Longitudinal Analysis Reveals Early Development of Three MPER-Directed Neutralizing Antibody Lineages from an HIV-1-Infected Individual

纵向分析揭示了HIV-1感染者体内三种MPER靶向中和抗体谱系的早期发育

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作者:Shelly J Krebs,Young D Kwon,Chaim A Schramm,William H Law,Gina Donofrio,Kenneth H Zhou,Syna Gift,Vincent Dussupt,Ivelin S Georgiev,Sebastian Schätzle,Jonathan R McDaniel,Yen-Ting Lai,Mallika Sastry,Baoshan Zhang,Marissa C Jarosinski,Amy Ransier,Agnes L Chenine,Mangaiarkarasi Asokan,Robert T Bailer,Meera Bose,Alberto Cagigi,Evan M Cale,Gwo-Yu Chuang,Samuel Darko,Jefferson I Driscoll,Aliaksandr Druz,Jason Gorman,Farida Laboune,Mark K Louder,Krisha McKee,Letzibeth Mendez,M Anthony Moody,Anne Marie O'Sullivan,Christopher Owen,Dongjun Peng,Reda Rawi,Eric Sanders-Buell,Chen-Hsiang Shen,Andrea R Shiakolas,Tyler Stephens,Yaroslav Tsybovsky,Courtney Tucker,Raffaello Verardi,Keyun Wang,Jing Zhou,Tongqing Zhou,George Georgiou,S Munir Alam,Barton F Haynes,Morgane Rolland,Gary R Matyas,Victoria R Polonis,Adrian B McDermott,Daniel C Douek,Lawrence Shapiro,Sodsai Tovanabutra,Nelson L Michael,John R Mascola,Merlin L Robb,Peter D Kwong,Nicole A Doria-Rose  0

Abstract

Lineage-based vaccine design is an attractive approach for eliciting broadly neutralizing antibodies (bNAbs) against HIV-1. However, most bNAb lineages studied to date have features indicative of unusual recombination and/or development. From an individual in the prospective RV217 cohort, we identified three lineages of bNAbs targeting the membrane-proximal external region (MPER) of the HIV-1 envelope. Antibodies RV217-VRC42.01, -VRC43.01, and -VRC46.01 used distinct modes of recognition and neutralized 96%, 62%, and 30%, respectively, of a 208-strain virus panel. All three lineages had modest levels of somatic hypermutation and normal antibody-loop lengths and were initiated by the founder virus MPER. The broadest lineage, VRC42, was similar to the known bNAb 4E10. A multimeric immunogen based on the founder MPER activated B cells bearing the unmutated common ancestor of VRC42, with modest maturation of early VRC42 intermediates imparting neutralization breadth. These features suggest that VRC42 may be a promising template for lineage-based vaccine design.

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