Rapidly Switchable Universal CAR-T Cells for Treatment of CD123-Positive Leukemia

被引:73
作者
Loff, Simon [1 ]
Dietrich, Josephine [2 ]
Meyer, Jan-Erik [2 ]
Riewaldt, Julia [2 ]
Spehr, Johannes [2 ]
von Bonin, Malte [3 ,6 ]
Gruender, Cordula [1 ]
Swayampakula, Mridula [1 ]
Franke, Kristin [1 ]
Feldmann, Anja [5 ]
Bachmann, Michael [4 ,5 ,6 ,7 ]
Ehninger, Gerhard [1 ,2 ]
Ehninger, Armin [1 ,2 ]
Cartellieri, Marc [1 ,2 ]
机构
[1] GEMoaB Monoclonals GmbH, D-01307 Dresden, Germany
[2] Cellex Patient Treatment GmbH, Tatzberg 47, D-01307 Dresden, Germany
[3] Tech Univ Dresden, Univ Hosp Carl Gustav Carus, Med Clin & Policlin 1, D-01307 Dresden, Germany
[4] Tech Univ Dresden, Tumor Immunol, Univ Canc Ctr Carl Gustav Carus, D-01307 Dresden, Germany
[5] Helmholtz Zentrum Dresden Rossendorf, Inst Radiopharmaceut Canc Res, D-01328 Dresden, Germany
[6] Tech Univ Dresden, German Canc Consortium Carl Gustav Carus, D-01307 Dresden, Germany
[7] Tech Univ Dresden, Natl Ctr Tumor Dis Carl Gustav Carus, D-01307 Dresden, Germany
来源
MOLECULAR THERAPY-ONCOLYTICS | 2020年 / 17卷
关键词
ACUTE MYELOID-LEUKEMIA; CHIMERIC ANTIGEN RECEPTORS; B-CELL; ALPHA CHAIN; CD123; THERAPY; CHEMOTHERAPY; MODULATION; ACTIVATION; EXPRESSION;
D O I
10.1016/j.omto.2020.04.009
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Chimeric antigen receptor T cells (CAR-T) targeting CD19 or B cell maturation antigen (BCMA) are highly effective against B cell malignancies. However, application of CAR-T to less differentially expressed targets remains a challenge due to lack of tumor-specific antigens and CAR-T controllability. CD123, a highly promising leukemia target, is expressed not only by leukemic and leukemia-initiating cells, but also by myeloid, hematopoietic progenitor, and certain endothelial cells. Thus, CAR-T lacking fine-tuned control mechanisms pose a high toxicity risk. To extend the CAR-T target landscape and widen the therapeutic window, we adapted our rapidly switchable universal CAR-T platform (UniCAR) to target CD123. UniCAR-T efficiently eradicated CD123(+) leukemia in vitro and in vivo. Activation, cytolytic response, and cytokine release were strictly dependent on the presence of the CD123-specific targeting module (TM123) with comparable efficacy to CD123-specific CAR-T in vitro. We further demonstrated a pre-clinical proof of concept for the safety-switch mechanism using a hematotoxicity mouse model wherein TM123-redirected UniCAR-T showed reversible toxicity toward hematopoietic cells compared to CD123 CAR-T. In conclusion, UniCAR-T maintain full anti-leukemic efficacy, while ensuring rapid controllability to improve safety and versatility of CD123-directed immunotherapy. The safety and efficacy of UniCAR-T in combination with TM123 will now be assessed in a phase I clinical trial.
引用
收藏
页码:408 / 420
页数:13
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