| Literature DB >> 31978365 |
Hesham Soliman1, Ben Paylor2, R Wilder Scott2, Dario R Lemos3, ChihKai Chang2, Martin Arostegui2, Marcela Low2, Christina Lee2, Daniela Fiore4, Paola Braghetta5, Vendula Pospichalova6, Christina E Barkauskas7, Vladimir Korinek6, Alessandra Rampazzo5, Kathleen MacLeod8, T Michael Underhill2, Fabio M V Rossi9.
Abstract
The cardiac stroma contains multipotent mesenchymal progenitors. However, lineage relationships within cardiac stromal cells are poorly defined. Here, we identified heart-resident PDGFRa+ SCA-1+ cells as cardiac fibro/adipogenic progenitors (cFAPs) and show that they respond to ischemic damage by generating fibrogenic cells. Pharmacological blockade of this differentiation step with an anti-fibrotic tyrosine kinase inhibitor decreases post-myocardial infarction (post-MI) remodeling and leads to improvement in cardiac function. In the undamaged heart, activation of cFAPs through lineage-specific deletion of the gene encoding the quiescence-associated factor HIC1 reveals additional pathogenic potential, causing fibrofatty infiltration within the myocardium and driving major pathological features pathognomonic in arrhythmogenic cardiomyopathy (AC). In this regard, cFAPs contribute to multiple pathogenic cell types within cardiac tissue and therapeutic strategies aimed at modifying their activity are expected to have tremendous benefit for the treatment of diverse cardiac diseases.Entities:
Keywords: Hic1; PDGFRa; arrhythmogenic cardiomyopathy; cFAP; cardiac fibrosis; fibroadipogenic progenitor; fibrofatty infiltration; mesenchymal progenitor; myocardial infarction; nilotinib
Mesh:
Year: 2020 PMID: 31978365 DOI: 10.1016/j.stem.2019.12.008
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633