Hybrid immunity from severe acute respiratory syndrome coronavirus 2 infection and vaccination in Canadian adults: A cohort study

Author:

Brown Patrick E1,Fu Sze Hang1,Newcombe Leslie1ORCID,Tang Xuyang1ORCID,Nagelkerke Nico1,Birnboim H Chaim1,Bansal Aiyush1,Colwill Karen2,Mailhot Geneviève2,Delgado-Brand Melanie2,Tursun Tulunay2,Qi Freda2,Gingras Anne-Claude2ORCID,Slutsky Arthur S3,Pasic Maria D3,Companion Jeffrey3,Bogoch Isaac I4,Morawski Ed5,Lam Teresa5,Reid Angus5,Jha Prabhat1ORCID,

Affiliation:

1. Centre for Global Health Research, Unity Health Toronto and University of Toronto

2. Lunenfeld-Tanenbaum Research Institute, Sinai Health

3. Unity Health Toronto

4. Toronto General Hospital, University Hospital Network

5. Angus Reid Institute

Abstract

Background:Few national-level studies have evaluated the impact of ‘hybrid’ immunity (vaccination coupled with recovery from infection) from the Omicron variants of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2).Methods:From May 2020 to December 2022, we conducted serial assessments (each of ~4000–9000 adults) examining SARS-CoV-2 antibodies within a mostly representative Canadian cohort drawn from a national online polling platform. Adults, most of whom were vaccinated, reported viral test-confirmed infections and mailed self-collected dried blood spots (DBSs) to a central lab. Samples underwent highly sensitive and specific antibody assays to spike and nucleocapsid protein antigens, the latter triggered only by infection. We estimated cumulative SARS-CoV-2 incidence prior to the Omicron period and during the BA.1/1.1 and BA.2/5 waves. We assessed changes in antibody levels and in age-specific active immunity levels.Results:Spike levels were higher in infected than in uninfected adults, regardless of vaccination doses. Among adults vaccinated at least thrice and infected more than 6 months earlier, spike levels fell notably and continuously for the 9-month post-vaccination. In contrast, among adults infected within 6 months, spike levels declined gradually. Declines were similar by sex, age group, and ethnicity. Recent vaccination attenuated declines in spike levels from older infections. In a convenience sample, spike antibody and cellular responses were correlated. Near the end of 2022, about 35% of adults above age 60 had their last vaccine dose more than 6 months ago, and about 25% remained uninfected. The cumulative incidence of SARS-CoV-2 infection rose from 13% (95% confidence interval 11–14%) before omicron to 78% (76–80%) by December 2022, equating to 25 million infected adults cumulatively. However, the coronavirus disease 2019 (COVID-19) weekly death rate during the BA.2/5 waves was less than half of that during the BA.1/1.1 wave, implying a protective role for hybrid immunity.Conclusions:Strategies to maintain population-level hybrid immunity require up-to-date vaccination coverage, including among those recovering from infection. Population-based, self-collected DBSs are a practicable biological surveillance platform.Funding:Funding was provided by the COVID-19 Immunity Task Force, Canadian Institutes of Health Research, Pfizer Global Medical Grants, and St. Michael’s Hospital Foundation. PJ and ACG are funded by the Canada Research Chairs Program.

Funder

COVID-19 Immunity Task Force

Canadian Institutes of Health Research

Pfizer Global Medical Grants

St. Michael's Hospital Foundation

Canada Research Chairs Program

Publisher

eLife Sciences Publications, Ltd

Reference30 articles.

1. Participant Information Sheet;Action to Beat Coronavirus Study,2021

2. Protection against the Omicron Variant from Previous SARS-CoV-2 Infection;Altarawneh;The New England Journal of Medicine,2022

3. Incidence of Omicron: One-in-five Canadians report COVID-19 infection in their household since Dec. 1. Angus Reid Forum;Angus Reid,2022

4. How we poll;Angus Reid Institute,2024

5. Protective effectiveness of previous SARS-CoV-2 infection and hybrid immunity against the omicron variant and severe disease: a systematic review and meta-regression;Bobrovitz;The Lancet. Infectious Diseases,2023

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