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依赖于Hfq的小非编码RNA NrrF直接介导脑膜炎奈瑟菌中琥珀酸脱氢酶的依赖于Fur的正调控。

The Hfq-dependent small noncoding RNA NrrF directly mediates Fur-dependent positive regulation of succinate dehydrogenase in Neisseria meningitidis.

作者信息

Metruccio Matteo M E, Fantappiè Laura, Serruto Davide, Muzzi Alessandro, Roncarati Davide, Donati Claudio, Scarlato Vincenzo, Delany Isabel

机构信息

Novartis Vaccines, Via Fiorentina 1, 53100 Siena, Italy.

出版信息

J Bacteriol. 2009 Feb;191(4):1330-42. doi: 10.1128/JB.00849-08. Epub 2008 Dec 5.

Abstract

Previous microarray studies have suggested that an indirect mechanism of Fur regulation may be present in meningococcus at the posttranscriptional level through a small regulatory RNA (sRNA) system analogous to that of Escherichia coli and Pseudomonas aeruginosa. Recently, a Fur-regulated sRNA, NrrF, was identified that is involved in the iron regulation of the sdhA and sdhC succinate dehydrogenase genes. Here we report a detailed transcriptional analysis of the nrrF gene and show that NrrF is a Hfq-dependent sRNA. The Hfq protein mediates nrrF downregulation and Fur-dependent upregulation of the sdhCDAB operon, the major in vivo NrrF-regulated operon. NrrF forms a duplex in vitro with a region of complementarity overlapping the sdhDA mRNA junction. Furthermore, Hfq binds to NrrF in vitro and considerably enhances the efficiency of the interaction of the sRNA with the identified target. Our data suggest that Hfq-meditated binding of NrrF to the in vivo target in the sdhCDAB mRNA may cause the rapid degradation of the transcript, resulting in Fur-dependent positive regulation of succinate dehydrogenase. In addition, while the upregulation of sodB and fumB by Fur is dependent on the Hfq protein, it is unaffected in the nrrF knockout, which suggests that there is more than one sRNA regulator involved in iron homeostasis in meningococcus.

摘要

先前的微阵列研究表明,在脑膜炎奈瑟菌中,Fur调控可能存在一种间接机制,该机制在转录后水平通过一个类似于大肠杆菌和铜绿假单胞菌的小调控RNA(sRNA)系统发挥作用。最近,一种受Fur调控的sRNA,即NrrF被鉴定出来,它参与了琥珀酸脱氢酶基因sdhA和sdhC的铁调控。在此,我们报告了对nrrF基因的详细转录分析,并表明NrrF是一种依赖Hfq的sRNA。Hfq蛋白介导nrrF的下调以及琥珀酸脱氢酶操纵子(体内主要受NrrF调控的操纵子)的Fur依赖性上调。NrrF在体外与sdhDA mRNA连接区域的互补区域形成双链体。此外,Hfq在体外与NrrF结合,并显著提高了sRNA与已鉴定靶点相互作用的效率。我们的数据表明,Hfq介导的NrrF与sdhCDAB mRNA体内靶点的结合可能导致转录本的快速降解,从而导致琥珀酸脱氢酶的Fur依赖性正调控。此外,虽然Fur对sodB和fumB的上调依赖于Hfq蛋白,但在nrrF基因敲除中不受影响,这表明在脑膜炎奈瑟菌的铁稳态中涉及不止一种sRNA调节因子。

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