首页> 外文OA文献 >A Novel Fur- and Iron-Regulated Small RNA, NrrF, Is Required for Indirect Fur-Mediated Regulation of the sdhA and sdhC Genes in Neisseria meningitidis▿ †
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A Novel Fur- and Iron-Regulated Small RNA, NrrF, Is Required for Indirect Fur-Mediated Regulation of the sdhA and sdhC Genes in Neisseria meningitidis▿ †

机译:脑膜炎奈瑟氏球菌中sdhA和sdhC基因的间接毛皮介导调控需要新型的毛皮和铁调控小RNA NrrF。

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摘要

Iron is both essential for bacterial growth and toxic at higher concentrations; thus, iron homeostasis is tightly regulated. In Neisseria meningitidis the majority of iron-responsive gene regulation is mediated by the ferric uptake regulator protein (Fur), a protein classically defined as a transcriptional repressor. Recently, however, microarray studies have identified a number of genes in N. meningitidis that are iron and Fur activated, demonstrating a new role for Fur as a transcriptional activator. Since Fur has been shown to indirectly activate gene transcription through the repression of small regulatory RNA molecules in other organisms, we hypothesized that a similar mechanism could account for Fur-dependent, iron-activated gene transcription in N. meningitidis. In this study, we used a bioinformatics approach to screen for the presence of Fur-regulated small RNA molecules in N. meningitidis MC58. This screen identified one small RNA, herein named NrrF (for neisserial regulatory RNA responsive to iron [Fe]), which was demonstrated to be both iron responsive and Fur regulated and which has a well-conserved orthologue in N. gonorrhoeae. In addition, this screen identified a number of other likely, novel small RNA transcripts. Lastly, we utilized a new bioinformatics approach to predict regulatory targets of the NrrF small RNA. This analysis led to the identification of the sdhA and sdhC genes, which were subsequently demonstrated to be under NrrF regulation in an nrrF mutant. This study is the first report of small RNAs in N. meningitidis and the first to use a bioinformatics approach to identify, a priori, regulatory targets of a small RNA.
机译:铁既是细菌生长必不可少的元素,也是高浓度的有毒物质。因此,铁稳态被严格调节。在脑膜炎奈瑟氏球菌中,大多数铁反应性基因调节是由铁摄取调节蛋白(Fur)介导的,该蛋白通常定义为转录阻遏物。然而,最近,微阵列研究已鉴定出脑膜炎奈瑟氏球菌中许多被铁和毛皮激活的基因,证明了毛皮作为转录激活因子的新作用。由于已显示出Fur可通过抑制其他生物中的小调节RNA分子间接激活基因转录,因此我们推测类似的机制可解释脑膜炎奈瑟氏球中Fur依赖性的铁激活基因转录。在这项研究中,我们使用了生物信息学方法来筛选脑膜炎奈瑟氏球菌MC58中Fur调节的小RNA分子的存在。该筛选鉴定了一种小RNA,本文称为NrrF(用于对铁[Fe]有反应的神经调节RNA),该RNA被证明具有铁反应性和Fur调节作用,并且在淋病奈瑟氏球菌中具有保守的直系同源物。此外,该屏幕还鉴定了许多其他可能的新颖小RNA转录物。最后,我们利用一种新的生物信息学方法来预测NrrF小RNA的调控靶标。该分析导致鉴定了sdhA和sdhC基因,随后证实它们在nrrF突变体中处于NrrF调控之下。这项研究是脑膜炎奈瑟氏球菌中小RNA的第一个报道,也是第一个使用生物信息学方法先验鉴定小RNA调控靶标的报告。

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