嵌合抗原受体
T细胞
抗原
免疫系统
受体
癌症研究
生物
免疫学
细胞
分子生物学
细胞生物学
化学
遗传学
作者
Fanlin Li,Huihui Zhang,Wanting Wang,Puyuan Yang,Yue Huang,Junshi Zhang,Yaping Yan,Yuan Wang,Xizhong Ding,Jie Liang,Xinyue Qi,Min Li,Ping Han,Xiaoqing Zhang,Xin Wang,Jiang Cao,Yang‐Xin Fu,Xuanming Yang
标识
DOI:10.1038/s41467-022-32092-8
摘要
Abstract The success of chimeric antigen receptor (CAR) T cells in treating B cell malignancies comes at the price of eradicating normal B cells. Even though T cell malignancies are aggressive and treatment options are limited, similar strategies for T cell malignancies are constrained by the severe immune suppression arising from bystander T cell aplasia. Here, we show the selective killing of malignant T cells without affecting normal T cell-mediated immune responses in vitro and in a mouse model of disseminated leukemia. Further, we develop a CAR construct that carries the single chain variable fragment of a subtype-specific antibody against the variable TCR β-chain region. We demonstrate that these anti-Vβ8 CAR-T cells are able to recognize and kill all Vβ8 + malignant T cells that arise from clonal expansion while sparing malignant or healthy Vβ8 − T cells, allowing sufficient T cell-mediated cellular immunity. In summary, we present a proof of concept for a selective CAR-T cell therapy to eradicate T cell malignancies while maintaining functional adaptive immunity, which opens the possibility for clinical development.
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