Analysis of the Diverse Antigenic Landscape of the Malaria Invasion Protein RH5 Identifies a Potent Vaccine-Induced Human Public Antibody Clonotype

Author:

Barrett Jordan R.ORCID,Pipini Dimitra,Wright Nathan D.,Cooper Andrew J. R.,Gorini Giacomo,Quinkert Doris,Lias Amelia M.,Davies Hannah,Rigby Cassandra,Aleshnick Maya,Williams Barnabas G.,Bradshaw William J.ORCID,Paterson Neil G.,Martinson Thomas,Kirtley Payton,Picard Luc,Wiggins Christine D.,Donnellan Francesca R.,King Lloyd D. W.,Wang Lawrence T.,Popplewell Jonathan F.,Silk Sarah E.,Swain Jed de Ruiter,Skinner Katherine,Kotraiah Vinayaka,Noe Amy R.,MacGill Randall S.,King C. Richter,Birkett Ashley J.,Soisson Lorraine A.,Minassian Angela M.ORCID,Lauffenburger Douglas A.,Miura Kazutoyo,Long Carole A.,Wilder Brandon K.,Koekemoer Lizbé,Tan Joshua,Nielsen Carolyn M.,McHugh KirstyORCID,Draper Simon J.ORCID

Abstract

SUMMARYThe highly conserved and essentialPlasmodium falciparumreticulocyte-binding protein homolog 5 (PfRH5) has emerged as the leading target for vaccines that seek to protect against the disease-causing blood-stage of malaria. However, the features of the human vaccine-induced antibody response that confer highly potent inhibition of malaria parasite invasion into red blood cells are not well defined. Here we characterize over 200 human IgG monoclonal antibodies induced by the most advanced PfRH5 vaccine. We define the antigenic landscape of this molecule, and establish epitope specificity, antibody association rate and intra-PfRH5 antibody interactions are key determinants of functional anti-parasitic potency. In addition, we identify a germline gene combination that results in an exceptionally potent class of antibody and demonstrate its prophylactic potential to protect againstP. falciparumparasite challengein vivo. This comprehensive dataset provides a framework to guide rational design of next-generation vaccines and prophylactic antibodies to protect against blood-stage malaria.

Publisher

Cold Spring Harbor Laboratory

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