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Age-associated contraction of tumor-specific T cells impairs antitumor immunity
Cancer Immunol Res. 2024 Aug 24. doi: 10.1158/2326-6066.CIR-24-0463.
Peter Georgiev 1, SeongJun Han 2, Amy Y Huang 3, Thao H Nguyen 4, Jefte M Drijvers 4, Hannah Creasey 5, Joseph A Pereira 6, Cong-Hui Yao 6, Joon Seok Park 5, Thomas S Conway 6, Megan E Fung 6, Dan Liang 6, Michael Peluso 7, Shakchhi Joshi 7, Jared H Rowe 8, Brian C Miller 9, Gordon J Freeman 8, Arlene H Sharpe 4, Marcia C Haigis 5, Alison E Ringel 10
Abstract:
...In this study, we set out to understand whether deficits in antitumor immunity with advanced age promote tumor progression and/or drive resistance to immunotherapy. We found that multiple syngeneic cancers grew more rapidly in aged versus young adult mice, driven by dysfunctional CD8+ T-cell responses. By systematically mapping immune cell profiles within tumors, we identified loss of tumor antigen-specific CD8+ T cells as a primary feature accelerating the growth of tumors in aged mice and driving resistance to immunotherapy. When antigen-specific T cells from young adult mice were administered to aged mice, tumor outgrowth was delayed and the aged animals became sensitive to PD-1 blockade. These studies reveal how age-associated CD8+ T-cell dysfunction may license tumorigenesis in elderly patients and have important implications for the use of aged mice as pre-clinical models of aging and cancer.