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Citations to this article

Integration of a Notch-dependent mesenchymal gene program and Bmp2-driven cell invasiveness regulates murine cardiac valve formation
Luis Luna-Zurita, … , José María Pérez-Pomares, José Luis de la Pompa
Luis Luna-Zurita, … , José María Pérez-Pomares, José Luis de la Pompa
Published September 20, 2010
Citation Information: J Clin Invest. 2010;120(10):3493-3507. https://doi.org/10.1172/JCI42666.
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Research Article Development

Integration of a Notch-dependent mesenchymal gene program and Bmp2-driven cell invasiveness regulates murine cardiac valve formation

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Abstract

Cardiac valve formation is crucial for embryonic and adult heart function. Valve malformations constitute the most common congenital cardiac defect, but little is known about the molecular mechanisms regulating valve formation and homeostasis. Here, we show that endocardial Notch1 and myocardial Bmp2 signal integration establish a valve-forming field between 2 chamber developmental domains. Patterning occurs through the activation of endocardial epithelial-to-mesenchymal transition (EMT) exclusively in prospective valve territories. Mice with constitutive endocardial Notch1 activity ectopically express Hey1 and Heyl. They also display an activated mesenchymal gene program in ventricles and a partial (noninvasive) EMT in vitro that becomes invasive upon BMP2 treatment. Snail1, TGF-β2, or Notch1 inhibition reduces BMP2-induced ventricular transformation and invasion, whereas BMP2 treatment inhibits endothelial Gsk3β, stabilizing Snail1 and promoting invasiveness. Integration of Notch and Bmp2 signals is consistent with Notch1 signaling being attenuated after myocardial Bmp2 deletion. Notch1 activation in myocardium extends Hey1 expression to nonchamber myocardium, represses Bmp2, and impairs EMT. In contrast, Notch deletion abrogates endocardial Hey gene transcription and extends Bmp2 expression to the ventricular endocardium. This embryonic Notch1-Bmp2-Snail1 relationship may be relevant in adult valve disease, in which decreased NOTCH signaling causes valve mesenchyme cell formation, fibrosis, and calcification.

Authors

Luis Luna-Zurita, Belén Prados, Joaquim Grego-Bessa, Guillermo Luxán, Gonzalo del Monte, Alberto Benguría, Ralf H. Adams, José María Pérez-Pomares, José Luis de la Pompa

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M Zhou, J Yan, Z Ma, Y Zhou, NN Abbood, J Liu, L Su, H Jia, AY Guo
PloS one 2012
Molecular Signatures of Cardiac Defects in Down Syndrome Lymphoblastoid Cell Lines Suggest Altered Ciliome and Hedgehog Pathways
C Ripoll, I Rivals, EA Yahya-Graison, L Dauphinot, E Paly, C Mircher, A Ravel, Y Grattau, H Bléhaut, A Mégarbane, G Dembour, B Fréminville, R Touraine, N Créau, MC Potier, JM Delabar
PloS one 2012
Co-ordinating Notch, BMP, and TGF-β signaling during heart valve development
VC Garside, AC Chang, A Karsan, PA Hoodless
Cellular and Molecular Life Sciences 2012
Bone morphogenetic protein-7 regulates Snail signaling in carbon tetrachloride-induced fibrosis in the rat liver
WR Bi, CX Jin, GT Xu, CQ Yang
Experimental and therapeutic medicine 2012
Bmp signaling regulates a dose-dependent transcriptional program to control facial skeletal development
M Bonilla-Claudio, J Wang, Y Bai, E Klysik, J Selever, JF Martin
Development (Cambridge, England) 2012
Notch Signaling Regulates Murine Atrioventricular Conduction and Formation of Accessory Pathways
Stacey Rentschler, Brett Harris, Laura Kuznekoff, Rajan Jain, Lauren Manderfield, Min Min Lu, Gregory Morley, Vickas Patel, Jonathan A Epstein
Journal of Clinical Investigation 2011
Tbx2 and Tbx3 induce atrioventricular myocardial development and endocardial cushion formation
R Singh, WM Hoogaars, P Barnett, T Grieskamp, MS Rana, H Buermans, HF Farin, M Petry, T Heallen, JF Martin, AF Moorman, PA Hoen, A Kispert, VM Christoffels
Cellular and Molecular Life Sciences 2011
Bmp Signaling in Congenital Heart Disease: New Developments and Future Directions
J Wang, SB Greene, JF Martin
Birth defects research. Part A, Clinical and molecular teratology 2011
Myocardial Tbx20 regulates early atrioventricular canal formation and endocardial epithelial-mesenchymal transition via Bmp2
X Cai, A Nomura-Kitabayashi, W Cai, J Yan, VM Christoffels, CL Cai
Developmental Biology 2011
Calcific Aortic Valve Stenosis: Methods, Models, and Mechanisms
JD Miller, RM Weiss, DD Heistad, DA Towler
Circulation research 2011
Distinct bone morphogenetic proteins activate indistinguishable transcriptional responses in nephron epithelia including Notch target genes
BW Larman, MJ Karolak, V Lindner, L Oxburgh
Cellular Signalling 2011
Nfatc1 Coordinates Valve Endocardial Cell Lineage Development Required for Heart Valve Formation
B Wu, Y Wang, W Lui, M Langworthy, KL Tompkins, AK Hatzopoulos, HS Baldwin, B Zhou
Circulation research 2011
Mmp15 is a direct target of Snai1 during endothelial to mesenchymal transformation and endocardial cushion development
G Tao, AK Levay, T Gridley, J Lincoln
Developmental Biology 2011
Notch1 binds and induces degradation of Snail in hepatocellular carcinoma
SO Lim, HS Kim, X Quan, SM Ahn, H Kim, D Hsieh, JK Seong, G Jung
BMC Biology 2011
Roles of STAT3 and ZEB1 proteins in E-cadherin down-regulation and human colorectal cancer epithelial-mesenchymal transition
H Xiong, J Hong, W Du, Y Lin, L Ren, Y Wang, W Su, J Wang, Y Cui, Z Wang, JY Fang
The Journal of biological chemistry 2011

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