Soluble prefusion-closed HIV-envelope trimers with glycan-covered bases

具有聚糖覆盖碱基的可溶性融合前封闭 HIV 包膜三聚体

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作者:Adam S Olia, Cheng Cheng, Tongqing Zhou, Andrea Biju, Darcy R Harris, Anita Changela, Hongying Duan, Vera B Ivleva, Wing-Pui Kong, Li Ou, Reda Rawi, Yaroslav Tsybovsky, David J Van Wazer, Angela R Corrigan, Christopher A Gonelli, Myungjin Lee, Krisha McKee, Sandeep Narpala, Sijy O'Dell, Danealle K P

Abstract

Soluble HIV-1-envelope (Env) trimers elicit immune responses that target their solvent-exposed protein bases, the result of removing these trimers from their native membrane-bound context. To assess whether glycosylation could limit these base responses, we introduced sequons encoding potential N-linked glycosylation sites (PNGSs) into base-proximal regions. Expression and antigenic analyses indicated trimers bearing six-introduced PNGSs to have reduced base recognition. Cryo-EM analysis revealed trimers with introduced PNGSs to be prone to disassembly and introduced PNGS to be disordered. Protein-base and glycan-base trimers induced reciprocally symmetric ELISA responses, in which only a small fraction of the antibody response to glycan-base trimers recognized protein-base trimers and vice versa. EM polyclonal epitope mapping revealed glycan-base trimers -even those that were stable biochemically- to elicit antibodies that recognized disassembled trimers. Introduced glycans can thus mask the protein base but their introduction may yield neo-epitopes that dominate the immune response.

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