Effectiveness of BNT162b2 mRNA vaccine third doses and previous infection in protecting against SARS-CoV-2 infections during the Delta and Omicron variant waves; the UK SIREN cohort study September 2021 to February 2022

Victoria J Hall; Ferdinando Insalata; Sarah Foulkes; Peter Kirwan; Dominic Sparkes; Ana Atti; Michelle Cole; Elen de Lacy; Lesley Price; Diane Corrigan; Colin S Brown; Jasmin Islam; Andre Charlett; Susan Hopkins; SIREN Study Group

doi:10.1016/j.jinf.2023.10.022

Effectiveness of BNT162b2 mRNA vaccine third doses and previous infection in protecting against SARS-CoV-2 infections during the Delta and Omicron variant waves; the UK SIREN cohort study September 2021 to February 2022

J Infect. 2024 Jan;88(1):30-40. doi: 10.1016/j.jinf.2023.10.022. Epub 2023 Nov 4.

Authors

Affiliations

¹ UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom. Electronic address: victoria.hall@ukhsa.gov.uk.
² UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom; Department of Mathematics, Imperial College London, London, SW7 2AZ, United Kingdom. Electronic address: ferdinando.insalata@ukhsa.gov.uk.
³ UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom. Electronic address: sarah.foulkes@ukhsa.gov.uk.
⁴ UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom; MRC Biostatistics Unit, University of Cambridge, Institute of Public Health, Forvie Site, Robinson Way, Cambridge CB2 0SR, United Kingdom. Electronic address: peter.kirwan@mrc-bsu.cam.ac.uk.
⁵ UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom. Electronic address: dominic.sparkes@ukhsa.gov.uk.
⁶ UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom. Electronic address: ana.atti@ukhsa.gov.uk.
⁷ UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom. Electronic address: michelle.cole@ukhsa.gov.uk.
⁸ Public Health Wales, 2 Capital Quarter, Tyndall Street, Cardiff CF10 4BZ, United Kingdom. Electronic address: elen.delacy@wales.nhs.uk.
⁹ Glasgow Caledonian University, Cowcaddens Road, Glasgow G4 0BA, United Kingdom; Public Health Scotland, Gyle Square 1 South Gyle Crescent, Edinburgh EH12 9EB, United Kingdom. Electronic address: l.price@gcu.ac.uk.
¹⁰ Public Health Agency Northern Ireland, Unit 12-22 Linenhall Street, Belfast BT2 8BS, United Kingdom. Electronic address: Diane.Corrigan@hscni.net.
¹¹ UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom. Electronic address: colin.brown@ukhsa.gov.uk.
¹² UK Health Security Agency, 10 South Colonnade, London E14 4PU, United Kingdom. Electronic address: jamin.islam@ukhsa.gov.uk.
¹³ UK Health Security Agency, UK Health Security Agency, Nobel House, 17 Smith Square, London, SW1P 3JR. Electronic address: andre.charlett@ukhsa.gov.uk.
¹⁴ UK Health Security Agency, UK Health Security Agency, Nobel House, 17 Smith Square, London, SW1P 3JR. Electronic address: susan.hopkins@ukhsa.gov.uk.

PMID: 37926119
DOI: 10.1016/j.jinf.2023.10.022

Abstract

Third doses of COVID-19 vaccines were widely deployed following the primary vaccine course waning and the emergence of the Omicron-variant. We investigated protection from third-dose vaccines and previous infection against SARS-CoV-2 infection during Delta-variant and Omicron-variant (BA.1 & BA.2) waves in our frequently PCR-tested cohort of healthcare-workers. Relative effectiveness of BNT162b2 third doses and infection-acquired immunity was assessed by comparing the time to PCR-confirmed infection in boosted participants with those with waned dose-2 protection (≥254 days after dose-2), by primary series vaccination type. Follow-up time was divided by dominant circulating variant: Delta 07 September 2021 to 30 November 2021, Omicron 13 December 2021t o 28 February 2022. We used a Cox regression model with adjustment/stratification for demographic characteristics and staff-type. We explored protection associated with vaccination, infection and both. We included 19,614 participants, 29% previously infected. There were 278 primary infections (4 per 10,000 person-days of follow-up) and 85 reinfections (0.8/10,000 person-days) during the Delta period and 2467 primary infections (43/10,000 person-days) and 881 reinfections (33/10,000) during the Omicron period. Relative Vaccine Effectiveness (VE) 0-2 months post-3rd dose (3rd dose) (3-doses BNT162b2) in the previously uninfected cohort against Delta infections was 63% (95% Confidence Interval (CI) 40%-77%) and was lower (35%) against Omicron infection (95% CI 21%-47%). The relative VE of 3rd dose (heterologous BNT162b2) was greater for primary course ChAdOX1 recipients, with VE 0-2 months post-3rd dose over ≥68% higher for both variants. Third-dose protection waned rapidly against Omicron, with no significant difference between two and three BNT162b2 doses observed after 4-months. Previous infection continued to provide additional protection against Omicron (67% (CI 56%-75%) 3-6 months post-infection), but this waned to about 25% after 9-months, approximately three times lower than against Delta. Infection rates surged with Omicron emergence. Third doses of BNT162b2 vaccine provided short-term protection, with rapid waning against Omicron infections. Protection associated with infections incurred before Omicron was markedly diminished against the Omicron wave. Our findings demonstrate the complexity of an evolving pandemic with the potential emergence of immune-escape variants and the importance of continued monitoring.

Keywords: COVID-19; Omicron; Reinfection; SARS-CoV-2; Vaccine Effectiveness.

MeSH terms

BNT162 Vaccine*
COVID-19 Vaccines
COVID-19* / prevention & control
Cohort Studies
Humans
Reinfection
SARS-CoV-2
United Kingdom / epidemiology
mRNA Vaccines

Substances

BNT162 Vaccine
COVID-19 Vaccines
mRNA Vaccines

Supplementary concepts

SARS-CoV-2 variants

Grants and funding

MR/W02067X/1/MRC_/Medical Research Council/United Kingdom