TY - JOUR
T1 - Alk3/Bmpr1a receptor is required for development of the atrioventricular canal into valves and annulus fibrosus
AU - Gaussin, Vinciane
AU - Morley, Gregory E.
AU - Cox, Luk
AU - Zwijsen, An
AU - Vance, Kendra M.
AU - Emile, Lorin
AU - Tian, Yimin
AU - Liu, Jing
AU - Hong, Chull
AU - Myers, Dina
AU - Conway, Simon J.
AU - Depre, Christophe
AU - Mishina, Yuji
AU - Behringer, Richard R.
AU - Hanks, Mark C.
AU - Schneider, Michael D.
AU - Huylebroeck, Danny
AU - Fishman, Glenn I.
AU - Burch, John B.E.
AU - Vatner, Stephen F.
PY - 2005/8/5
Y1 - 2005/8/5
N2 - Endocardial cushions are precursors of mature atrioventricular (AV) valves. Their formation is induced by signaling molecules originating from the AV myocardium, including bone morphogenetic proteins (BMPs), Here, we hypothesized that BMP signaling plays an important role in the AV myocardium during the maturation of AV valves from the cushions. To test our hypothesis, we used a unique Cre/lox system to target the deletion of a floxed Alk3 allele, the type IA receptor for BMPs, to cardiac myocytes of the AV canal (AVC). Lineage analysis indicated that cardiac myocytes of the AVC contributed to the tricuspid mural and posterior leaflets, the mitral septal leaflet, and the atrial border of the annulus fibrosus, When Alk3 was deleted in these cells, defects were seen in the same leaflets, ie, the tricuspid mural leaflet and mitral septal leaflet were longer, the tricuspid posterior leaflet was displaced and adherent to the ventricular wall, and the annulus fibrosus was disrupted resulting in ventricular preexcitation. The defects seen in mice with AVC-targeted deletion of Alk3 provide strong support for a role of Alk3 in human congenital heart diseases, such as Ebstein's anomaly. In conclusion, our mouse model demonstrated critical roles for Alk3 signaling in the AV myocardium during the development of AV valves and the annulus fibrosus.
AB - Endocardial cushions are precursors of mature atrioventricular (AV) valves. Their formation is induced by signaling molecules originating from the AV myocardium, including bone morphogenetic proteins (BMPs), Here, we hypothesized that BMP signaling plays an important role in the AV myocardium during the maturation of AV valves from the cushions. To test our hypothesis, we used a unique Cre/lox system to target the deletion of a floxed Alk3 allele, the type IA receptor for BMPs, to cardiac myocytes of the AV canal (AVC). Lineage analysis indicated that cardiac myocytes of the AVC contributed to the tricuspid mural and posterior leaflets, the mitral septal leaflet, and the atrial border of the annulus fibrosus, When Alk3 was deleted in these cells, defects were seen in the same leaflets, ie, the tricuspid mural leaflet and mitral septal leaflet were longer, the tricuspid posterior leaflet was displaced and adherent to the ventricular wall, and the annulus fibrosus was disrupted resulting in ventricular preexcitation. The defects seen in mice with AVC-targeted deletion of Alk3 provide strong support for a role of Alk3 in human congenital heart diseases, such as Ebstein's anomaly. In conclusion, our mouse model demonstrated critical roles for Alk3 signaling in the AV myocardium during the development of AV valves and the annulus fibrosus.
KW - Atrioventricular canal
KW - Bone morphogenetic protein signaling
KW - Cre-lox system
KW - Heart development
UR - http://www.scopus.com/inward/record.url?scp=23344439128&partnerID=8YFLogxK
U2 - 10.1161/01.RES.0000177862.85474.63
DO - 10.1161/01.RES.0000177862.85474.63
M3 - Article
C2 - 16037571
AN - SCOPUS:23344439128
SN - 0009-7330
VL - 97
SP - 219
EP - 226
JO - Circulation Research
JF - Circulation Research
IS - 3
ER -