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FGF Signaling is Required for Anterior but not Posterior Specification of the Murine Liver Bud

机译:鼠肝芽的前部而非后部规格需要FGF信号传导

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Background:The definitive endoderm arises as a naive epithelial sheet that produces the entire gut tube and associated organs including the liver, pancreas and lungs. Murine explant studies demonstrate that fibroblast growth factor (FGF) signaling from adjacent tissues is required to induce hepatic gene expression from isolated foregut endoderm. The requirement of FGF signaling during liver development is examined by means of small molecule inhibition during whole embryo culture. Results:Loss of FGF signaling before hepatic induction results in morphological defects and gene expression changes that are confined to the anterior liver bud. In contrast the posterior portion of the liver bud remains relatively unaffected. Because FGF is thought to act as a morphogen during endoderm organogenesis, the ventral pancreas was also examined after FGF inhibition. Although the size of the ventral pancreas is not affected, loss of FGF signaling results in a significantly higher density of ventral pancreas cells. Conclusions:The requirement for FGF-mediated induction of hepatic gene expression differs across the anterior/posterior axis of the developing liver bud. These results underscore the importance of studying tissue differentiation in the context of the whole embryo. Developmental Dynamics 244:431-443, 2015. (c) 2014 Wiley Periodicals, Inc.
机译:背景:定形内胚层是幼稚的上皮层,可产生整个肠管和相关器官,包括肝脏,胰腺和肺。小鼠外植体研究表明,从邻近的前肠内胚层诱导肝基因表达需要来自相邻组织的成纤维细胞生长因子(FGF)信号。通过在整个胚胎培养过程中抑制小分子来检查肝脏发育过程中FGF信号的需求。结果:肝诱导前FGF信号的丢失导致形态缺陷和基因表达变化,而这些变化仅限于前肝芽。相反,肝芽的后部保持相对不受影响。由于FGF被认为是内胚层器官发生过程中的一种形态发生原,因此在抑制FGF后也要检查腹胰。尽管腹胰脏的大小不受影响,但FGF信号传导的缺失会导致腹腔胰腺细胞的密度显着升高。结论:FGF介导的诱导肝基因表达的要求在发育中的肝芽的前后轴上是不同的。这些结果强调了在整个胚胎的背景下研究组织分化的重要性。 Developmental Dynamics 244:431-443,2015年。(c)2014 Wiley Periodicals,Inc.

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