B cell maturation restored ancestral germlines to control Omicron BA.2.86

Author:

Paciello IdaORCID,Pierleoni GiulioORCID,Pantano ElisaORCID,Antonelli GiadaORCID,Pileri PieroORCID,Maccari GiuseppeORCID,Cardamone Dario,Realini GiuliaORCID,Perrone FedericaORCID,Neto Martin MayoraORCID,Pozzessere Simone,Fabbiani MassimilianoORCID,Panza FrancescaORCID,Rancan IlariaORCID,Tumbarello MarioORCID,Montagnani FrancescaORCID,Medini DuccioORCID,Maes PietORCID,Temperton NigelORCID,Simon-Loriere EtienneORCID,Schwartz OlivierORCID,Rappuoli RinoORCID,Andreano EmanueleORCID

Abstract

ABSTRACTThe unceasing interplay between SARS-CoV-2 and the human immune system has led to a continuous maturation of the virus and B cell response providing an opportunity to track their evolution in real time. We longitudinally analyzed the functional activity of almost 1,000 neutralizing human monoclonal antibodies (nAbs) isolated from vaccinated people, and from individuals with hybrid and super hybrid immunity (SH), developed after three mRNA vaccine doses and two breakthrough infections. The most potent neutralization and Fc functions against highly mutated variants, including BA.2.86, were found in the SH cohort. Despite different priming, epitope mapping revealed a convergent maturation of the functional antibody response. Neutralization was mainly driven by Class 1/2 nAbs while Fc functions were induced by Class 3/4 antibodies. Remarkably, broad neutralization was mediated by restored IGHV3-53/3-66 B cell germlines which, after heterogenous exposure to SARS-CoV-2 S proteins, increased their level of somatic hypermutations. Our study shows the resilience of the human immune system which restored previously expanded germlines and activated naïve B cells to broaden the antibody repertoire of antibodies to control future SARS-CoV-2 variants.

Publisher

Cold Spring Harbor Laboratory

Reference42 articles.

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