在前心脏区域及其衍生物中,骨形态发生蛋白4(BMP4)对于心内膜垫重塑、流出道分隔和半月瓣发育是必需的。
BMP4 is required in the anterior heart field and its derivatives for endocardial cushion remodeling, outflow tract septation, and semilunar valve development.
作者信息
McCulley David J, Kang Ji-One, Martin James F, Black Brian L
机构信息
Cardiovascular Research Institute, University of California, San Francisco, California 94158-2517, USA.
出版信息
Dev Dyn. 2008 Nov;237(11):3200-9. doi: 10.1002/dvdy.21743.
Abstract
The endocardial cushions play a critical role in septation of the four-chambered mammalian heart and in the formation of the valve leaflets that control blood flow through the heart. Within the outflow tract (OFT), both cardiac neural crest and endocardial-derived mesenchymal cells contribute to the endocardial cushions. Bone morphogenetic protein 4 (BMP4) is required for endocardial cushion development and for normal septation of the OFT. In the present study, we show that anterior heart field (AHF)-derived myocardium is an essential source of BMP4 required for normal endocardial cushion expansion and remodeling. Loss of BMP4 from the AHF in mice results in an insufficient number of cells in the developing OFT endocardial cushions, defective cushion remodeling, ventricular septal defects, persistent truncus arteriosus, and abnormal semilunar valve formation.
摘要
心内膜垫在哺乳动物四腔心脏的分隔以及控制心脏血流的瓣膜小叶形成过程中发挥着关键作用。在流出道(OFT)内,心脏神经嵴细胞和心内膜衍生的间充质细胞都对心内膜垫有贡献。骨形态发生蛋白4(BMP4)是心内膜垫发育和OFT正常分隔所必需的。在本研究中,我们表明前心脏区域(AHF)衍生的心肌是正常心内膜垫扩张和重塑所需的BMP4的重要来源。小鼠AHF中BMP4的缺失导致发育中的OFT心内膜垫细胞数量不足、垫重塑缺陷、室间隔缺损、永存动脉干和半月瓣形成异常。
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