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TAR RNA剪接在恒河猴猿猴免疫缺陷病毒翻译调控中的作用。

Role of TAR RNA splicing in translational regulation of simian immunodeficiency virus from rhesus macaques.

作者信息

Viglianti G A, Rubinstein E P, Graves K L

机构信息

Program in Molecular Medicine, University of Massachusetts Medical Center, Worcester 01605.

出版信息

J Virol. 1992 Aug;66(8):4824-33. doi: 10.1128/JVI.66.8.4824-4833.1992.

Abstract

The untranslated leader sequences of rhesus macaque simian immunodeficiency virus mRNAs form a stable secondary structure, TAR. This structure can be modified by RNA splicing. In this study, the role of TAR splicing in virus replication was investigated. The proportion of viral RNAs containing a spliced TAR structure is high early after infection and decreases at later times. Moreover, proviruses containing mutations which prevent TAR splicing are significantly delayed in replication. These mutant viruses require approximately 20 days to achieve half-maximal virus production, in contrast to wild-type viruses, which require approximately 8 days. We attribute this delay to the inefficient translation of unspliced-TAR-containing mRNAs. The molecular basis for this translational effect was examined in in vitro assays. We found that spliced-TAR-containing mRNAs were translated up to 8.5 times more efficiently than were similar mRNAs containing an unspliced TAR leader. Furthermore, these spliced-TAR-containing mRNAs were more efficiently associated with ribosomes. We postulate that the level of TAR splicing provides a balance for the optimal expression of both viral proteins and genomic RNA and therefore ultimately controls the production of infectious virions.

摘要

恒河猴猿猴免疫缺陷病毒mRNA的未翻译前导序列形成一种稳定的二级结构,即反式激活应答元件(TAR)。这种结构可通过RNA剪接进行修饰。在本研究中,我们调查了TAR剪接在病毒复制中的作用。感染后早期,含有剪接后TAR结构的病毒RNA比例很高,而在后期则下降。此外,含有阻止TAR剪接突变的前病毒在复制中显著延迟。与野生型病毒(大约需要8天)相比,这些突变病毒需要大约20天才能达到最大病毒产量的一半。我们将这种延迟归因于含有未剪接TAR的mRNA翻译效率低下。在体外试验中研究了这种翻译效应的分子基础。我们发现,含有剪接后TAR的mRNA的翻译效率比含有未剪接TAR前导序列的类似mRNA高8.5倍。此外,这些含有剪接后TAR的mRNA与核糖体的结合更有效。我们推测,TAR剪接水平为病毒蛋白和基因组RNA的最佳表达提供了一种平衡,因此最终控制了传染性病毒粒子的产生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aff9/241310/55bfe90ccf18/jvirol00040-0213-a.jpg

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