Manufacturing CD20/CD19-targeted iCasp9 regulatable CAR-TSCM cells using a Quantum pBac-based CAR-T engineering system

Author:

Chang Peter S.ORCID,Chen Yi-Chun,Hua Wei-Kai,Hsu Jeff C.,Tsai Jui-Cheng,Huang Yi-Wun,Kao Yi-Hsin,Wu Pei-Hua,Wang Po-Nan,Chang Yi-Fang,Chang Ming-Chih,Chang Yu-Cheng,Jian Shiou-Ling,Lai Jiann-Shiun,Lai Ming-Tain,Yang Wei-Cheng,Shen Chia-Ning,Wen Kuo-Lan Karen,Wu Sareina Chiung-Yuan

Abstract

CD19-targeted chimeric antigen receptor (CAR) T cell therapies have driven a paradigm shift in the treatment of relapsed/refractory B-cell malignancies. However, >50% of CD19-CAR-T-treated patients experience progressive disease mainly due to antigen escape and low persistence. Clinical prognosis is heavily influenced by CAR-T cell function and systemic cytokine toxicities. Furthermore, it remains a challenge to efficiently, cost-effectively, and consistently manufacture clinically relevant numbers of virally engineered CAR-T cells. Using a highly efficient piggyBac transposon-based vector, Quantum pBac™ (qPB), we developed a virus-free cell-engineering system for development and production of multiplex CAR-T therapies. Here, we demonstrate in vitro and in vivo that consistent, robust and functional CD20/CD19 dual-targeted CAR-T stem cell memory (CAR-TSCM) cells can be efficiently produced for clinical application using qPB™. In particular, we showed that qPB™-manufactured CAR-T cells from cancer patients expanded efficiently, rapidly eradicated tumors, and can be safely controlled via an iCasp9 suicide gene-inducing drug. Therefore, the simplicity of manufacturing multiplex CAR-T cells using the qPB™ system has the potential to improve efficacy and broaden the accessibility of CAR-T therapies.

Funder

GenomeFrontier Therapeutics TW Co., Ltd.

Publisher

Public Library of Science (PLoS)

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