Redirection of Genetically Engineered CAR-T Cells Using Bifunctional Small Molecules
Chimeric antigen receptor (CAR)-engineered T cells (CAR-Ts) provide a potent antitumor response and have become a promising treatment option for cancer. However, despite their efficacy, CAR-T cells are associated with significant safety challenges related to the inability to control their activation and expansion and terminate their response. Herein, we demonstrate that a bifunctional small molecule switch consisting of folate conjugated to fluorescein isothiocyanate (folate-FITC) can redirect and regulate FITC-specific CAR-T cell activity toward folate receptor (FR)-overexpressing tumor cells. This system was shown to be highly cytotoxic to FR-positive cells with no activity against FR-negative cells, demonstrating the specificity of redirection by folate-FITC. Anti-FITC-CAR-T cell activation and proliferation was strictly dependent on the presence of both folate-FITC and FR-positive cells and was dose titratable with folate-FITC switch. This novel treatment paradigm may ultimately lead to increased safety for CAR-T cell immunotherapy.
- Publisher
- AMER CHEMICAL SOC
- Issue Date
- 2015-03
- Language
- English
- Article Type
- Article
- Keywords
FOLATE RECEPTOR-ALPHA; ANTIGEN RECEPTOR; ANTITUMOR-ACTIVITY; CANCER; IMMUNOTHERAPY; EXPRESSION; MALIGNANCIES; CARCINOMA; TOXICITY; LEUKEMIA
- Citation
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, v.137, no.8, pp.2832 - 2835
- ISSN
- 0002-7863
- Appears in Collection
- BS-Journal Papers(저널논문)
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