机构地区:[1]华中科技大学同济医学院附属同济医院内分泌科,武汉430030 [2]美国纽约州立基础研究所神经化学系
出 处:《中国生物化学与分子生物学报》2006年第11期902-908,共7页Chinese Journal of Biochemistry and Molecular Biology
摘 要:Tau蛋白过度磷酸化是Alzheimer病(Alzheimer disease,AD)的一个重要病理特征.采用1型糖尿病大鼠模型,研究胰岛素信号传导途径及葡萄糖代谢失调对tau蛋白过度磷酸化的形成机制进行探讨.以同龄Wistar大鼠做对照(CTL),胰腺大部分切除造低胰岛素组(PX),STZ较大剂量一次性注射造1型糖尿病模型即低胰岛素高血糖组(T1DM).葡萄糖氧化酶法检测血浆血糖,放免法检测血浆胰岛素,蛋白质印迹分析海马内总tau蛋白及tau蛋白上部分位点(Ser199、Thr212、Ser214、Ser396及Ser422)的磷酸化及神经细胞膜上葡萄糖转运子3(glucose transport3,GLUT3)水平.γ-32P-ATP和特异性底物肽检测海马内胰岛素信号传导系统中的关键酶糖原合成酶激酶-3β(glycogensynthase kinase-3β,GSK-3β)活性.发现3组大鼠海马回总tau蛋白水平无显著差异,但以高血糖、低胰岛素血症为特征的T1DM组在tau蛋白Ser199、Thr212、Ser214、Ser396及Ser422位点上,呈现过度磷酸化状态,以低胰岛素血症为特征而血糖正常的PX组在位点Ser199、Thr212及Ser396上磷酸化程度比对照组显著上升,在位点Ser214及Ser422上的磷酸化程度的改变不显著;T1DM及PX组大鼠海马GSK-3β活性显著高于对照组,而GLUT3水平在T1DM和PX组均降低,尤以T1DM组降低更显著.研究结果显示,胰岛素水平低下可能通过激活GSK-3β和下调细胞内葡萄糖代谢的双重作用引起脑内tau蛋白过度磷酸化.Abnormal hyperphosphorylation of tau plays a critical role in the pathogenesis of Alzheimer disease (AD) and decreased insulin and glucose are the causes of hyperphosphorylation of tau. The roles of dysregulation of insulin signaling and glucose metabolism in hyperphosphorylation of tau in type 1 diabetic rats were studied. Wistar rats were randomized into 3 groups, pancreatectomy (PX), type 1 diabetes mellitus (T1DM) and control group. The model of PX group characterized by low plasma insulin was made by partial (90%) pancreatectomy, and the model of T1DM group was made by single injection of STZ. The plasma insulin level was measured by RIA method, and the plasma glucose by glucose-oxidase method. Total tau level, the phosphorylation level of tau at individual phosphorylation sites (Ser199, Thr212, Ser214, Ser396 and Ser422) and glucose transport 3 (GLUT3) on neuronal membrane fractions were analyzed by Western blots. The activity of glycogen synthase kinase 3β (GSK-3 β), a key component of insulin signal transduction pathway and a known tan kinase, in the hippocampus of rats was determined by using γ-^32 P-ATP and the specific peptide substrate. It was found that neither pancreatectomy nor STZ injection changed the total level of tan protein in the hippocampus of rats. However, Tau was found to be hyperphosphorylated at several AD- related phosphorylation sites (Ser199,Thr212, Ser214, Ser396 and Ser422) in T1DM group. In PX group, Ser199 ,Thr212 and Ser396 of tau protein were hyperphosphorylated, but no significant changes at Ser214 and Ser422. The activity of GSK-313 was found to be increased dramatically in the hippocampi of rats in both PX and T1DM groups. The level of GLUT3 was also found to be decreased in both PX and T1DM groups, with a more dramatic decrease in T1DM group. These findings suggest that impaired insulin signaling could facilitate hyperphosphorylation of tau via both upregulation of GSK-313 and decreased intracellular glucose metabolism.
关 键 词:胰岛素 葡萄糖代谢 TAU蛋白 蛋白磷酸化 糖原合成酶激酶-3Β
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