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来自……的MltA晶体结构揭示的裂解转糖基酶二聚化的分子基础

Molecular basis of dimerization of lytic transglycosylase revealed by the crystal structure of MltA from .

作者信息

Jang Hyunseok, Do Hackwon, Kim Chang Min, Kim Gi Eob, Lee Jun Hyuck, Park Hyun Ho

机构信息

College of Pharmacy, Chung-Ang University, Seoul 06974, Republic of Korea.

Department of Global Innovative Drugs, Graduate School of Chung-Ang University, Seoul 06974, Republic of Korea.

出版信息

IUCrJ. 2021 Sep 23;8(Pt 6):921-930. doi: 10.1107/S2052252521008666. eCollection 2021 Nov 1.

Abstract

Peptidoglycan digestion by murein-degrading enzymes is a critical process in bacterial cell growth and/or cell division. The membrane-bound lytic murein transglycosylase A (MltA) is a murein-degrading enzyme; it catalyzes the cleavage of the β-1,4-glycosidic linkage between -acetylmuramic acid and -acetylglucosamine in peptidoglycans. Although substrate recognition and cleavage by MltA have been examined by previous structural and mutagenesis studies, the overall mechanism of MltA in conjunction with other functionally related molecules on the outer membrane of bacterial cells for peptidoglycan degradation has remained elusive. In this study, the crystal structure of MltA from the virulent human pathogen is characterized and presented. The study indicated that MltA from forms homodimers via an extra domain which is specific to this species. Furthermore, the working mechanism of MltA with various functionally related proteins on the bacterial outer membrane was modeled based on the structural and biochemical analysis.

摘要

由胞壁质降解酶进行的肽聚糖消化是细菌细胞生长和/或细胞分裂中的关键过程。膜结合的溶菌胞壁质转糖基酶A(MltA)是一种胞壁质降解酶;它催化肽聚糖中N-乙酰胞壁酸和N-乙酰葡糖胺之间的β-1,4-糖苷键的裂解。尽管先前的结构和诱变研究已经考察了MltA对底物的识别和裂解作用,但MltA与细菌细胞外膜上其他功能相关分子协同作用进行肽聚糖降解的整体机制仍不清楚。在本研究中,对来自强毒力人类病原体的MltA的晶体结构进行了表征和展示。该研究表明,来自该病原体的MltA通过一个特定于该物种的额外结构域形成同型二聚体。此外,基于结构和生化分析,对MltA与细菌外膜上各种功能相关蛋白的作用机制进行了建模。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ce78/8562663/0a56f39c691c/m-08-00921-fig1.jpg

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