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首页> 外文期刊>Journal of interferon and cytokine research: The official journal of the International Society for Interferon and Cytokine Research >Biochemical and genetic evidence for complex formation between the influenza A virus NS1 protein and the interferon-induced PKR protein kinase.
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Biochemical and genetic evidence for complex formation between the influenza A virus NS1 protein and the interferon-induced PKR protein kinase.

机译:甲型流感病毒NS1蛋白与干扰素诱导的PKR蛋白激酶之间形成复合物的生化和遗传证据。

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摘要

The interferon (IFN)-induced protein kinase (PKR) functions as a gatekeeper of mRNA translation initiation and is, therefore, a key mediator of the host IFN-induced antiviral defense system. Many viruses have invested countermeasures against PKR. Some apparently use more than one mechanism. The influenza virus can repress PKR activity through the use of at least two factors, the cellular P58IPK protein and the viral NS1 protein. The exact mode of action of the latter has not been established. Here, using a coprecipitation assay, we found that PKR could form a complex with NS1 in crude cell extracts prepared from influenza virus-infected HeLa cells. The NS1-PKR interaction was verified by using the yeast two-hybrid system and an in vitro binding assay. Deletion analysis mapped the NS1 binding site to the N-terminal 98 residues of PKR regulatory region. Furthermore, an NS1 mutant, which lacks PKR inhibitory activity, did not bind PKR. Finally, the functional role of NS1 in PKR inhibition was substantiated using an in vivo assay for PKR activity. These results support the role of NS1 in PKR modulation during viral infection that is mediated through a complex formation between the two proteins.
机译:干扰素(IFN)诱导的蛋白激酶(PKR)充当mRNA翻译起始的守门人,因此是宿主IFN诱导的抗病毒防御系统的关键介体。许多病毒已经投资了针对PKR的对策。有些人显然使用了不止一种机制。流感病毒可以通过使用至少两个因子来抑制PKR活性,即细胞P58IPK蛋白和病毒NS1蛋白。后者的确切作用方式尚未确定。在这里,使用共沉淀测定法,我们发现PKR可以与从流感病毒感染的HeLa细胞制备的粗细胞提取物中的NS1形成复合物。通过使用酵母双杂交系统和体外结合测定法验证了NS1-PKR相互作用。缺失分析将NS1结合位点定位于PKR调节区的N末端98个残基。此外,缺乏PKR抑制活性的NS1突变体不结合PKR。最后,使用体内PKR活性测定法证实了NS1在PKR抑制中的功能作用。这些结果支持NS1在病毒感染期间通过两种蛋白质之间的复杂形成介导的PKR调节中的作用。

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