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口服葡萄糖后肝脏胰岛素清除率的降低并非由胰高血糖素样肽1或胃抑制性多肽介导,此现象存在于人类中。

Reduction of hepatic insulin clearance after oral glucose ingestion is not mediated by glucagon-like peptide 1 or gastric inhibitory polypeptide in humans.

作者信息

Meier Juris J, Holst Jens J, Schmidt Wolfgang E, Nauck Michael A

机构信息

Department of Medicine I, St. Josef-Hospital, Ruhr-Univ. of Bochum, Gudrunstr. 56, 44791 Bochum, Germany.

出版信息

Am J Physiol Endocrinol Metab. 2007 Sep;293(3):E849-56. doi: 10.1152/ajpendo.00289.2007. Epub 2007 Jul 3.

DOI:10.1152/ajpendo.00289.2007
PMID:17609256
Abstract

Changes in hepatic insulin clearance can occur after oral glucose or meal ingestion. This has been attributed to the secretion and action of gastric inhibitory polypeptide (GIP) and glucagon-like peptide (GLP)-1. Given the recent availability of drugs based on incretin hormones, such clearance effects may be important for the future treatment of type 2 diabetes. Therefore, we determined insulin clearance in response to endogenously secreted and exogenously administered GIP and GLP-1. Insulin clearance was estimated from the molar C-peptide-to-insulin ratio calculated at basal conditions and from the respective areas under the curve after glucose, GIP, or GLP-1 administration. Oral glucose administration led to an approximately 60% reduction in the C-peptide-to-insulin ratio (P < 0.0001), whereas intravenous glucose administration had no effect (P = 0.09). The endogenous secretion of GIP or GLP-1 was unrelated to the changes in insulin clearance. The C-peptide-to-insulin ratio was unchanged after the intravenous administration of GIP or GLP-1 in the fasting state (P = 0.27 and P = 0.35, respectively). Likewise, infusing GLP-1 during a meal course did not alter insulin clearance (P = 0.87). An inverse nonlinear relationship was found between the C-peptide-to-insulin ratio and the integrated insulin levels after oral and during intravenous glucose administration. Insulin clearance is reduced by oral but not by intravenous glucose administration. Neither GIP nor GLP-1 has significant effects on insulin extraction. An inverse relationship between insulin concentrations and insulin clearance suggests that the secretion of insulin itself determines the rate of hepatic insulin clearance.

摘要

口服葡萄糖或进食后,肝脏胰岛素清除率会发生变化。这归因于胃抑制性多肽(GIP)和胰高血糖素样肽(GLP)-1的分泌及作用。鉴于近期基于肠促胰岛素激素的药物已可获得,这种清除效应可能对2型糖尿病的未来治疗很重要。因此,我们测定了内源性分泌和外源性给予GIP及GLP-1后的胰岛素清除率。胰岛素清除率通过基础状态下计算的摩尔C肽与胰岛素比值以及给予葡萄糖、GIP或GLP-1后各自的曲线下面积来估算。口服葡萄糖导致C肽与胰岛素比值降低约60%(P < 0.0001),而静脉注射葡萄糖则无影响(P = 0.09)。GIP或GLP-1的内源性分泌与胰岛素清除率的变化无关。在空腹状态下静脉注射GIP或GLP-1后,C肽与胰岛素比值未改变(分别为P = 0.27和P = 0.35)。同样,在进餐过程中输注GLP-1也未改变胰岛素清除率(P = 0.87)。口服和静脉注射葡萄糖期间,C肽与胰岛素比值和胰岛素整合水平之间呈反向非线性关系。口服葡萄糖可降低胰岛素清除率,而静脉注射则不然。GIP和GLP-1对胰岛素提取均无显著影响。胰岛素浓度与胰岛素清除率之间的反向关系表明,胰岛素自身的分泌决定了肝脏胰岛素清除率。

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