| Literature DB >> 27997827 |
Ivan Menendez-Montes1, Beatriz Escobar1, Beatriz Palacios1, Manuel Jose Gómez1, Jose Luis Izquierdo-Garcia2, Lorena Flores1, Luis Jesus Jiménez-Borreguero3, Julian Aragones4, Jesus Ruiz-Cabello5, Miguel Torres6, Silvia Martin-Puig7.
Abstract
While gene regulatory networks involved in cardiogenesis have been characterized, the role of bioenergetics remains less studied. Here we show that until midgestation, myocardial metabolism is compartmentalized, with a glycolytic signature restricted to compact myocardium contrasting with increased mitochondrial oxidative activity in the trabeculae. HIF1α regulation mirrors this pattern, with expression predominating in compact myocardium and scarce in trabeculae. By midgestation, the compact myocardium downregulates HIF1α and switches toward oxidative metabolism. Deletion of the E3 ubiquitin ligase Vhl results in HIF1α hyperactivation, blocking the midgestational metabolic shift and impairing cardiac maturation and function. Moreover, the altered glycolytic signature induced by HIF1 trabecular activation precludes regulation of genes essential for establishment of the cardiac conduction system. Our findings reveal VHL-HIF-mediated metabolic compartmentalization in the developing heart and the connection between metabolism and myocardial differentiation. These results highlight the importance of bioenergetics in ventricular myocardium specialization and its potential relevance to congenital heart disease.Entities:
Keywords: HIF; VHL; cardiac conduction system; cardiac maturation; glycolysis; heart development; hypoxia; metabolic reprogramming; mitochondria; transcriptional repression
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Year: 2016 PMID: 27997827 DOI: 10.1016/j.devcel.2016.11.012
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270