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A nitric oxide regulated small RNA controls expression of genes involved in redox homeostasis in Bacillus subtilis

机译:一氧化氮调节的小RNA控制枯草芽孢杆菌中参与氧化还原稳态的基因的表达

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摘要

RsaE is the only known trans-acting small regulatory RNA (sRNA) besides the ubiquitous 6S RNA that is conserved between the human pathogen Staphylococcus aureus and the soil-dwelling Firmicute Bacillus subtilis. Although a number of RsaE targets are known in S. aureus, neither the environmental signals that lead to its expression nor its physiological role are known. Here we show that expression of the B. subtilis homolog of RsaE is regulated by the presence of nitric oxide (NO) in the cellular milieu. Control of expression by NO is dependent on the ResDE two-component system in B. subtilis and we determined that the same is true in S. aureus. Transcriptome and proteome analyses revealed that many genes with functions related to oxidative stress and oxidation-reduction reactions were up-regulated in a B. subtilis strain lacking this sRNA. We have thus renamed it RoxS. The prediction of RoxS-dependent mRNA targets also suggested a significant enrichment for mRNAs related to respiration and electron transfer. Among the potential direct mRNA targets, we have validated the ppnKB mRNA, encoding an NAD(+)/NADH kinase, both in vivo and in vitro. RoxS controls both translation initiation and the stability of this transcript, in the latter case via two independent pathways implicating RNase Y and RNase III. Furthermore, RNase Y intervenes at an additional level by processing the 50 end of the RoxS sRNA removing about 20 nucleotides. Processing of RoxS allows it to interact more efficiently with a second target, the sucCD mRNA, encoding succinyl-CoA synthase, thus expanding the repertoire of targets recognized by this sRNA.
机译:除了在人病原体金黄色葡萄球菌和土壤中的枯草芽孢杆菌枯草芽孢杆菌之间保存的普遍存在的6S RNA以外,RsaE是唯一已知的反式作用小调控RNA(sRNA)。尽管在金黄色葡萄球菌中已知许多RsaE靶标,但导致其表达的环境信号及其生理作用均未知。在这里,我们显示RsaE枯草芽孢杆菌同源物的表达受细胞环境中一氧化氮(NO)的存在调节。 NO的表达控制取决于枯草芽孢杆菌中的ResDE两组分系统,我们确定在金黄色葡萄球菌中也是如此。转录组和蛋白质组分析表明,在缺乏该sRNA的枯草芽孢杆菌菌株中,许多具有与氧化应激和氧化还原反应相关的功能的基因上调。因此,我们将其重命名为RoxS。 RoxS依赖性mRNA靶标的预测也表明与呼吸作用和电子转移有关的mRNA大量富集。在潜在的直接mRNA靶标中,我们已经在体内和体外验证了ppnKB mRNA,它编码NAD(+)/ NADH激酶。 RoxS通过两个独立的途径牵涉RNase Y和RNase III来控制翻译起始和该转录物的稳定性。此外,RNase Y通过处理RoxS sRNA的50个末端去除了大约20个核苷酸,从而以更高的水平进行干预。 RoxS的加工使其能够更有效地与编码琥珀酰CoA合酶的第二个靶标sucCD mRNA相互作用,从而扩展了该sRNA识别的靶标库。

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