THEMIS-SHP1 通过 4-1BB 招募调控嵌合抗原受体重定向 T 细胞的 LCK 介导的启动。
THEMIS-SHP1 Recruitment by 4-1BB Tunes LCK-Mediated Priming of Chimeric Antigen Receptor-Redirected T Cells.
机构信息
Lineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.
Lineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA; Department of Microbiology and Immunology, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.
出版信息
Cancer Cell. 2020 Feb 10;37(2):216-225.e6. doi: 10.1016/j.ccell.2019.12.014. Epub 2020 Jan 30.
Abstract
Chimeric antigen receptor (CAR) T cell costimulation mediated by CD28 and 4-1BB is essential for CAR-T cell-induced tumor regression. However, CD28 and 4-1BB differentially modulate kinetics, metabolism and persistence of CAR-T cells, and the mechanisms governing these differences are not fully understood. We found that LCK recruited into the synapse of CD28-encoding CAR by co-receptors causes antigen-independent CAR-CD3ζ phosphorylation and increased antigen-dependent T cell activation. In contrast, the synapse formed by 4-1BB-encoding CAR recruits the THEMIS-SHP1 phosphatase complex that attenuates CAR-CD3ζ phosphorylation. We further demonstrated that the CAR synapse can be engineered to recruit either LCK to enhance the kinetics of tumor killing of 4-1BB CAR-T cells or SHP1 to tune down cytokine release of CD28 CAR-T cells.
摘要
嵌合抗原受体 (CAR) T 细胞共刺激由 CD28 和 4-1BB 介导,对于 CAR-T 细胞诱导的肿瘤消退至关重要。然而,CD28 和 4-1BB 对 CAR-T 细胞的动力学、代谢和持久性有不同的调节作用,其机制尚不完全清楚。我们发现,通过共受体募集到 CD28 编码的 CAR 突触中的 LCK 导致抗原非依赖性 CAR-CD3ζ 磷酸化和增加抗原依赖性 T 细胞激活。相比之下,由 4-1BB 编码的 CAR 形成的突触募集 THEMIS-SHP1 磷酸酶复合物,从而减弱 CAR-CD3ζ 磷酸化。我们进一步证明,可以对 CAR 突触进行工程改造,以募集 LCK 增强 4-1BB CAR-T 细胞的肿瘤杀伤动力学,或募集 SHP1 来调节 CD28 CAR-T 细胞的细胞因子释放。
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