AI Article Synopsis

  • CD4+ Th cells are crucial for immune responses, but the specific CD4+ Th cells that target tumors are not well defined.
  • Researchers identified a unique subset of CD4+ Th cells in head and neck squamous cell carcinoma and colorectal cancers that coexpress PD-1 and ICOS, distinguishing them from regulatory T cells (Tregs).
  • These tumor-infiltrating CD4+ Th cells show a memory-like behavior, proliferate within the tumor, and are capable of recognizing both tumor-associated and neoantigens, indicating their potential use in improving adoptive T cell therapies.

Article 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.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9197519PMC
http://dx.doi.org/10.1172/JCI156821DOI Listing

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