首页> 美国卫生研究院文献>Journal of Virology >The Cellular RNA Export Receptor TAP/NXF1 Is Required for ICP27-Mediated Export of Herpes Simplex Virus 1 RNA but the TREX Complex Adaptor Protein Aly/REF Appears To Be Dispensable
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The Cellular RNA Export Receptor TAP/NXF1 Is Required for ICP27-Mediated Export of Herpes Simplex Virus 1 RNA but the TREX Complex Adaptor Protein Aly/REF Appears To Be Dispensable

机译:ICP27介导的单纯疱疹病毒1 RNA的出口需要细胞RNA出口受体TAP / NXF1但似乎不需要TREX复合物衔接蛋白Aly / REF。

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摘要

Herpes simplex virus 1 (HSV-1) protein ICP27 has been shown to shuttle between the nucleus and cytoplasm and to bind viral RNA during infection. ICP27 was found to interact with the cellular RNA export adaptor protein Aly/REF, which is part of the TREX complex, and to relocalize Aly/REF to viral replication sites. ICP27 is exported to the cytoplasm through the export receptor TAP/NXF1, and ICP27 must be able to interact with TAP/NXF1 for efficient export of HSV-1 early and late transcripts. We examined the dynamics of ICP27 movement and its localization with respect to Aly/REF and TAP/NXF1 in living cells during viral infection. Recombinant viruses with a yellow fluorescent protein (YFP) tag on the N or C terminus of ICP27 were constructed. While the N-terminally tagged ICP27 virus behaved like wild-type HSV-1, the C-terminally tagged virus was defective in viral replication and gene expression, and ICP27 was confined to the nucleus, suggesting that the C-terminal YFP tag interfered with ICP27's C-terminal interactions, including the interaction with TAP/NXF1. To assess the role of Aly/REF and TAP/NXF1 in viral RNA export, these factors were knocked down using small interfering RNA. Knockdown of Aly/REF had little effect on the export of ICP27 or poly(A)+ RNA during infection. In contrast, a decrease in TAP/NXF1 levels severely impaired export of ICP27 and poly(A)+ RNA. We conclude that TAP/NXF1 is essential for ICP27-mediated export of RNA during HSV-1 infection, whereas Aly/REF may be dispensable.
机译:单纯疱疹病毒1(HSV-1)蛋白ICP27已显示在感染期间在细胞核与细胞质之间穿梭并结合病毒RNA。发现ICP27与作为TREX复合体一部分的细胞RNA出口衔接蛋白Aly / REF相互作用,并将Aly / REF重新定位到病毒复制位点。 ICP27通过出口受体TAP / NXF1出口到细胞质,并且ICP27必须能够与TAP / NXF1相互作用才能有效出口HSV-1早期和晚期转录本。我们检查了病毒感染过程中ICP27运动的动力学及其在活细胞中相对于Aly / REF和TAP / NXF1的定位。构建了在ICP27 N或C末端带有黄色荧光蛋白(YFP)标签的重组病毒。尽管N末端标记的ICP27病毒的行为类似于野生型HSV-1,但C末端标记的病毒在病毒复制和基因表达方面存在缺陷,并且ICP27局限于核内,这表明C末端的YFP标签会干扰ICP27的C端相互作用,包括与TAP / NXF1的相互作用。为了评估Aly / REF和TAP / NXF1在病毒RNA输出中的作用,使用小型干扰RNA敲低了这些因子。在感染过程中,敲除Aly / REF对ICP27或poly(A) + RNA的输出几乎没有影响。相反,TAP / NXF1水平的降低严重损害了ICP27和poly(A) + RNA的输出。我们得出结论,TAP / NXF1对于HSV-1感染期间ICP27介导的RNA出口至关重要,而Aly / REF可能是必需的。

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