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Role of Hfq in iron-dependent and -independent gene regulation in Neisseria meningitidis

机译:HFQ在脑内脑奈尼菌的铁依赖性和依赖性基因调控中的作用

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摘要

In Neisseria meningitidis, iron-responsive gene regulation is mediated primarily by the ferric uptake regulator (Fur) protein. When complexed with iron, Fur represses gene expression by preventing transcription initiation. Fur can also indirectly activate gene expression via the repression of regulatory small RNAs (sRNA). One such Fur- and iron-regulated sRNA, NrrF, was previously identified in N. meningitidis and shown to repress expression of the sdhA and sdhC genes encoding subunits of the succinate dehydrogenase complex. In the majority of Gram-negative bacteria, sRNA-mediated regulation requires a cofactor RNA-binding protein (Hfq) for proper gene regulation and stabilization. In this study, we examined the role of Hfq in NrrF-mediated regulation of the succinate dehydrogenase genes in N. meningitidis and the effect of an hfq mutation on iron-responsive gene regulation more broadly. We first demonstrated that the stability of NrrF, as well as the regulation of sdhC and sdhA in vivo, was unaltered in the hfq mutant. Secondly, we established that iron-responsive gene regulation of the Fur-regulated sodB gene was dependent on Hfq. Finally, we demonstrated that in N. meningitidis, Hfq functions in a global manner to control expression of many ORFs and intergenic regions via iron-independent mechanisms. Collectively these studies demonstrate that in N. meningitidis, iron- and NrrF-mediated regulation of sdhC and sdhA can occur independently of Hfq, although Hfq functions more globally to control regulation of other N. meningitidis genes primarily by iron-independent mechanisms.
机译:在脑膜炎脑奈尼虫病中,铁响应基因调节主要由丙铁吸收调节剂(毛皮)蛋白介导。当用铁复合时,通过防止转录开始,毛皮抑制基因表达。毛皮还可以通过抑制调节小RNA(SRNA)来间接激活基因表达。先前在N. Meningitidis中鉴定出一种这样的毛虫和铁调节的SRNA,NRRF,并显示为抑制编码琥珀酸脱氢酶复合物的亚基的SDHA和SDHC基因的表达。在大多数革兰氏阴性细菌中,SRNA介导的调节需要辅因子RNA结合蛋白(HFQ),以适当的基因调节和稳定化。在这项研究中,我们研究了HFQ在NRRF介导的NRRF介导的调节中的作用,培养芽孢杆菌在N.脑膜炎霉菌中的调节和HFQ突变更广泛地对铁响应基因调节的影响。我们首先表明NRRF的稳定性以及体内SDHC和SDHA的调节,在HFQ突变体中未被干扰。其次,我们确实确定了毛虫调节SODB基因的铁响应基因调节依赖于HFQ。最后,我们证明,在N. Meningitidis中,HFQ以全球性的方式用来通过无关的机制控制许多ORF和基因因子的表达。总体上这些研究表明,在N.脑膜炎,铁和NRRF介导的SDHC和SDHA调节中可以独立于HFQ发生,尽管HFQ功能更加全球,以控制主要通过铁无关机制的其他N.脑膜炎基因的调控。

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