TY - JOUR
T1 - Canonical Wnt signaling regulates atrioventricular junction programming and electrophysiological properties
AU - Gillers, Benjamin S.
AU - Chiplunkar, Aditi
AU - Aly, Haytham
AU - Valenta, Tomas
AU - Basler, Konrad
AU - Christoffels, Vincent M.
AU - Efimov, Igor R.
AU - Boukens, Bastiaan J.
AU - Rentschler, Stacey
N1 - Publisher Copyright:
© 2014 American Heart Association, Inc.
PY - 2014/11/6
Y1 - 2014/11/6
N2 - Rationale: Proper patterning of the atrioventricular canal (AVC) is essential for delay of electrical impulses between atria and ventricles, and defects in AVC maturation can result in congenital heart disease. Objective: To determine the role of canonical Wnt signaling in the myocardium during AVC development. Methods and Results: We used a novel allele of β-catenin that preserves β-catenin's cell adhesive functions but disrupts canonical Wnt signaling, allowing us to probe the effects of Wnt loss of function independently. We show that the loss of canonical Wnt signaling in the myocardium results in tricuspid atresia with hypoplastic right ventricle associated with the loss of AVC myocardium. In contrast, ectopic activation of Wnt signaling was sufficient to induce formation of ectopic AV junction-like tissue as assessed by morphology, gene expression, and electrophysiological criteria. Aberrant AVC development can lead to ventricular pre-excitation, a characteristic feature of Wolff-Parkinson-White syndrome. We demonstrate that postnatal activation of Notch signaling downregulates canonical Wnt targets within the AV junction. Stabilization of β-catenin protein levels can rescue Notch-mediated ventricular pre-excitation and dysregulated ion channel gene expression. Conclusions: Our data demonstrate that myocardial canonical Wnt signaling is an important regulator of AVC maturation and electric programming upstream of Tbx3. Our data further suggest that ventricular preexcitation may require both morphological patterning defects, as well as myocardial lineage reprogramming, to allow robust conduction across accessory pathway tissue.
AB - Rationale: Proper patterning of the atrioventricular canal (AVC) is essential for delay of electrical impulses between atria and ventricles, and defects in AVC maturation can result in congenital heart disease. Objective: To determine the role of canonical Wnt signaling in the myocardium during AVC development. Methods and Results: We used a novel allele of β-catenin that preserves β-catenin's cell adhesive functions but disrupts canonical Wnt signaling, allowing us to probe the effects of Wnt loss of function independently. We show that the loss of canonical Wnt signaling in the myocardium results in tricuspid atresia with hypoplastic right ventricle associated with the loss of AVC myocardium. In contrast, ectopic activation of Wnt signaling was sufficient to induce formation of ectopic AV junction-like tissue as assessed by morphology, gene expression, and electrophysiological criteria. Aberrant AVC development can lead to ventricular pre-excitation, a characteristic feature of Wolff-Parkinson-White syndrome. We demonstrate that postnatal activation of Notch signaling downregulates canonical Wnt targets within the AV junction. Stabilization of β-catenin protein levels can rescue Notch-mediated ventricular pre-excitation and dysregulated ion channel gene expression. Conclusions: Our data demonstrate that myocardial canonical Wnt signaling is an important regulator of AVC maturation and electric programming upstream of Tbx3. Our data further suggest that ventricular preexcitation may require both morphological patterning defects, as well as myocardial lineage reprogramming, to allow robust conduction across accessory pathway tissue.
KW - Arrhythmias
KW - Arrhythmogenic cardiomyopathy
KW - Cardiac
KW - Notch signaling pathway
KW - Septal defects
KW - Tricuspid atresia
KW - Ventricular pre-excitation
KW - Wnt signaling pathway
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U2 - 10.1161/CIRCRESAHA.116.304731
DO - 10.1161/CIRCRESAHA.116.304731
M3 - Article
C2 - 25599332
AN - SCOPUS:84927632105
SN - 0009-7330
VL - 116
SP - 398
EP - 406
JO - Circulation research
JF - Circulation research
IS - 3
ER -