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霍乱弧菌VI型分泌效应蛋白的易位需要宿主细胞对细菌进行内吞作用。

Translocation of a Vibrio cholerae type VI secretion effector requires bacterial endocytosis by host cells.

作者信息

Ma Amy T, McAuley Steven, Pukatzki Stefan, Mekalanos John J

机构信息

Department of Microbiology and Molecular Genetics, Harvard Medical School, 200 Longwood Avenue, Boston, MA 02115, USA.

出版信息

Cell Host Microbe. 2009 Mar 19;5(3):234-43. doi: 10.1016/j.chom.2009.02.005.

DOI:10.1016/j.chom.2009.02.005
PMID:19286133
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3142922/
Abstract

The type VI secretion system (T6SS) is a virulence mechanism common to several Gram-negative pathogens. In Vibrio cholerae, VgrG-1 is required for T6SS-dependent secretion. VgrG-1 is also secreted by T6SS and displays a C-terminal actin crosslinking domain (ACD). Using a heterologous reporter enzyme in place of the ACD, we show that the effector and secretion functions of VgrG-1 are genetically dissociable with the ACD being dispensable for secretion but required for T6SS-dependent phenotypes. Furthermore, internalization of bacteria is required for ACD translocation into phagocytic target cells. Inhibiting bacterial uptake abolishes actin crosslinking, while improving intracellular survival enhances it. Otherwise resistant nonphagocytic cells become susceptible to T6SS-mediated actin crosslinking when engineered to take up bacteria. Our results support a model for translocation of VgrG C-terminal effector domains into target cell cytosol by a process that requires trafficking of bacterial cells into an endocytic compartment where translocation is triggered by an unknown signal.

摘要

VI型分泌系统(T6SS)是几种革兰氏阴性病原体共有的一种毒力机制。在霍乱弧菌中,T6SS依赖性分泌需要VgrG-1。VgrG-1也由T6SS分泌,并显示出一个C端肌动蛋白交联结构域(ACD)。我们使用一种异源报告酶取代ACD,结果表明VgrG-1的效应器和分泌功能在遗传上是可分离的,其中ACD对于分泌是可有可无的,但对于T6SS依赖性表型是必需的。此外,细菌内化是ACD转运到吞噬靶细胞所必需的。抑制细菌摄取会消除肌动蛋白交联,而提高细胞内存活率则会增强这种交联。经过工程改造以摄取细菌的原本具有抗性的非吞噬细胞,会变得易受T6SS介导的肌动蛋白交联影响。我们的结果支持了一个模型,即VgrG C端效应器结构域通过一个需要将细菌细胞运输到内吞区室的过程转运到靶细胞胞质溶胶中,在该内吞区室中,转运由一个未知信号触发。

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