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阿托品和胃抑制性多肽对清醒犬肝脏葡萄糖摄取及胰岛素提取的影响。

Effects of atropine and gastric inhibitory polypeptide on hepatic glucose uptake and insulin extraction in conscious dogs.

作者信息

Chap Z, Ishida T, Chou J, Lewis R, Hartley C, Entman M, Field J B

机构信息

Diabetes Research Laboratory, St. Luke's Episcopal Hospital, Division of Endicrinology, Baylor College of Medicine, Houston, Texas, 77030, USA.

出版信息

J Clin Invest. 1985 Sep;76(3):1174-81. doi: 10.1172/JCI112073.

Abstract

Previous studies comparing the effects of oral, intraportal, and peripheral venous administration of glucose in conscious dogs demonstrated a significant increase in hepatic extraction of insulin only after oral glucose, but similar hepatic uptake of glucose after oral and intraportal glucose, which was greater than that after peripheral intravenous glucose infusion. This study evaluated the effect of atropine blockade of the parasympathetic nervous system on the increased fractional hepatic extraction of insulin and the role of gastric inhibitory polypeptide (GIP) on augmented hepatic uptake of oral glucose in conscious dogs with chronically implanted Doppler flow probes on the portal vein and hepatic artery, and catheters in the portal and hepatic veins and carotid artery. Since atropine infusion decreased absorption of glucose, and in order to achieve comparable portal vein levels of glucose and insulin, the dogs receiving atropine were given 1.9 +/- 0.1 g/kg glucose, compared with the control dogs who received 1.1 +/- 0.1 g/kg. The percentage of the glucose load that was absorbed was greater in the dogs not given atropine (80 +/- 4 vs. 44 +/- 7%), but because of the different loads, the absolute amount of glucose absorbed was similar in both groups (20.2 +/- 1.6 vs. 21.7 +/- 4.1 g). Although delayed by atropine, the peak portal vein glucose and insulin concentrations and the amounts presented to the liver were similar in both groups. However, the increased portal vein plasma flow and fractional hepatic extraction of insulin observed after oral glucose was not observed in the dogs infused with atropine. The net hepatic glucose uptake after oral glucose was significantly less at 10, 20, and 45 min in the atropine-treated dogs, and the area under the curve over the 180-min period was 44% less. However, the latter was not statistically significant. Infusion of GIP with peripheral intravenous glucose did not increase hepatic uptake of glucose or the fractional hepatic extraction of insulin compared with peripheral intravenous glucose alone. These results indicate an important role for parasympathetic innervation in the augmented fractional hepatic extraction of insulin, and increased portal vein plasma flow after oral glucose. Although a relationship between the augmented fractional extraction of insulin and the net hepatic glucose uptake may exist, it does not necessarily indicate that the former is required for the latter. Such parasympathetic innervation may be involved in the greater removal of glucose by the liver after oral compared with peripheral glucose administration. The augmented hepatic uptake of glucose and fractional hepatic extraction of insulin after oral glucose doesn not appear to be mediated by gastric inhibitory polypeptide.

摘要

以往在清醒犬身上比较口服、门静脉内和外周静脉注射葡萄糖效果的研究表明,仅在口服葡萄糖后肝脏对胰岛素的摄取显著增加,但口服和门静脉内注射葡萄糖后肝脏对葡萄糖的摄取相似,且大于外周静脉输注葡萄糖后的摄取。本研究评估了用阿托品阻断副交感神经系统对清醒犬肝脏胰岛素摄取分数增加的影响,以及胃抑制多肽(GIP)在增强口服葡萄糖后肝脏对葡萄糖摄取中的作用。这些清醒犬长期植入了门静脉和肝动脉的多普勒血流探头,以及门静脉、肝静脉和颈动脉的导管。由于输注阿托品会降低葡萄糖的吸收,为了使门静脉中的葡萄糖和胰岛素水平相当,接受阿托品的犬给予1.9±0.1 g/kg葡萄糖,而对照组犬给予1.1±0.1 g/kg。未给予阿托品的犬吸收的葡萄糖负荷百分比更高(80±4%对44±7%),但由于负荷不同,两组吸收的葡萄糖绝对量相似(20.2±1.6 g对21.7±4.1 g)。尽管被阿托品延迟,但两组门静脉葡萄糖和胰岛素浓度峰值以及输送到肝脏的量相似。然而,在输注阿托品的犬中未观察到口服葡萄糖后门静脉血浆流量增加和肝脏胰岛素摄取分数增加。在阿托品处理的犬中,口服葡萄糖后10、20和45分钟时肝脏净葡萄糖摄取显著减少,180分钟期间的曲线下面积减少44%。然而,后者无统计学意义。与单独外周静脉输注葡萄糖相比,外周静脉输注葡萄糖时同时输注GIP并未增加肝脏对葡萄糖的摄取或肝脏胰岛素摄取分数。这些结果表明,副交感神经支配在增强肝脏胰岛素摄取分数以及口服葡萄糖后门静脉血浆流量增加中起重要作用。尽管胰岛素摄取分数增加与肝脏净葡萄糖摄取之间可能存在关系,但这不一定表明前者是后者所必需的。这种副交感神经支配可能参与了口服葡萄糖后肝脏比外周葡萄糖给药后对葡萄糖的更大清除。口服葡萄糖后肝脏对葡萄糖摄取增加和肝脏胰岛素摄取分数增加似乎不是由胃抑制多肽介导的。

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