Litcius/Paper detail

Preclinical scenario of targeting myocardial fibrosis with chimeric antigen receptor (CAR) immunotherapy

Gemma Ferrer‐Curriu, Carolina Soler‐Botija, Sandra Charvátová, Benjamin Motais, Santiago Roura, Carolina Gálvez‐Montón, Marta Tortajada, Oriol Iborra‐Egea, Michele Emdin, Josep Lupón, Alberto Aimo, Juli R. Bagó, Antoni Bayés‐Genís

2022Biomedicine & Pharmacotherapy17 citationsDOIOpen Access PDF

Abstract

Fibrosis is present in an important proportion of myocardial disorders. Injury activates cardiac fibroblasts, which deposit excess extracellular matrix, increasing tissue stiffness, impairing cardiac function, and leading to heart failure. Clinical therapies that directly target excessive fibrosis are limited, and more effective treatments are needed. Immunotherapy based on chimeric antigen receptor (CAR) T cells is a novel technique that redirects T lymphocytes toward specific antigens to eliminate the target cells. It is currently used in haematological cancers but has demonstrated efficacy in mouse models of hypertensive cardiac fibrosis, with activated fibroblasts as the target cells. CAR T cell therapy is associated with significant toxicities, but CAR natural killer cells can overcome efficacy and safety limitations. The use of CAR immunotherapy offers a potential alternative to current therapies for fibrosis reduction and restoration of cardiac function in patients with myocardial fibrosis.

Topics & Concepts

Chimeric antigen receptorImmunotherapyFibrosisMedicineMyocardial fibrosisCancer researchAntigenImmunologyCardiac fibrosisCell therapyExtracellular matrixCellImmune systemInternal medicineBiologyCell biologyGeneticsCAR-T cell therapy researchAdvancements in Semiconductor Devices and Circuit DesignElectrostatic Discharge in Electronics