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Recent progress in the discovery and development of DNA gyrase B inhibitors

机译:DNA旋转酶B抑制剂发现与发展的最新进展

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New antibacterials that modulate less explored targets are needed to fight the emerging bacterial resistance. DNA gyrase and topoisomerase IV are attractive targets in this search. These are both type II topoisomerases that can cleave both DNA strands, and can thus alter DNA topology during replication or similar processes. Currently, there are no ATP-competitive inhibitors of these two enzymes on the market, as the only aminocoumarin representative, novobiocin, was withdrawn due to safety concerns. The search for novel ATP-competitive inhibitors is a focus of ongoing industrial and academical research. This review summarizes the recent efforts in the design, synthesis and evaluation of GyrB/ParE inhibitors. The various approaches to achieve improved antibacterial activities are described, with particular reference to Gram-negative bacteria.
机译:需要调节较少探索目标的新抗菌剂来对抗出现的细菌抗性。 DNA戊曲酶和拓扑异构酶IV在该搜索中是有吸引力的目标。 这些都是II型拓扑异构酶,其可以切割DNA链,因此可以在复制或类似过程中改变DNA拓扑。 目前,由于安全问题,目前在市场上没有这两种酶的ATP竞争性抑制剂,这两种酶在市场上唯一的诺比科霉素被撤回。 寻找新的ATP竞争性抑制剂是持续产业和学者研究的重点。 本综述总结了最近的设计,合成和评估GyrB / Pare抑制剂的努力。 描述了改善抗菌活性的各种方法,特别是革兰氏阴性细菌。

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