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BMP signaling regulates the fate of chondro-osteoprogenitor cells in facial mesenchyme in a stage-specific manner:BMP Levels Regulate Facial Chondrogenic Condensations

机译:BMP信号以特定阶段的方式调节面部间充质中软骨成骨祖细胞的命运:BMP水平调节面部软骨形成凝结

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摘要

Background: Lineage tracing has shown that most of the facial skeleton is derived from cranial neural crest cells. However, the local signals that influence postmigratory, neural crest-derived mesenchyme also play a major role in patterning the skeleton. Here, we study the role of BMP signaling in regulating the fate of chondro-osteoprogenitor cells in the face. Results: A single Noggin-soaked bead inserted into stage 15 chicken embryos induced an ectopic cartilage resembling the interorbital septum within the palate and other midline structures. In contrast, the same treatment in stage 20 embryos caused a loss of bones. The molecular basis for the stage-specific response to Noggin lay in the simultaneous up-regulation of SOX9 and downregulation of RUNX2 in the maxillary mesenchyme, increased cell adhesiveness as shown by N-cadherin induction around the beads and increased RA pathway gene expression. None of these changes were observed in stage 20 embryos. Conclusions: These experiments demonstrate how slight changes in expression of growth factors such as BMPs could lead to gain or loss of cartilage in the upper jaw during vertebrate evolution. In addition, BMPs have at least two roles: one in patterning the skull and another in regulating the skeletogenic fates of neural crest-derived mesenchyme.
机译:背景:沿袭追踪显示,大多数面部骨骼均来自颅神经rest细胞。但是,影响迁移后神经neural来源的间充质的局部信号在骨架构图中也起着重要作用。在这里,我们研究了BMP信号传导在调节软骨成骨祖细胞命运中的作用。结果:单个浸入Noggin的珠子插入第15阶段的鸡胚中,会诱发异位软骨,类似于the及其他中线结构中的眶间隔。相反,在20期胚胎中进行相同的处理会导致骨骼丢失。对Noggin的阶段特异性反应的分子基础在于上颌间充质细胞中同时上调SOX9和下调RUNX2,增加细胞粘附性,如磁珠周围的N-钙黏着蛋白诱导和RA途径基因表达增加。在20期胚胎中未观察到这些变化。结论:这些实验表明,在脊椎动物进化过程中,生长因子(如BMPs)表达的微小变化如何导致上颌软骨的增减。此外,BMP至少具有两个作用:一个作用是构图头骨,另一个作用是调节神经c衍生的间充质的骨骼生成。

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