首页> 外文期刊>Microbiology >The pmrF polymyxin-resistance operon of Yersinia pseudotuberculosis is upregulated by the PhoP–PhoQ two-component system but not by PmrA–PmrB, and is not required for virulence
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The pmrF polymyxin-resistance operon of Yersinia pseudotuberculosis is upregulated by the PhoP–PhoQ two-component system but not by PmrA–PmrB, and is not required for virulence

机译:yersinia伪核素愈伤症的PMRF多粘物抗性操纵子由PHOP-PHOQ双组分系统上调,但不是通过PMRA-PMRB来上调,并且不需要毒力

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The Yersinia pseudotuberculosis chromosome contains a seven-gene polycistronic unit (the pmrF operon) whose products share extensive homologies with their pmrF counterparts in Salmonella enterica serovar Typhimurium (S. typhimurium), another Gram-negative bacterial enteropathogen. This gene cluster is essential for addition of 4-aminoarabinose to the lipid moiety of LPS, as demonstrated by MALDI-TOF mass spectrometry of lipid A from both wild-type and pmrF-mutated strains. As in S. typhimurium, 4-aminoarabinose substitution of lipid A contributes to in vitro resistance of Y. pseudotuberculosis to the antimicrobial peptide polymyxin B. Whereas pmrF expression in S. typhimurium is mediated by both the PhoP–PhoQ and PmrA–PmrB two-component regulatory systems, it appears to be PmrA–PmrB-independent in Y. pseudotuberculosis, with the response regulator PhoP interacting directly with the pmrF operon promoter region. This result reveals that the ubiquitous PmrA–PmrB regulatory system controls different regulons in distinct bacterial species. In addition, pmrF inactivation in Y. pseudotuberculosis has no effect on bacterial virulence in the mouse, again in contrast to the situation in S. typhimurium. The marked differences in pmrF operon regulation in these two phylogenetically close bacterial species may be related to their dissimilar lifestyles.
机译:yersinia pseudotuberculosis染色体含有七种基因多函数单元(PMRF型摩押贷款),其产品与其PMRF对应于Salmonella肠道毒蕈醋酰莫硫核(S. typhimurium),另一个革兰氏阴性细菌肠道病理学分享着广泛的同源物。该基因簇对于向LPS的脂质部分添加4-氨基氨基糖至LPS的脂质部分是必不可少的,如来自野生型和PMRF突变的菌株的脂质A的MALDI-TOF质谱。如在S. Typhimurium,4-氨基喹啉糖代替脂质A含量为Y.Pseudotubliss对抗微生物肽多粘蛋白B的体外抗性有助于抗微生物肽B.,而PMRF表达在S.鼠脊酮中的培养基-Phoq和PMRB-PMRB两种 - 组件调节系统,它似乎是PMRA-PMRB无关的,在Y.Pseudotuberculosis中,响应调节剂PHOP直接与PMRF操纵子区域相互作用。该结果表明,普遍存在的PMRA-PMRB调节系统在不同的细菌种类中控制不同的调节件。此外,在Y.Pseudotuberculosis中的PMRF失活对小鼠的细菌毒力没有影响,再次与S. Typhimurium的情况相反。 PMRF操纵子调节在这两个系统近期细菌种类中的显着差异可能与其不同的生活方式有关。

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