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间质胰岛素浓度决定了瘦人和肥胖男性的葡萄糖摄取率,但不决定胰岛素抵抗。

Interstitial insulin concentrations determine glucose uptake rates but not insulin resistance in lean and obese men.

作者信息

Castillo C, Bogardus C, Bergman R, Thuillez P, Lillioja S

机构信息

Clinical Diabetes and Nutrition Section, National Institutes of Diabetes, and Digestive and Kidney Diseases, National Institutes of Health, Phoenix, Arizona 85016.

出版信息

J Clin Invest. 1994 Jan;93(1):10-6. doi: 10.1172/JCI116932.

Abstract

Insulin action and obesity are both correlated with the density of muscle capillary supply in humans. Since the altered muscle anatomy in the obese might affect interstitial insulin concentrations and reduce insulin action, we have cannulated peripheral lymphatic vessels in lean and obese males, and compared peripheral lymph insulin concentrations with whole body glucose uptake during a euglycemic, hyperinsulinemic clamp. Lymph insulin concentrations in the lower limb averaged only 34% of arterial insulin concentrations during 150 min of insulin infusion. Obese subjects had the highest arterial (P < or = 0.0001) and lymph insulin (P < 0.005) concentrations, but the lowest glucose uptake rates (P < 0.002). In contrast to the initial steep rise then plateau of arterial insulins, both lymph insulin and whole body glucose uptake rates rose slowly and did not consistently reach a plateau. In each individual, the glucose uptake closely correlated with peripheral lymphatic insulin concentrations (mean r2 = 0.95). The coupling between glucose uptake and lymph insulin (glucose uptake/pmol insulin) was much steeper in lean subjects than in the obese (P < or = 0.0001). These results indicate that even if insulin diffusion into tissues is rate limiting for insulin action, a tissue defect rather than an insulin diffusion defect causes insulin resistance in obese subjects.

摘要

胰岛素作用与肥胖均与人类肌肉毛细血管供应密度相关。由于肥胖者肌肉解剖结构的改变可能会影响组织间胰岛素浓度并降低胰岛素作用,我们已对瘦体型和肥胖男性的外周淋巴管进行插管,并在正常血糖、高胰岛素钳夹试验期间比较外周淋巴胰岛素浓度与全身葡萄糖摄取情况。在输注胰岛素的150分钟内,下肢淋巴胰岛素浓度平均仅为动脉胰岛素浓度的34%。肥胖受试者的动脉胰岛素浓度(P≤0.0001)和淋巴胰岛素浓度(P<0.005)最高,但葡萄糖摄取率最低(P<0.002)。与动脉胰岛素起初急剧上升然后趋于平稳不同,淋巴胰岛素和全身葡萄糖摄取率均上升缓慢,且未持续达到平稳状态。在每个个体中,葡萄糖摄取与外周淋巴胰岛素浓度密切相关(平均r2 = 0.95)。瘦体型受试者中葡萄糖摄取与淋巴胰岛素之间的耦合关系(葡萄糖摄取/皮摩尔胰岛素)比肥胖者陡峭得多(P≤0.0001)。这些结果表明,即使胰岛素向组织内的扩散是胰岛素作用的限速因素,但组织缺陷而非胰岛素扩散缺陷导致肥胖受试者出现胰岛素抵抗。

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