OncoImmunology (May 2018)

Expression of LLT1 and its receptor CD161 in lung cancer is associated with better clinical outcome

  • Véronique M. Braud,
  • Jérôme Biton,
  • Etienne Becht,
  • Samantha Knockaert,
  • Audrey Mansuet-Lupo,
  • Estelle Cosson,
  • Diane Damotte,
  • Marco Alifano,
  • Pierre Validire,
  • Fabienne Anjuère,
  • Isabelle Cremer,
  • Nicolas Girard,
  • Dominique Gossot,
  • Agathe Seguin-Givelet,
  • Marie-Caroline Dieu-Nosjean,
  • Claire Germain

DOI
https://doi.org/10.1080/2162402X.2017.1423184
Journal volume & issue
Vol. 7, no. 5

Abstract

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Co-stimulatory and inhibitory receptors expressed by immune cells in the tumor microenvironment modulate the immune response and cancer progression. Their expression and regulation are still not fully characterized and a better understanding of these mechanisms is needed to improve current immunotherapies. Our previous work has identified a novel ligand/receptor pair, LLT1/CD161, that modulates immune responses. Here, we extensively characterize its expression in non-small cell lung cancer (NSCLC). We show that LLT1 expression is restricted to germinal center (GC) B cells within tertiary lymphoid structures (TLS), representing a new hallmark of the presence of active TLS in the tumor microenvironment. CD161-expressing immune cells are found at the vicinity of these structures, with a global enrichment of NSCLC tumors in CD161+ CD4+ and CD8+ T cells as compared to normal distant lung and peripheral blood. CD161+ CD4+ T cells are more activated and produce Th1-cytokines at a higher frequency than their matched CD161-negative counterparts. Interestingly, CD161+ CD4+ T cells highly express OX40 co-stimulatory receptor, less frequently 4-1BB, and display an activated but not completely exhausted PD-1-positive Tim-3-negative phenotype. Finally, a meta-analysis revealed a positive association of CLEC2D (coding for LLT1) and KLRB1 (coding for CD161) gene expression with favorable outcome in NSCLC, independently of the size of T and B cell infiltrates. These data are consistent with a positive impact of LLT1/CD161 on NSCLC patient survival, and make CD161-expressing CD4+ T cells ideal candidates for efficient anti-tumor recall responses.

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