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大鼠脂肪细胞中胰岛素样生长因子II受体结合及胰岛素受体激酶活性的刺激作用。钒酸盐和过氧化氢的影响。

Stimulation of insulin-like growth factor II receptor binding and insulin receptor kinase activity in rat adipocytes. Effects of vanadate and H2O2.

作者信息

Kadota S, Fantus I G, Deragon G, Guyda H J, Posner B I

出版信息

J Biol Chem. 1987 Jun 15;262(17):8252-6.

PMID:3036804
Abstract

Autophosphorylation of the insulin receptor on tyrosine residues and activation of the endogenous insulin receptor kinase is postulated to be a critical step in the mechanism of action of insulin. To investigate this hypothesis, the insulin-mimicking effects of vanadate (sodium orthovanadate) and H2O2 (hydrogen peroxide) alone and in combination were examined in freshly isolated rat adipocytes. Vanadate and H2O2 stimulated the translocation of insulin-like growth factor II (IGF-II) receptors to the plasma membrane of rat adipocytes in a manner analogous to insulin. IGF-II binding was increased by maximally effective doses of vanadate (1 mM), H2O2 (1 mM), and insulin (10 ng/ml) to 172 +/- 10, 138 +/- 12, and 289 +/- 16% of control, respectively. Previously (Kadota, S., Fantus, I. G., Hersh, B., and Posner, B. I. (1986) Biochem. Biophys. Res. Commun. 138, 174-178), we showed that the combination of these concentrations of vanadate plus insulin was not more potent than insulin alone. In this study, similar results were found with H2O2 plus insulin. In contrast, the combination of vanadate plus H2O2 was synergistic, effecting an increase of IGF-II binding to 488 +/- 23% of control. Amiloride inhibited the effects of vanadate, H2O2, and insulin. Adipocyte insulin receptors purified by wheat germ agglutinin chromatography were assayed for tyrosine kinase activity using the synthetic substrate poly(Glu,Tyr) (4:1). Basal activity (no in vitro insulin) was stimulated by exposure of intact cells to vanadate, H2O2, insulin, and vanadate + H2O2 to 147.7 +/- 4.3, 178.2 +/- 43.4, 495.0 +/- 67.1, and 913.2 +/- 92.0% of control, respectively. The stimulation of tyrosine kinase activity by these agents was accounted for by the insulin receptor as the augmented activity was completely immunoprecipitated with insulin receptor antibody. In these studies, the increase in IGF-II binding correlated significantly with the activation of the insulin receptor-tyrosine kinase (r = 0.927, p less than 0.001). These data support the hypothesis that activation of the insulin receptor kinase is linked to insulin action.

摘要

胰岛素受体酪氨酸残基的自磷酸化以及内源性胰岛素受体激酶的激活被认为是胰岛素作用机制中的关键步骤。为了研究这一假说,我们在新鲜分离的大鼠脂肪细胞中检测了钒酸盐(原钒酸钠)和过氧化氢单独及联合使用时的胰岛素模拟效应。钒酸盐和过氧化氢以类似于胰岛素的方式刺激胰岛素样生长因子II(IGF-II)受体向大鼠脂肪细胞质膜的转位。最大有效剂量的钒酸盐(1 mM)、过氧化氢(1 mM)和胰岛素(10 ng/ml)分别将IGF-II结合增加至对照的172±10%、138±12%和289±16%。此前(Kadota, S., Fantus, I. G., Hersh, B., and Posner, B. I. (1986) Biochem. Biophys. Res. Commun. 138, 174 - 178),我们发现这些浓度的钒酸盐与胰岛素联合使用并不比单独使用胰岛素更有效。在本研究中,过氧化氢与胰岛素联合使用也得到了类似结果。相反,钒酸盐与过氧化氢联合使用具有协同作用,使IGF-II结合增加至对照的488±23%。氨氯地平抑制钒酸盐、过氧化氢和胰岛素的作用。使用合成底物聚(Glu,Tyr)(4:1)对通过麦胚凝集素层析纯化的脂肪细胞胰岛素受体进行酪氨酸激酶活性测定。完整细胞暴露于钒酸盐、过氧化氢、胰岛素和钒酸盐 + 过氧化氢时,基础活性(无体外胰岛素)分别被刺激至对照的147.7±4.3%、178.2±43.4%、495.0±67.1%和913.2±92.0%。这些试剂对酪氨酸激酶活性的刺激是由胰岛素受体引起的,因为增强的活性被胰岛素受体抗体完全免疫沉淀。在这些研究中,IGF-II结合的增加与胰岛素受体 - 酪氨酸激酶的激活显著相关(r = 0.927,p < 0.001)。这些数据支持胰岛素受体激酶的激活与胰岛素作用相关的假说。

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