胰腺和胰岛素敏感组织的脂肪储存与2型糖尿病的发病机制。

F Assimacopoulos-Jeannet
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引用次数: 70

摘要

肥胖与骨骼肌、肝脏和胰腺细胞等非脂肪组织中脂质储存增加有关。这些脂质构成了长链脂肪酰基辅酶a (LC-CoA)及其衍生代谢物如二酰基甘油和神经酰胺的连续来源,作为蛋白激酶活性(特别是PKCs家族)、离子通道、基因表达和蛋白酰化的信号分子。在骨骼肌中,LC-CoA和二酰基甘油的增加易位并激活特定的蛋白激酶C (PKC)异构体,使丝氨酸上的IRS-1磷酸化,阻止其在酪氨酸上的磷酸化并与PI3激酶结合。这阻断了胰岛素信号通路,导致葡萄糖运输的刺激。在胰腺β细胞中,短期过量的脂肪酸或LC-CoA可激活PKC,并直接刺激胰岛素胞吐。长期暴露于游离脂肪酸(FFA)中,通过影响基因表达、K(ATP)通道活性增加和线粒体解偶联,导致葡萄糖刺激的胰岛素分泌基础增加和钝化。此外,饱和脂肪酸棕榈酸酯通过增加神经酰胺合成增加细胞凋亡。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Fat storage in pancreas and in insulin-sensitive tissues in pathogenesis of type 2 diabetes.

Obesity is associated with increased storage of lipids in nonadipose tissues like skeletal muscle, liver, and pancreatic beta cells. These lipids constitute a continuous source of long-chain fatty acyl CoA (LC-CoA) and derived metabolites like diacylglycerol and ceramide, acting as signalling molecules on protein kinases activities (in particular, the family of PKCs), ion channel, gene expression, and protein acylation. In skeletal muscle, the increase in LC-CoA and diacylglycerol translocates and activates specific protein kinase C (PKC) isoforms, which will phosphorylate IRS-1 on serine, preventing its phosphorylation on tyrosine and association with PI3 kinase. This interrupts the insulin signalling pathway leading to the stimulation of glucose transport. In pancreatic beta cells, short-term excess of fatty acids or LC-CoA activates PKC and also directly stimulates insulin exocytosis. Long-term exposure to free fatty acids (FFA) leads to an increased basal and blunted glucose-stimulated insulin secretion by affecting gene expression, increase in K(ATP) channel activity, and uncoupling of the mitochondria. In addition, the saturated FFA palmitate increases cell death by apoptosis via increase in ceramide synthesis.

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