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RpoS与其他因子协同作用,在稳定期诱导嗜肺军团菌的毒力。

RpoS co-operates with other factors to induce Legionella pneumophila virulence in the stationary phase.

作者信息

Bachman M A, Swanson M S

机构信息

Department of Microbiology and Immunology, The University of Michigan Medical School, 6734 Medical Sciences II, Ann Arbor, MI 48109, USA.

出版信息

Mol Microbiol. 2001 Jun;40(5):1201-14. doi: 10.1046/j.1365-2958.2001.02465.x.

Abstract

Legionella pneumophila replicates within amoebae and macrophages and causes the severe pneumonia Legionnaires' disease. When broth cultures enter the post-exponential growth (PE) phase or experience amino acid limitation, L. pneumophila accumulates the stringent response signal (p)ppGpp and expresses traits likely to promote transmission to a new phagocyte. The hypothesis that a stringent response mechanism regulates L. pneumophila virulence was bolstered by our finding that the avirulent mutant Lp120 contains an internal deletion in the gene encoding the stationary phase sigma factor RpoS. To test directly whether RpoS co-ordinates virulence with stationary phase, isogenic wild-type, rpoS-120 and rpoS null mutant strains were constructed and analysed. PE phase L. pneumophila became cytotoxic by an RpoS-independent pathway, but their sodium sensitivity and maximal expression of flagellin required RpoS. Likewise, full induction of sodium sensitivity by experimentally induced (p)ppGpp synthesis required RpoS. To replicate efficiently in macrophages, L. pneumophila used both RpoS-dependent and -independent pathways. Like those containing the dotA type IV secretory apparatus mutant, phagosomes harbouring either rpoS or dotA rpoS mutants rapidly acquired the late endosomal protein LAMP-1, but not the lysosomal marker Texas red-ovalbumin. Together, the data support a model in which RpoS co-operates with other regulators to induce L. pneumophila virulence in the PE phase.

摘要

嗜肺军团菌在变形虫和巨噬细胞内复制,并引发严重的肺炎——军团病。当肉汤培养物进入指数生长后期(PE)阶段或经历氨基酸限制时,嗜肺军团菌会积累应急反应信号(p)ppGpp,并表达可能促进传播至新吞噬细胞的特性。无毒突变体Lp120在编码稳定期σ因子RpoS的基因中存在内部缺失,我们的这一发现支持了应急反应机制调节嗜肺军团菌毒力的假说。为了直接测试RpoS是否在稳定期协调毒力,构建并分析了同基因的野生型、rpoS - 120和rpoS缺失突变体菌株。PE期嗜肺军团菌通过一条不依赖RpoS的途径变得具有细胞毒性,但其对钠的敏感性和鞭毛蛋白的最大表达需要RpoS。同样,通过实验诱导(p)ppGpp合成来完全诱导钠敏感性也需要RpoS。为了在巨噬细胞中高效复制,嗜肺军团菌使用了依赖RpoS和不依赖RpoS的途径。与含有dotA IV型分泌装置突变体的情况一样,含有rpoS或dotA rpoS突变体的吞噬体迅速获得晚期内体蛋白LAMP - 1,但没有获得溶酶体标记物德克萨斯红 - 卵清蛋白。总之,这些数据支持了一个模型,即RpoS与其他调节因子协同作用,在PE期诱导嗜肺军团菌的毒力。

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