Discovery of a selective c-MET inhibitor with a novel binding mode

被引:6
|
作者
Collie, Gavin W. [1 ]
Barlind, Louise [2 ]
Bazzaz, Sana [3 ]
Borjesson, Ulf [2 ]
Dale, Ian L. [1 ]
Disch, Jeremy S. [3 ]
Habeshian, Sevan [3 ]
Jetson, Rachael [3 ,5 ]
Khurana, Puneet [1 ]
Madin, Andrew [1 ]
Michaelides, Iacovos N. [1 ]
Peng, Ling [4 ]
Snijder, Arjan [2 ]
Stubbs, Christopher J. [1 ]
机构
[1] AstraZeneca, R&D, Discovery Sci, Cambridge, England
[2] AstraZeneca, R&D, Discovery Sci, Gothenburg, Sweden
[3] X Chem Inc, Waltham, MA 02453 USA
[4] Pharmaron Beijing Co Ltd, 6 Taihe Rd BDA, Beijing 100176, Peoples R China
[5] Valo Hlth, Discovery Sci, R&D, Boston, MA USA
关键词
Kinase; Small molecule inhibitor; Drug-resistance; DNA-encoded chemical library; c-MET; ACQUIRED-RESISTANCE; CRIZOTINIB; MUTATION; NSCLC;
D O I
10.1016/j.bmcl.2022.128948
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
The c-MET receptor tyrosine kinase has received considerable attention as a cancer drug target yet there remains a need for inhibitors which are selective for c-MET and able to target emerging drug-resistant mutants. We report here the discovery, by screening a DNA-encoded chemical library, of a highly selective c-MET inhibitor which was shown by X-ray crystallography to bind to the kinase in an unprecedented manner. These results represent a novel mode of inhibiting c-MET with a small molecule and may provide a route to targeting drug-resistant forms of the kinase whilst avoiding potential toxicity issues associated with broad kinome inhibition.
引用
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页数:4
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