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Essential roles of zebrafish bmp2a, fgf10, and fgf24 in the specification of the ventral pancreas

机译:斑马鱼bmp2a,fgf10和fgf24在腹侧胰腺规范中的重要作用

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In vertebrates, pancreas and liver arise from bipotential progenitors located in the embryonic gut endoderm. Bone morphogenic protein (BMP) and fibroblast growth factor (FGF) signaling pathways have been shown to induce hepatic specification while repressing pancreatic fate. Here we show that BMP and FGF factors also play crucial function, at slightly later stages, in the specification of the ventral pancreas. By analyzing the pancreatic markers pdx1 , ptf1a , and hlxb9la in different zebrafish models of BMP loss of function, we demonstrate that the BMP pathway is required between 20 and 24 h postfertilization to specify the ventral pancreatic bud. Knockdown experiments show that bmp2a , expressed in the lateral plate mesoderm at these stages, is essential for ventral pancreas specification. Bmp2a action is not restricted to the pancreatic domain and is also required for the proper expression of hepatic markers. By contrast, through the analysis of fgf10 ?/?; fgf24 ?/? embryos, we reveal the specific role of these two FGF ligands in the induction of the ventral pancreas and in the repression of the hepatic fate. These mutants display ventral pancreas agenesis and ectopic masses of hepatocytes. Overall, these data highlight the dynamic role of BMP and FGF in the patterning of the hepatopancreatic region.
机译:在脊椎动物中,胰腺和肝脏来自位于胚胎肠道内胚层中的双能祖细胞。业已证明,骨形态发生蛋白(BMP)和成纤维细胞生长因子(FGF)信号通路可诱导肝脏规格,同时抑制胰腺命运。在这里,我们显示BMP和FGF因子在腹胰腺的规格中稍晚的阶段也起着至关重要的作用。通过分析不同斑马鱼BMP功能丧失的斑马鱼模型中的胰腺标记pdx1,ptf1a和hlxb9la,我们证明了受精后20至24小时之间需要BMP途径来指定腹侧胰腺芽。击倒实验表明,在这些阶段在外侧板中胚层中表达的bmp2a对于腹侧胰腺规范至关重要。 Bmp2a作用不仅限于胰腺结构域,对于肝标志物的正确表达也是必需的。相比之下,通过分析fgf10 ?/?; fgf24 ?/?胚胎,我们揭示了这两个FGF配体在腹侧胰腺的诱导和肝命运的抑制中的特定作用。这些突变体表现出腹胰腺发育不全和肝细胞异位肿块。总体而言,这些数据突出了BMP和FGF在肝胰腺区域形成图案中的动态作用。

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