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Characterization of human CD4 + EOMES + GzmK + T-cell subsets unveils an uncoupling of suppressive functions from IL-10-producing capacities.

Nadia PulvirentiYlenia SilvetriFrancesca ClementeRoberto BosottiElena CarelliGiorgia MoschettiPaola GruarinChiara VascoMaria Cristina CrostiMaria Lucia SarnicolaLuca ValentiDaniele PratiSergio AbrignaniJens Geginat
Published in: European journal of immunology (2024)
Human CD4 + EOMES + T cells are heterogeneous and contain Th1-cells, Tr1-cells, and CD4 + CTL. Tr1- cells and non-classical EOMES + Th1-cells displayed, respectively, anti- and pro-inflammatory cytokine profiles, but both expressed granzyme-K, produced IFN-γ, and suppressed T-cell proliferation. Diffusion map suggested a progressive CD4 + T-cell differentiation from naïve to cytotoxic cells and identified EOMES + Th1-cells as putative Tr1-cell precursors (pre-Tr1).
Keyphrases
  • induced apoptosis
  • cell cycle arrest
  • cell proliferation
  • stem cells
  • cell death
  • oxidative stress
  • multiple sclerosis
  • pi k akt
  • cell therapy
  • peripheral blood
  • anti inflammatory
  • pluripotent stem cells