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Discovery of (R)-1-(3-(4-Amino-3-(3-chloro-4-(pyridin-2-ylmethoxy)phenyl)-1H-pyrazolo [3,4-d]pyrimidin-1-yl)piperidin-1-yl)prop-2-en-1-one (CHMFL-EGFR-202) as a Novel Irreversible EGFR Mutant Kinase Inhibitor with a Distinct Binding Mode

Wang Aoli; Li Xixiang; Wu Hong; Zou Fengming; Yan Xiao-E; Chen Cheng; Hu Chen; Yu Kailin; Wang Wenchao; Zhao Peng; Wu Jiaxin; Qi Ziping; Wang Wei; Wang Beilei; Wang Li; Ren Tao; Zhang Shanchun; Yun Cai-Hong*; Liu Jing*; Liu Qingsong*
SCIE
中国科学技术大学

摘要

On the basis of Ibrutinib's core pharmacophore, which was moderately active to EGFR T790M mutant, we discovered novel epidermal growth factor receptor (EGFR) inhibitor compound 19 (CHMFL-EGFR-202), which potently inhibited EGFR primary mutants (L858R, del19) and drug-resistant mutant L858R/T790M. Compound 19 displayed a good selectivity profile among 468 kinases/mutants tested in the KINOMEscan assay (S score (1) = 0.02). In particular, it did not exhibit apparent activities against INSR and IGF1R kinases. The X-ray crystal structure revealed that this class of inhibitors formed a covalent bond with Cys797 in a distinct "DFG-in-C-helix-out" inactive EGFR conformation. Compound 19 displayed strong antiproliferative effects against EGFR mutant-driven nonsmall cell lung cancer (NSCLC) cell lines such as H1975, PC9, HCC827, and H3255 but not the wild-type EGFR expressing cells. In the H1975 and PC9 cell-inoculated xenograft mouse models, compound 19 exhibited dose-dependent tumor growth suppression efficacy without obvious toxicity. Compound 19 might be a potential drug candidate for EGFR mutant-driven NSCLC.

关键词

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出版信息

论文状态
公开发表
期刊名称
Journal of Medicinal Chemistry
发表日期
2017-4-13
卷
60
期
7
页码
2944-2962
DOI
10.1021/acs.jmedchem.6b01907

学科领域

临床医学兽医学

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