基于结构的变构抑制剂设计抑制拓扑异构酶 II。

Structure-guided design of antibacterials that allosterically inhibit DNA gyrase.

机构信息

GlaxoSmithKline, Collegeville, PA 19426, USA.

EVOTEC Center of Drug Discovery and Development, 37135 Verona, Italy.

出版信息

Bioorg Med Chem Lett. 2019 Jun 1;29(11):1407-1412. doi: 10.1016/j.bmcl.2019.03.029. Epub 2019 Mar 22.

DOI:10.1016/j.bmcl.2019.03.029

PMID:30962087

Abstract

A series of DNA gyrase inhibitors were designed based on the X-ray structure of a parent thiophene scaffold with the objective to improve biochemical and whole-cell antibacterial activity, while reducing cardiac ion channel activity. The binding mode and overall design hypothesis of one series was confirmed with a co-crystal structure with DNA gyrase. Although some analogs retained both biochemical activity and whole-cell antibacterial activity, we were unable to significantly improve the activity of the series and analogs retained activity against the cardiac ion channels, therefore we stopped optimization efforts.

摘要

设计了一系列 DNA 拓扑异构酶抑制剂，其基于具有母体噻吩支架的 X 射线结构，旨在提高生化和全细胞抗菌活性，同时降低心脏离子通道活性。通过与 DNA 拓扑异构酶的共晶结构证实了一个系列的结合模式和整体设计假设。尽管一些类似物保留了生化活性和全细胞抗菌活性，但我们无法显著提高该系列的活性，而且类似物仍保留对心脏离子通道的活性，因此我们停止了优化工作。

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基于结构的变构抑制剂设计抑制拓扑异构酶 II。

Structure-guided design of antibacterials that allosterically inhibit DNA gyrase.

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基于结构的变构抑制剂设计抑制拓扑异构酶 II。

Structure-guided design of antibacterials that allosterically inhibit DNA gyrase.

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