瘦素
肿瘤微环境
癌症研究
CD8型
细胞生物学
生物
内科学
医学
肿瘤细胞
免疫学
免疫系统
肥胖
作者
Feixiang Wang,Rujuan Bao,Shuiyu Xu,Wenyan Li,Haiyan Huang,Runchang Li,Xinyu Ding,Yuerong Zhang,Xiaoyan Yu,Qiaoqiao Han,Xian Du,Jie Wan,Hang Li,Yichuan Xiao,Ren Zhao,Xingang Cui,Youqiong Ye,Jiayuan Sun,Junke Zheng,Guoqiang Chen
标识
DOI:10.1016/j.xcrm.2025.102310
摘要
T cell dysfunction with age underlies an increased incidence of cancer in elderly individuals; however, how T cell aging is triggered in the tumor microenvironment is unclear. Here, we show that an age-associated reduction in adipocyte-derived leptin contributes to the accumulation of tumor-infiltrating senescent CD8+ T cells. Single-cell profiling of human and mouse cancer tissues reveals that the frequency of intratumoral senescent CD8+ T cells increases with age, leading to a weak antitumor effect. Moreover, decreased levels of adipocyte-derived leptin are an indispensable factor for CD8+ T cell aging. Leptin signaling prevents p38-dependent CD8+ T cell senescence. Furthermore, plasma leptin levels are negatively related to intratumoral CD8+ T cell senescence in cancer patients. Our findings identify an unappreciated interplay between metabolic perturbation and T cell aging and suggest that modulating adipocyte-derived leptin levels may be a promising therapeutic strategy for older cancer patients.
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