Kindlin-2 modulates MafA and β-catenin expression to regulate β-cell function and mass in mice

Kindlin-2 调节 MafA 和 β-catenin 表达以调节小鼠 β 细胞功能和质量

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作者：Ke Zhu, Yumei Lai, Huiling Cao, Xiaochun Bai, Chuanju Liu, Qinnan Yan, Liting Ma, Di Chen, Giedrius Kanaporis, Junqi Wang, Luyuan Li, Tao Cheng, Yong Wang, Chuanyue Wu, Guozhi Xiao

期刊：

Nature Communications

影响因子：

14.700

时间：

2020

起止号：

2020 Jan 24;11(1):484.

doi：

10.1038/s41467-019-14186-y

研究方向：

信号转导

细胞类型：

其它细胞

信号通路：

Wnt/β-Catenin

Abstract

β-Cell dysfunction and reduction in β-cell mass are hallmark events of diabetes mellitus. Here we show that β-cells express abundant Kindlin-2 and deleting its expression causes severe diabetes-like phenotypes without markedly causing peripheral insulin resistance. Kindlin-2, through its C-terminal region, binds to and stabilizes MafA, which activates insulin expression. Kindlin-2 loss impairs insulin secretion in primary human and mouse islets in vitro and in mice by reducing, at least in part, Ca2+ release in β-cells. Kindlin-2 loss activates GSK-3β and downregulates β-catenin, leading to reduced β-cell proliferation and mass. Kindlin-2 loss reduces the percentage of β-cells and concomitantly increases that of α-cells during early pancreatic development. Genetic activation of β-catenin in β-cells restores the diabetes-like phenotypes induced by Kindlin-2 loss. Finally, the inducible deletion of β-cell Kindlin-2 causes diabetic phenotypes in adult mice. Collectively, our results establish an important function of Kindlin-2 and provide a potential therapeutic target for diabetes.

Kindlin-2 modulates MafA and β-catenin expression to regulate β-cell function and mass in mice

Kindlin-2 调节 MafA 和 β-catenin 表达以调节小鼠 β 细胞功能和质量

Abstract

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