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Systems-level overview of host protein phosphorylation during Shigella flexneri infection revealed by phosphoproteomics

机译:磷酸蛋白组学揭示了弗氏志贺氏菌感染期间宿主蛋白磷酸化的系统级概述

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摘要

The enteroinvasive bacterium Shigella flexneri invades the intestinal epithelium of humans. During infection, several injected effector proteins promote bacterial internalization, and interfere with multiple host cell responses. To obtain a systems-level overview of host signaling during infection, we analyzed the global dynamics of protein phosphorylation by liquid chromatography-tandem MS and identified several hundred of proteins undergoing a phosphorylation change during the first hours of infection. Functional bioinformatic analysis revealed that they were mostly related to the cytoskeleton, transcription, signal transduction, and cell cycle. Fuzzy c-means clustering identified six temporal profiles of phosphorylation and a functional module composed of ATM-phosphorylated proteins related to genotoxic stress. Pathway enrichment analysis defined mTOR as the most overrepresented pathway. We showed that mTOR complex 1 and 2 were required for S6 kinase and AKT activation, respectively. Comparison with a published phosphoproteome of Salmonella typhimuriuminfected cells revealed a large subset of coregulated phosphoproteins. Finally, we showed that S. flexneri effector OspF affected the phosphorylation of several hundred proteins, thereby demonstrating the wide-reaching impact of a single bacterial effector on the host signaling network.
机译:肠侵袭性细菌弗氏志贺氏菌侵入人的肠上皮。在感染过程中,几种注射的效应蛋白促进细菌内在化,并干扰多种宿主细胞反应。为了获得感染期间宿主信号转导的系统级概述,我们通过液相色谱串联质谱分析了蛋白质磷酸化的整体动力学,并确定了在感染最初几个小时内发生磷酸化变化的数百种蛋白质。功能性生物信息学分析表明,它们主要与细胞骨架,转录,信号转导和细胞周期有关。模糊c均值聚类确定了六个时间的磷酸化轮廓和一个功能模块,该模块由与遗传毒性应激相关的ATM磷酸化蛋白组成。途径富集分析将mTOR定义为最具代表性的途径。我们显示mTOR复合物1和2是S6激酶和AKT激活所必需的。与已公布的鼠伤寒沙门氏菌感染细胞的磷酸化蛋白质组进行比较,发现有大量的核心化磷蛋白。最后,我们表明弗氏链球菌效应物OspF影响了数百种蛋白质的磷酸化,从而证明了单个细菌效应物对宿主信号网络的广泛影响。

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