Antibody-independent protection against heterologous SARS-CoV-2 challenge conferred by prior infection or vaccination

Author:

Fumagalli ValeriaORCID,Ravà MicolORCID,Marotta DavideORCID,Di Lucia Pietro,Bono Elisa B.,Giustini Leonardo,De Leo Federica,Casalgrandi Maura,Monteleone EmanueleORCID,Mouro Violette,Malpighi Chiara,Perucchini Chiara,Grillo Marta,De Palma Sara,Donnici LorenaORCID,Marchese SilviaORCID,Conti Matteo,Muramatsu Hiromi,Perlman StanleyORCID,Pardi NorbertORCID,Kuka MirelaORCID,De Francesco RaffaeleORCID,Bianchi Marco E.ORCID,Guidotti Luca G.ORCID,Iannacone MatteoORCID

Abstract

AbstractVaccines have reduced severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) morbidity and mortality, yet emerging variants challenge their effectiveness. The prevailing approach to updating vaccines targets the antibody response, operating under the presumption that it is the primary defense mechanism following vaccination or infection. This perspective, however, can overlook the role of T cells, particularly when antibody levels are low or absent. Here we show, through studies in mouse models lacking antibodies but maintaining functional B cells and lymphoid organs, that immunity conferred by prior infection or mRNA vaccination can protect against SARS-CoV-2 challenge independently of antibodies. Our findings, using three distinct models inclusive of a novel human/mouse ACE2 hybrid, highlight that CD8+ T cells are essential for combating severe infections, whereas CD4+ T cells contribute to managing milder cases, with interferon-γ having an important function in this antibody-independent defense. These findings highlight the importance of T cell responses in vaccine development, urging a broader perspective on protective immunity beyond just antibodies.

Funder

Associazione Italiana per la Ricerca sul Cancro

Ministero dell'Istruzione, dell'Università e della Ricerca

Publisher

Springer Science and Business Media LLC

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