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

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作者
Adam K. Wheatley
Jennifer A. Juno
Jing J. Wang
Kevin J. Selva
Arnold Reynaldi
Hyon-Xhi Tan
Wen Shi Lee
Kathleen M. Wragg
Hannah G. Kelly
Robyn Esterbauer
Samantha K. Davis
Helen E. Kent
Francesca L. Mordant
Timothy E. Schlub
David L. Gordon
David S. Khoury
Kanta Subbarao
Deborah Cromer
Tom P. Gordon
Amy W. Chung
Miles P. Davenport
Stephen J. Kent
机构
[1] University of Melbourne,Department of Microbiology and Immunology
[2] at The Peter Doherty Institute for Infection and Immunity,Australian Research Council Centre for Excellence in Convergent Bio
[3] University of Melbourne,Nano Science and Technology
[4] Flinders University,Department of Immunology, College of Medicine and Public Health
[5] Kirby Institute,Melbourne Sexual Health Centre and Department of Infectious Diseases, Alfred Hospital and Central Clinical School
[6] University of New South Wales,Sydney School of Public Health, Faculty of Medicine and Health
[7] Monash University,Department of Microbiology and Infectious Diseases
[8] University of Sydney,WHO Collaborating Centre for Reference and Research on Influenza
[9] Flinders University and SA Pathology,undefined
[10] Flinders Medical Centre,undefined
[11] The Peter Doherty Institute for Infection and Immunity,undefined
[12] Department of Immunology,undefined
[13] SA Pathology,undefined
[14] Flinders Medical Centre,undefined
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摘要
The 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.
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