Tumor-specific T cell dysfunction is a dynamic antigen-driven differentiation program initiated early during tumorigenesis Journal Article


Authors: Schietinger, A.; Philip, M.; Krisnawan, V. E.; Chiu, E. Y.; Delrow, J. J.; Basom, R. S.; Lauer, P.; Brockstedt, D. G.; Knoblaugh, S. E.; Hämmerling, G. J.; Schell, T. D.; Garbi, N.; Greenberg, P. D.
Article Title: Tumor-specific T cell dysfunction is a dynamic antigen-driven differentiation program initiated early during tumorigenesis
Abstract: CD8+ T cells recognizing tumor-specific antigens are detected in cancer patients but are dysfunctional. Here we developed a tamoxifen-inducible liver cancer mouse model with a defined oncogenic driver antigen (SV40 large T-antigen) to follow the activation and differentiation of naive tumor-specific CD8+ T (TST) cells after tumor initiation. Early during the pre-malignant phase of tumorigenesis, TST cells became dysfunctional, exhibiting phenotypic, functional, and transcriptional features similar to dysfunctional T cells isolated from late-stage human tumors. Thus, T cell dysfunction seen in advanced human cancers may already be established early during tumorigenesis. Although the TST cell dysfunctional state was initially therapeutically reversible, it ultimately evolved into a fixed state. Persistent antigen exposure rather than factors associated with the tumor microenvironment drove dysfunction. Moreover, the TST cell differentiation and dysfunction program exhibited features distinct from T cell exhaustion in chronic infections. Strategies to overcome this antigen-driven, cell-intrinsic dysfunction may be required to improve cancer immunotherapy. © 2016 Elsevier Inc.
Journal Title: Immunity
Volume: 45
Issue: 2
ISSN: 1074-7613
Publisher: Cell Press  
Date Published: 2016-08-16
Start Page: 389
End Page: 401
Language: English
DOI: 10.1016/j.immuni.2016.07.011
PROVIDER: scopus
PUBMED: 27521269
PMCID: PMC5119632
DOI/URL:
Notes: Article -- Export Date: 3 January 2017 -- Source: Scopus
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  1. Mary   Philip
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