Comparison of Omicron Breakthrough Infection Versus Monovalent SARS-CoV-2 Intramuscular Booster Reveals Differences in Mucosal and Systemic Humoral Immunity

Author:

Nantel Sabryna,Sheikh-Mohamed Salma,Chao Gary Y. C.,Kurtesi Alexandra,Hu Queenie,Wood Heidi,Colwill Karen,Li Zhijie,Liu Ying,Seifried Laurie,Bourdin Benoîte,McGeer Allison,Hardy William R.,Rojas Olga L.,Ostrowski Mario A.,Brockman Mark A.ORCID,Piccirillo Ciriaco A.,Quach Caroline,Rini James M.,Gingras Anne-Claude,Decaluwe HélèneORCID,Gommerman Jennifer L.ORCID

Abstract

ABSTRACTOur understanding of the quality of cellular and humoral immunity conferred by COVID-19 vaccination alone versus vaccination plus SARS-CoV-2 breakthrough (BT) infection remains incomplete. While the current (2023) SARS-CoV-2 immune landscape of Canadians is complex, in late 2021 most Canadians had either just received a third dose of COVID-19 vaccine, or had received their two dose primary series and then experienced an Omicron BT. Herein we took advantage of this coincident timing to contrast cellular and humoral immunity conferred by three doses of vaccine versus two doses plus BT. Our results show that mild BT infection induces cell-mediated immune responses to variants comparable to an intramuscular vaccine booster dose. In contrast, BT subjects had higher salivary IgG and IgA levels against the Omicron Spike and enhanced reactivity to the ancestral Spike for the IgA isotype, which also reacted with SARS-CoV-1. Serum neutralizing antibody levels against the ancestral strain and the variants were also higher after BT infection. Our results support the need for mucosal vaccines to emulate the enhanced mucosal and humoral immunity induced by Omicron without exposing individuals to the risks associated with SARS-CoV-2 infection.ONE SENTENCE SUMMARYOmicron breakthrough elicits cross-reactive systemic and mucosal immune responses in fully vaccinated adults.Graphical Abstract

Publisher

Cold Spring Harbor Laboratory

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