TGF-β-responsive CAR-T cells promote anti-tumor immune function

被引:84
作者
Hou, Andrew J. [1 ]
Chang, ZeNan L. [1 ,2 ]
Lorenzini, Michael H. [3 ]
Zah, Eugenia [1 ]
Chen, Yvonne Y. [1 ,4 ]
机构
[1] Univ Calif Los Angeles, Dept Chem & Biomol Engn, Los Angeles, CA 90095 USA
[2] Univ Calif Los Angeles, Inst Mol Biol, Los Angeles, CA 90095 USA
[3] Univ Calif Los Angeles, Dept Bioengn, Los Angeles, CA 90095 USA
[4] UCLA, Parker Inst Canc Immunotherapy Ctr, Los Angeles, CA 90095 USA
基金
美国国家卫生研究院;
关键词
Tumors - Cell proliferation - Cell culture - Antigens - Cell engineering - Diseases;
D O I
10.1002/btm2.10097
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
A chimeric antigen receptor (CAR) that responds to transforming growth factor beta (TGF-beta) enables the engineering of T cells that convert this immunosuppressive cytokine into a potent T-cell stimulant. However, clinical translation of TGF-beta CAR-T cells for cancer therapy requires the ability to productively combine TGF-beta responsiveness with tumor-targeting specificity. Furthermore, the potential concern that contaminating, TGF-beta-producing regulatory T (Treg) cells may preferentially expand during TGF-beta CAR-T cell manufacturing and suppress effector T (Teff) cells demands careful evaluation. Here, we demonstrate that TGF-beta CAR-T cells significantly improve the anti-tumor efficacy of neighboring cytotoxic T cells. Furthermore, the introduction of TGF-beta CARs into mixed T-cell populations does not result in the preferential expansion of Treg cells, nor do TGF-beta CAR-Treg cells cause CAR-mediated suppression of Teff cells. These results support the utility of incorporating TGF-beta CARs in the development of adoptive T-cell therapy for cancer.
引用
收藏
页码:75 / 86
页数:12
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