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Metabolic reprogramming of terminally exhausted CD8 T cells by IL-10 enhances anti-tumor immunity

Nat Immunol. 2021-05; 
Yugang Guo, Yu-Qing Xie, Min Gao, Yang Zhao, Fabien Franco, Mathias Wenes, Imran Siddiqui, Alessio Bevilacqua, Haiping Wang, Hanshuo Yang, Bing Feng, Xin Xie, Catherine M Sabatel, Benjamin Tschumi, Amphun Chaiboonchoe, Yuxi Wang, Weimin Li, Weihua Xiao, Werner Held, Pedro Romero, Ping-Chih Ho, Li Tang
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Mammalian Expression … ), as well as human gp100 25–33 or OVA 257-264 peptide (1 μM, GenScript) for PMEL or OT-I T cells, respectively. After a 3-d culture, live … 3g,h, Tcf7 DTR-GFP P14 T cells were primed by LCMV gp 33-41 peptide (1 µM, GenScript) and prepared similarly as described above for … Get A Quote

摘要

T cell exhaustion presents one of the major hurdles to cancer immunotherapy. Among exhausted CD8 tumor-infiltrating lymphocytes, the terminally exhausted subset contributes directly to tumor cell killing owing to its cytotoxic effector function. However, this subset does not respond to immune checkpoint blockades and is difficult to be reinvigorated with restored proliferative capacity. Here, we show that a half-life-extended interleukin-10-Fc fusion protein directly and potently enhanced expansion and effector function of terminally exhausted CD8 tumor-infiltrating lymphocytes by promoting oxidative phosphorylation, a process that was independent of the progenitor exhausted T cells. Interleukin-10-Fc was a saf... More

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