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Recruitment of host translation initiation factor eIF4G by the Vaccinia Virus ssDNA-binding protein I3

机译:牛痘病毒ssDNA结合蛋白I3募集宿主翻译起始因子eIF4G

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Poxviruses are large double-stranded DNA viruses that replicate exclusively in the cytoplasm of infected cells within discrete compartments termed viral factories. Recent work has shown that the prototypical poxvirus, Vaccinia Virus (VacV) sequesters components of the eukaryotic translation initiation complex eIF4F within viral factories while also stimulating formation of eIF4F complexes. However, the forces that govern these events remain unknown. Here, we show that maximal eIF4F formation requires viral DNA replication and the formation of viral factories, suggesting that sequestration functions to promote eIF4F assembly, and identify the ssDNA-binding protein, I3 as a viral factor that interacts and co-localizes with the eIF4F scaffold protein, eIF4G. Although it did not adversely affect host or viral protein synthesis, I3 specifically mediated the binding of eIF4G to ssDNA. Combined, our findings offer an explanation for the specific pattern and temporal process of eIF4G redistribution and eIF4F complex assembly within VacV-infected cells.
机译:痘病毒是大型的双链DNA病毒,仅在称为病毒工厂的离散隔室内的受感染细胞的细胞质中复制。最近的工作表明,原型痘病毒痘苗病毒(VacV)在病毒工厂中隔离了真核翻译起始复合物eIF4F的成分,同时还刺激了eIF4F复合物的形成。但是,控制这些事件的力量仍然未知。在这里,我们表明最大的eIF4F形成需要病毒DNA复制和病毒工厂的形成,这表明螯合功能可促进eIF4F装配,并鉴定ssDNA结合蛋白I3作为与eIF4F相互作用和共定位的病毒因子支架蛋白,eIF4G。尽管它不会对宿主或病毒蛋白的合成产生不利影响,但I3特异性介导了eIF4G与ssDNA的结合。综合起来,我们的发现为VacV感染细胞内eIF4G重新分布和eIF4F复杂装配的特定模式和时间过程提供了解释。

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