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首页> 外文期刊>Metabolic syndrome and related disorders >Mixed Meal and Intravenous L-Arginine Tests Both Stimulate Incretin Release Across Glucose Tolerance in Man: Lack of Correlation with Cell Function
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Mixed Meal and Intravenous L-Arginine Tests Both Stimulate Incretin Release Across Glucose Tolerance in Man: Lack of Correlation with Cell Function

机译:混合膳食和静脉注射L-精氨酸试验刺激胰岛素释放在人类中的葡萄糖耐受性:与细胞功能缺乏相关性

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Background: The aims of this study were to 1. define the responses of glucagon-like peptide-1 (GLP-1), glucose-dependent insulinotropic polypeptide (GIP), glucagon, and peptide YY (PYY) to an oral meal and to intravenous L-arginine; and 2. examine correlation of enteroendocrine hormones with insulin secretion. We hypothesized a relationship between circulating incretin concentrations and insulin secretion. Methods: Subjects with normal glucose tolerance (NGT, n=23), prediabetes (PDM, n=17), or with type 2 diabetes (T2DM, n=22) were studied twice, following a mixed test meal (470kCal) (mixed meal tolerance test [MMTT]) or intravenous L-arginine (arginine maximal stimulation test [AST], 5g). GLP-1 (total and active), PYY, GIP, glucagon, and cell function were measured before and following each stimulus. Results: Baseline enteroendocrine hormones differed across the glucose tolerance (GT) spectrum, T2DM generally NGT and PDM. In response to MMTT, total and active GLP-1, GIP, glucagon, and PYY increased in all populations. The incremental area-under-the-curve (0-120min) of analytes like total GLP-1 were often higher in T2DM compared with NGT and PDM (35-51%; P0.05). At baseline glucose, L-arginine increased total and active GLP-1 and glucagon concentrations in all GT populations (all P0.05). As expected, the MMTT and AST provoked differential glucose, insulin, and C-peptide responses across GT populations. Baseline or stimulated enteroendocrine hormone concentrations did not consistently correlate with either measure of cell function. Conclusions/interpretation: Both MMTT and AST resulted in insulin and enteroendocrine hormone responses across GT populations without consistent correlation between release of incretins and insulin, which is in line with other published research. If a defect is in the enteroendocrine/ cell axis, it is probably reduced response to rather than diminished secretion of enteroendocrine hormones.
机译:背景:本研究的目的是1。定义胰高血糖素样肽-1(GLP-1),葡萄糖依赖性胰岛素多肽(GIP),胰高血糖素和肽YY(PYY)到口服膳食的反应。静脉注射L-精氨酸; 2.检查肠内激素与胰岛素分泌的相关性。我们假设循环血管素浓度与胰岛素分泌之间的关系。方法:在混合试验膳食(470kcal)之后,研究了具有正常葡萄糖耐量(NGT,N = 23),前奶油(PDM,N = 17)或型糖尿病(T2DM,N = 22)的受试者进行两次(COND膳食耐受性测试[MMTT])或静脉注射L-精氨酸(精氨酸最大刺激测试[AST],5G)。在每次刺激之前和之后测量GLP-1(总和活性),PYY,GIP,胰高血糖素和细胞功能。结果:基线进肠癌激素在葡萄糖耐量(GT)光谱中不同,T2DM通常为GT; NGT和PDM。响应于MMTT,总和活跃的GLP-1,GIP,Glucagon和Pyy在所有人口中增加。与NGT和PDM(35-51%; P <0.05)相比,T2DM的分析物的增量区域曲线(0-120min)通常较高。在基线葡萄糖,L-精氨酸在所有GT种群中增加总和活性GLP-1和胰高血糖素浓度(所有P <0.05)。正如预期的那样,MMTT和AST激发差异血糖,胰岛素和C-肽反应在GT种群上。基线或刺激的肠内内分泌激素浓度与细胞功能的任一测量不始终相关。结论/解释:MMTT和AST均导致胰岛素和肠内内分泌激素响应GT种群,无需释放Incetins和胰岛素之间的一致相关性,这与其他公开的研究一致。如果缺陷在进肠内分/细胞轴上,则可能减少对进肠内分激素的分泌而不是减少的反应。

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