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Split-design approach enhances the therapeutic efficacy of ligand-based CAR-T cells against multiple B-cell malignancies

Nat Commun. 2024-11; 
Shuhong Li , Licai Shi , Lijun Zhao , Qiaoru Guo , Jun Li , Ze-Lin Liu , Zhi Guo , Yu J Cao
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Recombinant Proteins GenScript Biotech, Inc., synthesized the genes, which were subsequently inserted into the pCAGGS expression vector. The isolated T cells were thawed and activated with DynaBeads Human T-Activator CD3/CD28 (Gibco, 11141D) for 48 hours in X-VIVO 15 medium (LONZA, 04-418Q) supplemented with 5% FBS and 300 IU/mL IL-2 (GenScript, Z00368-50). CAR-T cells were expanded in X-VIVO15 medium (5% FBS) supplemented with 10 ng/mL IL-7 (GenScript, Z02704) and 5 ng/mL IL-15 (GenScript, Z03308). Genes encoding the full-length BCMA antigen were synthesized by GenScript and cloned into the pLV lentiviral plasmid. Get A Quote
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摘要

To address immune escape, multi-specific CAR-T-cell strategies use natural ligands that specifically bind multiple receptors on malignant cells. In this context, we propose a split CAR design comprising a universal receptor expressed on T cells and ligand-based switch molecules, which preserves the natural trimeric structure of ligands like APRIL and BAFF. Following optimization of the hinges and switch labeling sites, the split-design CAR-T cells ensure the native conformation of ligands, facilitating the optimal formation of immune synapses between target cancer cells and CAR-T cells. Our CAR-T-cell strategy demonstrates antitumor activities against various B-cell malignancy models in female mice, potentially... More

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