| Literature DB >> 24910328 |
Rabea Hinkel1, Teresa Trenkwalder2, Björn Petersen3, Wira Husada4, Florian Gesenhues4, Seungmin Lee4, Ewald Hannappel5, Ildiko Bock-Marquette6, Daniel Theisen7, Laura Leitner8, Peter Boekstegers4, Czeslaw Cierniewski9, Oliver J Müller10, Ferdinand le Noble11, Ralf H Adams12, Christine Weinl13, Alfred Nordheim13, Bruno Reichart14, Christian Weber15, Eric Olson16, Guido Posern17, Elisabeth Deindl18, Heiner Niemann3, Christian Kupatt19.
Abstract
Gradual occlusion of coronary arteries may result in reversible loss of cardiomyocyte function (hibernating myocardium), which is amenable to therapeutic neovascularization. The role of myocardin-related transcription factors (MRTFs) co-activating serum response factor (SRF) in this process is largely unknown. Here we show that forced MRTF-A expression induces CCN1 and CCN2 to promote capillary proliferation and pericyte recruitment, respectively. We demonstrate that, upon G-actin binding, thymosin ß4 (Tß4), induces MRTF translocation to the nucleus, SRF-activation and CCN1/2 transcription. In a murine ischaemic hindlimb model, MRTF-A or Tß4 promotes neovascularization, whereas loss of MRTF-A/B or CCN1-function abrogates the Tß4 effect. We further show that, in ischaemic rabbit hindlimbs, MRTF-A as well as Tß4 induce functional neovascularization, and that this process is inhibited by angiopoietin-2, which antagonizes pericyte recruitment. Moreover, MRTF-A improves contractile function of chronic hibernating myocardium of pigs to a level comparable to that of transgenic pigs overexpressing Tß4 (Tß4tg). We conclude that MRTF-A promotes microvessel growth (via CCN1) and maturation (via CCN2), thereby enabling functional improvement of ischaemic muscle tissue.Entities:
Mesh:
Substances:
Year: 2014 PMID: 24910328 DOI: 10.1038/ncomms4970
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919