Abstract
The prosurvival BCL-2 family protein BCL-XL is often overexpressed in solid tumors and renders malignant tumor cells resistant to anticancer therapeutics. Enhancing apoptotic responses by inhibiting BCL-XL will most likely have widespread utility in cancer treatment and, instead of inhibiting multiple prosurvival BCL-2 family members, a BCL-XL–selective inhibitor would be expected to minimize the toxicity to normal tissues. We describe the use of a high-throughput screen to discover a new series of small molecules targeting BCL-XL and their structure-guided development by medicinal chemistry. The optimized compound, WEHI-539 (7), has high affinity (subnanomolar) and selectivity for BCL-XL and potently kills cells by selectively antagonizing its prosurvival activity. WEHI-539 will be an invaluable tool for distinguishing the roles of BCL-XL from those of its prosurvival relatives, both in normal cells and notably in malignant tumor cells, many of which may prove to rely upon BCL-XL for their sustained growth.
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Acknowledgements
The authors thank J. Blyth, D. Buczek, A. Georgiou, H. Ierino, C. Rye, G. Siciliano, G. Thompson and A. Wardak for outstanding technical assistance; S. Cory (Walter and Eliza Hall Institute of Medical Research (WEHI)), L. Chen (WEHI), V. Dixit (Genentech (GNE)), M. Hijnen (GE Healthcare), S. Hymowitz (GNE), D. Segal (WEHI), V. Tsui (GNE), M.F. van Delft (WEHI), A.H. Wei (WEHI) and I. Wertz (GNE) for discussions and suggestions; P. Bouillet and A. Strasser (both from WEHI) for mice; W.D. Fairlie and E. Lee (both from WEHI) for expression constructs; W. Welch (University of California–San Francisco) for anti-HSP70; P. Pilling, V. Streltsov (both from Commonwealth Scientific and Industrial Research Organisation, Australia) and staff at the photon Factory BL6 for their help with collecting data for 2; and AbbVie for providing ABT-737. This work was supported by fellowships and grants from the Australian Research Council (fellowship to P.E.C.), the National Health and Medical Research Council (NHMRC) (fellowships to J.M.A., J.B.B., P.M.C. and D.C.S.H.; development grant 305536 and program grants 257502, 461221 and 1016701), the Leukemia and Lymphoma Society (specialized center of research grant nos. 7015 and 7413), the Cancer Council of Victoria (fellowship to P.M.C.; grant-in-aid 461239) and the Australian Cancer Research Foundation. Infrastructure support from the NHMRC Independent Research Institutes Infrastructure Support Scheme grant no. 361646 and a Victorian State Government OIS grant are gratefully acknowledged.
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G.L. devised synthetic strategies, synthesized compounds, supervised the chemistry team and wrote the manuscript. P.E.C. performed X-ray crystallization and solved and analyzed structures. B.E.S., K.Z., W.J.A.K., S.K. and K.D. designed and synthesized compounds. J.M.A. conceived the study and analyzed data and results. J.B.B., K.D., J.A.F. and K.G.W. designed synthetic strategies and oversaw chemistry efforts. P.M.C. conceived the study and designed and oversaw structural studies. K.N.L. performed biological experiments. P.G. and B.J.S. performed computational modeling. W.J.F. and J.A.F. designed studies and data analysis. R.M.M., J.P.P. and I.P.S. performed the high-throughput chemical screening campaign. H.Y. performed Biacore experiments. D.C.S.H. conceived the study, designed and oversaw biological experiments and wrote the manuscript.
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G.L., P.E.C., B.E.S., K.N.L., J.M.A., J.B.B., P.M.C., W.J.A.K., S.K., R.M.M., J.P.P., B.J.S., I.P.S., H.Y., D.C.S.H. and K.G.W. are or were employees of WEHI, which received commercial income and research funding from Genentech, Inc. for part of this work. W.J.F., J.A.F., K.D., P.G. and K.Z. are employees of Genentech, Inc., a member of the Roche group, and are stockholders of Roche Holding.
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Lessene, G., Czabotar, P., Sleebs, B. et al. Structure-guided design of a selective BCL-XL inhibitor. Nat Chem Biol 9, 390–397 (2013). https://doi.org/10.1038/nchembio.1246
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DOI: https://doi.org/10.1038/nchembio.1246
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