PD-1 and ICOS coexpression identifies tumor-reactive CD4+ T cells in human solid tumors
Rebekka Duhen, Olivier Fesneau, Kimberly A. Samson, Alexandra K. Frye, Michael Beymer, Venkatesh Rajamanickam, David Ross, Eric Tran, Brady Bernard, Andrew D. Weinberg, Thomas Duhen
Rebekka Duhen, Olivier Fesneau, Kimberly A. Samson, Alexandra K. Frye, Michael Beymer, Venkatesh Rajamanickam, David Ross, Eric Tran, Brady Bernard, Andrew D. Weinberg, Thomas Duhen
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Research Article Immunology Oncology

PD-1 and ICOS coexpression identifies tumor-reactive CD4+ T cells in human solid tumors

Abstract

CD4+ Th cells play a key role in orchestrating immune responses, but the identity of the CD4+ Th cells involved in the antitumor immune response remains to be defined. We analyzed the immune cell infiltrates of head and neck squamous cell carcinoma and colorectal cancers and identified a subset of CD4+ Th cells distinct from FOXP3+ Tregs that coexpressed programmed cell death 1 (PD-1) and ICOS. These tumor-infiltrating lymphocyte CD4+ Th cells (CD4+ Th TILs) had a tissue-resident memory phenotype, were present in MHC class II–rich areas, and proliferated in the tumor, suggesting local antigen recognition. The T cell receptor repertoire of the PD-1+ICOS+ CD4+ Th TILs was oligoclonal, with T cell clones expanded in the tumor, but present at low frequencies in the periphery. Finally, these PD-1+ICOS+ CD4+ Th TILs were shown to recognize both tumor-associated antigens and tumor-specific neoantigens. Our findings provide an approach for isolating tumor-reactive CD4+ Th TILs directly ex vivo that will help define their role in the antitumor immune response and potentially improve future adoptive T cell therapy approaches.

Authors

Rebekka Duhen, Olivier Fesneau, Kimberly A. Samson, Alexandra K. Frye, Michael Beymer, Venkatesh Rajamanickam, David Ross, Eric Tran, Brady Bernard, Andrew D. Weinberg, Thomas Duhen

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Figure 5

The presence of DP CD4+ Th cells positively correlates with DP CD8+ T cells in HNSCC, but not in CRC.

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The presence of DP CD4+ Th cells positively correlates with DP CD8+ T ce...
(A) Comparison of the percentage of DP CD4+ and DP CD8+ cells between HNSCC (n = 49) and CRC (n = 31) tumors. (B) Correlation between the frequencies of DP CD4+ and DP CD8+ cells in patients with HNSCC (n = 49) or CRC (n = 31). Red circles represent HPV+ HNSCC tumors. (C) qPCR analysis of CXCL9, CXCL10, and CXCL11 mRNA expression by the indicated CD4+ T cell subsets isolated from patients with HNSCC or CRC directly ex vivo. Horizontal lines indicate the mean ± SEM. *P < 0.05 and **P < 0.01, by unpaired 2-tailed t test (A) or 1-way ANOVA with Tukey’s post hoc test (C).