Discovery and Structural Optimization of N5-Substituted 6,7-Dioxo-6,7-dihydropteridines as Potent and Selective Epidermal Growth Factor Receptor (EGFR) Inhibitors against L858R/T790M Resistance Mutation

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• 作者：Yongjia Hao ; Xia Wang ; Tao Zhang ; Deheng Sun ; Yi Tong ; Yuqiong Xu ; Haiyang Chen ; Linjiang Tong ; Lili Zhu ; Zhenjiang Zhao ; Zhuo Chen ; Jian Ding ; Hua Xie ; Yufang Xu ; Honglin Li
• 刊名：Journal of Medicinal Chemistry
• 出版年：2016
• 出版时间：August 11, 2016
• 年：2016
• 卷：59
• 期：15
• 页码：7111-7124
• 全文大小：683K
• 年卷期：0
• ISSN：1520-4804

文摘

EGFR-targeted inhibitors (gefitinib and erlotinib) provided an effective strategy for the treatment of non-small-cell lung cancer. However, the EGFR T790M secondary mutation has become a leading cause of clinically acquired resistance to these agents. Herein, on the basis of the previously reported irreversible EGFR inhibitor (compound 9), we present a structure-based design approach, which is rationalized via analyzing its binding model and comparing the differences of gatekeeper pocket between the T790M mutant and wild-type (WT) EGFR kinases. Guided by these results, a novel 6,7-dioxo-6,7-dihydropteridine scaffold was discovered and hydrophobic modifications at N5-position were conducted to strengthen nonpolar contacts and improve mutant selectivity over EGFR^WT. Finally, the most representative compound 17d was identified. This work demonstrates the power of structure-based strategy in discovering lead compounds and provides molecular insights into the selectivity of EGFR^L858R/T790M over EGFR^WT, which may play an important role in designing new classes of mutant-selective EGFR inhibitors.