Humoral Immunity to SARS-CoV-2 and Inferred Protection from Infection in a French Longitudinal Community Cohort

Author:

Woudenberg Tom,Pinaud Laurie,Garcia Laura,Tondeur Laura,Pelleau Stéphane,De Thoisy Alix,Donnadieu Françoise,Backovic Marija,Attia Mikaël,Hozé Nathanael,Duru Cécile,Koffi Aymar Davy,Castelain Sandrine,Ungeheuer Marie-Noelle,Pellerin Sandrine Fernandes,Planas Delphine,Bruel TimothéeORCID,Cauchemez Simon,Schwartz Olivier,Fontanet Arnaud,White Michael

Abstract

AbstractPopulation-level immunity to SARS-CoV-2 is growing through vaccination as well as ongoing circulation. Given waning immunity and emergence of new variants, it is important to dynamically determine the risk of re-infection in the population. For estimating immune protection, neutralization titers are most informative, but these assays are difficult to conduct at a population level. Measurement of antibody levels can be implemented at high throughput, but has not been robustly validated as a correlate of protection. Here, we have developed a method that predicts neutralization and protection based on variant-specific antibody measurements to SARS-CoV-2 antigens. This approach allowed us to estimate population-immunity in a longitudinal cohort from France followed for up to 2 years. Participants with a single vaccination or immunity caused by infection only are especially vulnerable to COVID-19 or hospitalization due to SARS-CoV-2. While the median reduced risk to COVID-19 in participants with 3 vaccinations was 96%, the median reduced risk among participants with infection-acquired immunity only was 42%. The results presented here are consistent with data from vaccine-effectiveness studies indicating robustness of our approach. Our multiplex serological assay can be readily optimized and employed to study any new variant and provides a framework for development of an assay that would include protection estimates.

Publisher

Cold Spring Harbor Laboratory

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