Alexandra Tauzin, Étienne Bélanger, Jérémie Prévost, Halima Medjahed, Catherine Bourassa, Frederic Bibollet-Ruche, Jonathan Richard, Beatrice H Hahn, Andrés Finzi
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The small but significant accumulation of CD4 at the surface of cells infected with Env cytoplasmic tail-deleted viruses is sufficient to trigger Env to adopt a more \"open\" conformation. This prompted recognition of HIV-1-infected cells by plasma from people living with HIV (PLWH) and several families of CD4-induced (CD4i) antibodies, leading to the elimination of these cells by ADCC. While cytoplasmic tail truncations are known to enhance Env expression at the cell surface, this did not fully explain the increased recognition of infected cells by CD4i antibodies and plasma from PLWH. Introduction of the CD4bs D368R mutation, which abrogates CD4 interaction, decreased Env recognition and ADCC. 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引用次数: 0
摘要
hiv -1介导的CD4下调是一种众所周知的保护感染细胞免受抗体依赖性细胞毒性(ADCC)的机制。虽然HIV-1 Nef和Vpu蛋白对CD4下调的作用已被广泛研究,但HIV-1包膜糖蛋白(Env)在这一机制中的作用尚不清楚。虽然已知Env通过其CD4结合位点(CD4bs)将CD4保留在内质网(ER)中,但对这一过程的机制知之甚少。在这里,我们发现Env的细胞质尾部是CD4下调的主要决定因素。这一功能是高度保守的,因为它被观察到9个不同的传染性分子克隆从4支。被Env细胞质尾部缺失病毒感染的细胞表面少量但显著的CD4积累足以触发Env采用更“开放”的构象。这促使来自HIV感染者(PLWH)和几个cd4诱导(CD4i)抗体家族的血浆识别HIV-1感染细胞,导致ADCC消除这些细胞。虽然已知细胞质尾部截断可增强细胞表面的Env表达,但这并不能完全解释CD4i抗体和PLWH血浆对感染细胞的识别增加。引入CD4bs D368R突变,该突变消除了CD4相互作用,降低了Env识别和ADCC。总之,我们的研究结果表明,Env细胞质尾部的CD4下调有助于保护受感染的细胞免受ADCC的侵害。hiv -1介导的CD4下调是保护受感染细胞免受抗体依赖性细胞毒性(ADCC)的中心机制。CD4下调可防止HIV-1包膜糖蛋白(Env)和CD4之间的过早相互作用,否则会“打开”Env并暴露出存在于HIV感染者血浆中的CD4诱导抗体识别的易损表位。虽然已经阐明了病毒附属蛋白Nef和Vpu下调CD4的机制,但Env在这一过程中的作用尚不清楚。在这里,我们发现Env的细胞质尾部起着重要的作用,从而有助于保护受感染的细胞免受ADCC。
The HIV-1 envelope cytoplasmic tail protects infected cells from ADCC by downregulating CD4.
HIV-1-mediated CD4 downregulation is a well-known mechanism that protects infected cells from antibody-dependent cellular cytotoxicity (ADCC). While CD4 downregulation by HIV-1 Nef and Vpu proteins has been extensively studied, the contribution of the HIV-1 envelope glycoprotein (Env) in this mechanism is less understood. While Env is known to retain CD4 in the endoplasmic reticulum (ER) through its CD4-binding site (CD4bs), little is known about the mechanisms underlying this process. Here, we show that the cytoplasmic tail of Env is a major determinant in CD4 downregulation. This function is highly conserved as it was observed with nine different infectious molecular clones from four clades. The small but significant accumulation of CD4 at the surface of cells infected with Env cytoplasmic tail-deleted viruses is sufficient to trigger Env to adopt a more "open" conformation. This prompted recognition of HIV-1-infected cells by plasma from people living with HIV (PLWH) and several families of CD4-induced (CD4i) antibodies, leading to the elimination of these cells by ADCC. While cytoplasmic tail truncations are known to enhance Env expression at the cell surface, this did not fully explain the increased recognition of infected cells by CD4i antibodies and plasma from PLWH. Introduction of the CD4bs D368R mutation, which abrogates CD4 interaction, decreased Env recognition and ADCC. Overall, our results show that CD4 downregulation by the cytoplasmic tail of Env contributes to the protection of infected cells from ADCC.IMPORTANCEHIV-1-mediated CD4 downregulation is a central mechanism involved in the protection of infected cells from antibody-dependent cellular cytotoxicity (ADCC). CD4 downregulation prevents the premature interaction between HIV-1 envelope glycoproteins (Env) and CD4, which would otherwise "open" Env and expose vulnerable epitopes recognized by CD4-induced antibodies present in the plasma from people living with HIV. While the mechanisms of CD4 downregulation by the viral accessory proteins Nef and Vpu have been elucidated, the function of Env in this process is less clear. Here, we show that the cytoplasmic tail of Env plays an important role, thus contributing to the protection of infected cells from ADCC.
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