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对铜绿假单胞菌T6SS效应蛋白Tse3和Tse3-Tsi3复合物的结构研究揭示了一种钙依赖性膜结合机制。

Structural insights into the T6SS effector protein Tse3 and the Tse3-Tsi3 complex from Pseudomonas aeruginosa reveal a calcium-dependent membrane-binding mechanism.

作者信息

Lu Defen, Shang Guijun, Zhang Heqiao, Yu Qian, Cong Xiaoyan, Yuan Jupeng, He Fengjuan, Zhu Chunyuan, Zhao Yanyu, Yin Kun, Chen Yuanyuan, Hu Junqiang, Zhang Xiaodan, Yuan Zenglin, Xu Sujuan, Hu Wei, Cang Huaixing, Gu Lichuan

机构信息

State Key Laboratory of Microbial Technology, Shandong University, Jinan, 250100, Shandong, China; The Liver Centre of Fujian Province, MengChao Hepatobiliary Hospital of Fujian Medical University, Fuzhou, 350025, Fujian, China.

出版信息

Mol Microbiol. 2014 Jun;92(5):1092-112. doi: 10.1111/mmi.12616. Epub 2014 May 2.

DOI:10.1111/mmi.12616
PMID:24724564
Abstract

The opportunistic pathogen Pseudomonas aeruginosa uses the type VI secretion system (T6SS) to deliver the muramidase Tse3 into the periplasm of rival bacteria to degrade their peptidoglycan (PG). Concomitantly, P. aeruginosa uses the periplasm-localized immunity protein Tsi3 to prevent potential self-intoxication caused by Tse3, and thus gains an edge over rival bacteria in fierce niche competition. Here, we report the crystal structures of Tse3 and the Tse3-Tsi3 complex. Tse3 contains an annexin repeat-like fold at the N-terminus and a G-type lysozyme fold at the C-terminus. One loop in the N-terminal domain (Loop 12) and one helix (α9) from the C-terminal domain together anchor Tse3 and the Tse3-Tsi3 complex to membrane in a calcium-dependent manner in vitro, and this membrane-binding ability is essential for Tse3's activity. In the C-terminal domain, a Y-shaped groove present on the surface likely serves as the PG binding site. Two calcium-binding motifs are also observed in the groove and these are necessary for Tse3 activity. In the Tse3-Tsi3 structure, three loops of Tsi3 insert into the substrate-binding groove of Tse3, and three calcium ions present at the interface of the complex are indispensable for the formation of the Tse3-Tsi3 complex.

摘要

机会致病菌铜绿假单胞菌利用VI型分泌系统(T6SS)将溶菌酶Tse3输送到竞争细菌的周质中,以降解其肽聚糖(PG)。与此同时,铜绿假单胞菌利用定位于周质的免疫蛋白Tsi3来防止由Tse3引起的潜在自我中毒,从而在激烈的生态位竞争中比竞争细菌更具优势。在此,我们报道了Tse3和Tse3-Tsi3复合物的晶体结构。Tse3在N端包含一个类膜联蛋白重复折叠,在C端包含一个G型溶菌酶折叠。N端结构域中的一个环(环12)和C端结构域中的一个螺旋(α9)一起在体外以钙依赖的方式将Tse3和Tse3-Tsi3复合物锚定在膜上,这种膜结合能力对Tse3的活性至关重要。在C端结构域中,表面上存在的一个Y形凹槽可能作为PG结合位点。在该凹槽中还观察到两个钙结合基序,这些对Tse3活性是必需的。在Tse3-Tsi3结构中,Tsi3的三个环插入Tse3的底物结合凹槽中,复合物界面处存在的三个钙离子对于Tse3-Tsi3复合物的形成是不可或缺的。

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