A chimeric antigen receptor with antigen-independent OX40 signaling mediates potent antitumor activity

嵌合抗原受体 抗原 T细胞 蛋白激酶B MAPK/ERK通路 免疫学 生物 信号转导 癌症研究 细胞生物学 免疫系统
作者
Huihui Zhang,Fanlin Li,Jiang Cao,Xin Wang,Hai Cheng,Kunming Qi,Gang Wang,Kailin Xu,Junnian Zheng,Yang-Xin Fu,Xuanming Yang
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:13 (578) 被引量:100
标识
DOI:10.1126/scitranslmed.aba7308
摘要

Although chimeric antigen receptor (CAR)-modified T cells have shown great success in the treatment of B cell malignancies, this approach has limited efficacy in patients with solid tumors. Various modifications in CAR structure have been explored to improve this efficacy, including the incorporation of two costimulatory domains. Because costimulatory signals are transduced together with T cell receptor signals during T cell activation, we engineered a type of CAR-T cells with a costimulatory signal that was activated independently from the tumor antigen to recapitulate physiological stimulation. We screened 12 costimulatory receptors to identify OX40 as the most effective CAR-T function enhancer. Our data indicated that these new CAR-T cells showed superior proliferation capability compared to current second-generation CAR-T cells. OX40 signaling reduced CAR-T cell apoptosis through up-regulation of genes encoding Bcl-2 family members and enhanced proliferation through increased activation of the NF-κB (nuclear factor κB), MAPK (mitogen-activated protein kinase), and PI3K-AKT (phosphoinositide 3-kinase to the kinase AKT) pathways. OX40 signaling not only enhanced the cytotoxicity of CAR-T cells but also reduced exhaustion markers, thereby maintaining their function in immunosuppressive tumor microenvironments. In mouse tumor models and in patients with metastatic lymphoma, these CAR-T cells exhibited robust amplification and antitumor activity. Our findings provide an alternative option for CAR-T optimization with the potential to overcome the challenge of treating solid tumors.
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