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首页> 外文期刊>Archives of Microbiology >Artificial sRNAs activating the Gac/Rsm signal transduction pathway in Pseudomonas fluorescens
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Artificial sRNAs activating the Gac/Rsm signal transduction pathway in Pseudomonas fluorescens

机译:人工sRNA激活荧光假单胞菌Gac / Rsm信号转导途径

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In Pseudomonas fluorescens CHA0, the synthesis of antifungal compounds is post-transcriptionally activated by the Gac/Rsm cascade. The two-component system GacS/GacA promotes transcription of three small regulatory RNAs (i.e., sRNAs), RsmX, RsmY, and RsmZ, which remove the regulatory proteins RsmA and RsmE from the ribosome-binding sites of exoproduct-related mRNAs. The GacS/GacA-dependent accumulation of RsmX/Y/Z and formation of RsmX/Y/Z-RsmA/E complexes relieve mRNA translational repression. Other bacteria as E. coli and Vibrio spp. utilize similar sRNA–protein based systems to adjust mRNA translation (e.g., the E. coli Csr system for carbon storage, motility and biofilm regulation). The Rsm/Csr sRNAs are remarkably similar in that they contain several stem-loops with an invariant GGA trinucleotide exposed in the hairpin loop that would be the characteristic structural-sequence motifs relevant for sRNA activity and stability. Here it is shown that the dysfunctional Gac/Rsm cascade of P. fluorescens ΔrsmXYZ mutants could be restored by appropriate transcription levels of artificial genes encoding RNAs with unrelated primary sequence but with two or more hairpins displaying the RsmA/E binding motifs. The results support the hypothesis that the molecular mimicry of Rsm/Csr sRNAs is based on proper secondary structures that expose critical binding motifs irrespective of their overall sequence.
机译:在荧光假单胞菌CHA0中,抗真菌化合物的合成被Gac / Rsm级联转录后激活。两组分系统GacS / GacA促进三个小调节RNA(即sRNA),RsmX,RsmY和RsmZ的转录,后者从外产物相关mRNA的核糖体结合位点除去了调节蛋白RsmA和RsmE。 RsmX / Y / Z的GacS / GacA依赖性积累和RsmX / Y / Z-RsmA / E复合物的形成可缓解mRNA的翻译抑制。其他细菌如大肠杆菌和弧菌。利用类似的基于sRNA-蛋白质的系统来调节mRNA的翻译(例如,用于碳存储,运动性和生物膜调节的大肠杆菌Csr系统)。 Rsm / Csr sRNA非常相似,因为它们包含几个茎环,在发夹环中带有不变的GGA三核苷酸,这将是与sRNA活性和稳定性相关的特征性结构序列基序。此处显示荧光假单胞菌ΔrsmXYZ突变体的功能失调的Gac / Rsm级联可以通过编码具有无关一级序列但具有两个或更多个表现RsmA / E结合基序的RNA的人工基因的适当转录水平来恢复。结果支持以下假设:Rsm / Csr sRNA的分子模拟基于适当的二级结构,该二级结构暴露了关键的结合基序,而与它们的整体序列无关。

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