首页> 外文期刊>Nucleic Acids Research >Requirement for canonical base pairing in the short pseudoknot structure of genomic hepatitis delta virus ribozyme.
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Requirement for canonical base pairing in the short pseudoknot structure of genomic hepatitis delta virus ribozyme.

机译:在基因组肝炎三角洲病毒核酶的短假结结构中需要规范的碱基配对。

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摘要

The tertiary structure of the 3'-cleaved product of the genomic hepatitis delta virus (HDV) ribozyme was solved by X-ray crystallographic analysis. In this structure, three single-stranded regions (SSrA, -B and -C) interact intricately with one another via hydrogen bonds between nucleotide bases, phosphate oxygens and 2'-OHs to form a nested double pseudoknot structure. Among these interactions, two Watson-Crick (W-C) base pairs, 726G-710C and 727G-709C, that form between SSrA and SSrC (P1.1) seem to be especially important for compact folding. To characterize the importance of these base pairs, ribozymes were subjected to in vitro selection from a pool of RNA molecules randomly substituted at positions 709, 710, 726 and 727. The results establish the importance of the two W-C base pairs for activity, although some mutants are active with one G-C base pair. In addition, the kinetic parameters were analyzed in all 16 combinations with two canonical base pairs. Comparison of variant ribozymes with the wild-type ribozyme reveals that the difference in reaction rates for these variants (DeltaDelta G (double dagger)) is not simply accounted for by the differences in the stability of P1.1 (DeltaDelta G (0)(37)). The role played by Mg(2+)ions in formation of the P1.1 structure is also discussed.
机译:基因组肝炎三角洲病毒(HDV)核酶的3'裂解产物的三级结构通过X射线晶体学分析确定。在这种结构中,三个单链区(SSrA,-B和-C)通过核苷酸碱基,磷酸氧和2'-OH之间的氢键彼此复杂地相互作用,从而形成嵌套的双假结结构。在这些相互作用中,SSrA和SSrC(P1.1)之间形成的两个沃森-克里克(W-C)碱基对726G-710C和727G-709C对于紧凑折叠似乎特别重要。为了表征这些碱基对的重要性,对核酶进行了体外筛选,随机选择了709、710、726和727位的RNA分子库。结果确定了两个WC碱基对活性的重要性,尽管有些突变体具有一个GC碱基对。此外,还用两个标准碱基对分析了所有16种组合的动力学参数。将变体核酶与野生型核酶进行比较后发现,这些变体(DeltaDelta G(双匕首))的反应速率差异并非简单地由P1.1(DeltaDelta G(0)( 37))。还讨论了Mg(2+)离子在P1.1结构形成中的作用。

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