HIV-1 broadly neutralizing antibody precursor B cells revealed by germline-targeting immunogen

Joseph G. Jardine(Scripps Research Institute), Daniel W. Kulp(Scripps Research Institute), Colin Havenar‐Daughton(Scripps Research Institute), Anita Sarkar(Scripps Research Institute), Bryan Briney(Scripps Research Institute), Devin Sok(Scripps Research Institute), Fabian Sesterhenn(Scripps Research Institute), June Ereño‐Orbea(Hospital for Sick Children), Oleksandr Kalyuzhniy(Scripps Research Institute), Isaiah Deresa(Scripps Research Institute), Xiaozhen Hu(Scripps Research Institute), Skye Spencer(Scripps Research Institute), Meaghan Jones(Scripps Research Institute), Erik Georgeson(Scripps Research Institute), Yumiko Adachi(Scripps Research Institute), Michael Kubitz(Scripps Research Institute), Allan C. deCamp(Fred Hutch Cancer Center), Jean‐Philippe Julien(Scripps Research Institute), Ian A. Wilson(Scripps Research Institute), Dennis R. Burton(Scripps Research Institute), Shane Crotty(Scripps Research Institute), William R. Schief(Scripps Research Institute)
Science
March 24, 2016
Cited by 478Open Access
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Abstract

Induction of broadly neutralizing antibodies (bnAbs) is a major HIV vaccine goal. Germline-targeting immunogens aim to initiate bnAb induction by activating bnAb germline precursor B cells. Critical unmet challenges are to determine whether bnAb precursor naïve B cells bind germline-targeting immunogens and occur at sufficient frequency in humans for reliable vaccine responses. Using deep mutational scanning and multitarget optimization, we developed a germline-targeting immunogen (eOD-GT8) for diverse VRC01-class bnAbs. We then used the immunogen to isolate VRC01-class precursor naïve B cells from HIV-uninfected donors. Frequencies of true VRC01-class precursors, their structures, and their eOD-GT8 affinities support this immunogen as a candidate human vaccine prime. These methods could be applied to germline targeting for other classes of HIV bnAbs and for Abs to other pathogens.


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