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Discovery of novel selective inhibitors for EGFR-T790M/L858R
Authors:Bai Fang  Liu Hongyan  Tong Linjiang  Zhou Wei  Liu Li  Zhao Zhenjiang  Liu Xiaofeng  Jiang Hualiang  Wang Xicheng  Xie Hua  Li Honglin
Affiliation:Faculty of Chemical, Environmental and Biological Science and Technology, Dalian University of Technology, Dalian 116023, China.
Abstract:Through a receptor-based and ligand-based combined virtual screening protocol, 21 novel compounds covering 15 scaffolds were identified as novel inhibitors for EGFR-T790M/L858R, among which, 12 of them were identified as selective inhibitors for EGFR-T790M/L858R to wild-type EGFR, and 5 of them exhibited 'dual-effective' to wild-type and mutant EGFR. Meanwhile, their antiproliferative effects toward EGFR high-expressing human lung cancer cell (A549), epidermoid carcinoma cell (A431), and the mutant EGFR-dependent cell (NCI-H1975) were also evaluated.
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