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Unbiased in vitro selection reveals the unique character of the self-cleaving antigenomic HDV RNA sequence

机译:无偏见的体外选择揭示了自切割反基因组HDV RNA序列的独特特征

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In order to revisit the architecture of the catalytic center of the antigenomic hepatitis delta virus (HDV) ribozyme we developed an unbiased in vitro selection procedure that efficiently selected novel variants from a relatively small set of sequences. Using this procedure we examined all possible variants from a pool of HDV ribozymes that had been randomized at 25 positions (4(25)). The isolated set of sequences shows more variability than do the natural variants. Nucleotide variations were found at all randomized positions, even at positions when the general belief was that the specific base was absolutely required for catalytic activity. Covariation analysis supports the presence of several base pairs, although it failed to propose any new tertiary contacts. HDV ribozyme appears to possess a greater number of constraints, in terms of sequences capable of supporting the catalysed cleavage, than do other catalytic RNAs. This supports the idea that the appearance of this catalytic RNA structure has a low probability (i.e. is a rare event), which may explain why to date it has been found in nature only in the HDV. These contrasts with the hammerhead self-cleaving motif that is proposed to have multiple origins, and that is widespread among different organisms. Thus, just because a self-cleaving RNA motif is small does not imply that it occurs easily.
机译:为了重新审视反基因组肝炎三角洲病毒(HDV)核酶催化中心的结构,我们开发了一种无偏见的体外选择程序,该程序可以从相对较小的序列集中有效地选择新的变异体。使用此程序,我们检查了来自HDV核酶库的所有可能变异体,这些变异体已在25个位置随机分组(4(25))。分离的序列组比自然变体显示出更多的可变性。在所有随机位置都发现了核苷酸变异,即使在普遍认为特定碱基是催化活性绝对必需的位置上也是如此。协变分析支持多个碱基对的存在,尽管它未能提出任何新的三级联系。就能够支持催化裂解的序列而言,与其他催化RNA相比,HDV核酶似乎具有更多的限制条件。这支持了这种催化性RNA结构出现的可能性较低的想法(即罕见事件),这可以解释为什么迄今为止仅在HDV中才发现它的存在。这些与锤头自我切割基序形成鲜明对比,后者被认为具有多种起源,并且在不同生物中广泛分布。因此,仅由于自我切割的RNA基序较小并不意味着它容易发生。

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