Structural and genetic convergence of HIV-1 neutralizing antibodies in vaccinated non-human primates

接种疫苗的非人灵长类动物体内HIV-1中和抗体的结构和遗传趋同性

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作者:Fangping Cai ,Wei-Hung Chen ,Weimin Wu ,Julia A Jones ,Misook Choe ,Neelakshi Gohain ,Xiaoying Shen ,Celia LaBranche ,Amanda Eaton ,Laura Sutherland ,Esther M Lee ,Giovanna E Hernandez ,Nelson R Wu ,Richard Scearce ,Michael S Seaman ,M Anthony Moody ,Sampa Santra ,Kevin Wiehe ,Georgia D Tomaras ,Kshitij Wagh ,Bette Korber ,Mattia Bonsignori ,David C Montefiori ,Barton F Haynes ,Natalia de Val ,M Gordon Joyce ,Kevin O Saunders

Abstract

A primary goal of HIV-1 vaccine development is the consistent elicitation of protective, neutralizing antibodies. While highly similar neutralizing antibodies (nAbs) have been isolated from multiple HIV-infected individuals, it is unclear whether vaccination can consistently elicit highly similar nAbs in genetically diverse primates. Here, we show in three outbred rhesus macaques that immunization with Env elicits a genotypically and phenotypically conserved nAb response. From these vaccinated macaques, we isolated four antibody lineages that had commonalities in immunoglobulin variable, diversity, and joining gene segment usage. Atomic-level structures of the antigen binding fragments of the two most similar antibodies showed nearly identical paratopes. The Env binding modes of each of the four vaccine-induced nAbs were distinct from previously known monoclonal HIV-1 neutralizing antibodies, but were nearly identical to each other. The similarities of these antibodies show that the immune system in outbred primates can respond to HIV-1 Env vaccination with a similar structural and genotypic solution for recognizing a particular neutralizing epitope. These results support rational vaccine design for HIV-1 that aims to reproducibly elicit, in genetically diverse primates, nAbs with specific paratope structures capable of binding conserved epitopes.

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