Cancers (Apr 2021)

Activated Regulatory T-Cells, Dysfunctional and Senescent T-Cells Hinder the Immunity in Pancreatic Cancer

  • Shivan Sivakumar,
  • Enas Abu-Shah,
  • David J. Ahern,
  • Edward H. Arbe-Barnes,
  • Ashwin K. Jainarayanan,
  • Nagina Mangal,
  • Srikanth Reddy,
  • Aniko Rendek,
  • Alistair Easton,
  • Elke Kurz,
  • Michael Silva,
  • Zahir Soonawalla,
  • Lara R. Heij,
  • Rachael Bashford-Rogers,
  • Mark R. Middleton,
  • Michael L. Dustin

DOI
https://doi.org/10.3390/cancers13081776
Journal volume & issue
Vol. 13, no. 8
p. 1776

Abstract

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Pancreatic cancer has one of the worst prognoses of any human malignancy and leukocyte infiltration is a major prognostic marker of the disease. As current immunotherapies confer negligible survival benefits, there is a need to better characterise leukocytes in pancreatic cancer to identify better therapeutic strategies. In this study, we analysed 32 human pancreatic cancer patients from two independent cohorts. A multi-parameter mass-cytometry analysis was performed on 32,000 T-cells from eight patients. Single-cell RNA sequencing dataset analysis was performed on a cohort of 24 patients. Multiplex immunohistochemistry imaging and spatial analysis were performed to map immune infiltration into the tumour microenvironment. Regulatory T-cell populations demonstrated highly immunosuppressive states with high TIGIT, ICOS and CD39 expression. CD8+ T-cells were found to be either in senescence or an exhausted state. The exhausted CD8 T-cells had low PD-1 expression but high TIGIT and CD39 expression. These findings were corroborated in an independent pancreatic cancer single-cell RNA dataset. These data suggest that T-cells are major players in the suppressive microenvironment of pancreatic cancer. Our work identifies multiple novel therapeutic targets that should form the basis for rational design of a new generation of clinical trials in pancreatic ductal adenocarcinoma.

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