发现了一类含有喹啉结构的 N-取代-3-苯基-1,6-萘啶酮衍生物，作为选择性的 II 型 c-Met 激酶抑制剂，对 VEGFR-2 具有抑制作用。

Discovery of N-substituted-3-phenyl-1,6-naphthyridinone derivatives bearing quinoline moiety as selective type II c-Met kinase inhibitors against VEGFR-2.

机构信息

Key Laboratory of Pesticide & Chemical Biology of Ministry of Education, International Joint Research Center for Intelligent Biosensor Technology and Health, College of Chemistry, Central China Normal University, Wuhan 430079, China.

出版信息

Bioorg Med Chem. 2020 Jun 15;28(12):115555. doi: 10.1016/j.bmc.2020.115555. Epub 2020 May 12.

DOI:10.1016/j.bmc.2020.115555

PMID:32503697

Abstract

New N-substituted-3-phenyl-1,6-naphthyridinone derivatives are designed and synthesized, based on structural modification of our previously reported compound 3. Extensive enzyme-based SAR studies and PK evaluation led to the discovery of compound 4r, with comparable c-Met potency to that of Cabozantinib and high VEGFR-2 selectivity, while Cabozantinib displayed no VEGFR-2 selectivity. More importantly, at oral doses of 45 mg/kg (Q.D.), compound 4r exhibits significant tumor growth inhibition (93%) in a U-87MG human gliobastoma xenograft model. The promising selectivity against VEGFR-2 and excellent tumor growth inhibition of compound 4r suggest that it could be used as a new lead molecule for further discovery of selective type II c-Met inhibitors.

摘要

新型 N-取代-3-苯基-1,6-萘啶酮衍生物是在我们之前报道的化合物 3 的结构修饰基础上设计和合成的。广泛的基于酶的 SAR 研究和 PK 评估导致了化合物 4r 的发现，其 c-Met 活性与卡博替尼相当，并且对 VEGFR-2 具有高选择性，而卡博替尼对 VEGFR-2 没有选择性。更重要的是，在口服剂量为 45mg/kg（QD）时，化合物 4r 在 U-87MG 人神经胶质瘤异种移植模型中表现出显著的肿瘤生长抑制（93%）。化合物 4r 对 VEGFR-2 的良好选择性和出色的肿瘤生长抑制作用表明，它可能被用作进一步发现选择性 II 型 c-Met 抑制剂的新先导分子。

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发现了一类含有喹啉结构的 N-取代-3-苯基-1,6-萘啶酮衍生物，作为选择性的 II 型 c-Met 激酶抑制剂，对 VEGFR-2 具有抑制作用。

Discovery of N-substituted-3-phenyl-1,6-naphthyridinone derivatives bearing quinoline moiety as selective type II c-Met kinase inhibitors against VEGFR-2.

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