1. The functional and phenotypic diversity of single T-cell infiltrates in human colorectal cancer as correlated with clinical outcome
- Author
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Marlon Stoeckius, Kelley S. Yan, Vilma L. Rosario, Kerim Secener, Kazuya Masuda, Arnold Han, Nathan Suek, P. Ravi Kiran, Matthew Ingham, Ahmed M. Al-Masrou, Peter A. Sims, Adam E. Kornberg, Paul E. Oberstein, Peter Smibert, Sijie Lin, Patricia Ho, Alyssa M. Bacarella, and Steven A. Lee-Kong
- Subjects
Transcriptome ,medicine.anatomical_structure ,Colorectal cancer ,Effector ,T cell ,T-cell receptor ,medicine ,Cancer research ,Cytotoxic T cell ,Biology ,CD38 ,medicine.disease ,Phenotype - Abstract
Although degree of T-cell infiltration in CRC was shown to correlate with a positive prognosis, the contribution of phenotypically and functionally distinct T cell subtypes within tumors remains unclear. We analyzed 37,931 single T cells with respect to transcriptome, TCR sequence and 23 cell surface proteins, from tumors and adjacent normal colon of 16 patients. Our comprehensive analysis revealed two phenotypically distinct cytotoxic T cell populations within tumors, including positively prognostic effector memory cells and non-prognostic resident memory cells. These cytotoxic T cell infiltrates transitioned from effector memory to resident memory in a stage-dependent manner. We further defined several Treg subpopulations within tumors. While Tregs overall were associated with positive clinical outcomes, CD38+ peripherally-derived Tregs, phenotypically related to Th17 cells, correlated with poor outcomes independent of cancer stage. Thus, our data highlight the diversity of T cells in CRC and demonstrate the prognostic significance of distinct T cell subtypes, which could inform therapeutic strategies.
- Published
- 2020
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