Gremlin-1蛋白参与调控脂毒性介导的胰岛β细胞功能障碍的机制研究
基本信息
结项摘要
We have shown in our previous studies that heterozygous lipoprotein lipase (LPL) knockout mice (LPL+/-) develop lipotoxicity-induced glucose intolerance and islet β cell dysfunction. However, the underlying molecular basis for the β cell dysfunction is unclear. By gene chip screening and in vitro study, we have firstly found the Gremlin-1 protein and its downstream BMPs signaling pathway may be involved. We also discovered that lipotoxicity-induced Gremlin-1 down-regulation may activate islet β cell inflammation through non-BMPs signaling pathways, leading to its dysfunction. In this study, we will further elucidate the role of Gremlin-1 protein and its downstream BMPs/Smad signaling pathway, immune inflammatory response and also angiogenesis pathway in β-cell dysfunction. This project will provide novel information on the molecular etiology of type 2 diabetes mellitus (T2DM). Such knowledge may provide a new basis for pancreatic β cell-targeted therapy of T2DM in the future.
我们前期课题发现脂蛋白脂酶基因敲除杂合子(LPL+/-)小鼠通过脂毒性直接诱发了糖代谢异常。随后在机制研究中发现LPL+/-小鼠在胰腺通过脂毒性诱发了胰岛β细胞功能障碍,为了探讨其分子机制,通过基因芯片筛选和体外研究,我们首次发现Gremlin-1蛋白及其下游骨形态形成蛋白(BMPs)信号通路参与了脂毒性介导的β细胞功能障碍的发生发展;同时还发现脂毒性引起的Gremlin-1下调还通过非BMPs信号通路激活β细胞炎症反应,进而导致其功能紊乱。因此本课题将围绕Gremlin-1蛋白更加深入地阐明脂毒性如何导致胰岛β细胞功能受损以及Gremlin-1/BMPs信号通路在该过程中的调控机制,并进一步探索免疫炎症及其他如血管生成等通路如何参与Gremlin-1介导的β细胞功能障碍。本项目的开展不仅为2型糖尿病分子病因学研究提供了新的视角,同时也为将来针对糖尿病开展β细胞靶向治疗提供了新的依据。
项目摘要
本项目通过构建高脂胰岛β细胞模型,检测高脂环境下细胞中Gremlin-1蛋白表达量以及BMPs/Smads 信号通路的表达,发现高脂环境下胰岛β细胞脂质沉积,高浓度葡萄糖刺激的胰岛素分泌量显著降低,同时Gremlin-1表达降低,BMP4及其下游的Smad-1、Smad-5、p-Smad1/5表达增加;进一步利用重组Gremlin-1蛋白和BMP4/Smads信号通路抑制剂干预胰岛β细胞,以及构建Gremlin-1干扰及过表达的胰岛β细胞模型,同时测定胰岛β细胞增殖、分化、凋亡及胰岛素分泌功能的变化,发现增加Gremlin-1的表达以及抑制BMP4/Smads 信号通路可以改善高脂环境下胰岛β细胞功能,胰岛β细胞在高浓度葡萄糖刺激下的分泌量升高,同时细胞增殖、分化相关分子表达升高,凋亡相关分子表达降低。通过检测高脂小鼠胰岛组织中Gremlin-1及下游BMP4/Smads信号通路表达情况发现,高脂小鼠的Gremlin-1表达显著下降,BMP4、Smad1、Smad5、p-Smad1/5表达升高,非诺贝特治疗改善高脂后,Gremlin-1表达升高,BMP4、Smad1、Smad5、p-Smad1/5表达降低,同时糖代谢改善。本项目揭示了高脂条件下胰岛 Gremlin-1 表达变化与β细胞功能改变的相关性,并且证明了Gremlin-1 通过 BMP4/Smads 信号通路参与脂毒性介导胰岛β细胞功能障碍。本项目为脂毒性在2型糖尿病病因学中的研究提供了新的视角,同时也为将来针对糖尿病开展胰岛β细胞靶向治疗提供了新的依据。
项目成果
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数据更新时间:2023-05-31
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