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The role of a metastable RNA secondary structure in hepatitis delta virus genotype III RNA editing

机译:亚稳态RNA二级结构在乙型肝炎三角洲病毒基因型RNA编辑中的作用

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RNA editing plays a critical role in the life cycle of hepatitis delta virus (HDV). The host editing enzyme ADAR1 recognizes specific RNA secondary structure features around the amber/W site in the HDV antigenome and deaminates the amber/W adenosine. A previous report suggested that a branched secondary structure is necessary for editing in HDV genotype III. This branched structure, which is distinct from the characteristic unbranched rod structure required for HDV replication, was only partially characterized, and knowledge concerning its formation and stability was limited. Here, we examine the secondary structures, conformational dynamics, and amber/W site editing of HDV genotype III RNA using a miniaturized HDV genotype III RNA in vitro. Computational analysis of this RNA using the MPGAfold algorithm indicated that the RNA has a tendency to form both metastable and stable unbranched secondary structures. Moreover, native polyacrylamide gel electrophoresis demonstrated that this RNA forms both branched and unbranched rod structures when transcribed in vitro. As predicted, the branched structure is a metastable structure that converts readily to the unbranched rod structure. Only branched RNA was edited at the amber/W site by ADAR1 in vitro. The structural heterogeneity of HDV genotype III RNA is significant because not only are both conformations of the RNA functionally important for viral replication, but the ratio of the two forms could modulate editing by determining the amount of substrate RNA available for modification.
机译:RNA编辑在肝炎三角洲病毒(HDV)的生命周期中起着至关重要的作用。宿主编辑酶ADAR1识别HDV反基因组中琥珀色/ W位点周围的特定RNA二级结构特征,并使琥珀色/ W腺苷脱氨。先前的报告表明,分支二级结构对于在HDV基因型III中进行编辑是必需的。这种支化结构与HDV复制所需的特征性非支化棒状结构不同,仅被部分表征,有关其形成和稳定性的知识有限。在这里,我们研究了使用微型化的HDV基因型III RNA的HDV基因型III RNA的二级结构,构象动力学和琥珀/ W站点编辑。使用MPGAfold算法对该RNA的计算分析表明,RNA具有形成亚稳和稳定的直链二级结构的趋势。此外,天然聚丙烯酰胺凝胶电泳表明,在体外转录时,这种RNA既形成支链结构又形成非支链结构。如所预测的,支链结构是亚稳结构,其易于转化为直链的杆结构。在体外,ADAR1仅在琥珀/ W位点编辑了分支RNA。 HDV基因型III RNA的结构异质性很重要,因为不仅RNA的两个构象在功能上对病毒复制都非常重要,而且两种形式的比例可以通过确定可用于修饰的底物RNA的量来调节编辑。

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