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Genetic Evidence that Legionella pneumophila RpoS Modulates Expression of the Transmission Phenotype in Both the Exponential Phase and the Stationary Phase

机译:嗜肺军团菌RpoS调节指数期和固定期的传播表型表达的遗传证据。

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摘要

The opportunistic pathogen Legionella pneumophila alternates between two states: replication within phagocytes and transmission between host amoebae or macrophages. In broth cultures that model this life cycle, during the replication period, CsrA inhibits expression of transmission traits. When nutrients become limiting, the alarmone (p)ppGpp accumulates and the sigma factors RpoS and FliA and the positive activators LetA/S and LetE promote differentiation to the transmissible form. Here we show that when cells enter the postexponential growth phase, RpoS increases expression of the transmission genes fliA, flaA, and mip, factors L. pneumophila needs to establish a new replication niche. In contrast, in exponential (E)-phase cells whose (p)ppGpp levels are low, rpoS inhibits expression of transmission traits, on the basis of three separate observations. First, rpoS RNA levels peak in the E phase, suggestive of a role for RpoS during replication. Second, in multiple copies, rpoS decreases the amounts of csrA, letE, fliA, and flaA transcripts and inhibits the transmission traits of motility, infectivity, and cytotoxicity. Third, rpoS blocks expression of cytotoxicity and motility by E-phase bacteria that have been induced to express the LetA activator ectopically. The data are discussed in the context of a model in which the alarmone (p)ppGpp enables RpoS to outcompete other sigma factors for binding to RNA polymerase to promote transcription of transmission genes, while LetA/S acts in parallel to relieve CsrA posttranscriptional repression of the transmission regulon. By coupling transcriptional and posttranscriptional control pathways, intracellular L. pneumophila could respond to stress by rapidly differentiating to a transmissible form.
机译:机会病原体肺炎军团菌在两种状态之间交替:吞噬细胞内复制和宿主变形虫或巨噬细胞之间的传播。在复制过程中,模拟此生命周期的肉汤培养物中,CsrA抑制传递性状的表达。当养分变得有限时,警报蛋白(p)ppGpp积累,σ因子RpoS和FliA以及正激活剂LetA / S和LetE促进分化为可传播形式。在这里,我们显示,当细胞进入指数后生长阶段时,RpoS会增加传播基因fliA,flaA和mip的表达,因此嗜肺性粒细胞(L. pneumophila)需要建立新的复制位。相反,在(p)ppGpp水平较低的指数(E)期细胞中,rpoS根据三项独立的观察结果抑制了传输性状的表达。首先,rpoS RNA水平在E期达到峰值,这暗示了RpoS在复制过程中的作用。其次,在多个副本中,rpoS减少了csrA,letE,fliA和flaA转录本的数量,并抑制了运动性,感染性和细胞毒性的传播特性。第三,rpoS阻断了E期细菌的细胞毒性和运动性表达,这种E期细菌已被诱导异位表达LetA激活剂。在模型的背景下讨论了数据,在该模型中,警报蛋白(p)ppGpp使RpoS竞争于其他σ因子以与RNA聚合酶结合,从而促进传输基因的转录,而LetA / S并行发挥作用来缓解CsrA转录后抑制传输规则。通过耦合转录和转录后控制途径,细胞内肺炎链球菌可以通过迅速分化为可传播形式来应对压力。

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