C-JUN overexpressing CAR-T cells in acute myeloid leukemia: preclinical characterization and phase I trial

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作者：Zuo Shiyu, Li Chuo, Sun Xiaolei, Deng Biping, Zhang Yibing, Han Yajing, Ling Zhuojun, Xu Jinlong, Duan Jiajia, Wang Zelin, Yu Xinjian, Zheng Qinlong, Xu Xiuwen, Zong Jiao, Tian Zhenglong, Shan Lingling, Tang Kaiting, Huang Huifang, Song Yanzhi, Niu Qing, Zhou Dongming, Feng Sizhou, Han Zhongchao, Wang Guoling, Wu Tong, Pan Jing, Feng Xiaoming
期刊：Nature Communications
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Chimeric antigen receptor (CAR) T cells show suboptimal efficacy in acute myeloid leukemia (AML). We find that CAR T cells exposed to myeloid leukemia show impaired activation and cytolytic function, accompanied by impaired antigen receptor downstream calcium, ZAP70, ERK, and C-JUN signaling, compared to those exposed to B-cell leukemia. These defects are caused in part by the high expression of CD155 by AML. Overexpressing C-JUN, but not other antigen receptor downstream components, maximally restores anti-tumor function. C-JUN overexpression increases costimulatory molecules and cytokines through reinvigoration of ERK or transcriptional activation, independent of anti-exhaustion. We conduct an open-label, non-randomized, single-arm, phase I trial of C-JUN-overexpressing CAR-T in AML (NCT04835519) with safety and efficacy as primary and secondary endpoints, respectively. Of the four patients treated, one has grade 4 (dose-limiting toxicity) and three have grade 1–2 cytokine release syndrome. Two patients have no detectable bone marrow blasts and one patient has blast reduction after treatment. Thus, overexpressing C-JUN endows CAR-T efficacy in AML.