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重组人胰岛素样生长因子-I与胰岛素对人体葡萄糖和亮氨酸动力学影响的比较。

Comparison of the effects of recombinant human insulin-like growth factor-I and insulin on glucose and leucine kinetics in humans.

作者信息

Laager R, Ninnis R, Keller U

机构信息

Department of Research Medicine, University of Basel, Switzerland.

出版信息

J Clin Invest. 1993 Oct;92(4):1903-9. doi: 10.1172/JCI116783.

Abstract

To compare the metabolic effects of elevated plasma concentrations of IGF-I and insulin, overnight-fasted normal subjects were studied twice, once receiving IGF-I and once insulin at doses that resulted in identical increases in glucose uptake during 8-h euglycemic clamping. Recombinant human IGF-I or insulin were infused in one group at high doses (30 micrograms/kg per h IGF-I or 0.23 nmol/kg per h insulin) and in another group at low doses (5 micrograms/kg per h IGF-I or 0.04 nmol/kg per h insulin). Glucose rate of disappearance (measured by [6,6-D2]-glucose infusions) increased from baseline by 239 +/- 16% during high dose IGF-I vs 197 +/- 18% during insulin (P = 0.021 vs IGF-I). Hepatic glucose production decreased by 37 +/- 6% during high dose IGF-I vs 89 +/- 13% during insulin (P = 0.0028 vs IGF-I). IGF-I suppressed whole body leucine flux ([1-13C]-leucine infusion technique) more than insulin (42 +/- 4 vs 32 +/- 3% during high doses, P = 0.0082). Leucine oxidation rate decreased during high dose IGF-I more than during insulin (55 +/- 4 vs 32 +/- 6%, P = 0.0001). The decreases of plasma concentrations of free fatty acids, acetoacetate, and beta-hydroxybutyrate after 8 h of IGF-I and insulin administration were similar. Plasma C-peptide levels decreased by 57 +/- 4% during high doses of IGF-I vs 36 +/- 6% during insulin (P = 0.005 vs IGF-I). The present data demonstrate that, compared to insulin, an acute increase in plasma IGF-I levels results in preferential enhancement of peripheral glucose utilization, diminished suppression of hepatic glucose production, augmented decrease of whole body protein breakdown (leucine flux), and of irreversible leucine catabolism but in similar antilipolytic effects. The data suggest that insulin-like effects of IGF-I in humans are mediated in part via IGF-I receptors and in part via insulin receptors.

摘要

为比较血浆中胰岛素样生长因子-I(IGF-I)和胰岛素浓度升高的代谢效应,对过夜禁食的正常受试者进行了两次研究,一次给予IGF-I,一次给予胰岛素,剂量使在8小时血糖正常钳夹期间葡萄糖摄取有相同程度的增加。重组人IGF-I或胰岛素在一组中高剂量输注(30微克/千克每小时IGF-I或0.23纳摩尔/千克每小时胰岛素),在另一组中低剂量输注(5微克/千克每小时IGF-I或0.04纳摩尔/千克每小时胰岛素)。高剂量IGF-I期间葡萄糖消失率(通过[6,6-D2]-葡萄糖输注测量)较基线升高239±16%,而胰岛素期间为197±18%(与IGF-I相比,P = 0.021)。高剂量IGF-I期间肝葡萄糖生成减少37±6%,而胰岛素期间为89±13%(与IGF-I相比,P = 0.0028)。IGF-I对全身亮氨酸通量([1-13C]-亮氨酸输注技术)的抑制作用大于胰岛素(高剂量时分别为42±4%和32±3%,P = 0.0082)。高剂量IGF-I期间亮氨酸氧化率的降低大于胰岛素期间(分别为55±4%和32±6%,P = 0.0001)。给予IGF-I和胰岛素8小时后,游离脂肪酸、乙酰乙酸和β-羟基丁酸血浆浓度的降低相似。高剂量IGF-I期间血浆C肽水平降低57±4%,而胰岛素期间为36±6%(与IGF-I相比,P = 0.005)。目前的数据表明,与胰岛素相比,血浆IGF-I水平的急性升高导致外周葡萄糖利用优先增强、肝葡萄糖生成抑制减弱、全身蛋白质分解(亮氨酸通量)和不可逆亮氨酸分解代谢增加,但抗脂解作用相似。数据提示IGF-I在人体内的胰岛素样作用部分通过IGF-I受体介导,部分通过胰岛素受体介导。

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