OncoImmunology (Dec 2022)

Targeting NKG2A to boost anti-tumor CD8 T-cell responses in human colorectal cancer

  • Kathleen Ducoin,
  • Romain Oger,
  • Linda Bilonda Mutala,
  • Cécile Deleine,
  • Nicolas Jouand,
  • Juliette Desfrançois,
  • Juliette Podevin,
  • Emilie Duchalais,
  • Jonathan Cruard,
  • Houssem Benlalam,
  • Nathalie Labarrière,
  • Céline Bossard,
  • Anne Jarry,
  • Nadine Gervois-Segain

DOI
https://doi.org/10.1080/2162402X.2022.2046931
Journal volume & issue
Vol. 11, no. 1

Abstract

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Recently, the inhibitory CD94/NKG2A receptor has joined the group of immune checkpoints (ICs) and its expression has been documented in NK cells and CD8+ T lymphocytes in several cancers and some infectious diseases. In colorectal cancer (CRC), we previously reported that NKG2A+ tumor-infiltrating lymphocytes (TILs) are predominantly CD8+ αβ T cells and that CD94 overexpression and/or its ligand HLA-E were associated with a poor prognosis. This study aimed to thoroughly characterize the NKG2A+ CD8+ TIL subpopulation and document the impact of NKG2A on anti-tumor responses in CRC. Our findings highlight new features of this subpopulation: (i) enrichment in colorectal tumors compared to paired normal colonic mucosa, (ii) their character as tissue-resident T cells and their majority terminal exhaustion status, (iii) co-expression of other ICs delineating two subgroups differing mainly in the level of NKG2A expression and the presence of PD-1, (iv) high functional avidity despite reduced proliferative capacity and finally (v) inhibition of anti-tumor reactivity that is overcome by blocking NKG2A. From a clinical point of view, these results open a promising alternative for immunotherapies based on NKG2A blockade in CRC, which could be performed alone or in combination with other IC inhibitors, adoptive cell transfer or therapeutic vaccination.

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