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钙黏蛋白-11在心脏瓣膜中的表达模式与胚胎期心垫形成、瓣膜成熟及钙化过程中的关键功能相关。

Cadherin-11 expression patterns in heart valves associate with key functions during embryonic cushion formation, valve maturation and calcification.

作者信息

Zhou Jingjing, Bowen Caitlin, Lu Gloria, Knapp Iii Calvin, Recknagel Andrew, Norris Russell A, Butcher Jonathan T

机构信息

Department of Biomedical Engineering, Cornell University, Ithaca, N.Y., USA.

出版信息

Cells Tissues Organs. 2013;198(4):300-10. doi: 10.1159/000356762. Epub 2013 Dec 20.

Abstract

Proper fibroblast cell migration and differentiation are critical for valve formation and homeostasis, but uncontrolled myofibroblastic activation may precede osteogenic differentiation and calcification. Cadherin-11 (cad-11) is a cell-cell adhesion protein classically expressed at mesenchymal-osteoblast interfaces that participates in mesenchymal differentiation to osteochondral lineages. This suggests cad-11 may have an important role in heart valve development and pathogenesis, but its expression patterns in valves are largely unknown. In this study, we profiled the spatial and temporal expression patterns of cad-11 in embryonic chick and mouse heart development. We determined that cad-11 is expressed in both endocardial and mesenchymal cells of the atrioventricular and outflow tract cushions (pre-HH30/E14), but becomes restricted to the valve endocardial/endothelial cells during late fetal remodeling and throughout postnatal life. We then investigated changes in cad-11 expression in a murine aortic valve disease model (the ApoE(-/-)). Unlike wild-type mice, cad-11 becomes dramatically re-expressed in the interstitium. Similarly, in calcified human aortic valve leaflets, cad-11 loses endothelial confinement and becomes significantly re-expressed in the valve interstitium. Double labeling identified that 91% of myofibroblastic and 96% of osteoblastic cells in calcified aortic valves were also cad-11 positive. Collectively, our results suggest that cad-11 is important for proper embryonic cushion formation and remodeling, but may also participate in aortic valve pathogenesis if re-expressed in adulthood.

摘要

成纤维细胞的正常迁移和分化对于瓣膜形成和内环境稳定至关重要,但不受控制的肌成纤维细胞激活可能先于成骨分化和钙化。钙黏蛋白-11(cad-11)是一种细胞间黏附蛋白,经典地表达于间充质-成骨细胞界面,参与间充质向骨软骨谱系的分化。这表明cad-11可能在心脏瓣膜发育和发病机制中起重要作用,但其在瓣膜中的表达模式在很大程度上尚不清楚。在本研究中,我们描绘了cad-11在胚胎鸡和小鼠心脏发育过程中的时空表达模式。我们确定cad-11在房室和流出道垫的内皮细胞和间充质细胞中均有表达(HH30/E14之前),但在胎儿后期重塑及整个出生后阶段,其表达局限于瓣膜内皮细胞。然后,我们在小鼠主动脉瓣疾病模型(ApoE(-/-))中研究了cad-11表达的变化。与野生型小鼠不同,cad-11在间质中显著重新表达。同样,在钙化的人主动脉瓣小叶中,cad-11失去内皮限制并在瓣膜间质中显著重新表达。双重标记显示,钙化主动脉瓣中91%的肌成纤维细胞和96%的成骨细胞也为cad-11阳性。总体而言,我们的结果表明,cad-11对于胚胎垫的正常形成和重塑很重要,但如果在成年期重新表达,也可能参与主动脉瓣发病机制。

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