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Unprecedented tunability of riboswitch structure and regulatory function by sub-millimolar variations in physiological Mg2+

机译:通过生理MG2 +的亚毫米变化来前所未有的Riboswitch结构和监管功能的可调性。

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Riboswitches are cis-acting regulatory RNA biosensors that rival the efficiency of those found in proteins. At the heart of their regulatory function is the formation of a highly specific aptamer-ligand complex. Understanding how these RNAs recognize the ligand to regulate gene expression at physiological concentrations of Mg2+ ions and ligand is critical given their broad impact on bacterial gene expression and their potential as antibiotic targets. In this work, we used single-molecule FRET and biochemical techniques to demonstrate that Mg2+ ions act as fine-tuning elements of the amino acid-sensing lysC aptamer's ligand-free structure in the mesophile Bacillus subtilis. Mg2+ interactions with the aptamer produce encounter complexes with strikingly different sensitivities to the ligand in different, yet equally accessible, physiological ionic conditions. Our results demonstrate that the aptamer adapts its structure and folding landscape on a Mg2+-tunable scale to efficiently respond to changes in intracellular lysine of more than two orders of magnitude. The remarkable tunability of the lysC aptamer by sub-millimolar variations in the physiological concentration of Mg2+ ions suggests that some single-aptamer riboswitches have exploited the coupling of cellular levels of ligand and divalent metal ions to tightly control gene expression.
机译:Riboswitches是CIS作用的调节RNA生物传感器,其竞争蛋白质中存在的效率。在其调节功能的核心,是形成高度特异性的Aptamer-LigAnd复合物。了解这些RNA如何识别配体以调节Mg 2 +离子的生理浓度的基因表达,鉴于它们对细菌基因表达的广泛影响及其作为抗生素靶标的潜力至关重要。在这项工作中,我们使用单分子褶皱和生物化学技术来证明Mg2 +离子作为氨基酸感测的Lysc Aptamer在中间芽孢杆菌中的无氨基酸的韧带的韧带结构的微调元素。 Mg2 +与适体的相互作用产生与不同又同样可接近的生理离子条件的配体具有显着不同的敏感性的遇到复合物。我们的结果表明,Aptamer在MG2 + -Tucable规模上适应其结构和折叠景观,以有效地响应细胞内赖氨酸的变化超过两个数量级。通过Mg2 +离子的生理浓度的亚毫摩尔变化的LysC适体的显着可调性表明,一些单适体核糖织物已经利用了配体和二价金属离子的细胞水平的偶联以紧密控制基因表达。

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