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游离脂肪酸对分离的大鼠肝细胞中胰岛素结合、降解及作用的抑制作用。

Free-fatty acid inhibition of insulin binding, degradation, and action in isolated rat hepatocytes.

作者信息

Svedberg J, Björntorp P, Smith U, Lönnroth P

机构信息

Department of Medicine I, Sahlgren's Hospital, Gothenburg, Sweden.

出版信息

Diabetes. 1990 May;39(5):570-4. doi: 10.2337/diab.39.5.570.

DOI:10.2337/diab.39.5.570
PMID:2185108
Abstract

The effect of free fatty acids (FFAs) on insulin binding and action was investigated in isolated rat hepatocytes. Oleic acid (0.4 mM) added to the cells rapidly (within 45 min) reduced insulin binding and degradation (each by 45%; P less than 0.001, n = 7) without changing the apparent receptor affinity. The effect was concentration dependent; a half-maximal inhibitory effect occurred at 0.150 +/- 0.050 mM (mean +/- SE). Oleic acid exerted no effect on insulin binding in energy-depleted (KCN-treated) cells. Oleic, palmitic, stearic, palmitoleic, and eicosapentaenoic acids were equally effective in reducing insulin binding. FFA did not change insulin binding to partially purified insulin receptors, thus excluding a direct effect on the insulin receptor. Furthermore, binding to partially purified receptors from solubilized cells pretreated with 0.2 mM oleic acid was not changed, indicating the effect of FFA in intact cells is on the rate of receptor internalization and/or recycling. Concomitant with the effect on insulin binding, oleic acid elicited a concentration-dependent reduction in nonstimulated cellular [14C]aminoisobutyric acid uptake (AIB; 29 +/- 8%, P less than 0.05) and decreased the maximal effect of insulin (39 +/- 7%, P less than 0.05). Thus, in a concentration-dependent manner, different fatty acids can reduce the number of binding sites for insulin and the degradation of insulin by isolated liver cells. Basal and insulin-stimulated AIB transport was reduced, suggesting the presence of postbinding perturbations. These data suggest that FFA exerts an important modulating effect on insulin action in the liver.

摘要

在分离的大鼠肝细胞中研究了游离脂肪酸(FFA)对胰岛素结合及作用的影响。向细胞中添加油酸(0.4 mM)可迅速(45分钟内)降低胰岛素结合及降解(各降低45%;P<0.001,n = 7),而不改变表观受体亲和力。该效应呈浓度依赖性;在0.150±0.050 mM(平均值±标准误)时出现半数最大抑制效应。油酸对能量耗竭(经氰化钾处理)的细胞中的胰岛素结合无影响。油酸、棕榈酸、硬脂酸、棕榈油酸和二十碳五烯酸在降低胰岛素结合方面同样有效。FFA不会改变胰岛素与部分纯化的胰岛素受体的结合,因此排除了对胰岛素受体的直接作用。此外,用0.2 mM油酸预处理的溶解细胞中部分纯化受体的结合未发生改变,表明FFA在完整细胞中的作用是对受体内化和/或再循环速率的影响。与对胰岛素结合的影响同时,油酸引起非刺激细胞[14C]氨基异丁酸摄取(AIB)呈浓度依赖性降低(29±8%,P<0.05),并降低胰岛素的最大效应(39±7%,P<0.05)。因此,不同脂肪酸可通过分离的肝细胞以浓度依赖性方式减少胰岛素的结合位点数量及胰岛素的降解。基础及胰岛素刺激的AIB转运降低,提示存在结合后干扰。这些数据表明FFA对肝脏中的胰岛素作用发挥重要的调节作用。

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