Frontiers in Immunology (May 2023)

Omicron infection-associated T- and B-cell immunity in antigen-naive and triple-COVID-19-vaccinated individuals

  • Joana Barros-Martins,
  • Swantje I. Hammerschmidt,
  • Gema Morillas Ramos,
  • Anne Cossmann,
  • Laura Hetzel,
  • Ivan Odak,
  • Miriam Köhler,
  • Metodi V. Stankov,
  • Christiane Ritter,
  • Michaela Friedrichsen,
  • Inga Ravens,
  • Anja Schimrock,
  • Jasmin Ristenpart,
  • Anika Janssen,
  • Stefanie Willenzon,
  • Günter Bernhardt,
  • Ralf Lichtinghagen,
  • Berislav Bošnjak,
  • Georg M. N. Behrens,
  • Georg M. N. Behrens,
  • Georg M. N. Behrens,
  • Reinhold Förster,
  • Reinhold Förster,
  • Reinhold Förster

DOI
https://doi.org/10.3389/fimmu.2023.1166589
Journal volume & issue
Vol. 14

Abstract

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Since early 2022, various Omicron variants have dominated the SARS-CoV-2 pandemic in most countries. All Omicron variants are B-cell immune escape variants, and antibodies induced by first-generation COVID-19 vaccines or by infection with earlier SARS-CoV-2 variants largely fail to protect individuals from Omicron infection. In the present study, we investigated the effect of Omicron infections in triple-vaccinated and in antigen-naive individuals. We show that Omicron breakthrough infections occurring 2–3.5 months after the third vaccination restore B-cell and T-cell immune responses to levels similar to or higher than those measured 14 days after the third vaccination, including the induction of Omicron-neutralizing antibodies. Antibody responses in breakthrough infection derived mostly from cross-reacting B cells, initially induced by vaccination, whereas Omicron infections in antigen-naive individuals primarily generated B cells binding to the Omicron but not the Wuhan spike protein. Although antigen-naive individuals mounted considerable T-cell responses after infection, B-cell responses were low, and neutralizing antibodies were frequently below the limit of detection. In summary, the detection of Omicron-associated B-cell responses in primed and in antigen-naive individuals supports the application of Omicron-adapted COVID-19 vaccines, but calls into question their suitability if they also contain/encode antigens of the original Wuhan virus.

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