JCI Insight (Jan 2021)

PD-1 blockade restores helper activity of tumor-infiltrating, exhausted PD-1hiCD39+ CD4 T cells

  • Camille-Charlotte Balança,
  • Anna Salvioni,
  • Clara-Maria Scarlata,
  • Marie Michelas,
  • Carlos Martinez-Gomez,
  • Carlos Gomez-Roca,
  • Victor Sarradin,
  • Marie Tosolini,
  • Carine Valle,
  • Frédéric Pont,
  • Gwénaël Ferron,
  • Laurence Gladieff,
  • Sébastien Vergez,
  • Agnès Dupret-Bories,
  • Eliane Mery,
  • Philippe Rochaix,
  • Jean-Jacques Fournié,
  • Jean-Pierre Delord,
  • Christel Devaud,
  • Alejandra Martinez,
  • Maha Ayyoub

Journal volume & issue
Vol. 6, no. 2

Abstract

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Tumor antigen–specific CD4 T cells accumulate at tumor sites, evoking their involvement in antitumor effector functions in situ. Contrary to CD8 cytotoxic T lymphocyte exhaustion, that of CD4 T cells remains poorly appreciated. Here, using phenotypic, transcriptomic, and functional approaches, we characterized CD4 T cell exhaustion in patients with head and neck, cervical, and ovarian cancer. We identified a CD4 tumor-infiltrating lymphocyte (TIL) population, defined by high PD-1 and CD39 expression, which contained high proportions of cytokine-producing cells, although the quantity of cytokines produced by these cells was low, evoking an exhausted state. Terminal exhaustion of CD4 TILs was instated regardless of TIM-3 expression, suggesting divergence with CD8 T cell exhaustion. scRNA-Seq and further phenotypic analyses uncovered similarities with the CD8 T cell exhaustion program. In particular, PD-1hiCD39+ CD4 TILs expressed the exhaustion transcription factor TOX and the chemokine CXCL13 and were tumor antigen specific. In vitro, PD-1 blockade enhanced CD4 TIL activation, as evidenced by increased CD154 expression and cytokine secretion, leading to improved dendritic cell maturation and consequently higher tumor-specific CD8 T cell proliferation. Our data identify exhausted CD4 TILs as players in responsiveness to immune checkpoint blockade.

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