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甲型流感病毒基因组的核运输方向性是由核蛋白上核定位序列的选择性暴露驱动的。

The directionality of the nuclear transport of the influenza A genome is driven by selective exposure of nuclear localization sequences on nucleoprotein.

作者信息

Wu Winco Wh, Panté Nelly

机构信息

Department of Zoology, University of British Columbia, Vancouver, British Columbia, Canada.

出版信息

Virol J. 2009 Jun 2;6:68. doi: 10.1186/1743-422X-6-68.

Abstract

BACKGROUND

Early in infection, the genome of the influenza A virus, consisting of eight complexes of RNA and proteins (termed viral ribonucleoproteins; vRNPs), enters the nucleus of infected cells for replication. Incoming vRNPs are imported into the nucleus of infected cells using at least two nuclear localization sequences on nucleoprotein (NP; NLS1 at the N terminus, and NLS2 in the middle of the protein). Progeny vRNP assembly occurs in the nucleus, and later in infection, these are exported from the nucleus to the cytoplasm. Nuclear-exported vRNPs are different from incoming vRNPs in that they are prevented from re-entering the nucleus. Why nuclear-exported vRNPs do not re-enter the nucleus is unknown.

RESULTS

To test our hypothesis that the exposure of NLSs on the vRNP regulates the directionality of the nuclear transport of the influenza vRNPs, we immunolabeled the two NLSs of NP (NLS1 and NLS2) and analyzed their surface accessibility in cells infected with the influenza A virus. We found that the NLS1 epitope on NP was exposed throughout the infected cells, but the NLS2 epitope on NP was only exposed in the nucleus of the infected cells. Addition of the nuclear export inhibitor leptomycin B further revealed that NLS1 is no longer exposed in cytoplasmic NP and vRNPs that have already undergone nuclear export. Similar immunolabeling studies in the presence of leptomycin B and with cells transfected with the cDNA of NP revealed that the NLS1 on NP is hidden in nuclear exported-NP.

CONCLUSION

NLS1 mediates the nuclear import of newly-synthesized NP and incoming vRNPs. This NLS becomes hidden on nuclear-exported NP and nuclear-exported vRNPs. Thus the selective exposure of the NLS1 constitutes a critical mechanism to regulate the directionality of the nuclear transport of vRNPs during the influenza A viral life cycle.

摘要

背景

在感染早期,甲型流感病毒的基因组由八个RNA与蛋白质复合物(称为病毒核糖核蛋白;vRNPs)组成,进入被感染细胞的细胞核进行复制。进入的vRNPs利用核蛋白(NP)上至少两个核定位序列(N端的NLS1和蛋白中部的NLS2)被导入被感染细胞的细胞核。子代vRNP组装在细胞核中发生,且在感染后期,这些vRNPs从细胞核输出到细胞质。核输出的vRNPs与进入的vRNPs不同,它们被阻止重新进入细胞核。核输出的vRNPs为何不重新进入细胞核尚不清楚。

结果

为了检验我们的假设,即vRNP上NLSs的暴露调节甲型流感病毒vRNPs核运输的方向性,我们对NP的两个NLSs(NLS1和NLS2)进行免疫标记,并分析它们在感染甲型流感病毒的细胞中的表面可及性。我们发现NP上的NLS1表位在整个被感染细胞中都有暴露,但NP上的NLS2表位仅在被感染细胞的细胞核中暴露。添加核输出抑制剂雷帕霉素B进一步显示,NLS1在已经经历核输出的细胞质NP和vRNPs中不再暴露。在存在雷帕霉素B的情况下以及用NP的cDNA转染细胞进行的类似免疫标记研究表明,NP上的NLS1隐藏在核输出的NP中。

结论

NLS1介导新合成的NP和进入的vRNPs的核输入。这个NLS在核输出的NP和核输出的vRNPs上隐藏起来。因此,NLS1的选择性暴露构成了在甲型流感病毒生命周期中调节vRNPs核运输方向性的关键机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b481/2694790/eed2326d0d71/1743-422X-6-68-1.jpg

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