Coronavirus: how a large RNA viral genome is replicated and transcribed.

Infectious agents and disease Pub Date : 1994-04-01
M M Lai, C L Liao, Y J Lin, X Zhang
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Abstract

Coronaviruses are important human and animal pathogens and contain an extraordinarily long (27-31 kb) RNA genome. Its RNA synthesis involves complex mechanisms of regulation, similar to those of DNA viruses. In this treatise, mouse hepatitis virus (MHV) is used as a model for the discussion of the mechanism of viral RNA synthesis. We show that MHV RNA synthesis requires interactions of multiple RNA components, which are likely mediated by protein-RNA and protein-protein, as well as RNA-RNA, interactions. This virus also provides a unique example of a discontinuous transcription mechanism, which involves a trans-acting RNA component. Finally, study of the cis-acting signals for the various steps of RNA synthesis revealed an insight into the regulation of viral RNA synthesis. This discussion suggests that the regulation of RNA synthesis in coronavirus is more complex than previously thought possible for RNA viruses. Coronavirus RNA transcription and replication may serve as a paradigm of RNA synthesis for RNA viruses in general.

冠状病毒:大RNA病毒基因组如何复制和转录。
冠状病毒是重要的人类和动物病原体,含有超长(27-31 kb)的RNA基因组。它的RNA合成涉及复杂的调控机制,类似于DNA病毒。在这篇论文中,小鼠肝炎病毒(MHV)被用作模型来讨论病毒RNA合成的机制。我们发现MHV RNA的合成需要多种RNA组分的相互作用,这可能是由蛋白质-RNA、蛋白质-蛋白质以及RNA-RNA相互作用介导的。该病毒还提供了一个独特的不连续转录机制的例子,其中涉及反式作用RNA成分。最后,对RNA合成各个步骤的顺式作用信号的研究揭示了对病毒RNA合成的调控。这一讨论表明,冠状病毒中RNA合成的调控比以前认为的RNA病毒更复杂。总的来说,冠状病毒RNA转录和复制可以作为RNA病毒RNA合成的范例。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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