and use the table
below to interpret possible causes;

25.2.1 Management Protocol of a poison (specific and non-specific antidotes)


Investigations
The toxidromes are created to assist diagnosis. History may be inaccurate and hence the following
laboratory tests should usually be obtained for guidance:
• Complete blood count • Urine pregnancy test in all
• Liver function test women of childbearing
age
• Serum lactate
• Arterial blood gas • Basic serum electrolytes,
blood urea nitrogen
• Electrocardiogram (BUN), and creatinine

Sympathomimetics investigations - RBG-bedside, ECG, Serum electrolytes and Renal function test,
Liver function test, Creatinine kinase, Clotting screen: PT/PTT/INR, Full Blood Count, Arterial blood
gas, Serum osmolality and osmolality gap.
Abdominal X-ray may be useful in diagnosing.
Cholinergic investigations - Glucose, BUN, Electrolytes, Prothrombin time, Liver function test,
Cholinesterase measurements

Measurement of drug or toxin concentrations in body fluids is not required in most poisonings, but in
some exposures, it does influence management. The list of drug concentrations that may assist
patient assessment and management are shown here;

575

Table 25.3: List of drugs or toxins requiring measurement of drug concentrations.


Paracetamol Methanol
Carbamazepine Methotrexate
Carbon monoxide Organophosphorus
Digoxin Paraquat
Ethanol Phenobarbital
Ethylene glycol Phenytoin
Iron Salicylate
Lithium Theophylline
Methemoglobin Valproic acid

Table 25.4: Supportive Care


Toxic Feature Methods to reach Immediate Definitive Management
Diagnosis Stabilization
Signs of COPD H&P, CXR O2, NIPPV Bronchodilators, steroids
Pulmonary edema H&P, CXR, pro- O2, NIPPV Nitrates, diuretics
BNP
Pulmonary embolism H&P, d-dimer, O2 Anticoagulation,
chest CT thrombolysis (massive
PE only)
Acute respiratory distress H&P, CXR O2, NIPPV Ventilatory support
syndrome
Myocardial infarction H&P, ECG O2, nitrates, aspirin, Revascularization
anticoagulation (thrombolysis or PCI)
Metabolic acidosis H&P, metabolic O2 Directed at underlying
panel, blood gas cause

Psychosocial Intervention
• The investigations depend on the poison ingested:
• If the toxin cannot be identified, then toxidrome (signs and symptoms) can be used

25.2.2 Management of Ingested Poisons


Ingested toxins are suspected in any patient with signs and symptoms irrespective of reported dose
ingested

Clinical Presentations
• General clinical features: Nausea, vomiting, drowsiness, blurred vision, and dizziness
• Central Nervous System toxicity: Altered level of consciousness, convulsions, acute
confusion and coma,
• Renal Toxicity: Acute kidney injury/failure and papillary necrosis
• Metabolic derangement: Metabolic acidosis, respiratory acidosis, hypoglycemia.
• Allergic reactions: Urticaria, angioedema, anaphylaxis
• Haematological toxicity: Aplastic anaemia, agranulocytosis

Non-pharmacological Treatment
Gastric decontamination - practice of functionally removing an ingested toxin from the
gastrointestinal (GI) tract in order to decrease its absorption it includes gastric evacuation (forced
emesis or gastric lavage), intra-gastric binding (most commonly by single or multidose activated
charcoal), or speeding transit of toxins to decrease total absorption time (whole bowel irrigation or
cathartics).GI decontamination is most likely to benefit patients who present for care soon after
ingestion (usually within one to two hours).
• Gastric Lavage
• General care: Keep the patient under observation 4–24 hours depending on the poison
swallowed.

Contraindications to Gastric Lavage:


• An unprotected airway in an unconscious patient
• Ingestion of corrosives or petroleum products e.g. kerosene
• Bowel obstruction

576

• Bowel perforation
• GI bleeding
• Identify the specific agent and remove or adsorb it as soon as possible.

Note
• Treatment is most effective if given as quickly as possible after the poisoning event, ideally
within 1 hour.
• If the patient has swallowed kerosene, petrol, or petrol-based products (note that most
pesticides are in petrol-based solvents) or if the patient’s mouth and throat have been
burned (for example with bleach, toilet cleaner or battery acid) do not vomit the patient but
give water orally? Never use salt as an emetic as this can be fatal.

Pharmacological Treatment
A: activated charcoal (PO) single dose (if available) within one hour of ingestion and do
not induce vomiting; given by mouth or NG tube according to the dosage below:

Dose: Children below one year: 1g/kg


Children 1-12 years of age: 25–50g
Adolescents and adults: 25–100g
A: compound sodium lactate or 0.9% sodium chloride (IV) 30ml/kg 2liters for 24hours if
Shock is present
Note
Toxins for which multiple doses of activated charcoal are indicated includes Carbamazepine,
Dapsone, Digoxin, Paraquat, Phenobarbitone, Quinine, Slow-release preparations such as
theophylline, Amanita phalloides fungus, Multiple doses may also be considered in life threatening
overdose of other drugs (e.g. tricyclic antidepressants).

Content mixing:
• Mix the charcoal in 8–10 times the amount of water, e.g. 5g in 40 ml of water.
• If possible, give the whole amount at once; if the child has difficulty in tolerating it, the
charcoal dose can be divided.
• If charcoal is not available, then induce vomiting but only if the patient is conscious by
rubbing the back of the patient throat with a spatula or spoon handle;

Referral: Consider transferring patient to next referral level hospital, where this can be done safely,
if the patient is:
• Unconscious or deteriorating • Cyanosed
conscious level • Heart failure
• Burns to mouth and throat
• Severe respiratory distress

25.2.3 Food Poisoning


Food poisoning, also called foodborne illness, is illness caused by eating contaminated food.
Infectious organisms — including bacteria, viruses, and parasites — or their toxins are the most
common causes of food poisoning as listed in the table. Large intestine and small intestine have an
intermediate incubation from about 1 to 3 days.

Large intestine
Infections of the large intestine or colon can cause bloody, mucousy diarrhea associated with
crampy abdominal pain.
• Campylobacter spp, is the common one cause of food-borne disease
• Shigella spp contaminate food and water and cause dysentery (severe diarrhea often
containing mucus and blood).
• Salmonella spp infections often occur because of poorly or undercooked cooked and/or
poor handling of the chicken and eggs. In individuals with weakened immune systems,
including the elderly, the infection can enter the bloodstream and cause potentially life-
threatening infections.
• Vibrio parahaemolyticus can contaminate saltwater shellfish and cause a watery diarrhea.

577

Small Intestine Infection


Diarrhea due to small bowel infection tends not to be bloody, but infections may affect both the small
and large intestine at the same time.
• E. coli (enterotoxigenic) is the most common cause of traveler's diarrhea. It lacks
symptoms such as fever or bloody diarrhea.
• Vibrio cholerae, often from contaminated drinking, water produces a voluminous watery
diarrhea resembling rice-water.
• Viruses such as Norwalk, rotavirus and adenovirus tend to have other symptoms
associated with an infection including fever, chills, headache, and vomiting.
• Botulism is caused by Clostridium botulinum toxin and may present with fever, vomiting,
mild diarrhea, numbness, and weakness leading to paralysis.

Pharmacological Treatment
Adult:
A: 0.9% sodium chloride 30mL every 30minutes; not to exceed 8-10doses
AND
C: loratadine 10mg (PO) 24hourly
Children2 to 5 years:
A: 0.9% sodium chloride 7.5-15mL every 30minutes; not to exceed 8-10doses
AND
C: loratadine 5mg (PO) 24hourly
AND
Antibiotics based on the infection suspected.

25.2.4 Herbal Poisoning


Investigations
• Basic blood count, renal function, liver function, and electrocardiogram
• Heavy metal screening if suspected or if symptoms are non-specific
• Analysis methods exist for some herbal toxins only—Colchicines (HPLC, GCMS), tropane
alkaloids (GCMS, oxalate (GCMS), vinca alkaloids (HPLC), cardioactive steroids
(immunoassay)—check with local laboratory

Table25.5 Organ Toxicities and Toxidromes, and Common Dietary Supplements or Herbal
Medicines that can cause them
Clinical features Xenobiotics
Cardiac Sodium channel effects—Aconitum species (widen QRS, shock)
Digoxin-like effects—Digitalis species, bufo toads
Central nervous Seizures—strychnine, thujone, essential oils (camphor, eucalyptus)
system
Sedation—Valeriana species, kava kava
Dermatological Blistering—cantharidin (Chinese blister beetle)
Hematological Coagulopathies—G-herbs (ginger, garlic, gingko)
Agranulocytosis—anti-mitotic agents (colchicine, podophyllotoxin)
Hepatotoxic Hepatitis—multiple agents, germander commonly reported
Veno-occlusive disease—pyrrolizidine alkaloids
(comfrey, Senecio species, Heliotropium species)

Nephrotoxic Renal failure—Aristolochia species


Hypertension, hyperkalemia—licorice
Anticholinergic Datura metel commonly used in TCM
Hexing herbs (Atropa species, Hyoscyamus species, Mandrago
officinarum) common in Western herbal practice
Sympathomimetic Ephedra species, Citrus aurantium (bitter orange)
Salicylate poisoning Willow bark, checkerberry

578


Non-Pharmacological Treatment
• Ask specifically regarding the use of such products and a matched clinical feature using
the above Toxidrome
• Secure sample for identification
o Actual herbs or product used
o Prescription or packaging
• Good resuscitative, symptomatic, and supportive care
• Instruct patients and family to stop using the product
• Consider outpatient monitoring of renal function, liver function, and blood counts
• Report case to regulating authority
• Report unusual cases to National Poison Control Center

Pharmacological Treatment
Use antidote if appropriate, activated charcoal can be given in an acute overdose of toxic dietary
supplements and herbal medicines if there is adequate airway protection. Give:
A: compound sodium lactate or 0.9% sodium chloride (IV) 30ml/kg 2liters for 24hours if
shock is present

25.2.5 Management of Skin Contamination


• Remove all clothing and personal effects and thoroughly flush all exposed areas with
copious amounts of running water running for:
o 5-minutes for non-irritants or mild irritants
o 15-20 minutes for moderate to severe irritants and chemicals that cause acute
toxicity if absorbed through the skin
o 30 minutes for most corrosives
o 60 minutes for strong alkalis (e.g., sodium, potassium or calcium hydroxide)
• Use non-abrasive soapand water for oily substances
• Attending staff should take care to protect themselves from secondary contamination by
wearing gloves and apron
• Removed clothing and personal effects should be stored safely in a see-through plastic
bag that can be sealed, for later cleansing or disposal.

25.2.6 Management of Eye Contamination


Rinse the eye for with clean running water for 15-20 minutes, taking care that the run-off does not
enter the other eye.
• tetracaine hydrochloride 1-2drops into affected eye will assist irrigation. Evert the eyelids
and ensure that all surfaces are rinsed.
• In the case of an acid or alkali irrigate for 30 minutes and review for possible next 30
minutes
• Where possible, the eye should be thoroughly examined under fluorescein staining for
signs of corneal damage.
• If there is significant conjunctival or corneal damage, the patient should be seen urgently
by an ophthalmologist.
• Refer when further eye evaluation cannot be performed.

25.2.7 Management of Inhaled Poisoning


• Move the patient to the fresh air immediately. Victims to stay away from all toxic fumes and
gases.
• Thoroughly ventilate the involved area
Administer supplemental oxygen if cyanosis or difficulty in breathing
• Mild distress/ hypoxia gives 24–40% oxygen at a flow rate of 2–6 L/min (LPM), (nasal
canula)
• Moderate distress/ hypoxia gives 24–50% oxygen at a variable flow of 6 -10 L/min (Face
mask / Venture mask)
• Severe distress/ hypoxia gives 50–90% oxygen at 10-15L/min (Non-rebreather Mask / face
mask with reservoir bag)
• Apnea give nearly 100% oxygen at 10-15L/min (Bag valve Mask “BVM” device)
Oxygen flow should be moderated to achieve oxygen saturation levels, based on pulse
oximetry (with a target level of 94–96% in most, or 88–92% in people with COPD)

Apply Cardiopulmonary resuscitation (CPR) if there are signs of cardiac arrest

579

Inhalation of irritant gases may cause swelling and upper airway obstruction, bronchospasm and
delayed pneumonitis.
Intubation and provision of for bronchodilators;
A: salbutamol 4mg (PO) 6-8hourly
OR
A: adrenaline B: ephedrine (SC/MI) 25-50mg or (IV) 5-25mg slowly, repeated in 5-10
minutes, if necessary
OR
C: salmeterol (inhalation)
AND
12 years old give,
S: ipratropium bromide (inhalation) 250-500micrograms 6-8hourly daily maximum dose of
2mg.

6 to 12 years give,
S: ipratropium bromide (inhalation) 250micrograms 6-8hourly, maximum daily dose of 1mg

0-5 years give,


S: ipratropium bromide (inhalation) 125-250micrograms 6-8hourly, maximum daily dose
1mg

25.3 Specific poisons


25.3.1 Corrosive Compounds Poisoning
Examples — Sodium hydroxide (Soaps-drain/oven cleaners), potassium hydroxide, acids, bleaches
or disinfectants.

Non-Pharmacological Treatment
• Give 1Litre of water as soon as possible, beneficial within 30minutes.
• Give oxygen therapy at concentrations of 2–6litres per minute (LPM), 40–70% oxygen
(face mask with reservoir bag)

Surgical review
• Arrange for surgical review to check for:
o Esophageal damage/rupture, if severe.
o Perforation, mediastinitis and peritonitis if suspected

Note
Do notinduce vomiting or use activated charcoal

25.3.2 Petroleum Compounds Poisoning


Examples—Kerosene, Turpentine substitutes and petrol

Clinical Presentation:
• GIT-abdominal pain, bloody stool, vomiting
• RS-Throat swelling, pneumonitis and/or pulmonary oedema-cough, tachypnea, cyanosis,
crepitation and rhonchi
• CNS-Headache, dizziness, euphoria, restlessness, ataxia, convulsion, encephalopathy
and coma

Non-pharmacological Treatment
• Remove the patient from source
• Remove contaminated cloth and thoroughly wash the skin with soap and water
• Give supplemental oxygen 2–6litres per minute (LPM), delivering a concentration of 24–
40% oxygen (nasal cannula) or 28–50% oxygen (face mask) 40–70% oxygen (face mask
with reservoir bag)
• Oxygen flow should be moderated to achieve oxygen saturation levels, based on pulse
oximetry (with a target level of 94–96% in most, or 88–92% in people with COPD)
• If large amount of petroleum compound has been ingested less than an hour earlier lavage
may be considered and the patient should be intubated

Note
Do notinduce vomiting or use activated charcoal

580

Kerosene (Paraffin) Poisoning


There is a higher risk of kerosene poisoning among children. The respiratory system is the main
target organ affected. Pneumonia is in most cases interstitial and bilateral. Vomiting after
hydrocarbon ingestion is related to the rate of development of pneumonia; Symptoms of CNS
impairment correlated with hypoxemia, pneumonia, and fever.

Non-pharmacological Treatment
• Immediately remove the child from the source of the poisoning and ensure the airway is
open (this is always the first priority).
• Remove contaminated clothing and thoroughly wash the skin with soap and water.
• If possible, perform pulse oximetry and give supplemental oxygen if indicated. Intubation
and mechanical ventilation may be needed in a patient with severe hypoxia, respiratory
distress or decreased consciousness.
• Avoid gastric lavage because of the risk of inhalation and hence pneumonitis. If very large
amounts of kerosene have been ingested less than an hour earlier then lavage may be
considered if the airway can be protected by expert intubation.

Pharmacological Treatment,
A: compound sodium Lactate OR 0.9% sodium chloride (IV) 30ml/kg 2liters for 24hours if
Shock is present

Note
There is no evidence that corticosteroids are helpful in kerosene poisoning

25.3.3 Organo-Phosphorus and Carbamate Compounds Poisoning


Organophosphates and carbamates are common insecticides that inhibit cholinesterase activity,
causing acute muscarinic manifestations (e.g., salivation, lacrimation, urination, diarrhea, emesis,
bronchorrhea, bronchospasm, bradycardia, miosis) and some nicotinic symptoms, including muscle
fasciculation and weakness.
These can be absorbed through the skin, ingested or inhaled. Examples:
• Organophosphorus – Malathion, Parathion, Tetraethyl Pyrophosphate (TEPP), mevinphos
and
• Carbamates – methiocarb and carbaryl.

Clinical presentations
• Vomiting, diarrhoea, blurred vision or weakness.
• Signs of excess parasympathetic activation: salivation, sweating, lacrimation, slow pulse,
small pupils, convulsions, muscle weakness/twitching, then paralysis and loss of bladder
control, pulmonary oedema, and respiratory depression.

Non-pharmacological Treatment
• Remove poison by irrigating eye or washing skin (if in eye or on skin)
• Give activated charcoal if ingested and within 1 hour of the ingestion.
• Do not induce vomiting because most pesticides are in petrol-based solvents.
• In a serious ingestion where activated charcoal cannot be given, consider careful aspiration
of stomach contents by NG tube (the airway should be protected).
• Auscultate the chest for signs of respiratory secretions and monitor respiratory rate, heart
rate and coma score (if appropriate)
• Give oxygen saturation is less than 90%

Pharmacological Treatment
If there are signs of excess parasympathetic activation (see above) give:
A: atropine (IV) boluses of 5mg
o Repeat every 10minutes until satisfactory atropinization (i.e. no chest signs of
secretions, HR>80b/min, Systolic BP >80mmHg, pupils no longer pinpoint, Dry
axillae)
o Paediatric patient can start at 0.05mg/kg, then double the dose every five minutes,
stop doubling the dose when parameters have improved.
If muscle weakness gives:
S: pralidoxime (IV) (cholinesterase reactivator) 50mg/kg diluted with 15ml water by
infusion over 30 minutes

581

o Repeated once to twice.
o Followed by 10–20 mg/kg/hour, as necessary.

If other organophosphates are identified, the following table can be used:

Table 25.6 List of common Pesticides and Chemical Poisons with their antidotes
Group Poisons Antidote
Agricultural Organophosphates
pesticides
Malathion, Acephate, atropine sulfate
Dichlorvos, Dimethoate, A:2mg (IM) mid-lateral outer thigh
Fenitrothion, Monocrotop
hos, Phorate,
Quinalphos pralidoxime
S:1-2g IV infusion (10-20 mg/mL) over 15-30min,
repeat in 1hr if necessary and repeat 12hourly
thereafter PRN;
administer 30 mg/kg IV (IM, SC if no IV access)
over 20 min; follow by 4-8 mg/kg/hour
maintenance IV infusion
Carbamates; pralidoxime
propoxur, Aldicarb, Carbar S:1-2g (IV) infusion (10-20 mg/mL) over 15-30min,
yl, Carbofuran, repeat in 1 hour if necessary and repeat q12hr
Methomyl thereafter PRN;
administer 30 mg/kg (IV) (IM, SC if no IV access)
over 20 min; follow by 4-8 mg/kg/hour
maintenance (IV) infusion
Organochlorines; cholestyramine
Endosulfan, Gamma S: 4g (PO) 12-24hourly; increase gradually over
benzene hexachloride, 1month intervals
Heptachlor, Chlordane Maintenance: 8-16 g/day (PO) divided 12hourly;
Rodenticides not to exceed 24g/day
Cholestyramine vitamin K
bromadiolone Adults
A:Vitamin K (PO/SC) 2.5-10mg; may be increased
PRN to 25 mg or, rarely, to 50 mg; may be
repeated in 12-48 hours
Newborn
A:Vitamin K (IM) 0.5-1mg within 1hour of birth
D-Penicillamine
Industrial Arsenic B: Give D-penicillamine (PO) 30-40mg/kg/day 1-
chemicals 6months, 2hours before or three hours after
dimercaprol
D:dimercaprol (IM) 3mg/kg deep 4hourly for
48hours followed by 3mg/kg 12hourly for 10days
Ethanol
Methyl alcohol • Loading dose 600 mg/kg (IV) (i.e., 7.6mL/kg of
10% EtOH solution) 600-
700mg/kg oral/nasogastric (NG) using a 95%
solution diluted to 20% or less with water or juice.
• Oral maintenance of 0.15 mL/kg/hour (IV = 1.4
mL/kg/hour
• 10% ethanol.
folic acid/ folinic acid
Ethylene glycol S:folinic acid 60mg (IM) over 12-24 hours stat,
then 15mg (PO) 8hourly for 48 to 72 hours
Ethanol
• Loading dose 600 mg/kg intravenous (IV) (i.e., 7.6
mL/kg of 10% EtOH solution)
• 600-700 mg/kg oral/nasogastric (NG) using a 95%
solution diluted to 20% or less with water or juice
Oral maintenance of 0.15 mL/kg/hour (IV = 1.4

582
mL/kg/hour) 10% ethanol
pyridoxine hydrochloride
B:10-25 mg (PO) 8 hourly then observe in 6 hours
folinic acid
• S: Loading dose 600 mg/kg intravenous (IV) (i.e.,
7.6 mL/kg of 10% EtOH solution)
• 600-700 mg/kg oral/nasogastric (NG) using a 95%
solution diluted to 20% or less with water or juice
S: Oral maintenance of 0.15 mL/kg/hour (IV = 1.4
mL/kg/hour) 10% ethanol
thiamine
C: 100 mg IV; then 50-100 mg/day IM or IV; then
IM: 5-30 mg three times daily (if critically ill); then
5-30 mg three times daily for 1 month
Cyanide

hydroxocobalamin
C: 70 mg/kg (usually 5 g) (IV) infusion over 15
minutes; additional 5 g (IV) may be given
depending on severity of poisoning and clinical
response

Methemoglobinemia methylene blue


producing agents (nitrites, C:1 mg/kg (IV) over 5-30 minutes
nitrates, dapsone, copper, If Methemoglobin level remains >30% or if clinical
aniline, chlorates, symptoms persist, repeat dose up to 1 mg/kg
naphthalene) 1hour after the first dose
Drugs Acetaminophen N-Acetylcysteine
C:140 mg/kg of N-acetyl cysteine at first, followed
by 70mg/kg every 4 hours for 3days or until
acetaminophen is no longer detected in the blood
Iron deferoxamine
D:1g (IM) initially and then 500mg 8hourly for
48hours
Benzodiazepines flumazenil
A:0.2 mg (IV) for 15seconds then 0.1mg for
60second intervals, till consciousness is restored.
Maintain 0.3 and 0.6 mg depending on the
patient's characteristics and the benzodiazepine
used
Opioids naloxone
B:0.4 mg to 2mg (PO) depending on amount of
opioid taken, then repeat in 2 to 3minutes
Isoniazid pyridoxine
B:10-25 mg (PO) 8hourly for 48hours
Digoxin digoxin-specific antibodies
S: Each vial of DigiFab (40 mg of Fab) binds
0.5mg digoxin.
Equimolar dose to ingested digoxin (76/80 mg
FAB = 1 mg digoxin)
Environmen Datura physostigmine
tal toxins S:0.5-2mg slow IVP (not to exceed 1 mg/min);
keep atropine nearby for immediate use
If no response, repeat after 20min PRN
If initial dose effective, may give additional 1-4mg
q30-60min PRN
Snake bites Anti-snake venom
A: Anti–snake venom (ASV)– Polyvalent
For Mild Degree of envenomation give 5 vials (50
ml)
For Moderate Degree of envenomation give 5–10
vials (50–100 ml)

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Fore Severe Degree of envenomation give 10–20
vials (100–200 ml)
Dog bite Anti-rabies Immunoglobulins
A: Anti-rabies human immunoglobulin 20 IU/kg
half the dose given parenterally and the other half
injected into and around the wound for victims
suspected to be infected
Botulism Botulinum antitoxin
S: Administer slowly by (IV) infusion via volumetric
infusion pump; minimize allergic reactions by
starting at 0.5mL/min for initial 30minutes

25.3.4 Paracetamol Poisoning


It is the commonest taken drug overdose. The toxic dose is highly variable. In general, the
recommended maximum daily dose for healthy adults is 4 grams.
Chronic excessive alcohol consumption and Isoniazid can induce CYP2E1, antiepileptics
including carbamazepine, phenytoin, and barbiturates induces CYP enzymes thus increasing the
potential toxicity of Paracetamol.

Clinical Presentation
• Phase-1: 0.5–24 hours after ingestion: asymptomatic, to nonspecific symptoms (anorexia,
nausea, vomiting and malaise). Pallor, diaphoresis
• Phase-2: 18–72 hours after ingestion: Right upper quadrant abdominal pain, anorexia,
nausea and vomiting, Tender right upper quadrant, tachycardia, hypotension and oliguria.
• Phase-3: 72–96 hours after ingestion: all of the above and jaundice, coagulopathy,
hypoglycemia and hepatic encephalopathy, Acute Renal failure.
• Phase-4: 4th day to 3weeks after ingestion: patient who survive critical illness in phase 3,
have complete recovery.

Investigation
• Liver Function Test - Liver transaminases ALT, AST, ALP, Prothrombin Time (PT) with INR
(International Normalization Ratio)
• Serum Glucose
• Renal Function Test: Electrolytes, BUN, Creatinine
• ABG-Arterial Blood Gas

Non-pharmacological Treatment
• Resuscitation
• In adults, the initial treatment for paracetamol overdose is gastrointestinal decontamination.
• Usually there is no immediate threat to the airway, breathing and circulation with
paracetamol poisoning
• Correct hypoglycaemia (Give glucose or sugar or honey)
• If within 1 hour of ingestion of 150mg/kg or more paracetamol give activated charcoal, if
available, or induce vomiting.

Pharmacological Treatment
A: Activated charcoal (PO) (1gm/kg, up to 50gm) if less than 2hours.
If more than 8hours after ingestion, or the patient cannot take oral treatment, give:
AND
C: n-acetylcysteine (IV) 150mg/kg in 200mls of 5% Dextrose over 20 minutes, then
50mg/kg in in 500mls of 5% dextrose over 4 hours, then 100mg/kg in 1 liter of 5% dextrose
over 16 hours.
In severe poisoning a further 100mg/kg may be given over the next 24 hours
Children <20kg
C: n-acetylcysteine (IV)150mg/kg in 3ml/kg of 5% glucose, over 15 minutes, followed by 50
mg/kg in 7 ml/kg of 5% glucose over 4 hours, then 100 mg/kg IV in 14 ml/kg of 5% glucose
over 16 hours.

For conscious and not vomiting or when there is severe reaction to N-acetylcysteine give:
S: methionine (IV) (<6 years: 1 gram every 4 hours - 4 doses; 6 years and above: 2.5
grams every 4 hours for 4 doses).

584

Note
• Syrup of ipecac is contraindicated in inducing vomiting to control paracetamol overdose
because the vomiting it induces delays the effective administration of activated charcoal and
oral acetylcysteine

25.3.5 Acetylsalicylic Acid and other Salicylates Poisoning.


Clinical Presentation
• Initial signs and symptoms
o Tinnitus and impaired hearing, rapid breathing (acidotic-like breathing), vomiting,
dehydration, fever, double vision and feeling faint
• Late signs
o Drowsiness, bizarre behavior
o Unsteady walking and coma

Investigations
• Blood gases • ABG,
• pH and bicarbonates • LFTs,
• Serum electrolytes (Calcium and • Full Blood Picture (Leukocytosis and
Magnesium) thrombocytopenia)
• An ECG to evaluate for • Coagulation studies (PT and PTT)
dysrhythmias

Non-pharmacological Treatment
• Give activated charcoal within one hour of ingestion if available. If charcoal is not available
and a severely toxic dose has been given, then perform gastric lavage or induce vomiting
as above
• Monitor blood glucose every 6 hours and correct as necessary
• Monitor urine pH hourly.

Pharmacological Treatment
C: Fluid resuscitation: If hypokalemia, give
A: compound sodium lactate (IV) 1litre for 24hr if CNS hypoglycemia is seen give bolus of
20 mL 50% Dextrose then 5% Dextrose 1litre for 24hours
AND
C: sodium bicarbonate (IV) 1mmol/kg over 4hours to correct acidosis and to raise the pH
of the urine to above 7.5 so that salicylate excretion is increased.
AND
C: potassium chloride (IV) 8.4mEq/ml, maintain fluids until urine output is 2-3 mL/kg per
hour

Replace fluid losses (Plasma potassium concentration should be corrected before giving sodium
bicarbonate as hypokalaemia may complicate alkalinization of urine) Give;
A: 0.9% sodium chloride (IV) as maintenance requirements
OR
Hemodialysis is required if the concentration exceeds 700mg/liter or in presence of severe metabolic
acidosis

25.3.6 Iron Poisoning


Symptoms appear at doses greater than 20mg/kg. Iron levels above 350–500µg/dL are considered
toxic, and levels over 1000µg/dL indicate severe iron poisoning.Iron pills can look like candy to
children. Intentional overdose can occur among adults, but is rare.

Clinical Presentations
• Nausea, vomiting, abdominal pain and diarrhoea.
• The vomitus and stools are often grey or black.
• In severe poisoning there may be gastrointestinal haemorrhage, hypotension, drowsiness,
convulsions and metabolic acidosis.
• In a child, bloody vomit or stool gastrointestinal features usually appear in the first 6 hours
and a patient who has remained asymptomatic for this time probably does not require
antidote treatment.

585

Non-pharmacological Treatment
• Gastric lavage if potentially toxic amounts of iron were taken.

Pharmacological Treatment
Give antidote
D: deferoxamine (IM) 50mg/kg up to a maximum of 1g by repeated every 12hours; if very
ill, give (IV) infusion 15mg/kg/hour to a maximum of 80mg/kg in 24hours.

25.3.7 Carbon-monoxide Poisoning


Carbon monoxide is a byproduct of burning organic compounds, and may of its exposure occur in
private residences. So its toxicity is usually due to improper use of gasoline portable generators and
indoor use of charcoal for cooking and heating.

Clinical Presentations
• Common presentations includes "flu-like" and commonly include headache, dizziness,
weakness, vomiting, chest pain,
• Dizziness, nausea or vomiting
• Shortness of breath, blurred vision, loss of consciousness
Large exposures can result in loss of consciousness, arrhythmias, seizures, or death

Investigations
• Blood gases and serum electrolytes

Non-pharmacological Treatment
• Give 100% oxygen at 10-15L/min (BVM device) to accelerate removal of 50% carbon
monoxide (note patient can look pink but still be hypoxemic) until signs of hypoxia
disappear.
• Those who are unconscious may require CPR on site.

Table 24.7 Time to remove 50% carboxyhemoglobin.


Oxygen pressure О2 Time
21% oxygen at normal atmospheric pressure (fresh air) 5 hours 20 min
100% oxygen at normal atmospheric pressure (non-rebreather oxygen mask) 1 hours 20 min
100% hyperbaric oxygen (3 atmospheres absolute) 23 in

25.3.8 Opioid Poisoning


Physical and mental symptoms that occur after taking too many opioids, a substance found in
certain prescription pain medication and illegal drugs like heroin. It is caused by complications of
substance abuse, unintentional overdose, Intentional overdose, and Therapeutic drug error any time
from birth (Delivery/ maternal opioid usage) to terminal care. Drugs involved in substance
abuseincludes: Codeine, Diamorphene, Di Hydrocodeine, Fentanyl, Heroin, Loperamide,
Methadone, Morphine, opium, Tramadol (etc.) alone or in combination.

Risk factors for Toxicity


• Drug users • People who had used the drug
• Social disadvantaged earlier for treatment
• Those using alcohol and other
sedatives

Clinical Presentation
• Acute toxicity: drowsiness, nausea and vomiting
• Chronic toxicity: constipation, loss of appetite± nausea and vomiting
• Respiratory depression, tachycardia, hypotension and pin point pupils

Laboratory Investigations
• Full Blood Picture • Renal Function Test (Serum
• Liver Function Test (ALAT and Creatinine and Blood Urea
ASAT) Nitrogen, BUN)
• Creatinine kinase level
• Arterial blood gas determinations

586
• An ECG is recommended in all overdose.
patients with suspected opioid

Non-pharmacological Treatment
• Check the airway
• Intubate the patient who cannot protect their airway
• Give oxygen as described above.

Pharmacological Treatment
Antidote: Hypoventilating patient with spontaneous ventilation Naloxone

Adults & children> 20kg:


B: naloxone (IV) Initial dose 0.5mg titrated upward until Respiratory Rate is ≥12

Children (<20kg): 0.01mg/kg (IV) (Maximum 2mg/dose), increase till hypoventilation resolves

Note
• The starting dose of naloxone is between 0.4 to 1 mg in adults and 0.1 mg/kg in children. In
suspected chronic opiate abusers
• Naloxone must be administered slowly at doses of 0.1 to 0.4 mg IV every 1 to 3 minutes to
ensure a more controlled reversal of the opiate effects. If the naloxone is administered
rapidly in these patients, the patient may also start to feel the pain which was being
suppressed by the opiate.
• If the respiration is shallow, administer 100% oxygen or assisted with bag-valve ventilation
until patient becomes more alert and cooperative.
• The onset of action of naloxone is immediate with a peak response observed within 3 to 8
minutes.
• A repeat dose may be indicated if the patient still shows signs of opiate toxicity

Patients with apnoea:


• Newborn with apnoea secondary to maternal opioid: 0.01mg/kg (IV/IM) (Maximum
0.4mg/kg/dose)
• Children: <20kg 0.1mg/kg (Maximum 2mg/dose) start then repeat doses with continuous
infusion as required.
• Adults and children>20kg Higher dose of naloxone (0.2-1mg and titrate to clinical response

For life threatening Opioid toxicity


• Pediatrics (< 20kg) dosing: 0.1mg/kg/IV (Maximum 2mg/dose). Repeat dose/continuous
infusion as required
• Adults and children (More than 20kg): 2mg IV.
o The dose should be repeated every 3 min until improvement of Respiratory Distress
Syndrome
o If maximal cumulative dose of 10mg is reached and the respiratory insufficiency has
not improvement, consider other pathology

Note
Withdrawal reaction might be life threatening in neonatal period, hence low doses should be given.

Further management of Psychiatric Management of Opioid Toxicity refer Mental Disorders Chapter

25.3.9 Heavy Metal Poisoning


Lead Poisoning
Lead is a heavy metal, ubiquitous in our environment (Lead-based paint and its dust, in older
buildings) that has no physiologic role in biological systems. Lead poisoning occurs when lead builds
up in the body, often over months or years. Lead toxicity is a particularly insidious hazard with the
potential of causing irreversible health effects associated with chronic toxicity.

Clinical Presentation
The clinical presentation varies widely, depending upon the age at exposure, the amount of
exposure, and the duration of exposure
• New born: Be born prematurely, have lower birth weight, slowed growth,

587
• Children: Developmental delay, Learning difficulties, Irritability, Loss of appetite, Weight
loss, Sluggishness and fatigue, Abdominal pain, Vomiting, Constipation, Hearing loss,
Seizures, Eating things, such as paint chips, that aren't food (pica), lower IQ , anxiety,
depression and ADHD Like symptoms
• Adults: High blood pressure, joint and muscle pain, difficulties with memory or
concentration, headache, abdominal pain, mood disorders, reduced sperm count and
abnormal sperm, miscarriage, stillbirth or premature birth in pregnant women, anaemia,
Fanconi’s syndrome, wrist drop

Laboratory Investigations
• Lead blood levels > 10 µg/dL • Renal Function Test (Serum
• Free erythrocyte protoporphyrin Creatinine and Blood Urea Nitrogen,
(FEP) level BUN)
• Erythrocyte protoporphyrin (EP) > • Imaging studies according to
35µg/dL presentation, -chest, bones,
• FBC abdomen etc are ordered as
• Liver Function Test (ALAT and appropriate.
ASAT)

Non-pharmacological Treatment
• Remove the source of lead exposure in the community
• Closely monitor cardiovascular and mental status
• Maintain an adequate urine output.
• Assess renal and hepatic functions.

Pharmacological Treatment
Blood Lead levels are 25–40 µg/dL
D: d-penicillamine (PO) 30-40mg/kg/day 1-6months, 2hours before or three hours after
meals
OR
Blood Lead levels are 45–70 µg/dL Chelate the patient using,
D: 2,3-dimercapto-succinic acid (IM) 10mg/kg by deep 8 hourly for 5 days, followed by
10mg/kg 12hourly for 14 days.

Blood Lead levels of > 70 µg/dL and/or encephalopathy


D: dimercaprol 3mg/kg deep (IM) 4hourly for 48 hours followed by 3mg/kg 12 hourly for 10
days
AND
D: ethylene diamine tetra-acetic acid (CaNa2 EDTA) 10mg/kg (IV) 8hourly for 5 days
(calcium chelate of the disodium salt of ethylene-diamine-tetraacetic acid (EDTA))

Mercury Toxicity
Mercury in any form is poisonous. Poisoning can result from mercury vapour inhalation, mercury
injection and absorption of mercury through the skin. Methylmercury (organic mercury) poisoning is
largely linked to eating seafood, mercury-containing fish.

Clinical Presentation
• Inorganic Mercury:
o Ash-gray mucous membrane, haematochesia, severe abdominal pain, foul breath,
hypovolaemic shock, Metallic taste, stomatitis, gingival irritation loosening of teeth
and Renal tubular necrosis.
• Organic Mercury:
o Visual disturbances, - Eg, scotomata, visual field constriction, ataxia, paresthesias
(early signs), hearing loss, dysarthria, mental deterioration, muscle tremor,
movement disorders, paralysis, and death (with severe exposure).
Laboratory Investigations:
• Blood and Urine Mercury levels • Hair, Toenail, and CSF mercury level
• FBC for chronic exposure
• RFT • Plain X-ray of the abdomen

588
Non-pharmacological Treatment:
• Remove from the exposure, • Do gastric lavage if ingested
• Airway Breathing and Circulation mercury and observed in the
(ABC) abdominal radiographs
• Give oxygen • Do Hemodialysis when renal
• Copious irrigation of the skin if skin function has declined.
involvement

Pharmacological Treatment
Chelation therapy for acute inorganic mercury poisoning can be done with DMSA or
Dimercaprol. Occasionally 2,3-dimercapto-1-propanesulfonic acid (DMPS), D-
penicillamine (DPCN).
A: activated charcoal (PO) as in ingested poisons
OR
D: 2,3-dimercapto succinic acid (PO) (DMSA or succimer) 10 mg/kg 8 hourly for 5 days;
follow by 10 mg/kg/dose 12 hourly for 14 days; not to exceed 500 mg/dose

In acute inorganic mercury poisoning:


D: Dimercaprol:
o Day 1: 5mg/kg deep (IM) stat
o Day 2–11: 2.5mg deep (IM) 12 hourly for 10 days

Surgical intervention: To remove mercury that has been logged in the intestine or colon

25.4 Prevention of Poisoning


Educate the patient on Dos and Don’ts of poisoning prevention.
Do’s
• Keep medicines and poison in • Keep all products in their original
proper containers and out of reach of container
children. • Read medicine labels carefully to
• Use containers with child resistant avoid mistake
caps

Don’ts
• Leave container open • Put tablets into another container
• Transfer products from their origin such as purse or envelope
• Remove labels from the medicine • Medicine/tablets as sweet
products • Take your medicine in front of
children as they often copy
25.5 Alcohol Intoxication
Management of alcohol intoxication see mental health conditions chapter.

25.6 Bites and Stings


The insect that is responsible for the majority of serious sting related reactions belong to the order
hymenoptera. This includes bees, wasps, spiders, scorpions, ants andcentipedes.

Diagnostic Criteria
• Pain, swelling, redness, and itching to the affected area

Non-pharmacological Treatment
• Clean the area with soap and water to remove contaminated particles left behind by some
insects
• Refrain from scratching because this may cause the skin to break down and results to an
infection

Pharmacological Treatment
A: ibuprofen
Adults: 400–800mg (PO) 8hourly for 3days
Children: 10mg/kg 8hourly maximum 400mg per day for 3days
AND
A: prednisolone, 2mg/kg/day (PO) in single daily not to exceed 80mg/day for 5days
Where there is an anaphylactic reaction treat according to guideline.

589
AND
A: chlorpheniramine and be ready if allergic reaction occurs. Dosage as below
o Children under 6years: 4mg 8hourly needed
o 6–12 years: 8mg (PO) 12hours as needed
o >12 years and older 12mg 12hourly needed
OR
C: loratadine (PO) 10mg 24hourly
Usual Pediatric Dose:
2-5years: loratadine (PO) 5mg 24hourly (syrup)
6years or older: Loratadine (PO) 10 mg24hourly (tablets, capsule, and disintegrating
tablets)

25.6.1 Management of Specific Bites/Stings


25.6.1.1 Bee and Wasps Sting
Bee Venom contains many toxins including: Haemolytic enzyme, a neurotoxic factor, histamine and
lytic peptide. Wasp Venom contains Hyaluronidase and 5-hydroxytryptamine.

Prevention of Complications after Bites / Sting


• Move victims to a safe area to avoid more bites or stings.
• If needed, remove the stinger.
• Wash the area with soap and water.
• Apply a cool compression using a cloth dampened with cold water or filled with ice
• Apply 0.5 or 1 percent hydrocortisone cream, calamine lotion or a baking soda paste to the
bite or sting several times daily until your symptoms are alleviated.

Clinical Presentations
• Locally: Itching, pain, erythema, and swelling, cellulites
• Systemic: Oedema, fatigue, nausea, vomiting, fever, unconsciousness, Anaphylaxis,
diarrhea or stool incontinence, dizziness, hypotension, haemolysis, rhabdomyosid,
haemoglobinuria and myoglobinuria

Non-pharmacological Treatment:
• Airway and breathing
• Remove stingers by forceps or scrap with care
• Elevation of the affected limb
• Clean wound

Pharmacological Treatment
A: adrenaline 0.5mg (IV) (0.1Ml) of 1;1000 solution diluted in 10ml of 0.9% sodium chloride
slowly over 30minutes
AND
A: chlorpheniramine (PO) 4mg 4-6 hourly; not to exceed 24 mg/day; 8mg orally 8-12hourly
or 12mg every 12hourly; not to exceed 24mg/day
o Children under 2 years: Safety and efficacy not established
o Children 2-6 years: 1 mg (PO) 4-6hourly; not to exceed 6mg/day
o Children 6-12 years: 2mg (PO) 4-6hourly; not to exceed 12mg/day or sustained
release at bedtime.
o Children over 12 years: 8 mg (PO) 8-12hourly or 12 mg 12hourly; not to exceed
24 mg/day
OR
A: promethazine (PO/Rectal) 6.25 to 12.5 mg orally or rectally before meals and at
bedtime, if necessary,
OR
A: promethazine 25mg orally or rectally 24hourly at bedtime
OR
A: promethazine 25mg (IM or IV) stat, and may be repeated within 2hours if necessary
OR
C: loratadine (PO) 10mg24hourly

590
Pediatric Dose:
2-5years: loratadine (PO) 5mg 24hourly (syrup)
6 years or older: loratadine (PO) 10mg 24hourly (tablets, capsule, and disintegrating
tablets)
AND
A: 0.9% sodium chloride 10–20mls/kg as a bolus
AND
A: paracetamol (PO) 1g for adult or 15mg/kg for children 8hourly for 48hours
OR
D: methylprednisolone (IV) 125mg stat inpatient with respiratory and cardiovascular
compromised.

Note
• Patient with multiple stings: observe for 24hours
• Healthy adults >50stings,
• Children 1 sting

25.6.1.2 Scorpion Sting (Envenoming)


Scorpion stings can be very painful for days. Systemic effects of venom are much more common in
children than adults.

Clinical Presentations
• Local pain and/or paresthesia at the site of envenomation,
• Pain and/or paresthesia remote from the site of sting,
• Autonomic disturbances such as tachy/bradycardia, hyper/hypotension, hypersalivation and
lacrimation, urinary and faecal incontinence and pulmonary oedema.
• Blurred vision, roving eye movement, tongue fasculation, dysphagia, dysphonia, restless,
• Severe involuntary shaking or jerking extremities
• Cardiogenic shock
Deaths from scorpion stings are usually due to cardiogenic shock and pulmonary oedema.

Grading of Envenomation
• Grade I involves local pain and paresthesias at the sting site. The puncture wound may not
be noticeable in this grade.
• Grade II involves local pain and paresthesias existing at the sting site as well as proximal to
the sting site.
• Grade III includes grade 2 classification factors with added cranial nerve (increased oral
secretions, blurry vision, rapid tongue movement, nystagmus), or skeletal neuromuscular
dysfunction (flailing of the extremities and tetanus-like arching of the back) and can also be
accompanied by autonomic dysfunction.
• Grade IV includes both 3 and hyperthermia, up to 104 ⁰F, rhabdomyolysis, pulmonary
edema, and multiple organ failures.

Non-pharmacological Treatment
• Provide adequate airway, ventilation and perfusion
• Calm the patient to lower the heart rate and blood pressure, thus limiting the spread of the
venom
• Give oxygen as above
• Monitor vitals: oxygen saturation, heart rate respiratory rate and blood pressure

Pharmacological Treatment
A: Cleaning of the sting area with Normal saline
AND
A: compound sodium lactate (IV) 2L for 24hours
AND
A: adrenalin (IM) dose of 1:1000 (Repeat after 5 min if no improvement)

591
Children > 12 years and Adults 500 µg (0.5ml)
Children 6-12 years 300 µg (0.3ml)
Children < 6 years 150 µg IM (0.15ml)
Intubation equipment should be made available before the administration of the antivenom in case of
anaphylactic shock
OR
S: equine antivenom (Centruroides Scorpion) for (Grade III or IV envenomations) -
intravenous scorpion-specific F(ab’)2 equine antivenom at a maximum of three vials in 20
to 50 mL of normal saline and infused over 30 minutes.
Initial dose: infuse 1vial of the 3vials over 10minutes, observe for 60minutes If symptoms
persist you may repeat the remaining 2 vials, one vial at a 30minutes interval.
AND
A: paracetamol (PO) or IV 1g for adult or 15mg/kg for children (PO) 8hourly for 48hours
OR
A: ibuprofen
Adults: 400–800mg (PO) 8hourly for 3days
Children: 10mg/kg 8hourly maximum 400mg per day for 8hourly a day
OR
C: morphine (PO) or (IM) according to severity
If very severe, infiltrate site with
A: 1% lignocaine.

25.6.1.3 Snake Bite


A snake bite can be life-threatening if the snake is venomous. Less than 10% of 3500 snake species
are poisonous and they include cobras and mamba’sblack mamba, king cobra, banded krait, saw-
scaled viper and rattlesnake. (Elapidac), sea snakes (hydrophidac) and the boom slang and vine
snakes (columbidac). Clinical ccondition depends on the type of snake bite and amount of poison
(venom) injected.

Hence envenomation (poisoning) are:


• Neurotoxin in cobra, mambas and sea snakes
• Haemotoxic in vipers and boom slang.

Snake bites should be considered in any severe pain or swelling of a limb or in any unexplained
illness presenting with bleeding or abnormal neurological signs. Some cobras spit venom into the
eyes of victims causing pain and inflammation.

Table: 25.8 Various snakebites, their fatal dose, quantity of venom injected, and time to
fatality
LD50 in mine Fatal dose Average Average
Snake for delivered dose fatal period
humans per bite
Indian cobra (Naja naja) 0.28 mg/kg 12 mg 60 mg 8h
Common krait (Bungarus 0.09 mg/kg 6 mg 20 mg 18 h
caeruleus)
Russell's viper (Daboia russelii) 0.1 mg/kg 15 mg 63 mg 3 days
Saw-scaled viper (Echis carinatus) 6.65 mg/kg 8 mg 13–40 mg 41 days

Clinical Presentations
• General signs include pain in the affected area, skin redness, swelling, bleeding, bruise,
• fast heart rate, nausea, or sweating vomiting and headache
• Shock
• Bite for local necrosis, bleeding or tender local lymph node enlargement

592
• Specific signs and level of envomation are shown in the table below depending on the
venom and its effects.

Table 25.9: Assessment of severity of Snake envenomation


Level of Intoxication Presentation
No envenomation Absence of local or systemic reactions; fang marks (+/−)
Mild envenomation Fang marks (+), moderate pain, minimal local edema (0–15 ce), erythema (+),
ecchymosis (+/−), no systemic reactions
Moderate Fang marks (+), severe pain, moderate local edema (15–30 cm), erythema and
envenomation ecchymosis (+), systemic weakness, sweating, syncope, nausea, vomiting,
anemia, or thrombocytopenia
Severe envenomation Fang marks (+), severe pain, severe local edema (>30 cm), erythema and
ecchymosis (+), hypotension, paresthesia, coma, pulmonary edema,
respiratory failure

Additionally, the patient may present with


• These include:
o Shock
o Local swelling that may gradually extend up the bitten limb
o Bleeding: external from gums, wounds or sores; internal especially intracranial
o Signs of neurotoxicity: respiratory arrest or paralysis, ptosis, bulbar palsy (difficulty
swallowing and talking), limb weakness
o Signs of muscle breakdown: muscle pains and black urine

Note
• Avoid picking up the snake or try to wrap it up or kill it, as this will increase your chances of
getting bitten again.
• Avoid applying a tourniquet.
• Avoid cutting into the wound at all.
• Avoid trying to suck out the venom.
• Avoid applying ice or use water to submerge the wound.
• Avoid drinking alcohol.
• Avoid drinking beverages with caffeine.
• Avoid taking any pain-relieving medication, such as ibuprofen

Investigations
Specific investigations
No specific investigations, history is more useful.
• The 20-min whole blood clotting test (20 WBCT)
• Enzyme linked immunosorbent assay (ELISA)

Supportive investigations may include


• Hemogram: Presence of neutrophilic leucocytosis signifies systemic absorption of venom.
Thrombocytopenia may be a feature of viper envenomation.
• Serum creatinine: This is necessary to rule out renal failure after viper and sea snake bite.
• Serum amylase and creatinine phosphokinase (CPK): Elevated levels of these markers
suggests muscle damage (caution for renal damage).
• Prothrombin time (PT) and activated partial thromboplastin time (aPTT): Prolongation may
be present in viper bite.
• Fibrinogen and fibrin degradation products (FDPs): Low fibrinogen with elevated FDP is
present when venom interferes with the clotting mechanism.
• Arterial blood gas and electrolyte determinations: These test are necessary for patients with
systemic symptoms.
• Urine examination: Can reveal hematuria, proteinuria, hemoglobinuria, or myoglobinuria

593
• Electrocardiogram (ECG): Nonspecific ECG changes such as bradycardia and
atrioventricular block with ST-T changes may be seen.
• Electroencephalogram (EEG): Recently, EEG changes have been noted in up to 96% of
patients bitten by snakes.

Non-pharmacological Treatment:
• Reassure the patient;
• Splint the limb to reduce movement and absorption of venom.
• If the bite was likely to have come from a snake with neurotoxin venom,
o Clean the site with clean water to remove any poison and remove any fangs;
• If any of the above signs, transport to hospital which has antivenom as soon as possible.
• Paralysis of respiratory muscles can last for days and requires intubation and mechanical
ventilation or manual ventilation (with a mask or endotracheal tube and bag) by relays of
staff and/or relatives until respiratory function returns.
• Do endotracheal intubation +/- elective tracheotomy.
• Elevate limb if swollen
• Monitor very closely immediately after admission, then hourly for at least 24 hours as
envenoming can develop rapidly.

Pharmacological Treatment
Give
A: Anti-Tetanus prophylaxis
Treat shock, if present.
A: 0.9% sodium chloride (IV) 10–20mls/kg bolus, repeat after 30min if still in shock
Give fluids orally or by NG tube according to daily requirements. Keep a close record of
fluid intake and output fluid daily requirements to be inserted
If there are systemic signs or severe local signs (swelling of more than half of the limb or severe
necrosis), give
A: Anti–snake venom (IV) (ASV)are polyvalent immunoglobulins prepared to control venom
of poisonous snakes) using indications shown below. Follow the directions given on the
antivenom preparation.
o Dilute antivenom in 2–3 volumes of 0.9% Normal saline and give intravenously over 1
hour
o Give more slowly initially and monitor closely for anaphylaxis or other serious adverse
reactions.
For mild degree of envenomation give 5 vials (50 ml)
For moderate degree of envenomation give 5–10 vials (50–100 ml)
Fore severe degree of envenomation gives 10–20 vials (100–200 ml)

594
Table 25.10: Indications for Anti-Snake Venom
System Clinical features
Spontaneous systemic bleeding
Whole blood clotting time >20 min
Thrombocytopenia (platelets <100,000/mm3)
Cardiovascular
Shock
Arrhythmia
Abnormal electrocardiogram

Neurological Ptosis and paralysis


Acute renal failure
Generalized rhabdomyolysis and muscular pains
Renal Hyperkalemia
Local swelling involving more than half of the bitten limb
Rapid extension of swelling
Development of an enlarged lymph node draining the bitten limb

A: adrenaline (IM) dose of 1:1000 (Repeat after 5minutes if no improvement)


o Children > 12 years and Adults 500 µg (0.5ml)
o Children 6-12 years 300 µg (0.3ml)
o Children < 6 years 150 µg IM (0.15ml)
AND
A: chlorpheniramine and be ready if allergic reaction occurs. Dosage as below
o Children under 6years: 4mg 8hourly needed
o 6–12 years: 8mg (PO) 12hours as needed.
o >12 years and older 12mg 12hourly needed

Note
• If itching/urticarial rash, restlessness, fever, cough or difficult breathing develop, then stop
antivenom and give
A: adrenalin 0.01 ml/kg of 1/1000 or 0.1 ml/kg of 1/10,000 solution subcutaneously and IM
or IV/SC Chlorpheniramine 250 micrograms/kg.
• When the patient is stable, re-start antivenom infusion slowly.
• More antivenom should be given after 6 hours if there is recurrence of blood in-coagulability
or after 1–2hour if the patient is continuing to bleed briskly or has deteriorating neurotoxin or
cardiovascular signs.
• Blood transfusion should not be required if antivenom is given.
• Response of abnormal neurological signs to antivenom is more variable and depends on
type of venom.

Surgical Intervention
• Excision of dead tissue from wound
• Incision of facial membranes to relieve pressure in limb compartments, if necessary
• Skin grafting, if extensive necrosis
• Tracheotomy if paralysis of muscles involved in swallowing occurs

595
CONTRIBUTORS
National Medicines and Therapeutic Committee (NMTC) Members
SN Name Membership
1 Prof. Abel Makubi Chief Medical Officer and Chairperson NMTC
2 Pharm. Daudi Msasi Director, Pharmaceutical Services Unit- MoHCDGEC and
Secretary NMTC

3 Dr. John Rwegasha Gastroenterologist, Muhimbili National Hospital (Member)


4 Dr. David Mwenesano Director Medical and Technical Services, National Insurance
Fund, (Member)
5 Dr. Peter Masunga Clinical Microbiologist, Kibong'oto Special Hospital
Mbelele
6 Pharm. Samiri Saitoti Clinical Pharmacologist, University of Dodoma l (Member)
7 Dr. Delfina Mkenda Gynacologist, Mbeya Zonal Referral Hospital(Member)
8 Dr. Deus Buma Clinical Pharmacist, Muhimbili National Hospital (Member)
9 Pharm. Silvester Maige Clinical Pharmacologist, Medical Store Department (Member)
10 Dr. John Meda Cardiologist, Benjamini Mkapa Zonal Referral Hospital
(Member)
11 Dr. Vickfarajael Daudi Pediatrician, Hydom Lutheran Hospital (Member)
12 Pharm. Kauke B. Zimbwe Clinical Pharmacist, Benjamini Mkapa Zonal Referral Hospital
13 Dr. Mark Mseti Oncologist, Ocean Road Cancer Institute(Member )
14 Pharm.Walter Ombeni Clinical Pharmacist, Mirembe Psychatric Hospital ( Member)
15 Dr. Michael Irira Paeditrician, Mawenzi Regional Referral Hospital ( Member)
16 Dr. Azma Simba Epidemiologist, Directorate of Preventive Services-
MoHCDGEC (Member)
17 Dr .Phillipina Philipo District Medical Officer In charge, Bahi DC (Member)
18 Dr. Linda Ezekiel Nephrologist, Directorate of Curative Services, MoHCDGEC
(Co-opted Member)
20 Pharm. Cosmas Mogasa Principal Pharmacist, National Insurance Fund (Co-opted
Member)
21 Pharm. Mary Masanja Principal Pharmacist, Tanzania Medicines and Medical
Devices Authority (Co-opted Member)
22 Pharm. Regina J. Senior Pharmacist, POLARG (Co-opted Member)
Richard
23 Pharm. Ibrahim Mwandu Pharmacist, Pharmacy Council (Co-opted Member)
24 Pharm. Siana G. Principal Pharmacist, Pharmaceutical Services Unit-
Mapunjo MoHCDGEC (Secretariat)
25 Pharm. Noel Mhadu Senior Pharmacist, Pharmaceutical Services Unit-
MoHCDGEC (Secretariat)
26 Pharm. Marco Salingu Senior Pharmacist, Pharmaceutical Services Unit-
MoHCDGEC (Secretariat)
27 Pharm. Emiliana Francis Pharmacist I, Pharmaceutical Services Unit-MoHCDGEC
(Secretariat)
28 Pharm. Aneth Wilbroad Pharmacist I, Pharmaceutical Services Unit-MoHCDGEC
(Secretariat)
29 Pharm. Lucy Mziray Pharmacist I, Directorate Curative Services-MoHCDGEC
(Secretariat)

596
Lead Reviewers
SN Leader Reviewrs Chapters
1 Dr. Patrick Shayo (Emergency Physician) - Muhimbili Emergency and Critical Care
National Hospital
2 Dr. Alex Loth (Anethetics) - Muhimbili National Hospital Anesthesia
3 Dr. Mwashungi Ally (Hematologist) - Temeke Regional Hematological Disease
Referral Hospital Conditions
4 Dr. Rogath Kishimba (Epidemiologist) - MoHCDGEC Notifiable Diseases
5 Dr. Issa Garimo, National Malaria Control Programme Malaria
6 Dr. Aneth Rwebembera, National AIDS Control Programme HIV/AIDS
7 Pharm. Jumanne Mkumbo, TB and Leprosy Programme TB and Leprosy
8 Dr. Raymond Makundi (Neurologist) - Muhimbili National Nervous Disease Conditions
Hospital (Mloganzila)
9 Dr. Jude Tarimo (Pulmonologist) - Muhimbili National Respiratory Disease Conditions
Hospital
10 Dr. Amunga Meda (Gastroenterologist) - Muhimnbili Gastrointestinal Disease
National Hospital Conditions
11 Dr. France Rwegoshora (Gynecologist)-Mbeya Zonal Obstetrics, Gynecology and
Referral Hospital Contraception
12 Dr. Gisenga Lija (Dermatovenereologist) - Kibaha College Sexually Transmitted Infections
of Health and Allied Sciences
13 Dr. Julia Wang'ari (Dermatologists) - Bombo Regional Skin Disease and Allergic
Referral Hospital Reactions
14 Dr. Bernadetha Shilio (Opthalimologist) - Directorate of Eye Disease Conditions
Curative Services, MoHCDGEC
15 Dr. Baraka Nzobo (Dental surgeon) - Morogoro Regional Oral and Dental Conditions
Referral Hospital
16 Dr. Martin Elimath (ENT Specialist) - Muhimbili National Ear, Nose and Throat Diseases
Hospital
17 Dr. Bryceson Kiwelu (Orthopedic Surgeon) - Tumbi Musculorskeletal Disorders
Regional Referral Hospital
18 Dr. Deogratius Banuba (Orthopedic Surgeon) - Singida Trauma and Injuries
Regional Referral Hospital
19 Prof. Andrew Swai (Endocrinologist) - Tanzania Diabetes Metabolic and Endocrine
Association Disease Conditions
20 Dr. Engerasiya Kifai (Cardiologist) - Jakaya Kikwete Heart Cardiovascular Disease
Institute Conditions
21 Dr. Kajiru Kilonzo (Nephrologist) - Kilimanjaro Christian Kidney and Urological Disorders
Medical Centre
22 Dr. Jerry Ndumbalo (Oncologist) - Ocean Road Cancer Malignant Disease Conditions
Institute
23 Dr. Enock Changarawe (Psychiatrist) - Mirembe Psychiatric Mental Health Conditions
Hospital
24 Mrs. Elizabeth Lyimo (Nutritionist) - Tanzania Food and Nutrition Disorders
Nutrition Centre
25 Dr. Benard Mbwele (Epidermiologist) - UDSM Mbeya Poisoning
collage of Health and Allied Sciences
26 Prof. Jeremiah Seni (Microbiologist) - Catholic University of UTI (Section)
Health and Allied Sciences

597
Other Contributors
SN Name Background Institution
1 Dr. Sirili Harya Neural Surgeon Muhimbili National Hospital

2 Dr. Francis Fredrick Furia Nephrologist Muhimbili National Hospital

3 Dr. Lugano Wilson Anesthetics Muhimbili National Hospital

4 Dr. Emmanuel Balandya Hematologist Muhimbili National Hospital

5 Dr. Jackson Ilangali Publi Health Specialist MTaPs - MSH

6 Mr. Machumu Miyeye Pharmacist RCHS Programme,


MoHCDGEC
7 Ms. Fiona Chilunda Advisor Health System Strengthening
Project - Dodoma

598

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