Co-expression of CD39 and CD103 identifies tumor-reactive CD8 T cells in human solid tumors.
Thomas DuhenRebekka DuhenRyan MontlerJake MosesTarsem MoudgilNoel F de MirandaCheri P GoodallTiffany C BlairBernard A FoxJason E McDermottShu-Ching ChangGary GrunkemeierRom LeidnerRichard Bryan BellAndrew D WeinbergPublished in: Nature communications (2018)
Identifying tumor antigen-specific T cells from cancer patients has important implications for immunotherapy diagnostics and therapeutics. Here, we show that CD103+CD39+ tumor-infiltrating CD8 T cells (CD8 TIL) are enriched for tumor-reactive cells both in primary and metastatic tumors. This CD8 TIL subset is found across six different malignancies and displays an exhausted tissue-resident memory phenotype. CD103+CD39+ CD8 TILs have a distinct T-cell receptor (TCR) repertoire, with T-cell clones expanded in the tumor but present at low frequencies in the periphery. CD103+CD39+ CD8 TILs also efficiently kill autologous tumor cells in a MHC-class I-dependent manner. Finally, higher frequencies of CD103+CD39+ CD8 TILs in patients with head and neck cancer are associated with better overall survival. Our data thus describe an approach for detecting tumor-reactive CD8 TILs that will help define mechanisms of existing immunotherapy treatments, and may lead to future adoptive T-cell cancer therapies.
Keyphrases
- squamous cell carcinoma
- small cell lung cancer
- stem cells
- oxidative stress
- immune response
- gene expression
- bone marrow
- induced apoptosis
- small molecule
- cell death
- deep learning
- patient safety
- genome wide
- mesenchymal stem cells
- quality improvement
- regulatory t cells
- dna methylation
- big data
- dendritic cells
- signaling pathway
- endoplasmic reticulum stress