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Publication
Featured researches published by Xilu Wang.
Journal of Medicinal Chemistry | 2008
Cheol-Min Park; Milan Bruncko; Jessica Adickes; Joy Bauch; Hong Ding; Aaron R. Kunzer; Kennan Marsh; Paul Nimmer; Alexander R. Shoemaker; Xiaohong Song; Stephen K. Tahir; Christin Tse; Xilu Wang; Michael D. Wendt; Xiufen Yang; Haichao Zhang; Stephen W. Fesik; Saul H. Rosenberg; Steven W. Elmore
Overexpression of prosurvival proteins such as Bcl-2 and Bcl-X L has been correlated with tumorigenesis and resistance to chemotherapy, and thus, the development of antagonists of these proteins may provide a novel means for the treatment of cancer. We recently described the discovery of 1 (ABT-737), which binds Bcl-2, Bcl-X L, and Bcl-w with high affinity, shows robust antitumor activity in murine tumor xenograft models, but is not orally bioavailable. Herein, we report that targeted modifications at three key positions of 1 resulted in a 20-fold improvement in the pharmacokinetic/pharmacodynamic relationship (PK/PD) between oral exposure (AUC) and in vitro efficacy in human tumor cell lines (EC 50). The resulting compound, 2 (ABT-263), is orally efficacious in an established xenograft model of human small cell lung cancer, inducing complete tumor regressions in all animals. Compound 2 is currently in multiple phase 1 clinical trials in patients with small cell lung cancer and hematological malignancies.
Chemical Biology & Drug Design | 2007
Jeffrey R. Huth; Chang Park; Andrew M. Petros; Aaron R. Kunzer; Michael D. Wendt; Xilu Wang; Christopher L. Lynch; Jamey Mack; Kerry M. Swift; Russell A. Judge; Jun Chen; Paul L. Richardson; Sha Jin; Stephen K. Tahir; Edward D. Matayoshi; Sarah A. Dorwin; Uri S. Ladror; Jean M. Severin; Karl A. Walter; Diane Bartley; Stephen W. Fesik; Steven W. Elmore; Philip J. Hajduk
The molecular chaperone HSP90 has been shown to facilitate cancer cell survival by stabilizing key proteins responsible for a malignant phenotype. We report here the results of parallel fragment‐based drug design approaches in the design of novel HSP90 inhibitors. Initial aminopyrimidine leads were elaborated using high‐throughput organic synthesis to yield nanomolar inhibitors of the enzyme. Second site leads were also identified which bound to HSP90 in two distinct conformations, an ‘open’ and ‘closed’ form. Intriguingly, linked fragment approaches targeting both of these conformations were successful in producing novel, micromolar inhibitors. Overall, this study shows that, with only a few fragment hits, multiple lead series can be generated for HSP90 due to the inherent flexibility of the active site. Thus, ample opportunities exist to use these lead series in the development of clinically useful HSP90 inhibitors for the treatment of cancers.
ACS Medicinal Chemistry Letters | 2014
Zhi-Fu Tao; Lisa A. Hasvold; Le Wang; Xilu Wang; Andrew M. Petros; Chang H. Park; Erwin R. Boghaert; Nathaniel D. Catron; Jun Chen; Peter M. Colman; Peter E. Czabotar; Kurt Deshayes; Wayne J. Fairbrother; John A. Flygare; Sarah G. Hymowitz; Sha Jin; Russell A. Judge; Michael F. T. Koehler; Peter Kovar; Guillaume Lessene; Michael J. Mitten; Chudi Ndubaku; Paul Nimmer; Hans E. Purkey; Anatol Oleksijew; Darren C. Phillips; Brad E. Sleebs; Brian J. Smith; Morey L. Smith; Stephen K. Tahir
A-1155463, a highly potent and selective BCL-XL inhibitor, was discovered through nuclear magnetic resonance (NMR) fragment screening and structure-based design. This compound is substantially more potent against BCL-XL-dependent cell lines relative to our recently reported inhibitor, WEHI-539, while possessing none of its inherent pharmaceutical liabilities. A-1155463 caused a mechanism-based and reversible thrombocytopenia in mice and inhibited H146 small cell lung cancer xenograft tumor growth in vivo following multiple doses. A-1155463 thus represents an excellent tool molecule for studying BCL-XL biology as well as a productive lead structure for further optimization.
Journal of Medicinal Chemistry | 2015
Milan Bruncko; Le Wang; George S. Sheppard; Darren C. Phillips; Stephen K. Tahir; John Xue; Scott A. Erickson; Steve D. Fidanze; Elizabeth E. Fry; Lisa A. Hasvold; Gary J. Jenkins; Sha Jin; Russell A. Judge; Peter Kovar; David J. Madar; Paul Nimmer; Chang Park; Andrew M. Petros; Saul H. Rosenberg; Morey L. Smith; Xiaohong Song; Chaohong Sun; Zhi-Fu Tao; Xilu Wang; Yu Xiao; Haichao Zhang; Chris Tse; Joel D. Leverson; Steve W. Elmore; Andrew J. Souers
Myeloid cell leukemia 1 (MCL-1) is a BCL-2 family protein that has been implicated in the progression and survival of multiple tumor types. Herein we report a series of MCL-1 inhibitors that emanated from a high throughput screening (HTS) hit and progressed via iterative cycles of structure-guided design. Advanced compounds from this series exhibited subnanomolar affinity for MCL-1 and excellent selectivity over other BCL-2 family proteins as well as multiple kinases and GPCRs. In a MCL-1 dependent human tumor cell line, administration of compound 30b rapidly induced caspase activation with associated loss in cell viability. The small molecules described herein thus comprise effective tools for studying MCL-1 biology.
Bioorganic & Medicinal Chemistry Letters | 2010
Andrew M. Petros; Jeffrey R. Huth; Thorsten Oost; Cheol-Min Park; H. Ding; Xilu Wang; Haichao Zhang; Paul Nimmer; Renaldo Mendoza; Chaohong Sun; Jamey Mack; Karl A. Walter; Sarah A. Dorwin; Emily Gramling; Uri S. Ladror; Saul H. Rosenberg; Steven W. Elmore; Stephen W. Fesik; Philip J. Hajduk
The Bcl-2 family of proteins plays a major role in the regulation of apoptosis, or programmed cell death. Overexpression of the anti-apoptotic members of this family (Bcl-2, Bcl-x(L), and Mcl-1) can render cancer cells resistant to chemotherapeutic agents and therefore these proteins are important targets for the development of new anti-cancer agents. Here we describe the discovery of a potent, highly selective, Bcl-2 inhibitor using SAR by NMR and structure-based drug design which could serve as a starting point for the development of a Bcl-2 selective anti-cancer agent. Such an agent would potentially overcome the Bcl-x(L) mediated thrombocytopenia observed with ABT-263.
Journal of Medicinal Chemistry | 2007
Milan Bruncko; Thorsten Oost; Barbara A. Belli; Hong Ding; Mary K. Joseph; Aaron R. Kunzer; Darlene Martineau; William J. McClellan; Michael J. Mitten; Shi-Chung Ng; Paul Nimmer; Tilman Oltersdorf; Cheol-Min Park; Andrew M. Petros; Alexander R. Shoemaker; Xiaohong Song; Xilu Wang; Michael D. Wendt; Haichao Zhang; Stephen W. Fesik; Saul H. Rosenberg; Steven W. Elmore
Journal of Medicinal Chemistry | 2006
Andrew M. Petros; Jurgen Dinges; David J. Augeri; Steven A. Baumeister; David A. Betebenner; Mark G. Bures; Steven W. Elmore; Philip J. Hajduk; Mary K. Joseph; Shelley K. Landis; David G. Nettesheim; Saul H. Rosenberg; Wang Shen; Sheela A. Thomas; Xilu Wang; Irini Zanze; Haichao Zhang; Stephen W. Fesik
Archive | 2004
David J. Augeri; Steven A. Baumeister; Milan Bruncko; Daniel A. Dickman; H. Ding; Jurgen Dinges; Stephen W. Fesik; Philip J. Hajduk; Aaron R. Kunzer; William J. McClellan; David D. Nettesheim; Thorsten Oost; Andrew M. Petros; Saul H. Rosenberg; Wang Shen; Sheela A. Thomas; Xilu Wang; Michael D. Wendt
Archive | 2010
Milan Bruncko; Hong Ding; George Doherty; Steven W. Elmore; Lisa A. Hasvold; Laura Hexamer; Aaron R. Kunzer; Xiaohong Song; Andrew J. Souers; Gerard M. Sullivan; Zhi-Fu Tao; Gary T. Wang; Le Wang; Xilu Wang; Michael D. Wendt; Robert A. Mantei; Todd M. Hansen
Archive | 2008
Xilu Wang; Xiaohong Song; Steven W. Elmore; Milan Bruncko; David J. Madar; Andrew J. Souers; Lisa A. Hasvold; Le Wang; Zhi-Fu Tao; Aaron R. Kunzer
