IL-7R licenses a population of epigenetically poised memory CD8 + T cells with superior antitumor efficacy that are critical for melanoma memory

黑色素瘤 人口 癌症研究 细胞毒性T细胞 免疫疗法 免疫学 CD8型 免疫系统 生物 免疫检查点 记忆T细胞 抗原 低甲基化剂 医学 DNA甲基化 基因表达 遗传学 环境卫生 基因 体外
作者
Goran Micevic,Andrew Daniels,Karine Flem-Karlsen,Koonam Park,Ronan Talty,Meaghan K. McGeary,Haris Mirza,Holly N. Blackburn,Esen Sefik,Julie F. Cheung,Noah I. Hornick,Lilach Aizenbud,Nikhil S. Joshi,Harriet M. Kluger,Akiko Iwasaki,Marcus W. Bosenberg,Richard A. Flavell
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [National Academy of Sciences]
卷期号:120 (30) 被引量:4
标识
DOI:10.1073/pnas.2304319120
摘要

Recurrence of advanced melanoma after therapy is a major risk factor for reduced survival, and treatment options are limited. Antitumor immune memory plays a critical role in preventing melanoma recurrence and memory T cells could be a potent cell-based therapy, but the identity, and functional properties of the required immune cells are incompletely understood. Here, we show that an IL-7R hi tumor-specific CD8 + population is critical for antitumor memory and can be epigenetically augmented to drive powerful antitumor immune responses. Using a model of functional antimelanoma memory, we found that high IL-7R expression selectively marks a CD8 + population in lymphoid organs that plays critical roles in maintaining tumor remission after immunotherapy or surgical resection. This population has intrinsic cytotoxic activity, lacks markers of exhaustion and has superior antitumor efficacy. IL-7Rhi cells have a functionally poised epigenetic landscape regulated by DNA methylation, which can be augmented by hypomethylating agents to confer improved survival and complete melanoma clearance in naive mice. Importantly, greater than 95% of tumor-specific T cells in draining lymph nodes after therapy express high levels of IL-7R. This overlap between IL-7R hi and antigen-specific T cells allows for enrichment of a potent functional CD8 + population without determining antigen-specificity, which we demonstrate in a melanoma model without a known antigen. We identify that IL-7R expression in human melanoma is an independent prognostic factor of improved survival. These findings advance our basic understanding of antitumor memory and suggest a cell-based therapy using high IL-7R expression to enrich for a lymph node population with superior antitumor activity that can be augmented by hypomethylating agents.
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