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In vivo and in witro Techniques to Study Pancreas Dewelopment and Islet Cell Function

机译:体内和体外技术研究胰腺发育和胰岛电池功能

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Over the last decades, pancreas development has been widely investigated. Understanding the mechanisms that control beta-cell development should allow progress towards the regeneration of these cells in humans. Particularly, it is well established that inductive signals from the mesenchyme play an essential role in the proliferation of precursor cells. In the present review, we focused on the roles of fibroblast growth factors (FGFs) in pancreas development. Improvements of the in vivo and in vitro techniques were used to define the function of FGF10. Experiments on FGF10 knockout mice showed that FGF10 is required forthe proliferation of precursor cells and the pancreas development. Several laboratories used different in vitro techniques to study the effect of FGF10 on beta-cell differentiation. These methods of investigation are described here. In our experiments, pancreases were placed at the air-liquid interface to define the precise mechanism of action of FGF10. We showed that FGF10 positively regulates the beta-cell mass by increasing the proliferation of the early precursors and by extending the window of expression of the endocrine precursor marker Ngn3. These data are compared with studies performed with other culture systems. Finally, the role of other FGFs is discussed.
机译:在过去的几十年中,胰腺发展已被广泛调查。了解控制β细胞开发的机制应允许在人类中进行这些细胞的再生。特别地,很好地确定,来自间充质的电感信号在前体细胞的增殖中起重要作用。在本综述中,我们专注于成纤维细胞生长因子(FGF)在胰腺发育中的作用。使用体内和体外技术的改进用于定义FGF10的功能。 FGF10敲除小鼠的实验表明FGF10是前体细胞的增殖和胰腺发育的需求。几个实验室使用了不同的体外技术来研究FGF10对β细胞分化的影响。这里描述了这些调查方法。在我们的实验中,将胰腺释放在空气液体界面处,以定义FGF10的精确作用机制。我们展示FGF10通过增加早期前体的增殖并通过延长内分泌前体标记NGN3的表达窗口来肯定地调节β细胞质量。将这些数据与与其他培养系统进行的研究进行比较。最后,讨论了其他FGF的作用。

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