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梭状芽胞杆菌的缀合蛋白 TcpC 在结构上与革兰氏阴性菌的 IV 型分泌系统蛋白 VirB8 有关。

The conjugation protein TcpC from Clostridium perfringens is structurally related to the type IV secretion system protein VirB8 from Gram-negative bacteria.

机构信息

ARC Centre of Excellence in Structural and Functional Microbial Genomics, Clayton, Vic. 3800, Australia.

出版信息

Mol Microbiol. 2012 Jan;83(2):275-88. doi: 10.1111/j.1365-2958.2011.07930.x. Epub 2011 Dec 11.

DOI:10.1111/j.1365-2958.2011.07930.x
PMID:22150951
Abstract

Bacterial conjugation is important for the acquisition of virulence and antibiotic resistance genes. We investigated the mechanism of conjugation in Gram-positive pathogens using a model plasmid pCW3 from Clostridium perfringens. pCW3 encodes tetracycline resistance and contains the tcp locus, which is essential for conjugation. We showed that the unique TcpC protein (359 amino acids, 41 kDa) was required for efficient conjugative transfer, localized to the cell membrane independently of other conjugation proteins, and that membrane localization was important for its function, oligomerization and interaction with the conjugation proteins TcpA, TcpH and TcpG. The crystal structure of the C-terminal component of TcpC (TcpC(99-359)) was determined to 1.8-Å resolution. TcpC(99-359) contained two NTF2-like domains separated by a short linker. Unexpectedly, comparative structural analysis showed that each of these domains was structurally homologous to the periplasmic region of VirB8, a component of the type IV secretion system from Agrobacterium tumefaciens. Bacterial two-hybrid studies revealed that the C-terminal domain was critical for interactions with other conjugation proteins. The N-terminal region of TcpC was required for efficient conjugation, oligomerization and protein-protein interactions. We conclude that by forming oligomeric complexes, TcpC contributes to the stability and integrity of the conjugation apparatus, facilitating efficient pCW3 transfer.

摘要

细菌接合对于获得毒力和抗生素耐药基因非常重要。我们使用来自产气荚膜梭菌的模型质粒 pCW3 研究了革兰氏阳性病原体的接合机制。pCW3 编码四环素抗性,并包含 tcp 基因座,这对于接合是必不可少的。我们表明,独特的 TcpC 蛋白(359 个氨基酸,41kDa)是有效接合转移所必需的,它独立于其他接合蛋白定位在细胞膜上,并且膜定位对于其功能、寡聚化和与接合蛋白 TcpA、TcpH 和 TcpG 的相互作用很重要。TcpC 的 C 端成分(TcpC(99-359))的晶体结构已确定至 1.8Å 分辨率。TcpC(99-359)包含两个 NTF2 样结构域,由一个短接头隔开。出乎意料的是,比较结构分析表明,这些结构域中的每一个都与根癌农杆菌 IV 型分泌系统的 VirB8 成分的周质区结构同源。细菌双杂交研究表明,C 端结构域对于与其他接合蛋白的相互作用至关重要。TcpC 的 N 端区域对于有效的接合、寡聚化和蛋白质-蛋白质相互作用是必需的。我们得出结论,通过形成寡聚复合物,TcpC 有助于维持接合装置的稳定性和完整性,从而促进 pCW3 的有效转移。

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