糖耐量受损的非肥胖受试者口服葡萄糖后的胰岛素分泌及肠促胰岛素激素
Insulin secretion and incretin hormones after oral glucose in non-obese subjects with impaired glucose tolerance.
作者信息
Rask E, Olsson T, Söderberg S, Holst Jj J j, Tura A, Pacini G, Ahrén B
机构信息
Department of Medicine, Umeå University, Umeå, Sweden.
出版信息
Metabolism. 2004 May;53(5):624-31. doi: 10.1016/j.metabol.2003.11.011.
Subjects with impaired glucose tolerance (IGT) are usually overweight and exhibit insulin resistance with a defective compensation of insulin secretion. In this study, we sought to establish the interrelation between insulin secretion and insulin sensitivity after oral glucose in non-obese subjects with IGT and we also examined this interrelation in relation to the 2 main incretins, glucagon-like peptide (GLP-1) and gastric inhibitory polypeptide (GIP). To that end, 13 women with IGT and 17 women with normal glucose tolerance (NGT) underwent an oral glucose tolerance test (OGTT) with measurements of glucose, insulin, C-peptide, GLP-1, and GIP. Insulin secretion (TIS) and insulin sensitivity (OGIS) were assessed using models describing the relationship between glucose, insulin and C-peptide data. These models allowed estimation also of the hepatic extraction of insulin. The age (54.2 +/- 9.7 [mean +/- SD] years) and body mass index (BMI; 26.0 +/- 4.0 kg/m(2)) did not differ between the groups. Subjects with IGT displayed lower TIS during the initial 30 minutes after oral glucose (0.97 +/- 0.17 [mean +/- SEM] v 1.75 +/- 0.23 nmol/L in NGT; P =.018) and lower OGIS (397 +/- 21 v 463 +/- 12 mL/min/m(2); P =.005). The incremental 30-minute TIS times OGIS (reflecting insulin secretion in relation to insulin sensitivity) was significantly reduced in IGT (359 +/- 51 v 774 +/- 91 nmol/min/m(2), P =.001). This measure correlated inversely to the 2-hour glucose level (r = -0.71; P <.001). In contrast, TIS over the whole 180-minute period was higher in IGT (26.2 +/- 2.4 v 20.0 +/- 2.0 nmol/L; P =.035). Hepatic insulin extraction correlated linearly with OGIS (r = 0.71; P <.001), but was not significantly different between the groups although there was a trend with lower extraction in IGT (P =.055). Plasma levels of GLP-1 and GIP increased after oral glucose. Total secretion of these incretin hormones during the 3-hour test did not differ between the 2 groups. However, the 30-minute increase in GLP-1 concentrations was lower in IGT than in NGT (P =.036). We conclude that also in non-obese subjects with IGT, when adiposity is controlled for in relation to NGT, defective early insulin secretion after oral glucose is a key factor. This defective beta-cell function is associated with, and may be caused by, a reduced early GLP-1 response.
糖耐量受损(IGT)的受试者通常超重,表现出胰岛素抵抗,且胰岛素分泌的代偿功能存在缺陷。在本研究中,我们试图确定非肥胖IGT受试者口服葡萄糖后胰岛素分泌与胰岛素敏感性之间的相互关系,并且我们还研究了这种相互关系与两种主要肠促胰岛素,即胰高血糖素样肽(GLP - 1)和胃抑制多肽(GIP)的关系。为此,13名IGT女性和17名糖耐量正常(NGT)的女性接受了口服葡萄糖耐量试验(OGTT),并测量了葡萄糖、胰岛素、C肽、GLP - 1和GIP。使用描述葡萄糖、胰岛素和C肽数据之间关系的模型评估胰岛素分泌(TIS)和胰岛素敏感性(OGIS)。这些模型还可以估计胰岛素的肝脏摄取。两组之间的年龄(54.2±9.7 [平均值±标准差]岁)和体重指数(BMI;26.0±4.0 kg/m²)没有差异。IGT受试者在口服葡萄糖后的最初30分钟内TIS较低(0.97±0.17 [平均值±标准误]对比NGT中的1.75±0.23 nmol/L;P = 0.018),OGIS也较低(397±21对比463±12 mL/min/m²;P = 0.005)。IGT中30分钟的TIS增量乘以OGIS(反映与胰岛素敏感性相关的胰岛素分泌)显著降低(359±51对比774±91 nmol/min/m²,P = 0.001)。该指标与2小时血糖水平呈负相关(r = -0.71;P < 0.001)。相比之下,IGT在整个180分钟期间的TIS较高(26.2±2.4对比20.0±2.0 nmol/L;P = 0.035)。肝脏胰岛素摄取与OGIS呈线性相关(r = 0.71;P < 0.001),尽管IGT中有肝脏摄取较低的趋势(P = 0.055),但两组之间没有显著差异。口服葡萄糖后血浆GLP - 1和GIP水平升高。这两种肠促胰岛素激素在3小时试验期间的总分泌量在两组之间没有差异。然而,IGT中GLP - 1浓度的30分钟增量低于NGT(P = 0.036)。我们得出结论,在非肥胖IGT受试者中,当相对于NGT控制肥胖因素时,口服葡萄糖后早期胰岛素分泌缺陷是一个关键因素。这种β细胞功能缺陷与早期GLP - 1反应降低有关,并且可能由其引起。
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