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Recombinant viral RdRps can initiate RNA synthesis from circular templates.

机译:重组病毒RdRps可以从环状模板启动RNA合成。

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摘要

The crystal structure of the recombinant hepatitis C virus (HCV) RNA-dependent RNA polymerase (RdRp) revealed extensive interactions between the fingers and the thumb subdomains, resulting in a closed conformation with an established template channel that should specifically accept single-stranded templates. We made circularized RNA templates and found that they were efficiently used by the HCV RdRp to synthesize product RNAs that are significantly longer than the template, suggesting that RdRp could exist in an open conformation prior to template binding. RNA synthesis using circular RNA templates had properties similar to those previously documented for linear RNA, including a need for higher GTP concentration for initiation, usage of GTP analogs, sensitivity to salt, and involvement of active-site residues for product formation. Some products were resistant to challenge with the template competitor heparin, indicating that the elongation complexes remain bound to template and are competent for RNA synthesis. Other products were not elongated in the presence of heparin, indicating that the elongation complex was terminated. Lastly, recombinant RdRps from two other flaviviruses and from the Pseudomonas phage phi6 also could use circular RNA templates for RNA-dependent RNA synthesis, although the phi6 RdRp could only use circular RNAs made from the 3'-terminal sequence of the phi6 genome.
机译:重组丙型肝炎病毒(HCV)RNA依赖性RNA聚合酶(RdRp)的晶体结构揭示了手指和拇指亚结构域之间的广泛相互作用,从而导致与已建立的模板通道形成封闭构象,该通道应专门接受单链模板。我们制作了环化的RNA模板,发现HCV RdRp有效地使用了它们来合成比模板更长的产物RNA,这表明RdRp可以在模板结合之前以开放构象存在。使用环状RNA模板进行RNA合成的性质与先前针对线性RNA记录的性质相似,包括需要更高的GTP浓度进行起始,GTP类似物的使用,对盐的敏感性以及活性位点残基参与产物形成。一些产品对模板竞争者肝素具有抗性,表明延伸复合物仍与模板结合并具有RNA合成能力。在肝素存在下,其他产品未伸长,表明伸长复合物已终止。最后,来自其他两种黄病毒和假单胞菌噬菌体phi6的重组RdRps也可以使用环状RNA模板进行RNA依赖的RNA合成,尽管phi6 RdRp只能使用由phi6基因组3'端序列制成的环状RNA。

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