首款基于三氯生的 InhA 酶大环抑制剂。

First triclosan-based macrocyclic inhibitors of InhA enzyme.

机构信息

LSPCMIB, UMR-CNRS 5068, Université Paul Sabatier-Toulouse III, 118 Route de Narbonne, 31062 Toulouse Cedex 9, France.

Institut de Chimie de Toulouse, FR2599, 118 Route de Narbonne, 31062 Toulouse, France.

出版信息

Bioorg Chem. 2020 Jan;95:103498. doi: 10.1016/j.bioorg.2019.103498. Epub 2019 Dec 6.

DOI:10.1016/j.bioorg.2019.103498

PMID:31855823

Abstract

Two macrocyclic derivatives based on the triclosan frame were designed and synthesized as inhibitors of Mycobacterium tuberculosis InhA enzyme. One of the two molecules M02 displayed promising inhibitory activity against InhA enzyme with an IC of 4.7 μM. Molecular docking studies of these two compounds were performed and confirmed that M02 was more efficient as inhibitor of InhA activity. These molecules are the first macrocyclic direct inhibitors of InhA enzyme able to bind into the substrate pocket. Furthermore, these biaryl ether compounds exhibited antitubercular activities comparable to that of triclosan against M. tuberculosis H37Rv strain.

摘要

设计并合成了两种基于三氯生骨架的大环衍生物，作为结核分枝杆菌 InhA 酶的抑制剂。这两个分子中的一个 M02 对 InhA 酶表现出有希望的抑制活性，IC 为 4.7μM。对这两种化合物进行了分子对接研究，证实 M02 作为 InhA 活性抑制剂更有效。这些分子是能够结合到底物口袋中的第一个大环直接 InhA 酶抑制剂。此外，这些联苯醚化合物对结核分枝杆菌 H37Rv 株的抗结核活性与三氯生相当。

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首款基于三氯生的 InhA 酶大环抑制剂。

First triclosan-based macrocyclic inhibitors of InhA enzyme.

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