Litcius/Paper detail

Targeting cardiac fibrosis in heart failure with preserved ejection fraction: mirage or miracle?

Mark Sweeney, Ben Corden, Stuart A. Cook

2020EMBO Molecular Medicine195 citationsDOIOpen Access PDF

Abstract

Cardiac fibrosis is central to the pathology of heart failure, particularly heart failure with preserved ejection fraction (HFpEF). Irrespective of the underlying profibrotic condition (e.g. ageing, diabetes, hypertension), maladaptive cardiac fibrosis is defined by the transformation of resident fibroblasts to matrix-secreting myofibroblasts. Numerous profibrotic factors have been identified at the molecular level (e.g. TGFβ, IL11, AngII), which activate gene expression programs for myofibroblast activation. A number of existing HF therapies indirectly target fibrotic pathways; however, despite multiple clinical trials in HFpEF, a specific clinically effective antifibrotic therapy remains elusive. Therapeutic inhibition of TGFβ, the master-regulator of fibrosis, has unfortunately proven toxic and ineffective in clinical trials to date, and new approaches are needed. In this review, we discuss the pathophysiology and clinical implications of interstitial fibrosis in HFpEF. We provide an overview of trials targeting fibrosis in HFpEF to date and discuss the promise of potential new therapeutic approaches and targets in the context of underlying molecular mechanisms.

Topics & Concepts

Heart failureCardiac fibrosisFibrosisHeart failure with preserved ejection fractionMedicineMyofibroblastContext (archaeology)Ejection fractionMyocardial fibrosisClinical trialCardiologyInternal medicineBioinformaticsBiologyPaleontologyCardiac Fibrosis and RemodelingCardiac Structural Anomalies and RepairPeptidase Inhibition and Analysis