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CesT是一种多效应伴侣蛋白和募集因子,对于肠致病性大肠杆菌中LEE编码效应蛋白和非LEE编码效应蛋白的有效III型分泌而言是必需的。

CesT is a multi-effector chaperone and recruitment factor required for the efficient type III secretion of both LEE- and non-LEE-encoded effectors of enteropathogenic Escherichia coli.

作者信息

Thomas Nikhil A, Deng Wanyin, Puente Jose L, Frey Elizabeth A, Yip Calvin K, Strynadka Natalie C J, Finlay B Brett

机构信息

Michael Smith Laboratories, University of British Columbia, Vancouver, BC, Canada.

出版信息

Mol Microbiol. 2005 Sep;57(6):1762-79. doi: 10.1111/j.1365-2958.2005.04802.x.

DOI:10.1111/j.1365-2958.2005.04802.x
PMID:16135239
Abstract

Enteropathogenic Escherichia coli (EPEC) is an intestinal attaching and effacing pathogen that utilizes a type III secretion system (T3SS) for the delivery of effectors into host cells. The chaperone CesT has been shown to bind and stabilize the type III translocated effectors Tir and Map in the bacterial cytoplasm prior to their delivery into host cells. In this study we demonstrate a role for CesT in effector recruitment to the membrane embedded T3SS. CesT-mediated effector recruitment was dependent on the presence of the T3SS membrane-associated ATPase EscN. EPEC DeltacesT carrying a C-terminal CesT variant, CesT(E142G), exhibited normal cytoplasmic Tir stability function, but was less efficient in secreting Tir, further implicating CesT in type III secretion. In vivo co-immunoprecipitation studies using CesT-FLAG containing EPEC lysates demonstrated that CesT interacts with Tir and EscN, consistent with the notion of CesT recruiting Tir to the T3SS. CesT was also shown to be required for the efficient secretion of several type III effectors encoded within and outside the locus of enterocyte effacement (LEE) in addition to Tir and Map. Furthermore, a CesT affinity column was shown to specifically retain multiple effector proteins from EPEC culture supernatants. These findings indicate that CesT is centrally involved in recruiting multiple type III effectors to the T3SS via EscN for efficient secretion, and functionally redefine the role of CesT in multiple type III effector interactions.

摘要

肠致病性大肠杆菌(EPEC)是一种肠道黏附性和致病变性病原菌,它利用III型分泌系统(T3SS)将效应蛋白递送至宿主细胞。伴侣蛋白CesT已被证明在III型易位效应蛋白Tir和Map递送至宿主细胞之前,能在细菌细胞质中结合并稳定它们。在本研究中,我们证明了CesT在效应蛋白募集至膜嵌入的T3SS中发挥作用。CesT介导的效应蛋白募集依赖于T3SS膜相关ATP酶EscN的存在。携带C端CesT变体CesT(E142G)的EPEC DeltacesT表现出正常的细胞质Tir稳定功能,但在分泌Tir方面效率较低,这进一步表明CesT参与III型分泌。使用含CesT-FLAG的EPEC裂解物进行的体内共免疫沉淀研究表明,CesT与Tir和EscN相互作用,这与CesT将Tir募集至T3SS的观点一致。除了Tir和Map外,CesT还被证明是有效分泌肠细胞脱落位点(LEE)内外编码的几种III型效应蛋白所必需的。此外,CesT亲和柱被证明能特异性保留EPEC培养上清液中的多种效应蛋白。这些发现表明,CesT通过EscN在将多种III型效应蛋白募集至T3SS以实现有效分泌方面发挥核心作用,并在功能上重新定义了CesT在多种III型效应蛋白相互作用中的作用。

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