Glycan-reactive antibodies isolated from human HIV-1 vaccine trial participants show broad pathogen cross-reactivity

Parker J. Jamieson
Xiaoying Shen
Alexandra A. Abu-Shmais
Perry T. Wasdin
Katarzyna Janowska
Robert J. Edwards
Garrett Scapellato
Simone I. Richardson
Nelia P. Manamela
Shuying Liu
Maggie Barr
Rebecca A. Gillespie
Jessica Mimms
Naveenchandra Suryadevara
Ty A. Sornberger
Seth Zost
Rob Parks
Shelby Flaherty
Alexis K. Janke
Bethany N. Howard
Yukthi P. Suresh
Ruth M. Ruprecht
James E. Crowe
Robert H. Carnahan
Justin R. Bailey
Kanekiyo Masaru
Barton F. Haynes
Penny L. Moore
Priyamvada Acharya
David C. Montefiori
Spyros A. Kalams
Shan Lu
Ivelin S. Georgiev

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Abstract

HIV-1 continues to pose a significant global health challenge, requiring ongoing research into effective prevention and treatment strategies. Understanding the B cell repertoire that can be engaged upon vaccination in humans is crucial for the development of future preventive vaccines. In this study, PBMCs from HIV-negative participants in the multivalent HVTN124 human HIV-1 vaccine clinical trial were interrogated for HIV-reactive B cells using LIBRA-seq, a high-throughput B cell mapping technology. We report the discovery of glycan-reactive antibodies capable of neutralizing diverse heterologous HIV-1 virus strains. Further, isolated antibodies showed broad cross-reactivity against antigens from a variety of other pathogens, while remaining mostly negative on autoreactivity assays. The emerging class of glycan- reactive virus-neutralizing antibodies with exceptional breadth of pathogen cross- reactivity may present an effective target for vaccination at the population level.

Version published to 10.1101/2025.01.17.633475v1 on bioRxiv
Jan 20, 2025

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