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细胞外基质蛋白介导HIV-1 gp120与αβ的相互作用。

Extracellular Matrix Proteins Mediate HIV-1 gp120 Interactions with αβ.

作者信息

Plotnik David, Guo Wenjin, Cleveland Brad, von Haller Priska, Eng Jimmy K, Guttman Miklos, Lee Kelly K, Arthos James, Hu Shiu-Lok

机构信息

Department of Pharmaceutics, University of Washington, Seattle, Washington, USA.

Department of Genome Sciences, University of Washington, Seattle, Washington, USA.

出版信息

J Virol. 2017 Oct 13;91(21). doi: 10.1128/JVI.01005-17. Print 2017 Nov 1.

Abstract

Gut-homing αβ CD4 T lymphocytes have been shown to be preferentially targeted by human immunodeficiency virus type 1 (HIV-1) and are implicated in HIV-1 pathogenesis. Previous studies demonstrated that HIV-1 envelope protein gp120 binds and signals through αβ and that this likely contributes to the infection of αβ T cells and promotes cell-to-cell virus transmission. Structures within the second variable loop (V2) of gp120, including the tripeptide motif LDV/I, are thought to mediate gp120-αβ binding. However, lack of αβ binding has been reported in gp120 proteins containing LDV/I, and the precise determinants of gp120-αβ binding are not fully defined. In this work, we report the novel finding that fibronectins mediate indirect gp120-αβ interactions. We show that Chinese hamster ovary (CHO) cells used to express recombinant gp120 produced fibronectins and other extracellular matrix proteins that copurified with gp120. CHO cell fibronectins were able to mediate the binding of a diverse panel of gp120 proteins to αβ in an cell binding assay. The V2 loop was not required for fibronectin-mediated binding of gp120 to αβ, nor did V2-specific antibodies block this interaction. Removal of fibronectin through anion-exchange chromatography abrogated V2-independent gp120-αβ binding. Additionally, we showed a recombinant human fibronectin fragment mediated gp120-αβ interactions similarly to CHO cell fibronectin. These findings provide an explanation for the apparently contradictory observations regarding the gp120-αβ interaction and offer new insights into the potential role of fibronectin and other extracellular matrix proteins in HIV-1 biology. Immune tissues within the gut are severely damaged by HIV-1, and this plays an important role in the development of AIDS. Integrin αβ plays a major role in the trafficking of lymphocytes, including CD4 T cells, into gut lymphoid tissues. Previous reports indicate that some HIV-1 gp120 envelope proteins bind to and signal through αβ, which may help explain the preferential infection of gut CD4 T cells. In this study, we demonstrate that extracellular matrix proteins can mediate interactions between gp120 and αβ This suggests that the extracellular matrix may be an important mediator of HIV-1 interaction with αβ-expressing cells. These findings provide new insight into the nature of HIV-1-αβ interactions and how these interactions may represent targets for therapeutic intervention.

摘要

归巢至肠道的αβ CD4 T淋巴细胞已被证明是1型人类免疫缺陷病毒(HIV-1)的优先靶向目标,并与HIV-1发病机制有关。先前的研究表明,HIV-1包膜蛋白gp120通过αβ结合并发出信号,这可能有助于αβ T细胞的感染并促进细胞间病毒传播。gp120第二个可变环(V2)内的结构,包括三肽基序LDV/I,被认为介导gp120与αβ的结合。然而,在含有LDV/I的gp120蛋白中已报道缺乏与αβ的结合,并且gp120与αβ结合的确切决定因素尚未完全明确。在这项工作中,我们报告了一个新发现,即纤连蛋白介导间接的gp120与αβ的相互作用。我们表明,用于表达重组gp120的中国仓鼠卵巢(CHO)细胞产生了纤连蛋白和其他与gp120共纯化的细胞外基质蛋白。在细胞结合试验中,CHO细胞纤连蛋白能够介导多种gp120蛋白与αβ的结合。V2环对于纤连蛋白介导的gp120与αβ的结合不是必需的,V2特异性抗体也不能阻断这种相互作用。通过阴离子交换色谱法去除纤连蛋白消除了不依赖V2的gp120与αβ的结合。此外,我们表明重组人纤连蛋白片段介导gp120与αβ的相互作用,其方式与CHO细胞纤连蛋白类似。这些发现为关于gp120与αβ相互作用的明显矛盾的观察结果提供了解释,并为纤连蛋白和其他细胞外基质蛋白在HIV-1生物学中的潜在作用提供了新的见解。肠道内的免疫组织受到HIV-1的严重破坏,这在艾滋病的发展中起重要作用。整合素αβ在淋巴细胞,包括CD4 T细胞向肠道淋巴组织的运输中起主要作用。先前的报告表明,一些HIV-1 gp120包膜蛋白与αβ结合并通过αβ发出信号,这可能有助于解释肠道CD4 T细胞的优先感染。在这项研究中,我们证明细胞外基质蛋白可以介导gp120与αβ之间的相互作用。这表明细胞外基质可能是HIV-1与表达αβ的细胞相互作用的重要介质。这些发现为HIV-1与αβ相互作用的性质以及这些相互作用如何可能成为治疗干预靶点提供了新的见解。

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