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Different developmental histories of beta-cells generate functional and proliferative heterogeneity during islet growth

机译:β细胞的不同发育史在胰岛生长过程中产生功能性和增殖性异质性

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The proliferative and functional heterogeneity among seemingly uniform cells is a universal phenomenon. Identifying the underlying factors requires single-cell analysis of function and proliferation. Here we show that the pancreatic beta-cells in zebrafish exhibit different growth-promoting and functional properties, which in part reflect differences in the time elapsed since birth of the cells. Calcium imaging shows that the beta-cells in the embryonic islet become functional during early zebrafish development. At later stages, younger beta-cells join the islet following differentiation from post-embryonic progenitors. Notably, the older and younger beta-cells occupy different regions within the islet, which generates topological asymmetries in glucose responsiveness and proliferation. Specifically, the older beta-cells exhibit robust glucose responsiveness, whereas younger beta-cells are more proliferative but less functional. As the islet approaches its mature state, heterogeneity diminishes and beta-cells synchronize function and proliferation. Our work illustrates a dynamic model of heterogeneity based on evolving proliferative and functional beta-cell states.
机译:看起来均匀的细胞之间的增殖和功能异质性是普遍现象。识别潜在因素需要对功能和增殖进行单细胞分析。在这里,我们显示了斑马鱼中的胰腺β细胞表现出不同的促生长和功能特性,部分反映了自细胞诞生以来经过的时间的差异。钙成像显示,在斑马鱼早期发育过程中,胚胎胰岛中的β细胞开始起作用。在以后的阶段,年轻的β细胞在与胚胎后祖细胞分化后加入胰岛。值得注意的是,较年轻和较年轻的β细胞占据胰岛内的不同区域,从而在葡萄糖反应性和增殖中产生拓扑不对称性。具体而言,年龄较大的β细胞表现出强大的葡萄糖反应能力,而年龄较小的β细胞则具有更强的增殖能力,但功能更弱。当胰岛接近其成熟状态时,异质性会降低,β细胞会同步功能和增殖。我们的工作说明了基于不断发展的增殖和功能性β细胞状态的异质性动态模型。

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