Expression of Foxp3 by T follicular helper cells in end-stage germinal centers

Johanne T. Jacobsen(Rockefeller University), Wei Hu(Memorial Sloan Kettering Cancer Center), Tiago B. R. Castro(Rockefeller University), Sigrid Solem(Rockefeller University), Alice Galante(Rockefeller University), Zeran Lin(Rockefeller University), Samuel J. Allon(Broad Institute), Luka Mesin(Rockefeller University), Angelina M. Bilate(Rockefeller University), Ariën Schiepers(Rockefeller University), Alex K. Shalek(Broad Institute), Alexander Y. Rudensky(Memorial Sloan Kettering Cancer Center), Gabriel D. Victora(Rockefeller University)
Science
July 15, 2021
10.1126/science.abe5146
Cited by 128Open Access
Full Text

Abstract

Regulating germinal center contraction Germinal centers (GCs) in secondary lymphoid organs are where mature B cells expand and differentiate. Although GC formation is well studied, the control of GC duration and contraction is less well understood. Using intravital imaging of mouse GCs and single-cell RNA sequencing, Jacobsen et al. report that T follicular helper (T FH ) cells are a critical player in this process. They found that some late-GC T FH cells upregulate the transcription factor FOXP3 and acquire a regulatory T cell–like phenotype. These cells are distinct from T follicular regulatory (T FR ) cells and, unlike T FR cells, are needed to shut down the GC reaction. Tweaking this process may be key to extending GC lifetimes and enhancing antibody responses in the context of vaccination. Science , abe5146, this issue p. eabe5146

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