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分枝杆菌 VII 型分泌系统的结构。

Architecture of the mycobacterial type VII secretion system.

机构信息

Institute for Molecular Infection Biology, Julius-Maximilians-University Würzburg, Würzburg, Germany.

Rudolf Virchow Center for Experimental Biomedicine, Julius-Maximilians-University Würzburg, Würzburg, Germany.

出版信息

Nature. 2019 Dec;576(7786):321-325. doi: 10.1038/s41586-019-1633-1. Epub 2019 Oct 9.

DOI:10.1038/s41586-019-1633-1
PMID:31597161
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6914368/
Abstract

Host infection by pathogenic mycobacteria, such as Mycobacterium tuberculosis, is facilitated by virulence factors that are secreted by type VII secretion systems. A molecular understanding of the type VII secretion mechanism has been hampered owing to a lack of three-dimensional structures of the fully assembled secretion apparatus. Here we report the cryo-electron microscopy structure of a membrane-embedded core complex of the ESX-3/type VII secretion system from Mycobacterium smegmatis. The core of the ESX-3 secretion machine consists of four protein components-EccB3, EccC3, EccD3 and EccE3, in a 1:1:2:1 stoichiometry-which form two identical protomers. The EccC3 coupling protein comprises a flexible array of four ATPase domains, which are linked to the membrane through a stalk domain. The domain of unknown function (DUF) adjacent to the stalk is identified as an ATPase domain that is essential for secretion. EccB3 is predominantly periplasmatic, but a small segment crosses the membrane and contacts the stalk domain. This suggests that conformational changes in the stalk domain-triggered by substrate binding at the distal end of EccC3 and subsequent ATP hydrolysis in the DUF-could be coupled to substrate secretion to the periplasm. Our results reveal that the architecture of type VII secretion systems differs markedly from that of other known secretion machines, and provide a structural understanding of these systems that will be useful for the design of antimicrobial strategies that target bacterial virulence.

摘要

宿主被致病性分枝杆菌(如结核分枝杆菌)感染,这是由 VII 型分泌系统分泌的毒力因子促成的。由于缺乏完全组装的分泌装置的三维结构,因此对 VII 型分泌机制的分子理解受到了阻碍。在这里,我们报告了来自耻垢分枝杆菌的 ESX-3/ VII 型分泌系统的膜嵌入核心复合物的冷冻电子显微镜结构。ESX-3 分泌机器的核心由四个蛋白成分-EccB3、EccC3、EccD3 和 EccE3-以 1:1:2:1 的比例组成,形成两个相同的原体。EccC3 偶联蛋白由四个 ATP 酶结构域组成,这些结构域通过一个柄结构域与膜相连。与柄结构域相邻的未知功能域(DUF)被鉴定为 ATP 酶结构域,对于分泌是必需的。EccB3 主要位于周质中,但一小段穿过膜并与柄结构域接触。这表明,由 EccC3 远端的底物结合和随后在 DUF 中的 ATP 水解触发的柄结构域的构象变化,可能与底物分泌到周质相偶联。我们的结果表明,VII 型分泌系统的结构与其他已知的分泌机器明显不同,并为这些系统的结构理解提供了基础,这对于设计针对细菌毒力的抗菌策略将是有用的。

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