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首页> 外文期刊>Molecular Microbiology >The two-component system ArlS-ArlR is a regulator of virulence gene expression in Staphylococcus aureus.
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The two-component system ArlS-ArlR is a regulator of virulence gene expression in Staphylococcus aureus.

机译:两组分系统ArlS-ArlR是金黄色葡萄球菌中毒力基因表达的调节剂。

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Staphylococcus aureus is a major human pathogen that produces many virulence factors in a temporally regulated manner controlled by at least two global virulence regulatory loci (agr and sarA). We identified previously a two-component system, ArlS-ArlR, that modifies the activity of extracellular serine protease and may be involved in virulence regulation. Here, we show that mutations in either arlR or arlS increase the production of secreted proteins [alpha-toxin (Hla), beta-haemolysin, lipase, coagulase, serine protease (Ssp)] and especially protein A (Spa). Furthermore, the pattern of proteins secreted by both mutants was strikingly different from that of the wild-type strain. Transcriptional fusions showed that expression of hla, ssp and spa was higher in both mutants than in the wild-type strain, indicating that the arl operon decreases the production of virulence factors by downregulating the transcription of their genes. The arl mutation did not change spa expression in an agrA mutant or in a sarA mutant, suggesting that both the sarA and the agr loci are required for the action of arl on spa. Northern blot analyses indicated that the arl mutation increased the synthesis of both RNA II and RNA III, but decreased sarA transcription. Finally, arl was not autoregulated, but its expression was stimulated by agr and sarA. These results suggest that the Arl system interacts with both agr and sarA regulatory loci to modulate the virulence regulation network.
机译:金黄色葡萄球菌是主要的人类病原体,其以时间调控的方式产生多种毒力因子,该方式由至少两个全球毒力调控位点(agr和sarA)控制。我们以前确定了一种两组分系统,ArlS-ArlR,它可以修饰细胞外丝氨酸蛋白酶的活性,并可能参与毒力调节。在这里,我们显示arlR或arlS中的突变会增加分泌蛋白[α-毒素(Hla),β-溶血素,脂肪酶,凝固酶,丝氨酸蛋白酶(Ssp)]的产生,尤其是蛋白A(Spa)。此外,两个突变体分泌的蛋白质的模式与野生型菌株显着不同。转录融合显示,在两个突变体中,hla,ssp和spa的表达均高于野生型菌株,表明arl操纵子通过下调其基因的转录而降低了毒力因子的产生。 arl突变不会改变agrA突变体或sarA突变体中spa的表达,这表明sarA和agr基因座都需要arl对spa的作用。 Northern印迹分析表明,arl突变增加了RNA II和RNA III的合成,但降低了sarA转录。最后,arl没有被自动调节,但是其表达受到agr和sarA的刺激。这些结果表明,Arl系统与agr和sarA调节基因座相互作用,以调节毒力调节网络。

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