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Tetherin Inhibits HIV-1 Release by Directly Tethering Virions to Cells

机译:Tetherin通过直接将病毒颗粒束缚到细胞来抑制HIV-1释放

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摘要

Tetherin is an interferon-induced protein whose expression blocks the release of HIV-1 and other enveloped viral particles. The underlying mechanism by which tetherin functions and whether it directly or indirectly causes virion retention are unknown. Here, we elucidate the mechanism by which tetherin exerts its antiviral activity. We demonstrate, through mutational analyses and domain replacement experiments, that tetherin configuration rather than primary sequence is critical for antiviral activity. These findings allowed the design of a completely artificial protein, lacking sequence homology with native tetherin, that nevertheless mimicked its antiviral activity. We further show that tetherin is incorporated into HIV-1 particles as a parallel homodimer using either of its two membrane anchors. These results indicate that tetherin functions autonomously and directly and that infiltration of virion envelopes by one or both of tetherin's membrane anchors is necessary, and likely sufficient, to tether enveloped virus particles that bud through the plasma membrane.
机译:Tetherin是一种干扰素诱导的蛋白,其表达可阻止HIV-1和其他包膜病毒颗粒的释放。系链素起作用的基本机制以及它是直接还是间接引起病毒体保留的原因尚不清楚。在这里,我们阐明了系链素发挥其抗病毒活性的机制。通过突变分析和域替换实验,我们证明了系链蛋白构型而不是一级序列对于抗病毒活性至关重要。这些发现允许设计出一种完全人工的蛋白质,该蛋白质与天然系链素缺乏序列同源性,但仍模仿其抗病毒活性。我们进一步显示,使用其两个膜锚之一,将系链素作为平行同型二聚体掺入HIV-1颗粒中。这些结果表明,系链素可以自主和直接发挥功能,并且系链膜的一个或两个膜渗透物对病毒体包膜的渗透对于系留通过质膜发芽的被包​​膜的病毒颗粒是必要的,而且可能足够。

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