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沙门氏菌 III 型分泌效应物/伴侣复合物形成六聚体环状结构。

A Salmonella type three secretion effector/chaperone complex adopts a hexameric ring-like structure.

机构信息

INRA Biopolymères, Interactions et Assemblages, Nantes, France Synchrotron SOLEIL, Gif sur Yvette, France.

Unité de Glycobiologie Structurale et Fonctionnelle, CNRS UMR8576, Université Lille Nord de France, Villeneuve d'Ascq, France.

出版信息

J Bacteriol. 2015 Feb 15;197(4):688-98. doi: 10.1128/JB.02294-14. Epub 2014 Nov 17.

Abstract

Many bacterial pathogens use type three secretion systems (T3SS) to inject virulence factors, named effectors, directly into the cytoplasm of target eukaryotic cells. Most of the T3SS components are conserved among plant and animal pathogens, suggesting a common mechanism of recognition and secretion of effectors. However, no common motif has yet been identified for effectors allowing T3SS recognition. In this work, we performed a biochemical and structural characterization of the Salmonella SopB/SigE chaperone/effector complex by small-angle X-ray scattering (SAXS). Our results showed that the SopB/SigE complex is assembled in dynamic homohexameric-ring-shaped structures with an internal tunnel. In this ring, the chaperone maintains a disordered N-terminal end of SopB molecules, in a good position to be reached and processed by the T3SS. This ring dimensionally fits the ring-organized molecules of the injectisome, including ATPase hexameric rings; this organization suggests that this structural feature is important for ATPase recognition by T3SS. Our work constitutes the first evidence of the oligomerization of an effector, analogous to the organization of the secretion machinery, obtained in solution. As effectors share neither sequence nor structural identity, the quaternary oligomeric structure could constitute a strategy evolved to promote the specificity and efficiency of T3SS recognition.

摘要

许多细菌病原体利用 III 型分泌系统(T3SS)将毒力因子(称为效应子)直接注射到真核靶细胞的细胞质中。大多数 T3SS 成分在植物和动物病原体中都保守,这表明效应子的识别和分泌具有共同的机制。然而,尚未确定用于 T3SS 识别的通用效应子基序。在这项工作中,我们通过小角度 X 射线散射(SAXS)对沙门氏菌 SopB/SigE 伴侣/效应子复合物进行了生化和结构表征。我们的结果表明,SopB/SigE 复合物组装成动态同六聚体环形状结构,具有内部隧道。在这个环中,伴侣蛋白保持 SopB 分子的无序 N 端,处于可被 T3SS 到达和加工的良好位置。这个环的尺寸与注射器的环组织分子相匹配,包括 ATP 酶六聚体环;这种组织表明,这种结构特征对于 T3SS 对 ATP 酶的识别很重要。我们的工作首次在溶液中获得了效应子的寡聚化证据,类似于分泌机制的组织。由于效应子既没有序列也没有结构同一性,因此四元寡聚结构可能是一种进化策略,用于促进 T3SS 识别的特异性和效率。

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