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首页> 外文期刊>Development >Bmp signaling regulates proximal-distal differentiation of endoderm in mouse lung development.
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Bmp signaling regulates proximal-distal differentiation of endoderm in mouse lung development.

机译:Bmp信号传导调节小鼠肺发育中内胚层的近端-远端分化。

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In the mature mouse lung, the proximal-distal (P-D) axis is delineated by two distinct epithelial subpopulations: the proximal bronchiolar epithelium and the distal respiratory epithelium. Little is known about the signaling molecules that pattern the lung along the P-D axis. One candidate is Bone Morphogenetic Protein 4 (Bmp4), which is expressed in a dynamic pattern in the epithelial cells in the tips of growing lung buds. Previous studies in which Bmp4 was overexpressed in the lung endoderm (Bellusci, S., Henderson, R., Winnier, G., Oikawa, T. and Hogan, B. L. M. (1996) Development 122, 1693-1702) suggested that this factor plays an important role in lung morphogenesis. To further investigate this question, two complementary approaches were utilized to inhibit Bmp signaling in vivo. The Bmp antagonist Xnoggin and, independently, a dominant negative Bmp receptor (dnAlk6), were overexpressed using the surfactant protein C (Sp-C) promoter/enhancer. Inhibiting Bmp signaling results in a severe reduction in distal epithelial cell types and a concurrent increase in proximal cell types, as indicated by morphology and expression of marker genes, including the proximally expressed hepatocyte nuclear factor/forkhead homologue 4 (Hfh4) and Clara cell marker CC10, and the distal marker Sp-C. In addition, electron microscopy demonstrates the presence of ciliated cells, a proximal cell type, in the most peripheral regions of the transgenic lungs. We propose a model in which Bmp4 is a component of an apical signaling center controlling P-D patterning. Endodermal cells at the periphery of the lung, which are exposed to high levels of Bmp4, maintain or adopt a distal character, while cells receiving little or no Bmp4 signal initiate a proximal differentiation program.
机译:在成熟的小鼠肺中,近端-远端(P-D)轴由两个不同的上皮亚群描绘:近端细支气管上皮和远端呼吸上皮。关于沿着P-D轴对肺部进行构图的信号分子知之甚少。一种候选物是骨形态发生蛋白4(Bmp4),它以动态模式在生长中的肺芽顶端的上皮细胞中表达。先前关于Bmp4在肺内胚层中过表达的研究(Bellusci,S.,Henderson,R.,Winnier,G.,Oikawa,T.和Hogan,BLM(1996)Development 122,1693-1702)建议在肺形态发生中起重要作用。为了进一步研究这个问题,采用了两种互补的方法在体内抑制Bmp信号传导。使用表面活性剂蛋白C(Sp-C)启动子/增强子过表达Bmp拮抗剂Xnoggin和独立的显性负Bmp受体(dnAlk6)。抑制Bmp信号传导会导致远端上皮细胞类型的严重减少和近端细胞类型的同时增加,这由标记基因的形态和表达所表明,包括近端表达的肝细胞核因子/叉头同源物4(Hfh4)和Clara细胞标记CC10和远端标记Sp-C。另外,电子显微镜证明在转基因肺的最外围区域中存在纤毛细胞(近端细胞类型)。我们提出了一个模型,其中Bmp4是控制P-D模式的顶端信号中心的组成部分。暴露于高水平Bmp4的肺部周围的内胚层细胞维持或采取远端特征,而几乎不接收或不接收Bmp4信号的细胞启动近端分化程序。

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