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沙眼衣原体 Slc1 是一种 III 型分泌接头蛋白,可增强其入侵效应子底物 TARP 的易位。

Chlamydia trachomatis Slc1 is a type III secretion chaperone that enhances the translocation of its invasion effector substrate TARP.

机构信息

Centre for Molecular Microbiology and Infection, Division of Cell and Molecular Biology, Imperial College, London SW72AZ, UK.

出版信息

Mol Microbiol. 2011 Oct;82(1):131-44. doi: 10.1111/j.1365-2958.2011.07802.x. Epub 2011 Sep 2.

Abstract

Bacterial type III secretion system (T3SS) chaperones pilot substrates to the export apparatus in a secretion-competent state, and are consequently central to the translocation of effectors into target cells. Chlamydia trachomatis is a genetically intractable obligate intracellular pathogen that utilizes T3SS effectors to trigger its entry into mammalian cells. The only well-characterized T3SS effector is TARP (translocated actin recruitment protein), but its chaperone is unknown. Here we exploited a known structural signature to screen for putative type III secretion chaperones encoded within the C. trachomatis genome. Using bacterial two-hybrid, co-precipitation, cross-linking and size exclusion chromatography we show that Slc1 (SycE-like chaperone 1; CT043) specifically interacts with a 200-amino-acid residue N-terminal region of TARP (TARP¹⁻²⁰⁰). Slc1 formed homodimers in vitro, as shown in cross-linking and gel filtration experiments. Biochemical analysis of an isolated Slc1-TARP¹⁻²⁰⁰ complex was consistent with a characteristic 2:1 chaperone-effector stoichiometry. Furthermore, Slc1 was co-immunoprecipitated with TARP from C. trachomatis elementary bodies. Also, coexpression of Slc1 specifically enhanced host cell translocation of TARP by a heterologous Yersinia enterocolitica T3SS. Taken together, we propose Slc1 as a chaperone of the C. trachomatis T3SS effector TARP.

摘要

细菌 III 型分泌系统 (T3SS) 伴侣将底物引导至分泌功能状态下的出口装置,因此对于效应物向靶细胞的易位至关重要。沙眼衣原体是一种遗传上难以处理的专性细胞内病原体,它利用 T3SS 效应物引发其进入哺乳动物细胞。唯一被充分研究的 T3SS 效应物是 TARP(易位肌动蛋白募集蛋白),但其伴侣未知。在这里,我们利用已知的结构特征筛选了沙眼衣原体基因组中编码的潜在 III 型分泌伴侣。使用细菌双杂交、共沉淀、交联和大小排阻层析,我们表明 Slc1(SycE 样伴侣 1;CT043)特异性地与 TARP(TARP¹⁻²⁰⁰)的 200 个氨基酸残基 N 端区域相互作用。Slc1 在体外形成同源二聚体,如交联和凝胶过滤实验所示。对分离的 Slc1-TARP¹⁻²⁰⁰ 复合物的生化分析与特征性 2:1 伴侣-效应物比例一致。此外,Slc1 从沙眼衣原体原体中与 TARP 一起被共同免疫沉淀。此外,Slc1 的共表达特异性增强了异源耶尔森氏菌 T3SS 中 TARP 的宿主细胞易位。综上所述,我们提出 Slc1 是沙眼衣原体 T3SS 效应物 TARP 的伴侣。

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