首页> 外文期刊>Journal of bacteriology >Bacteriocin Activity of Streptococcus pneumoniae Is Controlled by the Serine Protease HtrA via Posttranscriptional Regulation
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Bacteriocin Activity of Streptococcus pneumoniae Is Controlled by the Serine Protease HtrA via Posttranscriptional Regulation

机译:丝氨酸蛋白酶HtrA通过转录后调控来控制肺炎链球菌的细菌活性。

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The blp locus of a type 6A strain of Streptococcus pneumoniae encodes a two-peptide bacteriocin, pneumocin MN, which mediates intraspecies competition during mouse nasopharyngeal colonization. This locus is regulated by a quorum-sensing mechanism consisting of a dedicated two-component regulatory system and a peptide pheromone. Like most clinical isolates, this type 6A strain can be separated into opaque and transparent colony variants, each playing a different role during pneumococcal infection. In this study, we show that the blp locus is differentially regulated at the posttranscriptional level in pneumococcal opacity variants. Transparent and opaque variants produce equivalent amounts of blpMNPO transcript when stimulated with a synthetic pheromone, but transparent variants have no pneumocin MN-mediated inhibitory activity while opaque variants produce large zones of inhibitory activity. The differential regulation in opacity variants is driven by the two-component regulatory system CiaRH via its regulation of the serine protease HtrA. Transparent mutants deficient in CiaH or HtrA show increased pneumocin MN-mediated inhibition. In addition, these mutants demonstrate alterations in their dose response to a synthetic peptide pheromone, suggesting that HtrA activity impacts pneumocin MN production at the level of signaling. This, in addition to its known effects on competence, suggests that HtrA is a pleiotropic regulator whose protease activity affects several important bacterial pathways. The complex regulation of pneumocins may allow the pneumococcus to reserve the secretion of active peptides for situations where the benefit of their inhibitory activity outweighs the cost of their production.
机译:6em型肺炎链球菌株的 blp 基因座编码一种两肽细菌素,肺炎球菌素MN,在小鼠鼻咽菌落定殖过程中介导种内竞争。该基因座由群体感应机制调控,该机制由专用的两组分调控系统和肽信息素组成。像大多数临床分离株一样,这种6A型菌株可以分为不透明和透明菌落变体,每种变体在肺炎球菌感染过程中起着不同的作用。在这项研究中,我们显示在肺炎球菌混浊度变异体中,在转录后水平上, blp 基因座受到差异调节。透明和不透明变体在用合成信息素刺激时产生等量的 blpMNPO 转录本,但是透明变体没有肺炎球菌MN介导的抑制活性,而不透明变体则产生较大的抑制活性区。两组分调节系统CiaRH通过其对丝氨酸蛋白酶HtrA的调节来驱动不透明度变体中的差异调节。缺乏CiaH或HtrA的透明突变体显示增加的肺炎球菌MN介导的抑制作用。另外,这些突变体显示出它们对合成肽信息素的剂量反应的改变,表明HtrA活性在信号水平上影响肺炎球蛋白MN的产生。除了其对能力的已知影​​响外,这还表明HtrA是一种多效调节剂,其蛋白酶活性影响几种重要的细菌途径。肺炎球菌的复杂调控可能使肺炎球菌在其抑制活性的益处超过其生产成本的情况下保留活性肽的分泌。

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