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IFP35 Is Involved in the Antiviral Function of Interferon by Association with the Viral Tas Transactivator of Bovine Foamy Virus▿

机译:IFP35与牛泡沫病毒的病毒Tas反式激活因子相关,参与干扰素的抗病毒功能▿

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摘要

Interferon-induced proteins (IFPs) exert multiple functions corresponding to diverse interferon signals. However, the intracellular functions of many IFPs are not fully characterized. Here, we report that IFP35, a member of the IFP family with a molecular mass of 35 kDa, can interact with the bovine Tas (BTas) regulatory protein of bovine foamy virus (BFV). The interaction involves NID2 (IFP35/Nmi homology domain) of IFP35 and the central domain of BTas. The overexpression of IFP35 disturbs the ability of BTas to activate viral-gene transcription and inhibits viral replication. The depletion of endogenous IFP35 by interfering RNA can promote the activation of BFV, suggesting an inhibitory function of IFP35 in viral-gene expression. In addition, IFP35 can interact with the homologous regulatory protein of prototype FV and arrest viral replication and repress viral transcription. Our study suggests that IFP35 may represent a novel pathway of interferon-mediated antiviral activity in host organisms that plays a role in the maintenance of FV latency.
机译:干扰素诱导蛋白(IFP)发挥多种功能,对应于多种干扰素信号。但是,许多IFP的细胞内功能尚未完全表征。在这里,我们报告IFP35,IFP家族的一个成员,分子量为35 kDa,可以与牛泡沫病毒(BFV)的牛Tas(BTas)调节蛋白相互作用。相互作用涉及IFP35的NID2(IFP35 / Nmi同源结构域)和BTas的中央结构域。 IFP35的过表达干扰BTas激活病毒基因转录的能力,并抑制病毒复制。内源性IFP35通过干扰RNA的消耗可以促进BFV的激活,提示IFP35在病毒基因表达中具有抑制功能。此外,IFP35可以与原型FV的同源调节蛋白相互作用,并阻止病毒复制并抑制病毒转录。我们的研究表明,IFP35可能代表了在宿主生物中干扰素介导的抗病毒活性的新途径,该途径在维持FV潜伏期中发挥作用。

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