首页> 外文期刊>Developmental dynamics: an official publication of the American Association of Anatomists >Fgf10 maintains notch activation, stimulates proliferation, and blocks differentiation of pancreatic epithelial cells.
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Fgf10 maintains notch activation, stimulates proliferation, and blocks differentiation of pancreatic epithelial cells.

机译:Fgf10维持缺口激活,刺激增殖并阻止胰腺上皮细胞分化。

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摘要

The pancreas is an endodermally derived organ that initially appears as a dorsal and ventral protrusion of the primitive gut epithelium. The pancreatic progenitor cells present in these early pancreatic anlagen proliferate and eventually give rise to all pancreatic cell types. The fibroblast growth factor receptor (FGFR) 2b high-affinity ligand FGF10 has been linked to pancreatic epithelial cell proliferation, and we have shown previously that Notch signalling controls pancreatic cell differentiation by means of lateral inhibition. In the developing pancreas, activated intracellular Notch appears to be required for maintaining cells in the progenitor state, in part by blocking the expression of the pro-endocrine gene neurogenin 3 (ngn3), and hence endocrine cell differentiation. Here, we show that persistent expression of Fgf10 in the embryonic pancreas of transgenic mice also inhibits pancreatic cell differentiation, while stimulating pancreatic epithelial cell proliferation. We provide evidence that one of the effects of the persistent expression of Fgf10 in the developing pancreas is maintained Notch activation, which results in impaired expression of ngn3 within the pancreatic epithelium. Together, our data suggest a role for FGF10/FGFR2b signalling in regulation of pancreatic cell proliferation and differentiation and that FGF10/FGFR2b signalling affects the Notch-mediated lateral inhibition pathway. Developmental Dynamics 228:185-193, 2003.
机译:胰腺是一种真皮内源性器官,最初表现为原始肠道上皮的背侧和腹侧突出。这些早期胰腺胶原蛋白中存在的胰腺祖细胞增殖并最终产生所有类型的胰腺细胞。成纤维细胞生长因子受体(FGFR)2b高亲和力配体FGF10已与胰腺上皮细胞增殖相关,并且我们以前已经证明,Notch信号通过侧向抑制来控制胰腺细胞分化。在发育中的胰腺中,激活细胞内Notch似乎是维持细胞处于祖细胞状态所必需的,部分是通过阻断前内分泌基因Neurogenin 3(ngn3)的表达,从而阻止内分泌细胞分化。在这里,我们显示Fgf10在转基因小鼠的胚胎胰腺中的持续表达也抑制了胰腺细胞的分化,同时刺激了胰腺上皮细胞的增殖。我们提供的证据表明,在发育中的胰腺中Fgf10持续表达的影响之一是维持Notch激活,这会导致胰腺上皮内ngn3的表达受损。在一起,我们的数据表明FGF10 / FGFR2b信号传导在调节胰腺细胞增殖和分化中的作用,并且FGF10 / FGFR2b信号传导影响Notch介导的侧向抑制途径。发展动力学228:185-193,2003年。

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