Litcius/Paper detail

Vaccination-induced T cell responses maintain polyclonality with high antigen receptor avidity

Katharina Kocher, Felix Drost, Abel Tesfaye, Carolin Moosmann, Christine Schülein, M. Grotz, Elvira D’Ippolito, Frederik Graw, B. Spriewald, Dirk H. Busch, Christian Bogdan, Matthias Tenbusch, Benjamin Schubert, Kilian Schober

2025Science Immunology9 citationsDOI

Abstract

Clonal expansion is a hallmark of adaptive immunity and has been challenging to investigate in humans in a standardized manner compared with animal models. We studied a cohort of 29 healthy individuals who received three mRNA vaccinations against SARS-CoV-2 before a breakthrough infection. We characterized the magnitude, phenotype, and clonal composition of CD8 T cell responses against 16 epitope specificities by ELISpot; flow cytometry; and single-cell RNA, protein, and T cell receptor (TCR) sequencing. One hundred six TCRs from five epitope-specific repertoires were reexpressed and tested for peptide sensitivity. Whereas vaccination-recruited T cell repertoires were enriched for high-avidity TCRs, differential clonal expansion was not linked to fine avidity differences. Instead, maintenance of polyclonality ensured robustness in counteracting viral mutational escape through altered epitopes. Deciphering the functionality of human antigen-specific T cell repertoires instructs our understanding of human T cell biology and may guide the development of vaccines and other immunotherapies.

Topics & Concepts

AvidityBiologyT cellEpitopeT-cell receptorCD8ImmunologyAntigenImmunityVirologyImmune systemCytotoxic T cellCellCell biologyAcquired immune systemReceptorFlow cytometryB cellAntigen-presenting cellImmunotherapyCell growthMajor histocompatibility complexDendritic cellMonoclonal antibodyT lymphocyteCAR-T cell therapy researchT-cell and B-cell ImmunologyImmunotherapy and Immune Responses