Mutations in Bcl9 and Pygo genes cause congenital heart defects by tissue-specific perturbation of Wnt/β-catenin signaling

Bcl9 and Pygopus (Pygo) are obligate Wnt/β-catenin cofactors in Drosophila, yet their contribution to Wnt signaling during vertebrate development remains unresolved. Combining zebrafish and mouse genetics, we document a conserved, β-catenin-associated function for BCL9 and Pygo proteins during vertebrate heart development. Disrupting the β-catenin–BCL9–Pygo complex results in a broadly maintained canonical Wnt response yet perturbs heart development and proper expression of key cardiac regulators. Our work highlights BCL9 and Pygo as selective β-catenin cofactors in a subset of canonical Wnt responses during vertebrate development. Moreover, our results implicate alterations in BCL9 and BCL9L in human congenital heart defects.

Mutations in Bcl9 and Pygo genes cause congenital heart defects by tissue-specific perturbation of Wnt/β-catenin signaling

Cantu C.;Felker A.;Zimmerli D.;Prummel K. D.;Cabello E. M.;Chiavacci E.;Mendez-Acevedo K. M.;Kirchgeorg L.;Burger S.;Ripoll J.;Valenta T.;Hausmann G.;Vilain N.;Aguet M.;Burger A.;Panakova D.;Basler K.;Mosimann C.

2018

Abstract

Bcl9 and Pygopus (Pygo) are obligate Wnt/β-catenin cofactors in Drosophila, yet their contribution to Wnt signaling during vertebrate development remains unresolved. Combining zebrafish and mouse genetics, we document a conserved, β-catenin-associated function for BCL9 and Pygo proteins during vertebrate heart development. Disrupting the β-catenin–BCL9–Pygo complex results in a broadly maintained canonical Wnt response yet perturbs heart development and proper expression of key cardiac regulators. Our work highlights BCL9 and Pygo as selective β-catenin cofactors in a subset of canonical Wnt responses during vertebrate development. Moreover, our results implicate alterations in BCL9 and BCL9L in human congenital heart defects.

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	Anno di pubblicazione
	
			2018
		
	Settore Scientifico Disciplinare
	
			Settore BIO/11 - Biologia Molecolare
		
	Titolo Rivista
	
			GENES & DEVELOPMENT
		
	DOI
	
			https://dx.doi.org/10.1101/gad.315531.118
		
	Parole chiave
	
			Cardiovascular development; Congenital heart disease; CRISPR-Cas9; Heart; Transcription; Wnt signaling
		
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11384/134427

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