Chimeric antigen receptors containing the OX40 signalling domain enhance the persistence of T cells even under repeated stimulation with multiple myeloma target cells

嵌合抗原受体 CD28 医学 癌症研究 抗原 细胞毒性T细胞 免疫学 T细胞 药理学
作者
Jingwen Tan,Yujie Jia,Meixia Zhou,Chengcheng Fu,Israth Jahan Tuhin,Jing Ye,Masuma Akter Monty,Nan Xu,Liqing Kang,Minghao Li,Jiaqi Shao,Xiaoyan Fang,Hongjia Zhu,Lingzhi Yan,Changju Qu,Shengli Xue,Zhengming Jin,Suning Chen,Haiwen Huang,Yang Xu,Jia Chen,Miao Miao,Xiaowen Tang,Caixia Li,Zhiqiang Yan,Depei Wu,Lei Yu
出处
期刊:Journal of Hematology & Oncology [Springer Nature]
卷期号:15 (1)
标识
DOI:10.1186/s13045-022-01244-0
摘要

Persistence of CAR-T cell function is associated with relapse rate after CAR-T therapy, while co-stimulatory agents are highly concerned with the persistence of CAR-T cells. In this study, we designed and constructed a series of BCMA-targeting second-generation CAR constructs containing CD28, 41BB, and OX40 molecules, respectively, to identify the costimulatory domains most favorable for persistence. The results of routine in vitro studies showed that OX40-CAR-T and 41BB-CAR-T had similar antitumor effects and were superior to CD28-CAR-T in terms of proliferation and cytotoxicity. Although difficult to distinguish by conventional functional assays, OX40-CAR-T cells exhibited greater proliferation and enhanced immune memory than 41BB-CAR-T cells with the repeated stimulation assay by BCMA-expressing target cells. In vivo studies further demonstrated that OX40-CAR-T cells had stronger proliferative activity than 41BB-CAR-T cells, which was highly consistent with the in vitro antitumor activity and proliferation results. Our study provides for the first time a scientific basis for designing OX40-CAR-T cell therapy to improve relapse in patients with MM after CAR-T treatment.
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