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Cleavage strongly influences whether soluble HIV-1 envelope glycoprotein trimers adopt a native-like conformation

机译:切割强烈影响可溶性HIV-1包膜糖蛋白三聚体是否采用天然样构象

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摘要

We compare the antigenicity and conformation of soluble, cleaved vs. uncleaved envelope glycoprotein (Env gp) 140 trimers from the subtype A HIV type 1 (HIV-1) strain BG505. The impact of gp120-gp41 cleavage on trimer structure, in the presence or absence of trimer-stabilizing modifications (i.e., a gp120-gp41 disulfide bond and an I559P gp41 change, together designated SOSIP), was assessed. Without SOSIP changes, cleaved trimers disintegrate into their gp120 and gp41-ectodomain (gp41(ECTO)) components; when only the disulfide bond is present, they dissociate into gp140 monomers. Uncleaved gp140s remain trimeric whether SOSIP substitutions are present or not. However, negative-stain electron microscopy reveals that only cleaved trimers form homogeneous structures resembling native Env spikes on virus particles. In contrast, uncleaved trimers are highly heterogeneous, adopting a variety of irregular shapes, many of which appear to be gp120 subunits dangling from a central core that is presumably a trimeric form of gp41(ECTO). Antigenicity studies with neutralizing and nonneutralizing antibodies are consistent with the EM images; cleaved, SOSIP-stabilized trimers express quaternary structure-dependent epitopes, whereas uncleaved trimers expose nonneutralizing gp120 and gp41(ECTO) epitopes that are occluded on cleaved trimers. These findings have adverse implications for using soluble, uncleaved trimers for structural studies, and the rationale for testing uncleaved trimers as vaccine candidates also needs to be reevaluated
机译:我们比较了A型亚型HIV 1型(HIV-1)菌株BG505的可溶性,裂解的和未裂解的包膜糖蛋白(Env gp)140三聚体的抗原性和构象。在存在或不存在三聚体稳定修饰(即,gp120-gp41二硫键和I559P gp41改变,一起称为SOSIP)的情况下,评估了gp120-gp41裂解对三聚体结构的影响。没有SOSIP的变化,裂解的三聚体会分解成其gp120和gp41胞外域(gp41(ECTO))成分;当仅存在二硫键时,它们解离为gp140单体。无论是否存在SOSIP取代,未切割的gp140都保持三聚体。然而,负染色电子显微镜显示只有被切割的三聚体才能形成均质的结构,类似于病毒颗粒上的天然Env尖峰。相反,未切割的三聚体是高度异质的,采用各种不规则形状,其中许多似乎是悬挂于中央核心的gp120亚基,可能是gp41(ECTO)的三聚体形式。用中和和非中和抗体进行的抗原性研究与EM图像一致;裂解的,SOSIP稳定的三聚体表达依赖于四级结构的表位,而未裂解的三聚体暴露了在裂解的三聚体上闭塞的未中和的gp120和gp41(ECTO)表位。这些发现对将可溶性,未裂解的三聚体用于结构研究具有不利影响,并且测试未裂解的三聚体的原理也需要重新评估,因为候选疫苗也需要重新评估

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