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Hand2 Is an Essential Regulator for Two Notch-Dependent Functions within the Embryonic Endocardium

Authors

VanDusen, Nathan J. , Casanovas, Jose , Vincentz, Joshua W. , Firulli, Beth A. , Osterwalder, Marco , LÓPEZ-RÍOS MORENO, JAVIER, Zeller, Rolf , Zhou, Bin , Grego-Bessa, Joaquim , Luis De La Pompa, Jose , Shou, Weinian , Firulli, Anthony B.

External publication

Si

Means

Cell Reports

Scope

Article

Nature

Científica

JCR Quartile

SJR Quartile

JCR Impact

8.358

SJR Impact

8.415

Publication date

24/12/2014

ISI

000346852400010

Abstract

The basic-helix-loop-helix (bHLH) transcription factor Hand2 plays critical roles during cardiac morphogenesis via expression and function within myocardial, neural crest, and epicardial cell populations. Here, we show that Hand2 plays two essential Notch-dependent roles within the endocardium. Endocardial ablation of Hand2 results in failure to develop a patent tricuspid valve, intraventricular septum defects, and hypotrabeculated ventricles, which collectively resemble the human congenital defect tricuspid atresia. We show endocardial Hand2 to be an integral downstream component of a Notch endocardium-to-myocardium signaling pathway and a direct transcriptional regulator of Neuregulin1. Additionally, Hand2 participates in endocardium-to-endocardium-based cell signaling, with Hand2 mutant hearts displaying an increased density of coronary lumens. Molecular analyses further reveal dysregulation of several crucial components of Vegf signaling, including VegfA, VegfR2, Nrp1, and VegfR3. Thus, Hand2 functions as a crucial downstream transcriptional effector of endocardial Notch signaling during both cardiogenesis and coronary vasculogenesis.

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