Conformational trajectory of the HIV-1 fusion peptide during CD4-induced envelope opening

Bhishem Thakur, Revansiddha H Katte, Wang Xu, Katarzyna Janowska, Salam Sammour, Rory Henderson, Maolin Lu, Peter D Kwong, Priyamvada Acharya
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Abstract

The hydrophobic fusion peptide (FP), a critical component of the HIV-1 entry machinery, is located at the N terminal stretch of the envelope (Env) gp41 subunit. The receptor-binding gp120 subunit of Env forms a heterodimer with gp41 and assembles into a trimer, in which FP is accessible for antibody binding. Env conformational changes or opening that follow receptor binding result in FP relocating to a newly formed interprotomer pocket at the gp41-gp120 interface where it is sterically inaccessible to antibody. The mechanistic steps connecting the entry-related transition of antibody accessible-to-inaccessible FP configurations remain unresolved. Here, using SOSIP-stabilized Env ectodomains, we visualized atomic-level details of a functional entry intermediate, where partially open Env was bound to receptor CD4, co-receptor mimetic antibody 17b, and FP-targeting antibody VRC34.01, demonstrating that FP remains antibody accessible despite substantial receptor-induced Env opening. We determined a series of structures delineating stepwise opening of Env from its closed state to a newly resolved intermediate and defining downstream re-organizations of the gp120-gp41 interface that ultimately resulted in FP burial in an antibody-inaccessible configuration. Our studies improve our understanding of HIV-1 entry and provide information on entry-related conformation reorganization of a key site of HIV vulnerability to neutralizing antibody.
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CD4 诱导包膜打开过程中 HIV-1 融合肽的构象轨迹
疏水融合肽(FP)是 HIV-1 进入机制的重要组成部分,位于包膜(Env)gp41 亚基的 N 端。与受体结合的 Env gp120 亚基与 gp41 形成异源二聚体并组装成三聚体,其中的 FP 可被抗体结合。受体结合后,Env构象发生变化或开放,导致FP转移到gp41-gp120界面上新形成的原体间口袋中,在那里,抗体无法接触到FP。连接抗体可进入到不可进入的 FP 构型的进入相关转变的机理步骤仍未解决。在这里,我们使用 SOSIP 稳定的 Env 外结构域,观察了功能性进入中间体的原子级细节,其中部分开放的 Env 与受体 CD4、共受体模拟抗体 17b 和 FP 靶向抗体 VRC34.01 结合,表明尽管受体诱导 Env 大量开放,但 FP 仍可与抗体结合。我们确定了一系列结构,描述了 Env 从封闭状态逐步开放到新解析的中间体的过程,并确定了 gp120-gp41 界面的下游重组,最终导致 FP 埋藏在抗体无法访问的构型中。我们的研究增进了我们对 HIV-1 进入的了解,并提供了 HIV 易受中和抗体影响的关键位点与进入相关的构象重组信息。
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