人体摄入葡萄糖后胃排空及肠促胰岛素激素的释放

Gastric emptying and release of incretin hormones after glucose ingestion in humans.

作者信息

Schirra J, Katschinski M, Weidmann C, Schäfer T, Wank U, Arnold R, Göke B

机构信息

Clinical Research Unit of Gastrointestinal Endocrinology, Philipps-University, Marburg, Germany.

出版信息

J Clin Invest. 1996 Jan 1;97(1):92-103. doi: 10.1172/JCI118411.

DOI:10.1172/JCI118411

PMID:8550855

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC507066/

Abstract

This study investigated in eight healthy male volunteers (a) the gastric emptying pattern of 50 and 100 grams of glucose; (b) its relation to the phase of interdigestive motility (phase I or II) existing when glucose was ingested; and (c) the interplay between gastric emptying or duodenal perfusion of glucose (1.1 and 2.2 kcal/min; identical total glucose loads as orally given) and release of glucose-dependent insulinotropic peptide (GIP), glucagon-like peptide-1(7-36)amide (GLP-1), C-peptide, insulin, and plasma glucose. The phase of interdigestive motility existing at the time of glucose ingestion did not affect gastric emptying or any metabolic parameter. Gastric emptying of glucose displayed a power exponential pattern with a short initial lag period. Duodenal delivery of glucose was not constant but exponentially declined over time. Increasing the glucose load reduced the rate of gastric emptying by 27.5% (P < 0.05) but increased the fractional duodenal delivery of glucose. Both glucose loads induced a fed motor pattern which was terminated by an antral phase III when approximately 95% of the meal had emptied. Plasma GLP-1 rose from basal levels of approximately 1 pmol/liter of peaks of 3.2 +/- 0.6 pmol/liter with 50 grams of glucose and of 7.2 +/- 1.6 pmol/liter with 100 grams of glucose. These peaks occurred 20 min after glucose intake irrespective of the load. A duodenal delivery of glucose exceeding 1.4 kcal/min was required to maintain GLP-1 release in contrast to ongoing GIP release with negligibly low emptying of glucose. Oral administration of glucose yielded higher GLP-1 and insulin releases but an equal GIP release compared with the isocaloric duodenal perfusion. We conclude that (a) gastric emptying of glucose displays a power exponential pattern with duodenal delivery exponentially declining over time and (b) a threshold rate of gastric emptying of glucose must be exceeded to release GLP-1, whereas GIP release is not controlled by gastric emptying.

摘要

本研究在8名健康男性志愿者中进行，调查了：(a) 50克和100克葡萄糖的胃排空模式；(b) 其与摄入葡萄糖时存在的消化间期运动相（I相或II相）的关系；以及(c) 葡萄糖胃排空或十二指肠灌注（1.1和2.2千卡/分钟；与口服给予的葡萄糖总负荷相同）与葡萄糖依赖性促胰岛素多肽（GIP）、胰高血糖素样肽-1(7-36)酰胺（GLP-1）、C肽、胰岛素和血浆葡萄糖释放之间的相互作用。摄入葡萄糖时存在的消化间期运动相不影响胃排空或任何代谢参数。葡萄糖的胃排空呈现幂指数模式，初始延迟期较短。十二指肠葡萄糖输送并不恒定，而是随时间呈指数下降。增加葡萄糖负荷使胃排空速率降低27.5%（P<0.05），但增加了十二指肠葡萄糖的分数输送。两种葡萄糖负荷均诱导出进食运动模式，当约95%的餐食排空时，该模式由胃窦III相终止。血浆GLP-1从基础水平约1皮摩尔/升升至峰值，50克葡萄糖时为3.2±0.6皮摩尔/升，100克葡萄糖时为7.2±1.6皮摩尔/升。无论负荷如何，这些峰值均在葡萄糖摄入后20分钟出现。与葡萄糖排空极低时持续释放GIP相反，维持GLP-1释放需要十二指肠葡萄糖输送超过1.4千卡/分钟。与等热量十二指肠灌注相比，口服葡萄糖产生更高的GLP-1和胰岛素释放，但GIP释放相等。我们得出结论：(a) 葡萄糖的胃排空呈现幂指数模式，十二指肠输送随时间呈指数下降；(b) 必须超过葡萄糖胃排空的阈值速率才能释放GLP-1，而GIP释放不受胃排空控制。

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