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非胰岛素依赖型糖尿病(NIDDM)患者及肥胖者成纤维细胞和骨骼肌中葡萄糖转运异常及葡萄糖转运蛋白1(GLUT1)细胞表面含量变化

Abnormal glucose transport and GLUT1 cell-surface content in fibroblasts and skeletal muscle from NIDDM and obese subjects.

作者信息

Miele C, Formisano P, Condorelli G, Caruso M, Oriente F, Andreozzi F, Tocchetti C G, Riccardi G, Beguinot F

机构信息

C.N.R. Center of Experimental Endocrinology and Oncology, Naples, Italy.

出版信息

Diabetologia. 1997 Apr;40(4):421-9. doi: 10.1007/s001250050696.

Abstract

Glucose transport and GLUT1 expression were studied in fibroblasts from 7 lean and 5 obese non-insulin-dependent diabetic (NIDDM) subjects with at least 2 NIDDM first-degree relatives and from 12 lean and 5 obese non-diabetic subjects with no family history of diabetes. The obese individuals also had a strong family history of obesity. Fibroblasts from all of the subjects exhibited no difference in insulin receptor binding, autophosphorylation, and kinase and hexokinase activity. At variance, basal 2-deoxyglucose (2-DG) uptake and 3H-cytochalasin B binding were 50% increased in cells from individuals with NIDDM (p < 0.001) and/or obesity (p < 0.01) as compared to the lean non-diabetic subjects. Insulin-dependent (maximally stimulated-basal) 2-DG uptake and cytochalasin B binding were decreased three-fold in cells from the diabetic and/or obese subjects (p < 0.01). GLUT1 mRNA and total protein levels were comparable in fibroblasts from all the groups. However, basal GLUT1 cell-surface content was 50% greater in fibroblasts from the NIDDM and/or obese subjects as compared to the lean non-diabetic individuals while insulin-dependent GLUT1 recruitment at the cell surface was diminished three-fold. Increased basal GLUT1 content in the plasma membrane was also observed in skeletal muscle of 4 NIDDM and 3 non-diabetic obese individuals (p < 0.05 vs the lean non diabetic subjects). Basal 2-DG uptake in fibroblasts from diabetic/obese individuals and lean control subjects strongly correlated with the in vivo fasting plasma insulin concentration of the donor. A negative correlation was demonstrated between the magnitude of insulin-dependent glucose uptake by the fibroblasts and plasma insulin levels in vivo. We conclude that a primary abnormality in glucose transport and GLUT1 cell-surface content is present in fibroblasts from NIDDM and obese individuals. The abnormal GLUT1 content is also present in skeletal muscle plasma membranes from NIDDM and obese individuals.

摘要

对7名体型偏瘦且患有非胰岛素依赖型糖尿病(NIDDM)的受试者、5名体型肥胖且患有非胰岛素依赖型糖尿病且至少有2名NIDDM一级亲属的受试者,以及12名体型偏瘦且无糖尿病家族史的非糖尿病受试者、5名体型肥胖且无糖尿病家族史的非糖尿病受试者的成纤维细胞进行了葡萄糖转运和GLUT1表达的研究。这些肥胖个体也有肥胖的家族病史。所有受试者的成纤维细胞在胰岛素受体结合、自身磷酸化、激酶和己糖激酶活性方面均无差异。与此不同的是,与体型偏瘦的非糖尿病受试者相比,NIDDM患者(p < 0.001)和/或肥胖患者(p < 0.01)的细胞中基础2-脱氧葡萄糖(2-DG)摄取量和3H-细胞松弛素B结合量增加了50%。糖尿病和/或肥胖受试者的细胞中胰岛素依赖型(最大刺激-基础)2-DG摄取量和细胞松弛素B结合量降低了三倍(p < 0.01)。所有组的成纤维细胞中GLUT1 mRNA和总蛋白水平相当。然而,与体型偏瘦的非糖尿病个体相比,NIDDM和/或肥胖受试者的成纤维细胞中基础GLUT1细胞表面含量高出50%,而胰岛素依赖型GLUT1在细胞表面的募集减少了三倍。在4名NIDDM患者和3名非糖尿病肥胖个体的骨骼肌中也观察到质膜中基础GLUT1含量增加(与体型偏瘦的非糖尿病受试者相比,p < 0.05)。糖尿病/肥胖个体和成纤维细胞的体型偏瘦对照受试者的基础2-DG摄取量与供体的体内空腹血浆胰岛素浓度密切相关。成纤维细胞的胰岛素依赖型葡萄糖摄取量与体内血浆胰岛素水平之间呈负相关。我们得出结论,NIDDM患者和肥胖个体的成纤维细胞中存在葡萄糖转运和GLUT1细胞表面含量的原发性异常。NIDDM患者和肥胖个体的骨骼肌质膜中也存在异常的GLUT1含量。

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