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hnRNP E1 and E2 have distinct roles in modulating HIV-1 gene expression

机译:hnRNP E1和E2在调节HIV-1基因表达中具有不同的作用

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摘要

Pre-mRNA processing, including 5' end capping, splicing, and 3' end cleavage/polyadenylation, are events coordinated by transcription that can influence the subsequent export and translation of mRNAs. Coordination of RNA processing is crucial in retroviruses such as HIV-1, where inefficient splicing and the export of intron-containing RNAs are required for expression of the full complement of viral proteins. RNA processing can be affected by both viral and cellular proteins, and in this study we demonstrate that a member of the hnRNP E family of proteins can modulate HIV-1 RNA metabolism and expression. We show that hnRNP E1/E2 are able to interact with the ESS3a element of the bipartite ESS in tat/rev exon 3 of HIV-1 and that modulation of hnRNP E1 expression alters HIV-1 structural protein synthesis. Overexpression of hnRNP E1 leads to a reduction in Rev, achieved in part through a decrease in rev mRNA levels. However, the reduction in Rev levels cannot fully account for the effect of hnRNP E1, suggesting that hmRNP E1 might also act to suppress viral RNA translation. Deletion mutagenesis determined that the C-terminal end of hnRNP E1 was required for the reduction in Rev expression and that replacing this portion of hnRNP E1 with that of hnRNP E2, despite the high degree of conservation, could not rescue the loss of function.
机译:mRNA的前加工,包括5'末端加帽,剪接和3'末端切割/聚腺苷酸化,是转录所协调的事件,可影响后续的mRNA输出和翻译。 RNA加工的协调在诸如HIV-1等逆转录病毒中至关重要,在后者中,表达完整的病毒蛋白需要低效率的剪接和含内含子RNA的输出。 RNA加工会受到病毒和细胞蛋白的影响,在这项研究中,我们证明hnRNP E蛋白家族的成员可以调节HIV-1 RNA的代谢和表达。我们显示,hnR​​NP E1 / E2能够与HIV-1的tat / rev外显子3中二分体ESS的ESS3a元素相互作用,并且hnRNP E1表达的调节改变了HIV-1结构蛋白的合成。 hnRNP E1的过表达导致Rev降低,部分是通过rev mRNA水平的降低实现的。但是,Rev水平的降低不能完全说明hnRNP E1的作用,这表明hmRNP E1也可能起到抑制病毒RNA翻译的作用。缺失诱变确定hnRNP E1的C末端是Rev表达降低所必需的,尽管高度保守,用hnRNP E2取代hnRNP E1的这一部分仍无法挽救功能丧失。

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