Litcius/Paper detail

GRK5 is a regulator of fibroblast activation and cardiac fibrosis

Akito Eguchi, Ryan C. Coleman, Kenneth S. Gresham, Erhe Gao, Jessica Ibetti, J. Kurt Chuprun, Walter J. Koch

2021Proceedings of the National Academy of Sciences74 citationsDOIOpen Access PDF

Abstract

-CAM)-dependent manner, promoting hypertrophic gene transcription through activation of nuclear factor of activated T cells (NFAT). Interestingly, NFAT is also involved in fibroblast activation. GRK5 is highly expressed and active in cardiac fibroblasts; however, its pathophysiological role in these crucial cardiac cells is unknown. We demonstrate using adult cardiac fibroblasts that genetic deletion of GRK5 inhibits angiotensin II (AngII)-mediated fibroblast activation. Fibroblast-specific deletion of GRK5 in mice led to decreased fibrosis and cardiac hypertrophy after chronic AngII infusion or after ischemic injury compared to nontransgenic littermate controls (NLCs). Mechanistically, we show that nuclear translocation of GRK5 is involved in fibroblast activation. These data demonstrate that GRK5 is a regulator of fibroblast activation in vitro and cardiac fibrosis in vivo. This adds to previously published data which demonstrate the potential beneficial effects of GRK5 inhibition in the context of cardiac disease.

Topics & Concepts

NFATCardiac fibrosisFibroblastAngiotensin IIBiologyFibrosisCell biologyHeart failureEndocrinologyInternal medicineCancer researchReceptorTranscription factorMedicineIn vitroBiochemistryGeneCardiac Fibrosis and RemodelingSignaling Pathways in DiseaseCardiac electrophysiology and arrhythmias