Evolution of immune responses to SARS-CoV-2 in mild-moderate COVID-19

Author:

Wheatley Adam K.ORCID,Juno Jennifer A.ORCID,Wang Jing J.,Selva Kevin J.,Reynaldi ArnoldORCID,Tan Hyon-Xhi,Lee Wen ShiORCID,Wragg Kathleen M.,Kelly Hannah G.,Esterbauer RobynORCID,Davis Samantha K.ORCID,Kent Helen E.,Mordant Francesca L.ORCID,Schlub Timothy E.ORCID,Gordon David L.,Khoury David S.ORCID,Subbarao KantaORCID,Cromer Deborah,Gordon Tom P.,Chung Amy W.ORCID,Davenport Miles P.ORCID,Kent Stephen J.ORCID

Abstract

AbstractThe durability of infection-induced SARS-CoV-2 immunity has major implications for reinfection and vaccine development. Here, we show a comprehensive profile of antibody, B cell and T cell dynamics over time in a cohort of patients who have recovered from mild-moderate COVID-19. Binding and neutralising antibody responses, together with individual serum clonotypes, decay over the first 4 months post-infection. A similar decline in Spike-specific CD4+ and circulating T follicular helper frequencies occurs. By contrast, S-specific IgG+ memory B cells consistently accumulate over time, eventually comprising a substantial fraction of circulating the memory B cell pool. Modelling of the concomitant immune kinetics predicts maintenance of serological neutralising activity above a titre of 1:40 in 50% of convalescent participants to 74 days, although there is probably additive protection from B cell and T cell immunity. This study indicates that SARS-CoV-2 immunity after infection might be transiently protective at a population level. Therefore, SARS-CoV-2 vaccines might require greater immunogenicity and durability than natural infection to drive long-term protection.

Funder

Department of Health | National Health and Medical Research Council

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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