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CsrA对高度适应人类胃部的病原体幽门螺杆菌毒力和应激反应的全局调控

Global regulation of virulence and the stress response by CsrA in the highly adapted human gastric pathogen Helicobacter pylori.

作者信息

Barnard Faye M, Loughlin Michael F, Fainberg Hernan P, Messenger Michael P, Ussery David W, Williams Paul, Jenks Peter J

机构信息

Institute of Infections, Immunity and Inflammation, University of Nottingham, Nottingham, United Kingdom.

出版信息

Mol Microbiol. 2004 Jan;51(1):15-32. doi: 10.1046/j.1365-2958.2003.03788.x.

Abstract

Although successful and persistent colonization of the gastric mucosa depends on the ability to respond to changing environmental conditions and co-ordinate the expression of virulence factors during the course of infection, Helicobacter pylori possesses relatively few transcriptional regulators. We therefore investigated the contribution of the regulatory protein CsrA to global gene regulation in this important human pathogen. CsrA was necessary for full motility and survival of H. pylori under conditions of oxidative stress. Loss of csrA expression deregulated the oxidant-induced transcriptional responses of napA and ahpC, the acid induction of napA, cagA, vacA, the urease operon, and fur, as well as the heat shock responses of napA, groESL and hspR. Although the level of napA transcript was higher in the csrA mutant, its stability was similar in the wild-type and mutant strains, and less NapA protein was produced in the mutant strain. Finally, H. pylori strains deficient in the production of CsrA were significantly attenuated for virulence in a mouse model of infection. This work provides evidence that CsrA has a broad role in regulating the physiology of H. pylori in response to environmental stimuli, and may be important in facilitating adaptation to the different environments encountered during colonization of the gastric mucosa. Furthermore, CsrA appears to mediate its effects in H. pylori at the post-transcriptional level by influencing the processing and translation of target transcripts, with minimal effect on the stability of the target mRNAs.

摘要

尽管胃黏膜的成功且持续定植取决于应对不断变化的环境条件以及在感染过程中协调毒力因子表达的能力,但幽门螺杆菌拥有相对较少的转录调节因子。因此,我们研究了调节蛋白CsrA对这种重要人类病原体全局基因调控的作用。CsrA对于幽门螺杆菌在氧化应激条件下的完全运动性和存活是必需的。csrA表达缺失使napA和ahpC的氧化剂诱导转录反应、napA、cagA、vacA、脲酶操纵子和fur的酸诱导以及napA、groESL和hspR的热休克反应失调。尽管csrA突变体中napA转录本水平较高,但其在野生型和突变体菌株中的稳定性相似,且突变体菌株中产生的NapA蛋白较少。最后,在感染小鼠模型中,缺乏CsrA产生的幽门螺杆菌菌株的毒力显著减弱。这项工作提供了证据,表明CsrA在响应环境刺激调节幽门螺杆菌生理方面具有广泛作用,并且在促进适应胃黏膜定植过程中遇到的不同环境方面可能很重要。此外,CsrA似乎通过影响靶转录本的加工和翻译在转录后水平介导其在幽门螺杆菌中的作用,对靶mRNA的稳定性影响最小。

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