In vivo imaging of β-cell function reveals glucose-mediated heterogeneity of β-cell functional development

β 细胞功能体内成像揭示了葡萄糖介导的 β 细胞功能发育的异质性

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作者:Jia Zhao, Weijian Zong, Yiwen Zhao, Dongzhou Gou, Shenghui Liang, Jiayu Shen, Yi Wu, Xuan Zheng, Runlong Wu, Xu Wang, Fuzeng Niu, Aimin Wang, Yunfeng Zhang, Jing-Wei Xiong, Liangyi Chen, Yanmei Liu

Abstract

How pancreatic β-cells acquire function in vivo is a long-standing mystery due to the lack of technology to visualize β-cell function in living animals. Here, we applied a high-resolution two-photon light-sheet microscope for the first in vivo imaging of Ca2+activity of every β-cell in Tg (ins:Rcamp1.07) zebrafish. We reveal that the heterogeneity of β-cell functional development in vivo occurred as two waves propagating from the islet mantle to the core, coordinated by islet vascularization. Increasing amounts of glucose induced functional acquisition and enhancement of β-cells via activating calcineurin/nuclear factor of activated T-cells (NFAT) signaling. Conserved in mammalians, calcineurin/NFAT prompted high-glucose-stimulated insulin secretion of neonatal mouse islets cultured in vitro. However, the reduction in low-glucose-stimulated insulin secretion was dependent on optimal glucose but independent of calcineurin/NFAT. Thus, combination of optimal glucose and calcineurin activation represents a previously unexplored strategy for promoting functional maturation of stem cell-derived β-like cells in vitro.

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