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Localization to detergent-resistant membranes and HIV-1 core entry inhibition correlate with HIV-1 restriction by SERINC5

机译:对洗涤剂抗性膜的定位和HIV-1核心进入抑制与Serinc5的HIV-1限制相关

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摘要

Abstract SERINC5(S5) is a multi-span transmembrane protein that potently blocks the infectivity of HIV-1 produced by human T-cells. The ability of S5 to restrict infectivity correlates with its presence in the virion, but the exact mechanism by which S5 restricts HIV-1 is unknown. Here we tested whether the core from HIV-1 virions containing S5 is delivered to the cytoplasm. Using the “fate of the capsid” assay, we demonstrated that the viral core of S5-restricted HIV-1 does not reach the cytoplasm of target cells, suggesting a block in the delivery of the core to the cytoplasm. In agreement with evidence suggesting that the viral determinants for S5 restriction map to the envelope of HIV-1, we observed that S5 induces conformational changes to the HIV-1 envelope. Further, we demonstrated that S5 localizes to detergent-resistant membranes (DRMs), as has been shown previously for the HIV-1 envelope in producer cells. In order to identify the determinants of S5 restriction, we explored the ability of all human SERINC proteins to restrict HIV-1. In contrast to human S5, we observed that human SERINC2(S2) did not restrict HIV-1, and was inefficiently incorporated into HIV-1 virions when compared to S5. Experiments using S5-S2 chimeric proteins revealed two functional domains for restriction: one necessary for S5 incorporation into virions, which does not seem to be necessary for restriction, and a second one necessary to change the HIV-1 envelope conformation, localize to DRMs, and block infection. Highlights ? SERINC5 prevents the delivery of HIV-1 cores to the cytoplasm of target cells. ? SERINC5 contains specific domains important for viral incorporation and restriction. ? HIV-1 restriction by SERINC5 correlates with localization to DRMs and a change in envelope conformation.
机译:摘要Serinc5(S5)是一种多跨度跨膜蛋白,其效果地阻断了人T细胞产生的HIV-1的感染性。 S5限制感染性的能力与其在病毒夫中的存在相关,但是S5限制HIV-1的确切机制是未知的。在这里,我们测试了含有S5的HIV-1病毒粒子的核心是否递送到细胞质。使用测定法“衣壳的命运”,我们表明,S5-限制HIV-1的病毒核心没有达到靶细胞的细胞质中,这表明在芯到细胞质的递送的块。在一致的证据表明S5限制图的病毒决定因素到HIV-1的包络,我们观察到S5诱导HIV-1封套的构象变化。此外,我们证明S5定位于耐洗涤剂膜(DRM),如前所述用于生产者细胞中的HIV-1封套。为了鉴定S5限制的决定因素,我们探讨了所有人筛查蛋白质限制HIV-1的能力。与人S5相反,我们观察到,与S5相比,人乳突2(S2)没有限制HIV-1,并且在HIV-1病毒中尚未掺入HIV-1病毒中。使用S5-S2嵌合蛋白的实验显示了用于限制的两个功能结构域:S5掺入病毒粒子必需的,这似乎没有必要的限制,并且第二个是改变HIV-1包络构象的第二个必要的,并阻止感染。强调 ? SerIC5防止将HIV-1核心递送到靶细胞的细胞质。还是Serinc5含有特异性域,对于病毒掺入和限制很重要。还是HIV-1 SerIC3的限制与DRM的定位相关,并且包络构象的变化。

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