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利用冷冻电镜断层成像术确定了三聚合的猴免疫缺陷病毒包膜糖蛋白与可溶性 CD4 结合状态的三维结构。

Three-dimensional structures of soluble CD4-bound states of trimeric simian immunodeficiency virus envelope glycoproteins determined by using cryo-electron tomography.

机构信息

Laboratory of Cell Biology, Center for Cancer Research, National Cancer Institute, NIH, Bethesda, MD 20892, USA.

出版信息

J Virol. 2011 Dec;85(23):12114-23. doi: 10.1128/JVI.05297-11. Epub 2011 Sep 21.

Abstract

The trimeric envelope glycoprotein (Env) spikes displayed on the surfaces of simian immunodeficiency virus (SIV) and human immunodeficiency virus type 1 (HIV-1) virions are composed of three heterodimers of the viral glycoproteins gp120 and gp41. Although binding of gp120 to cell surface CD4 and a chemokine receptor is known to elicit conformational changes in gp120 and gp41, changes in quaternary structure of the trimer have only recently been elucidated. For the HIV-1 BaL isolate, CD4 attachment results in a striking rearrangement of the trimer from a "closed" to an "open" conformation. The effect of CD4 on SIV trimers, however, has not been described. Using cryo-electron tomography, we have now determined molecular architectures of the soluble CD4 (sCD4)-bound states of SIV Env trimers for three different strains (SIVmneE11S, SIVmac239, and SIV CP-MAC). In marked contrast to HIV-1 BaL, SIVmneE11S and SIVmac239 Env showed only minor conformational changes following sCD4 binding. In SIV CP-MAC, where trimeric Env displays a constitutively "open" conformation similar to that seen for HIV-1 BaL Env in the sCD4-complexed state, we show that there are no significant further changes in conformation upon the binding of either sCD4 or 7D3 antibody. The density maps also show that 7D3 and 17b antibodies target epitopes on gp120 that are on opposites sides of the coreceptor binding site. These results provide new insights into the structural diversity of SIV Env and show that there are strain-dependent variations in the orientation of sCD4 bound to trimeric SIV Env.

摘要

病毒表面展示的三聚体包膜糖蛋白(Env)刺突由病毒糖蛋白 gp120 和 gp41 的三种异二聚体组成。虽然已知 gp120 与细胞表面 CD4 和趋化因子受体的结合会引起 gp120 和 gp41 的构象变化,但三聚体的四级结构变化直到最近才被阐明。对于 HIV-1 BaL 分离株,CD4 的附着会导致三聚体从“封闭”构象到“开放”构象的惊人重排。然而,CD4 对 SIV 三聚体的影响尚未描述。通过冷冻电子断层扫描,我们现在已经确定了三种不同毒株(SIVmneE11S、SIVmac239 和 SIV CP-MAC)的可溶性 CD4(sCD4)结合状态下 SIV Env 三聚体的分子结构。与 HIV-1 BaL 形成鲜明对比的是,SIVmneE11S 和 SIVmac239 Env 在结合 sCD4 后仅发生微小的构象变化。在 SIV CP-MAC 中,三聚体 Env 显示出类似于 HIV-1 BaL Env 在 sCD4 复合物状态下的固有“开放”构象,我们表明,在结合 sCD4 或 7D3 抗体时,构象没有进一步发生显著变化。密度图还表明,7D3 和 17b 抗体针对 gp120 上的表位,这些表位位于核心受体结合位点的相对两侧。这些结果提供了对 SIV Env 结构多样性的新见解,并表明存在与三聚体 SIV Env 结合的 sCD4 方向的菌株依赖性变化。

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