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空肠弯曲杆菌CsrA调节代谢和毒力相关蛋白,是小鼠定殖所必需的。

Campylobacter jejuni CsrA Regulates Metabolic and Virulence Associated Proteins and Is Necessary for Mouse Colonization.

作者信息

Fields Joshua A, Li Jiaqi, Gulbronson Connor J, Hendrixson David R, Thompson Stuart A

机构信息

Department of Medicine, Division of Infectious Diseases, Augusta University, Augusta, GA, 30912, United States of America.

Department of Natural Sciences, Georgia Military College - Augusta, Augusta, GA, 30907, United States of America.

出版信息

PLoS One. 2016 Jun 3;11(6):e0156932. doi: 10.1371/journal.pone.0156932. eCollection 2016.

DOI:10.1371/journal.pone.0156932
PMID:27257952
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4892619/
Abstract

Campylobacter jejuni infection is a leading bacterial cause of gastroenteritis and a common antecedent leading to Gullian-Barré syndrome. Our previous data suggested that the RNA-binding protein CsrA plays an important role in regulating several important phenotypes including motility, biofilm formation, and oxidative stress resistance. In this study, we compared the proteomes of wild type, csrA mutant, and complemented csrA mutant C. jejuni strains in an effort to elucidate the mechanisms by which CsrA affects virulence phenotypes. The putative CsrA regulon was more pronounced at stationary phase (111 regulated proteins) than at mid-log phase (25 regulated proteins). Proteins displaying altered expression in the csrA mutant included diverse metabolic functions, with roles in amino acid metabolism, TCA cycle, acetate metabolism, and various other cell processes, as well as pathogenesis-associated characteristics such as motility, chemotaxis, oxidative stress resistance, and fibronectin binding. The csrA mutant strain also showed altered autoagglutination kinetics when compared to the wild type. CsrA specifically bound the 5' end of flaA mRNA, and we demonstrated that CsrA is a growth-phase dependent repressor of FlaA expression. Finally, the csrA mutant exhibited reduced ability to colonize in a mouse model when in competition with the wild type, further underscoring the role of CsrA in C. jejuni colonization and pathogenesis.

摘要

空肠弯曲菌感染是导致肠胃炎的主要细菌病因,也是引发格林-巴利综合征的常见诱因。我们之前的数据表明,RNA结合蛋白CsrA在调节包括运动性、生物膜形成和氧化应激抗性等多种重要表型方面发挥着重要作用。在本研究中,我们比较了野生型、csrA突变体和互补的csrA突变体空肠弯曲菌菌株的蛋白质组,以阐明CsrA影响毒力表型的机制。假定的CsrA调控子在稳定期(111种受调控蛋白)比在对数中期(25种受调控蛋白)更为明显。在csrA突变体中表达发生改变的蛋白质包括多种代谢功能,涉及氨基酸代谢、三羧酸循环、乙酸代谢和各种其他细胞过程,以及与发病机制相关的特征,如运动性、趋化性、氧化应激抗性和纤连蛋白结合。与野生型相比,csrA突变体菌株还表现出自凝动力学的改变。CsrA特异性结合flaA mRNA的5'端,并且我们证明CsrA是FlaA表达的生长阶段依赖性阻遏物。最后,当与野生型竞争时,csrA突变体在小鼠模型中的定殖能力降低,这进一步强调了CsrA在空肠弯曲菌定殖和发病机制中的作用。

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本文引用的文献

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The post-transcriptional regulatory system CSR controls the balance of metabolic pools in upper glycolysis of Escherichia coli.转录后调控系统CSR控制大肠杆菌上糖酵解中代谢池的平衡。
Mol Microbiol. 2016 May;100(4):686-700. doi: 10.1111/mmi.13343. Epub 2016 Feb 26.
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KEGG as a reference resource for gene and protein annotation.KEGG作为基因和蛋白质注释的参考资源。
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Pancreatic amylase is an environmental signal for regulation of biofilm formation and host interaction in Campylobacter jejuni.
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CemR atypical response regulator impacts energy conversion in .CemR 非典型应答调节子影响. 中的能量转换。
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Helicobacter pylori Modulates Heptose Metabolite Biosynthesis and Heptose-Dependent Innate Immune Host Cell Activation by Multiple Mechanisms.幽门螺旋杆菌通过多种机制调节庚糖代谢物的生物合成和庚糖依赖性固有免疫宿主细胞的激活。
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Identification and Regulatory Roles of a New Csr Small RNA from Arctic Pseudoalteromonas fuliginea BSW20308 in Temperature Responses.从北极假交替单胞菌 BSW20308 中鉴定出的一个新的 Csr 小 RNA 在温度响应中的调控作用。
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