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抑制剂/抗抑制剂系统控制溶菌转糖苷酶 MltF 的活性。

An inhibitor/anti-inhibitor system controls the activity of lytic transglycosylase MltF in .

机构信息

Department of Microbiology, New York University Grossman School of Medicine, New York, New York, USA.

出版信息

mBio. 2023 Dec 19;14(6):e0202223. doi: 10.1128/mbio.02022-23. Epub 2023 Dec 4.

Abstract

A peptidoglycan cell wall is an essential component of almost all bacterial cell envelopes, which determines cell shape and prevents osmotic rupture. Antibiotics that interfere with peptidoglycan synthesis have been one of the most important treatments for bacterial infections. Peptidoglycan must also be hydrolyzed to incorporate new material for cell growth and division and to help accommodate important envelope-spanning systems. However, the enzymes that hydrolyze peptidoglycan must be carefully controlled to prevent autolysis. Exactly how this control is achieved is poorly understood in most cases but is a highly active area of current research. Identifying hydrolase control mechanisms has the potential to provide new targets for therapeutic intervention. The work here reports the important discovery of a novel inhibitor/anti-inhibitor system that controls the activity of a cell wall hydrolase in the human pathogen , which also affects resistance to an antibiotic used in the clinic.

摘要

肽聚糖细胞壁是几乎所有细菌细胞膜的重要组成部分,它决定了细胞的形状并防止渗透压破裂。干扰肽聚糖合成的抗生素一直是治疗细菌感染的最重要手段之一。肽聚糖还必须被水解以掺入新的物质以促进细胞生长和分裂,并帮助容纳重要的膜贯穿系统。然而,用于水解肽聚糖的酶必须被仔细控制,以防止自溶。在大多数情况下,这种控制是如何实现的还了解甚少,但这是当前研究的一个非常活跃的领域。确定水解酶的控制机制有可能为治疗干预提供新的靶点。这里的工作报道了一个重要的发现,即一种新型的抑制剂/抗抑制剂系统控制着人类病原体中细胞壁水解酶的活性,这也影响了临床使用的抗生素的耐药性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7766/10746161/c4359376fccf/mbio.02022-23.f001.jpg

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