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弗氏志贺氏菌毒力因子IcsA/VirG的结构解析以及参与极性分布和分泌的基序

Structural insights into the architecture of the Shigella flexneri virulence factor IcsA/VirG and motifs involved in polar distribution and secretion.

作者信息

Leupold Stefan, Büsing Petra, Mas Philippe J, Hart Darren J, Scrima Andrea

机构信息

Structural Biology of Autophagy, Helmholtz-Centre for Infection Research, Inhoffenstraße 7, 38124 Braunschweig, Germany.

European Molecular Biology Laboratory Grenoble Outstation and Unit of Virus Host-Cell Interactions, University Grenoble Alpes-CNRS-EMBL, 71 Avenue des Martyrs, CS 90181, 38042 Grenoble Cedex 9, France.

出版信息

J Struct Biol. 2017 Apr;198(1):19-27. doi: 10.1016/j.jsb.2017.03.003. Epub 2017 Mar 6.

Abstract

IcsA/VirG is a key virulence factor of the human pathogen Shigella flexneri, acting as both an adhesin and actin-polymerizing factor during infection. We identified a soluble expression construct of the IcsA/VirG α-domain using the ESPRIT library screening system and determined its structure to 1.9Å resolution. In addition to the previously characterized autochaperone domain, our structure reveals a new domain, which shares a common fold with the autochaperone domains of various autotransporters. We further provide insight into the previously structurally uncharacterized β-helix domain that harbors the polar targeting motif and passenger-associated transport repeat. This structure is the first of any member of the recently identified passenger-associated transport repeat-containing autotransporters. Thus, it provides new insights into the overall architecture of this class of autotransporters, the function of the identified additional autochaperone domain and the structural properties of motifs involved in polar targeting and secretion of the Shigella flexneri virulence factor IcsA/VirG.

摘要

IcsA/VirG是人类病原体福氏志贺菌的关键毒力因子,在感染过程中兼具黏附素和肌动蛋白聚合因子的作用。我们利用ESPRIT文库筛选系统鉴定出IcsA/VirG α结构域的可溶性表达构建体,并将其结构解析到1.9Å的分辨率。除了先前已鉴定特征的自伴侣结构域外,我们的结构还揭示了一个新结构域,它与各种自转运蛋白的自伴侣结构域具有共同的折叠方式。我们进一步深入研究了先前结构未明确的β螺旋结构域,该结构域包含极性靶向基序和与乘客相关的转运重复序列。此结构是最近鉴定出的含与乘客相关转运重复序列的自转运蛋白家族中首个成员的结构。因此,它为这类自转运蛋白的整体结构、鉴定出的额外自伴侣结构域的功能以及福氏志贺菌毒力因子IcsA/VirG的极性靶向和分泌所涉及基序的结构特性提供了新的见解。

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