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Nat Med . Antibody responses and correlates of protection in the general population after two doses of the ChAdOx1 or BNT162b2 vaccines

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  • Nat Med . Antibody responses and correlates of protection in the general population after two doses of the ChAdOx1 or BNT162b2 vaccines


    Nat Med


    . 2022 Feb 14.
    doi: 10.1038/s41591-022-01721-6. Online ahead of print.
    Antibody responses and correlates of protection in the general population after two doses of the ChAdOx1 or BNT162b2 vaccines


    Jia Wei # 1 2 , Koen B Pouwels # 3 4 , Nicole Stoesser 1 3 5 6 , Philippa C Matthews 1 6 , Ian Diamond 7 , Ruth Studley 7 , Emma Rourke 7 , Duncan Cook 7 , John I Bell 8 , John N Newton 9 , Jeremy Farrar 10 , Alison Howarth 1 6 , Brian D Marsden 1 11 , Sarah Hoosdally 1 , E Yvonne Jones 1 , David I Stuart 1 , Derrick W Crook 1 3 5 6 , Tim E A Peto 1 3 5 6 , A Sarah Walker 1 2 3 12 , David W Eyre 13 14 15 16 , COVID-19 Infection Survey team



    Collaborators, Affiliations

    Abstract

    Antibody responses are an important part of immunity after Coronavirus Disease 2019 (COVID-19) vaccination. However, antibody trajectories and the associated duration of protection after a second vaccine dose remain unclear. In this study, we investigated anti-spike IgG antibody responses and correlates of protection after second doses of ChAdOx1 or BNT162b2 vaccines for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in the United Kingdom general population. In 222,493 individuals, we found significant boosting of anti-spike IgG by the second doses of both vaccines in all ages and using different dosing intervals, including the 3-week interval for BNT162b2. After second vaccination, BNT162b2 generated higher peak levels than ChAdOX1. Older individuals and males had lower peak levels with BNT162b2 but not ChAdOx1, whereas declines were similar across ages and sexes with ChAdOX1 or BNT162b2. Prior infection significantly increased antibody peak level and half-life with both vaccines. Anti-spike IgG levels were associated with protection from infection after vaccination and, to an even greater degree, after prior infection. At least 67% protection against infection was estimated to last for 2-3 months after two ChAdOx1 doses, for 5-8 months after two BNT162b2 doses in those without prior infection and for 1-2 years for those unvaccinated after natural infection. A third booster dose might be needed, prioritized to ChAdOx1 recipients and those more clinically vulnerable.


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