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<scp>mRNA</scp>‐laden lipid nanoparticle‐enabled humanized <scp>CD19 CAR</scp>‐T‐cell engineering for the eradication of leukaemic cells

Zhaozhao Chen, Anqi Ren, Yingying Li, Jinhui Shu, Jianghua Wu, Hekuan Huang, Jingming Wang, Yu Hu, Heng Mei

2025British Journal of Haematology24 citationsDOIOpen Access PDF

Abstract

Chimeric antigen receptor T-cell (CAR-T) therapy has shown transformative potential in treating malignant tumours, with increasing global approval of CAR-T products. However, high-production costs and risks associated with viral vector-based CAR-T cells-such as insertional mutagenesis and secondary tumour formation-remain challenges. Our study introduces an innovative CAR-T engineering approach using mRNA delivered via lipid nanoparticles (LNPs), aiming to reduce costs and enhance safety while maintaining strong anti-tumour efficacy. We developed an LNP-based transfection protocol for efficient delivery of mRNA encoding full-human CAR constructs, achieving high CAR expression and significant cytotoxicity against leukaemic cells in vitro. Co-culture with Raji cells showed increased cytokine secretion and tumour cell killing by mRNA-LNP CAR-T cells. Therapeutic efficacy was further demonstrated in an NOD-scid-IL2Rγnull (NSG) mouse model with Raji engraftment, where treated mice exhibited marked tumour regression and extended survival. These findings underscore the potential of mRNA-LNPs as a non-viral, effective CAR-T engineering platform, offering a promising alternative to traditional methods that could improve CAR-T safety, efficacy and accessibility in clinical cancer immunotherapy.

Topics & Concepts

Chimeric antigen receptorCD19Cancer immunotherapyImmunotherapyRaji cellCancer researchAntigenBiologyImmunologyImmune systemVirusCAR-T cell therapy researchVirus-based gene therapy researchViral Infectious Diseases and Gene Expression in Insects
<scp>mRNA</scp>‐laden lipid nanoparticle‐enabled humanized <scp>CD19 CAR</scp>‐T‐cell engineering for the eradication of leukaemic cells | Litcius