首页> 美国卫生研究院文献>Nucleic Acids Research >The secondary structure of the 5-noncoding region of beet necrotic yellow vein virus RNA 3: evidence for a role in viral RNA replication.
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The secondary structure of the 5-noncoding region of beet necrotic yellow vein virus RNA 3: evidence for a role in viral RNA replication.

机译:甜菜坏死性黄脉病毒RNA 5:5非编码区的二级结构:在病毒RNA复制中起作用的证据。

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摘要

Secondary structure-sensitive chemical and enzymatic probes have been used to produce a model for the folding of the first 312 residues of the long 5'-noncoding region of beet necrotic yellow vein virus RNA 3. The structure consists of two major domains, one of which includes long distance base-pairing interactions between two short sequence elements (Box I and Box II) situated between positions 237 and 292 and complementary elements (Box I' and II') near the 5'-terminus. Previous studies have shown that base pairing between these sequence elements (in either the plus-strand or minus-strand RNA) is important for RNA 3 accumulation during infection. RNA 3 transcripts were produced containing mutations which preferentially disrupted Box II-II' base pairing in either the plus- or minus-strand. In infection experiments, transcripts with mutations which disrupted the Box II-II' interaction in the plus-strand structure replicated less efficiently than mutants in which the Box II-II' interaction was disrupted in the minus-strand. These findings indicate that the complex 5'-proximal plus-strand structure to which the Box II-II' interaction contributes comprises at least part of the promoter for plus-strand RNA synthesis.
机译:二级结构敏感的化学和酶探针已用于产生甜菜坏死性黄脉病毒RNA 3长5'-非编码区的前312个残基的折叠模型。该结构由两个主要域组成,一个为它包括位于位置237和292之间的两个短序列元素(框I和框II)与5'端附近的互补元素(框I'和II')之间的长距离碱基配对相互作用。先前的研究表明,这些序列元素之间的碱基配对(在正链或负链RNA中)对于感染期间RNA 3的积累很重要。产生了含有突变的RNA 3转录本,该突变优先破坏了正链或负链的Box II-II'碱基配对。在感染实验中,具有破坏正链结构中Box II-II'相互作用的突变体的转录本,其复制效率低于其中负链中Box II-II'相互作用被破坏的突变体。这些发现表明,Box II-II'相互作用所贡献的复杂的5'-近端正链结构包括至少一部分用于正链RNA合成的启动子。

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