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胃泌素对人体基础及葡萄糖刺激的胰岛素分泌的影响。

The effect of gastrin on basal- and glucose-stimulated insulin secretion in man.

作者信息

Rehfeld J F, Stadil F

出版信息

J Clin Invest. 1973 Jun;52(6):1415-26. doi: 10.1172/JCI107315.

Abstract

The effect of gastrin on basal- and glucose-stimulated insulin secretion was studied in 32 normal, young subjects. The concentration of gastrin and insulin in serum was measured radioimmunochemically. Maximal physiologic limit for the concentration of gastrin in serum was of the order of 160 pmol per liter as observed during a protein-rich meal. Oral ingestion of 50 g glucose produced a small gastrin response from 28+/-3 to 39+/-5 pmol per liter (mean +/-SEM, P < 0.01). Intravenous injection or prolonged infusion of gastrin increased the concentration of insulin in peripheral venous blood to a maximum within 2 min followed by a decline to basal levels after a further 10 min. The minimum dose required to induce a significant insulin response (31.2 ng gastrin per kg) increased the gastrin level in serum above the physiologic range. Maximum effect was obtained with 500 ng gastrin per kg. When 15.6 ng (7.1 pmol) gastrin per kg body weight and 25 g glucose were injected simultaneously, the glucose-induced insulin response was potentiated (from 2.32+/-0.33 to 4.33+/-0.98 nmol per liter per 20 min, P < 0.02), even though gastrin concentrations only increased to 71.2+/-6.6 pmol per liter. No effect, however, was noted on glucose disposal. 15.6 ng gastrin per kg given i.v. 30 min before an i.v. glucose tolerance test was without significant effect on the insulin response. The results indicate that gastrin can stimulate a rapid and short-lived release of insulin. In physiologic concentrations gastrin potentiates the glucose-stimulated insulin secretion and is without effect on basal insulin secretion. A small release of gastrin during oral glucose ingestion may to a limited extent contribute to the nonglycemic insulin secretion. During protein ingestion, gastrin probably stimulates insulin secretion significantly.

摘要

在32名正常年轻受试者中研究了胃泌素对基础及葡萄糖刺激的胰岛素分泌的影响。采用放射免疫化学法测定血清中胃泌素和胰岛素的浓度。在富含蛋白质的餐食期间观察到血清中胃泌素浓度的最大生理极限约为每升160皮摩尔。口服50克葡萄糖可使胃泌素反应轻微增加,从每升28±3皮摩尔增至39±5皮摩尔(均值±标准误,P<0.01)。静脉注射或长时间输注胃泌素可使外周静脉血中胰岛素浓度在2分钟内升至最高,随后再过10分钟降至基础水平。诱导显著胰岛素反应所需的最小剂量(每千克体重31.2纳克胃泌素)会使血清中胃泌素水平升高至生理范围之上。每千克体重500纳克胃泌素可获得最大效应。当每千克体重同时注射15.6纳克(7.1皮摩尔)胃泌素和25克葡萄糖时,葡萄糖诱导的胰岛素反应增强(从每20分钟每升2.32±0.33纳摩尔增至4.33±0.98纳摩尔,P<0.02),尽管胃泌素浓度仅增至每升71.2±6.6皮摩尔。然而,未观察到对葡萄糖处置有影响。在静脉葡萄糖耐量试验前30分钟静脉给予每千克体重15.6纳克胃泌素对胰岛素反应无显著影响。结果表明胃泌素可刺激胰岛素快速且短暂的释放。在生理浓度下,胃泌素可增强葡萄糖刺激的胰岛素分泌,而对基础胰岛素分泌无影响。口服葡萄糖期间胃泌素的少量释放可能在一定程度上促成非血糖性胰岛素分泌。在摄入蛋白质期间,胃泌素可能显著刺激胰岛素分泌。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f020/302406/6dcdf8b1d0e6/jcinvest00182-0128-a.jpg

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