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CAR T cells produced in vivo to treat cardiac injury

Joel G. Rurik, István Tombácz, Amir Yadegari, Pedro O. Méndez Fernández, Swapnil V. Shewale, Li Li, Toru Kimura, Ousamah Younoss Soliman, Tyler E. Papp, Ying K. Tam, Barbara L. Mui, Steven M. Albelda, Ellen Puré, Carl H. June, Haig Aghajanian, Drew Weissman, Hamideh Parhiz, Jonathan A. Epstein

2022Science1,244 citationsDOIOpen Access PDF

Abstract

Fibrosis affects millions of people with cardiac disease. We developed a therapeutic approach to generate transient antifibrotic chimeric antigen receptor (CAR) T cells in vivo by delivering modified messenger RNA (mRNA) in T cell–targeted lipid nanoparticles (LNPs). The efficacy of these in vivo–reprogrammed CAR T cells was evaluated by injecting CD5-targeted LNPs into a mouse model of heart failure. Efficient delivery of modified mRNA encoding the CAR to T lymphocytes was observed, which produced transient, effective CAR T cells in vivo. Antifibrotic CAR T cells exhibited trogocytosis and retained the target antigen as they accumulated in the spleen. Treatment with modified mRNA-targeted LNPs reduced fibrosis and restored cardiac function after injury. In vivo generation of CAR T cells may hold promise as a therapeutic platform to treat various diseases.

Topics & Concepts

In vivoChimeric antigen receptorCardiac fibrosisFibrosisCardiac function curveEx vivoAntigenMessenger RNAMedicineIn vitroImmunologyFunction (biology)Cancer researchPharmacologyT cellCell biologyT lymphocyteAntigen-presenting cellImmune systemReceptorBiologyChemistryCell therapyGenetic enhancementCAR-T cell therapy researchTissue Engineering and Regenerative MedicineViral Infections and Immunology Research
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