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

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

Nature communications (2020-01-26)

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

PMID31980627

摘要

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.

材料

产品编号

品牌

产品描述

T5648

Sigma-Aldrich

泰莫西芬, ≥99%

11684795910

Roche

原位细胞死亡检测试剂盒，荧光素法, sufficient for ≤50 tests, suitable for detection

C9263

Sigma-Aldrich

胶原酶来源于溶组织梭菌, Type V, ≥1 FALGPA units/mg solid, >125 CDU/mg solid

G2654

Sigma-Aldrich

单克隆抗胰高血糖素小鼠抗, clone K79bB10, ascites fluid