The challenge of limited vaccine supplies: impact of prior infection on anti-spike IgG antibody trajectories after a single COVID-19 vaccination

Author:

Wei JiaORCID,Matthews Philippa C.ORCID,Stoesser NicoleORCID,Diamond Ian,Studley Ruth,Rourke Emma,Cook Duncan,Bell John I,Newton John N,Farrar Jeremy,Howarth Alison,Marsden Brian D.,Hoosdally Sarah,Jones E Yvonne,Stuart David I,Crook Derrick W.,Peto Tim E. A.,Walker A. Sarah,Eyre David W.,Pouwels Koen B.,

Abstract

AbstractGiven high SARS-CoV-2 incidence, coupled with slow and inequitable vaccine roll-out, there is an urgent need for evidence to underpin optimum vaccine deployment, aiming to maximise global population immunity at speed. We evaluate whether a single vaccination in previously infected individuals generates similar initial and subsequent antibody responses to two vaccinations in those without prior infection. We compared anti-spike IgG antibody responses after a single dose of ChAdOx1, BNT162b2, or mRNA-1273 SARS-CoV-2 vaccines in the COVID-19 Infection Survey in the UK general population. In 100,849 adults who received at least one vaccination, 13,404 (13.3%) had serological and/or PCR evidence of prior infection. Prior infection significantly boosted antibody responses for all three vaccines, producing a higher peak level and longer half-life, and a response comparable to those without prior infection receiving two vaccinations. In those with prior infection, median time above the positivity threshold was estimated to last for >1 year after the first dose. Single-dose vaccination targeted to those previously infected may provide protection in populations with high rates of previous infection faced with limited vaccine supply, as an interim measure while vaccine campaigns are scaled up.

Publisher

Cold Spring Harbor Laboratory

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