发现选择性 EGFR 调节剂，以抑制具有 N-9-二苯基-9H-嘌呤-2-胺骨架的 L858R/T790M 双突变体。

Discovery of selective EGFR modulator to inhibit L858R/T790M double mutants bearing a N-9-Diphenyl-9H-purin-2-amine scaffold.

机构信息

Key Laboratory of Structure-Based Drug Design and Discovery (Shenyang Pharmaceutical University), Ministry of Education, 103 Wenhua Road, Shenhe District, Shenyang 110016, PR China.

出版信息

Bioorg Med Chem. 2018 May 1;26(8):1810-1822. doi: 10.1016/j.bmc.2018.02.029. Epub 2018 Feb 17.

DOI:10.1016/j.bmc.2018.02.029

PMID:29486953

Abstract

Based upon the modeling binding mode of marketed AZD9291 with T790M, a series of N-9-Diphenyl-9H-purin-2-amine derivatives were designed and synthesized with the purpose to overcome the drug resistance resulted from T790M/L858R double mutations. The most potent compound 23a showed excellent enzyme inhibitory activities and selectivity with nanomolar IC values for both the single T790M and double T790M/L858R mutant EGFRs, and was more than 8-fold selective for wild type EGFR. Compound 23a displayed strong antiproliferative activity against the H1975 non-small cell lung cancer (NSCLC) cells bearing T790M/L858R. And it was less potent against A549 (WT EGFR and k-Ras mutation) and HT-29 (non-special gene type) cells, showing a high safety index.

摘要

基于已上市药物 AZD9291 与 T790M 的结合模式，设计并合成了一系列 N-9-二苯基-9H-嘌呤-2-胺衍生物，旨在克服由 T790M/L858R 双突变引起的耐药性。最有效的化合物 23a 对单突变 T790M 和双突变 T790M/L858R 突变型 EGFR 均具有优异的酶抑制活性和选择性，其纳摩尔 IC 值对野生型 EGFR 的选择性超过 8 倍。化合物 23a 对携带 T790M/L858R 的 H1975 非小细胞肺癌（NSCLC）细胞具有很强的增殖抑制活性。而对 A549（WT EGFR 和 k-Ras 突变）和 HT-29（非特殊基因类型）细胞的活性较低，显示出较高的安全指数。

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发现选择性 EGFR 调节剂，以抑制具有 N-9-二苯基-9H-嘌呤-2-胺骨架的 L858R/T790M 双突变体。

Discovery of selective EGFR modulator to inhibit L858R/T790M double mutants bearing a N-9-Diphenyl-9H-purin-2-amine scaffold.

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