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首页> 外文期刊>Nucleic Acids Research >Attenuation of loop-receptor interactions with pseudoknot formation
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Attenuation of loop-receptor interactions with pseudoknot formation

机译:具有假结形成的环-受体相互作用的减弱

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摘要

RNA tetraloops can recognize receptors to mediate long-range interactions in stable natural RNAs. In vitro selected GNRA tetraloop/receptor interactions are usually more 'G/C-rich' than their 'A/U-rich' natural counterparts. They are not as widespread in nature despite comparable biophysical and chemical properties. Moreover, while AA, AC and GU dinucleotide platforms occur in natural GAAA/11 nt receptors, the AA platform is somewhat preferred to the others. The apparent preference for 'A/U-rich' GNRA/receptor interactions in nature might stem from an evolutionary adaptation to avoid folding traps at the level of the larger molecular context. To provide evidences in favor of this hypothesis, several riboswitches based on natural and artificial GNRA receptors were investigated in vitro for their ability to prevent inter-molecular GNRA/receptor interactions by trapping the receptor sequence into an alternative intra-molecular pseudoknot. Extent of attenuation determined by native gel-shift assays and co-transcriptional assembly is correlated to the G/C content of the GNRA receptor. Our results shed light on the structural evolution of natural long-range interactions and provide design principles for RNA-based attenuator devices to be used in synthetic biology and RNA nanobiotechnology.
机译:RNA四环可以识别受体,以介导稳定的天然RNA中的长距离相互作用。体外选择的GNRA四环/受体相互作用通常比其“富含A / U”的天然对应物更具“富含G / C”的特性。尽管具有相当的生物物理和化学性质,但它们在自然界中并不那么广泛。此外,虽然AA,AC和GU二核苷酸平台存在于天然GAAA / 11 nt受体中,但AA平台在某种程度上优于其他平台。自然界中对“富含A / U”的GNRA /受体相互作用的明显偏爱可能来自进化适应,以避免在较大分子环境下折叠陷阱。为了提供支持该假设的证据,在体外研究了几种基于天然和人工GNRA受体的核糖开关通过将受体序列捕获到另一种分子内假结中来阻止分子间GNRA /受体相互作用的能力。通过天然凝胶移位测定和共转录装配确定的衰减程度与GNRA受体的G / C含量相关。我们的研究结果揭示了自然远程相互作用的结构演变,并为合成生物学和RNA纳米生物技术中使用的基于RNA的衰减器设备提供了设计原理。

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