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III型分泌系统中底物特异性开关蛋白上尺子蛋白相互作用界面的表征

Characterization of the Ruler Protein Interaction Interface on the Substrate Specificity Switch Protein in the Type III Secretion System.

作者信息

Ho Oanh, Rogne Per, Edgren Tomas, Wolf-Watz Hans, Login Frédéric H, Wolf-Watz Magnus

机构信息

Department of Chemistry, Chemical Biological Centre.

Department of Molecular Biology and The Laboratory for Molecular Infection Medicine Sweden (MIMS), Umeå University, S-901 87 Umeå, Sweden.

出版信息

J Biol Chem. 2017 Feb 24;292(8):3299-3311. doi: 10.1074/jbc.M116.770255. Epub 2016 Dec 30.

DOI:10.1074/jbc.M116.770255
PMID:28039361
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5336164/
Abstract

Many pathogenic Gram-negative bacteria use the type III secretion system (T3SS) to deliver effector proteins into eukaryotic host cells. In , the switch to secretion of effector proteins is induced first after intimate contact between the bacterium and its eukaryotic target cell has been established, and the T3SS proteins YscP and YscU play a central role in this process. Here we identify the molecular details of the YscP binding site on YscU by means of nuclear magnetic resonance (NMR) spectroscopy. The binding interface is centered on the C-terminal domain of YscU. Disrupting the YscU-YscP interaction by introducing point mutations at the interaction interface significantly reduced the secretion of effector proteins and HeLa cell cytotoxicity. Interestingly, the binding of YscP to the slowly self-cleaving YscU variant P264A conferred significant protection against autoproteolysis. The YscP-mediated inhibition of YscU autoproteolysis suggests that the cleavage event may act as a timing switch in the regulation of early late T3SS substrates. We also show that YscU binds to the inner rod protein YscI with a dissociation constant ( ) of 3.8 μm and with 1:1 stoichiometry. The significant similarity among different members of the YscU, YscP, and YscI families suggests that the protein-protein interactions discussed in this study are also relevant for other T3SS-containing Gram-negative bacteria.

摘要

许多致病性革兰氏阴性细菌利用Ⅲ型分泌系统(T3SS)将效应蛋白输送到真核宿主细胞中。在[具体情况未提及]中,效应蛋白分泌的转换首先在细菌与其真核靶细胞建立紧密接触后被诱导,并且T3SS蛋白YscP和YscU在这一过程中发挥核心作用。在这里,我们通过核磁共振(NMR)光谱法确定了YscU上YscP结合位点的分子细节。结合界面以YscU的C末端结构域为中心。通过在相互作用界面引入点突变破坏YscU - YscP相互作用,显著降低了效应蛋白的分泌和对HeLa细胞的细胞毒性。有趣的是,YscP与缓慢自我切割的YscU变体P264A的结合赋予了对自身蛋白水解的显著保护作用。YscP介导的对YscU自身蛋白水解的抑制表明,切割事件可能在早期和晚期T3SS底物的调节中充当定时开关。我们还表明,YscU以3. μM的解离常数( )和1:1的化学计量比与内杆蛋白YscI结合。YscU、YscP和YscI家族不同成员之间的显著相似性表明,本研究中讨论的蛋白质 - 蛋白质相互作用也与其他含T3SS的革兰氏阴性细菌相关。

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Role of autocleavage in the function of a type III secretion specificity switch protein in Salmonella enterica serovar Typhimurium.自切割在鼠伤寒沙门氏菌III型分泌特异性开关蛋白功能中的作用
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YscU/FlhB of Yersinia pseudotuberculosis Harbors a C-terminal Type III Secretion Signal.假结核耶尔森菌的YscU/FlhB含有一个C端III型分泌信号。
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Negatively charged lipid membranes promote a disorder-order transition in the Yersinia YscU protein.带负电荷的脂质膜促进耶尔森氏菌YscU蛋白的无序-有序转变。
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The inner rod protein controls substrate switching and needle length in a Salmonella type III secretion system.杆状内蛋白控制沙门氏菌 III 型分泌系统中底物的转换和针的长度。
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