Immune evasion of dormant disseminated tumor cells is due to their scarcity and can be overcome by T cell immunotherapies

免疫疗法 嵌合抗原受体 免疫学 免疫系统 抗原 T细胞 主要组织相容性复合体 生物 细胞毒性T细胞 过继性细胞移植 癌症研究 生物化学 体外
作者
Erica T. Goddard,Miles H. Linde,Shivani Srivastava,Grant Klug,Tamer B. Shabaneh,Santino Iannone,Candice Alexandra Grzelak,Sydney Marsh,Alessandra I. Riggio,Ryann E. Shor,Ian L. Linde,Marissa Guerrero,Joshua R. Veatch,Annelise G. Snyder,Alana L. Welm,Stanley R. Riddell,Cyrus M. Ghajar
出处
期刊:Cancer Cell [Cell Press]
卷期号:42 (1): 119-134.e12 被引量:18
标识
DOI:10.1016/j.ccell.2023.12.011
摘要

Summary

The period between "successful" treatment of localized breast cancer and the onset of distant metastasis can last many years, representing an unexploited window to eradicate disseminated disease and prevent metastases. We find that the source of recurrence—disseminated tumor cells (DTCs) —evade endogenous immunity directed against tumor neoantigens. Although DTCs downregulate major histocompatibility complex I, this does not preclude recognition by conventional T cells. Instead, the scarcity of interactions between two relatively rare populations—DTCs and endogenous antigen-specific T cells—underlies DTC persistence. This scarcity is overcome by any one of three immunotherapies that increase the number of tumor-specific T cells: T cell-based vaccination, or adoptive transfer of T cell receptor or chimeric antigen receptor T cells. Each approach achieves robust DTC elimination, motivating discovery of MHC-restricted and -unrestricted DTC antigens that can be targeted with T cell-based immunotherapies to eliminate the reservoir of metastasis-initiating cells in patients.
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