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Functional impact of mutational activation on the Listeria monocytogenes central virulence regulator PrfA

机译:突变激活对李斯特菌单核细胞增生中央毒力调节器PRFA的功能影响

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The transcriptional activator PrfA is required for the expression of virulence factors necessary for Listeria monocytogenes pathogenesis. PrfA is believed to become activated following L. monocytogenes entry into the cytosol of infected host cells, resulting in the induction of target genes whose products are required for bacterial intracellular growth and cell-to-cell spread. Several mutations have been identified that appear to lock PrfA into its highly activated cytosolic form (known as prfA* mutations). In this study PrfA and five PrfA* mutant proteins exhibiting differing degrees of activity were purified and analysed to define the influences of the mutations on distinct aspects of PrfA activity. Based on limited proteolytic digestion, conformational changes were detected for the PrfA* mutant proteins in comparison to wild-type PrfA. For all but one mutant (PrfA Y63C), the DNA binding affinity as measured by electophoretic mobility shift assay appeared to directly correlate with levels of PrfA mutational activation, such that the high-activity mutants exhibited the largest increases in DNA binding affinity and moderately activated mutants exhibited more moderate increases. Surprisingly, the ability of PrfA and PrfA* mutants to form dimers in solution appeared to inversely correlate with levels of PrfA-dependent gene expression. Based on comparisons of protein activity and structural similarities with PrfA family members Crp and CooA, the prfA* mutations modify distinct aspects of PrfA activity that include DNA binding and protein–protein interactions.
机译:转录活化剂PRFA是表达李斯特菌单核细胞增生的毒力因子所必需的毒力因子所必需的。 PRFA被认为在L.单核细胞化进入感染宿主细胞的细胞溶胶中被激活,导致靶基因的诱导,其产品需要细菌细胞内生长和细胞对细胞扩散。已经确定了几种突变,其似乎将PRFA锁定成其高活性的细胞溶质形式(称为PRFA *突变)。在本研究中,纯化并分析了表现出不同活性程度的5个PRFA *突变蛋白以定义突变对PRFA活性的独特方面的影响。基于有限的蛋白水解消解,与野生型PRFA相比,检测PRFA *突变蛋白的构象变化。对于所有但一个突变体(PRFA Y63C),通过电子迁移率移位测定的DNA结合亲和力似乎与PRFA突变激活的水平直接相关,使得高活性突变体表现出DNA结合亲和力和中度活化的最大增加突变体表现出更温和的增加。令人惊讶的是,PRFA和PRFA *突变体在溶液中形成二聚体的能力似乎与PRFA依赖性基因表达的水平相反。基于与PRFA家族成员CRP和COOA的蛋白质活性和结构相似性的比较,PRFA *突变改变了PRFA活性的独特方面,包括DNA结合和蛋白质 - 蛋白质相互作用。

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