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PepO, a CovRS-controlled endopeptidase, disrupts Streptococcus pyogenes quorum sensing

机译:PevO,一种受CovRS控制的内肽酶,可破坏化脓性链球菌的群体感应

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摘要

Group A Streptococcus (GAS, Streptococcus pyogenes) is a human-restricted pathogen with a capacity to both colonize asymptomatically and cause illnesses ranging from pharyngitis to necrotizing fasciitis. An understanding of how and when GAS switches between genetic programs governing these different lifestyles has remained an enduring mystery and likely requires carefully tuned environmental sensors to activate and silence genetic schemes when appropriate. Herein, we describe the relationship between the Control of Virulence (CovRS, CsrRS) two-component system and the Rgg2/3 quorum-sensing pathway. We demonstrate that responses of CovRS to the stress signals Mg2+ and a fragment of the antimicrobial peptide LL-37 result in modulated activity of pheromone signaling of the Rgg2/3 pathway through a means of proteolysis of SHP peptide pheromones. This degradation is mediated by the cytoplasmic endopeptidase PepO, which is the first identified enzymatic silencer of an RRNPP-type quorum-sensing pathway. These results suggest that under conditions in which the virulence potential of GAS is elevated (i.e. enhanced virulence gene expression), cellular responses mediated by the Rgg2/3 pathway are abrogated and allow individuals to escape from group behavior. These results also indicate that Rgg2/3 signaling is instead functional during non-virulent GAS lifestyles.
机译:A组链球菌(GAS,化脓性链球菌)是一种人类限制性病原体,能够无症状地定殖并引起从咽炎到坏死性筋膜炎的各种疾病。对GAS如何以及何时在控制这些不同生活方式的基因计划之间进行切换的理解一直是一个长期的谜,并且可能需要仔细调整环境传感器以在适当时激活和沉默基因计划。本文中,我们描述了毒力控制(CovRS,CsrRS)两组分系统与Rgg2 / 3群体感应途径之间的关系。我们证明,CovRS对应激信号Mg2 +和抗菌肽LL-37片段的响应通过SHP肽信息素的蛋白水解手段导致Rgg2 / 3途径的信息素信号传导的调节活性。这种降解是由细胞质内肽酶PepO介导的,PepO是RRNPP型群体感应途径的第一个酶促沉默子。这些结果表明,在GAS的毒力潜力升高的条件下(即,毒力基因表达增强),由Rgg2 / 3途径介导的细胞应答被消除,并允许个体逃避群体行为。这些结果还表明,在无毒的GAS生活方式中,Rgg2 / 3信号转而起作用。

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