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杂环并苯的简单合成及其作为孵化阻断物抑制 c-Met 活性的研究*。

Simple Synthesis of a Heterocyclophane Exhibiting Anti-c-Met Activity by Acting as a Hatch Blocking Access to the Active Site*.

机构信息

Faculty of Pharmaceutical Sciences, Kobe Gakuin University, Minatojima, chuo-ku, Kobe, 650-8586, Japan.

Graduate School of Human and Environmental Studies, Kyoto University, Yoshida Nihonmatsu-cho, Sakyo-ku, Kyoto, 606-8501, Japan.

出版信息

Chemistry. 2021 Jan 21;27(5):1648-1654. doi: 10.1002/chem.202001382. Epub 2020 Dec 15.

Abstract

A simple approach to the synthesis of heterocyclophane consisting of two 4,4'-bithiazoles has been developed in mild conditions. The heterocyclophane with two short chains was conveniently prepared by Hantzsch thiazoles synthesis using the reaction of 3-tert-butoxycarbonyl-3-azapentanethiocarboxamide with 1,4-dibromobutane-2,3-dione in methanol under reflux for only 15 min. Amino groups at the linkers of this heterocyclophane can be functionalized to give acylated and carbamate derivatives. Their properties as protein kinase inhibitors were investigated, and one of the heterocyclophanes exhibited specific anti-activity for c-mesenchymal epithelial transition factor (IC =603 nm), among seven types of protein kinases investigated. The computational site identification by ligand competitive saturation method was used to determine why the one heterocyclophane exhibited strong anti-activity for c-mesenchymal epithelial transition factor.

摘要

已开发出一种在温和条件下由两个 4,4'-联噻唑组成的杂环并苯的简便合成方法。使用 3-叔丁氧羰基-3-氮杂戊烷硫代甲酰胺与 1,4-二溴-2,3-丁二酮在甲醇中回流仅 15 分钟的 Hantzsch 噻唑合成,方便地制备了带有两条短链的杂环并苯。该杂环并苯的连接体上的氨基可进一步官能化得到酰化和氨基甲酸酯衍生物。研究了它们作为蛋白激酶抑制剂的性质,在所研究的七种蛋白激酶中,一种杂环并苯对 c-间充质上皮转化因子(IC =603nm)表现出特异性的抑制活性。通过配体竞争饱和方法的计算位点鉴定,确定了为什么一种杂环并苯对 c-间充质上皮转化因子具有很强的抑制活性。

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