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本文引用的文献

1
Structural Basis of Type 2 Secretion System Engagement between the Inner and Outer Bacterial Membranes.2 型分泌系统在细菌内外膜之间结合的结构基础。
mBio. 2017 Oct 17;8(5):e01344-17. doi: 10.1128/mBio.01344-17.
2
The trans-envelope architecture and function of the type 2 secretion system: new insights raising new questions.2型分泌系统的跨内膜结构与功能:新见解引发新问题
Mol Microbiol. 2017 Jul;105(2):211-226. doi: 10.1111/mmi.13704. Epub 2017 May 18.
3
Expanding Role of Type II Secretion in Bacterial Pathogenesis and Beyond.II型分泌系统在细菌致病及其他方面的作用扩展
Infect Immun. 2017 Apr 21;85(5). doi: 10.1128/IAI.00014-17. Print 2017 May.
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cryoSPARC: algorithms for rapid unsupervised cryo-EM structure determination.cryoSPARC:用于快速无监督低温电子显微镜结构测定的算法。
Nat Methods. 2017 Mar;14(3):290-296. doi: 10.1038/nmeth.4169. Epub 2017 Feb 6.
5
Structural insights into the secretin translocation channel in the type II secretion system.结构洞察 II 型分泌系统中分泌素易位通道。
Nat Struct Mol Biol. 2017 Feb;24(2):177-183. doi: 10.1038/nsmb.3350. Epub 2017 Jan 9.
6
Near-atomic-resolution cryo-EM analysis of the Salmonella T3S injectisome basal body.鼠伤寒沙门氏菌三型分泌注射体基体的近原子分辨率冷冻电镜分析。
Nature. 2016 Dec 22;540(7634):597-601. doi: 10.1038/nature20576. Epub 2016 Dec 14.
7
Prepore Stability Controls Productive Folding of the BAM-independent Multimeric Outer Membrane Secretin PulD.前孔稳定性控制不依赖BAM的多聚体外膜分泌素PulD的有效折叠。
J Biol Chem. 2017 Jan 6;292(1):328-338. doi: 10.1074/jbc.M116.759498. Epub 2016 Nov 30.
8
Accelerated cryo-EM structure determination with parallelisation using GPUs in RELION-2.在RELION-2中使用图形处理器(GPU)并行化加速冷冻电镜结构测定
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9
Differential Regulation of the Surface-Exposed and Secreted SslE Lipoprotein in Extraintestinal Pathogenic Escherichia coli.肠道外致病性大肠杆菌中表面暴露和分泌的SslE脂蛋白的差异调控
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Giant MACPF/CDC pore forming toxins: A class of their own.巨型MACPF/CDC孔形成毒素:独树一帜的一类毒素。
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肠致病性大肠杆菌 II 型分泌系统 Vibrio 型分泌通路上的结构和膜拓扑结构

Structure and Membrane Topography of the Vibrio-Type Secretin Complex from the Type 2 Secretion System of Enteropathogenic Escherichia coli.

机构信息

Infection and Immunity Program, Biomedicine Discovery Institute and Department of Microbiology, Monash University, Clayton, Australia.

Infection and Immunity Program, Biomedicine Discovery Institute and Department of Microbiology, Monash University, Clayton, Australia

出版信息

J Bacteriol. 2018 Feb 7;200(5). doi: 10.1128/JB.00521-17. Print 2018 Mar 1.

DOI:10.1128/JB.00521-17
PMID:29084860
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5809698/
Abstract

The β-barrel assembly machinery (BAM) complex is the core machinery for the assembly of β-barrel membrane proteins, and inhibition of BAM complex activity is lethal to bacteria. Discovery of integral membrane proteins that are key to pathogenesis and yet do not require assistance from the BAM complex raises the question of how these proteins assemble into bacterial outer membranes. Here, we address this question through a structural analysis of the type 2 secretion system (T2SS) secretin from enteropathogenic O127:H6 strain E2348/69. Long β-strands assemble into a barrel extending 17 Å through and beyond the outer membrane, adding insight to how these extensive β-strands are assembled into the outer membrane. The substrate docking chamber of this secretin is shown to be sufficient to accommodate the substrate mucinase SteC. In order to cause disease, bacterial pathogens inhibit immune responses and induce pathology that will favor their replication and dissemination. In Gram-negative bacteria, these key attributes of pathogenesis depend on structures assembled into or onto the outer membrane. One of these is the T2SS. The -type T2SS mediates cholera toxin secretion in , and in O127:H6 strain E2348/69, the same machinery mediates secretion of the mucinases that enable the pathogen to penetrate intestinal mucus and thereby establish deadly infections.

摘要

β-桶状膜蛋白装配机器(BAM)复合体是β-桶状膜蛋白装配的核心机器,抑制 BAM 复合体活性对细菌是致命的。发现对发病机制至关重要但不需要 BAM 复合体辅助的整合膜蛋白,这就提出了一个问题,即这些蛋白如何装配到细菌外膜中。在这里,我们通过对肠致病性 O127:H6 菌株 E2348/69 的 II 型分泌系统(T2SS)分泌蛋白的结构分析来解决这个问题。长的β-链组装成一个桶状结构,通过并超出外膜延伸 17 Å,这为这些广泛的β-链如何组装到外膜中提供了新的见解。该分泌蛋白的底物结合腔足以容纳底物粘蛋白酶 SteC。为了引起疾病,细菌病原体抑制免疫反应并诱导有利于其复制和传播的病理。在革兰氏阴性菌中,这些发病机制的关键属性取决于组装到外膜上或外膜上的结构。其中之一是 T2SS。- 型 T2SS 在霍乱弧菌中介导霍乱毒素的分泌,而在 O127:H6 菌株 E2348/69 中,相同的机器介导粘蛋白酶的分泌,使病原体能够穿透肠道粘液,从而建立致命的感染。