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十二指肠内给予盐酸和葡萄糖对循环中免疫反应性促胰液素和胰岛素浓度的影响。

Effects of intraduodenal administration of HCl and glucose on circulating immunoreactive secretin and insulin concentrations.

作者信息

Boden G, Essa N, Owen O E, Reichle F A

出版信息

J Clin Invest. 1974 Apr;53(4):1185-93. doi: 10.1172/JCI107657.

Abstract

A new radioimmunoassay for secretin was used to investigate (a) serum secretin responses to intraduodenally infused HCl and glucose, (b) the metabolic half-life and the volume of distribution of exogenous secretin and (c) the effect of endogenously released secretin on insulin secretion in 25 anesthetized dogs. Portal and femoral venous blood samples were taken simultaneously before, during, and after intraduodenal infusion of HCl (21 meq/30 min) and glucose (131 ml/30 min). Control experiments were performed with intraduodenal infusion of saline. Mean portal venous immunoreactive secretin concentration of six dogs rose from 313 muU/ml before to 1,060 muU/ml 10 min after initiation of the intestinal acidification (P < 0.005). Femoral venous immunoreactive secretin concentration rose from 220 muU/ml before to 567 muU/ml 15 min after intestinal acidification (P < 0.01). Secretin concentrations remained elevated during the remainder of the infusion. In the same six dogs mean portal venous immunoreactive insulin concentration rose from 38 muU/ml before to 62 muU/ml at the end of the infusion (P < 0.05). Peripheral immunoreactive insulin, glucose, and free fatty acid concentrations, however, did not change significantly. Pancreatic exocrine function was studied in four dogs. The rise in secretin concentration was followed promptly by a highly significant increase in exocrine pancreatic flow rate and bicarbonate secretion, indicating biological activity of the circulating immunoreactive secretin. The effect of intraduodenal infusion of glucose on immunoreactive secretin concentration was studied in 12 dogs. Glucose in concentrations ranging from 2.5% to 10% had no detectable influence on portal or peripheral secretin concentration. Infusion of 50% glucose caused a slight decline in secretin concentration. The metabolic clearance rate, half-life of disappearance, and volume of distribution of exogenous secretin was studied in three dogs by the constant infusion technic. The metabolic clearance rate was 730+/-34 ml/min, volume of distribution was 17.4+/-0.8% of body weight, and the half-life of disappearance was 2.8+/-0.1 min. It could be calculated that 1.38 U/kg-h(-1) of endogenous secretin was released into the peripheral circulation during the steady state period of the HCl infusion experiments. The data indicated that immunoreactive secretin was released rapidly after intestinal acidification, continued to be secreted throughout the duration of HCl infusion, and was promptly distributed in the extracellular compartment. Furthermore, they suggested that endogenously released secretin could stimulate insulin secretion. The HCl-mediated insulinogenic effect of immunoreactive secretin, however, was too weak to influence peripheral immunoreactive insulin, glucose, and free fatty acid concentrations. The failure of intraduodenal glucose to stimulate secretin release suggests that secretin is not the insulin-stimulatory factor released from the gastrointestinal tract in response to glucose.

摘要

采用一种新的促胰液素放射免疫分析法,对25只麻醉犬进行了以下研究:(a) 十二指肠内注入盐酸和葡萄糖后血清促胰液素的反应;(b) 外源性促胰液素的代谢半衰期和分布容积;(c) 内源性释放的促胰液素对胰岛素分泌的影响。在十二指肠内注入盐酸(21毫当量/30分钟)和葡萄糖(131毫升/30分钟)之前、期间和之后,同时采集门静脉和股静脉血样。用十二指肠内注入生理盐水进行对照实验。6只犬的门静脉平均免疫反应性促胰液素浓度从酸化前的313微单位/毫升升至酸化开始后10分钟的1060微单位/毫升(P<0.005)。股静脉免疫反应性促胰液素浓度从酸化前的220微单位/毫升升至酸化后15分钟的567微单位/毫升(P<0.01)。在输注的其余时间里,促胰液素浓度一直升高。在同6只犬中门静脉平均免疫反应性胰岛素浓度从输注前的38微单位/毫升升至输注结束时的62微单位/毫升(P<0.05)。然而,外周免疫反应性胰岛素、葡萄糖和游离脂肪酸浓度没有明显变化。在4只犬中研究了胰腺外分泌功能。促胰液素浓度升高后,胰腺外分泌流速和碳酸氢盐分泌立即显著增加,表明循环中的免疫反应性促胰液素具有生物活性。在12只犬中研究了十二指肠内注入葡萄糖对免疫反应性促胰液素浓度的影响。浓度范围为2.5%至10%的葡萄糖对门静脉或外周促胰液素浓度没有可检测到的影响。注入5G%葡萄糖导致促胰液素浓度略有下降。通过持续输注技术在3只犬中研究了外源性促胰液素的代谢清除率、消失半衰期和分布容积。代谢清除率为730±34毫升/分钟,分布容积为体重的17.4±0.8%,消失半衰期为2.8±0.1分钟。可以计算出,在盐酸输注实验的稳态期,每千克每小时有1.38单位的内源性促胰液素释放到外周循环中。数据表明,肠道酸化后免疫反应性促胰液素迅速释放,在盐酸输注期间持续分泌,并迅速分布在细胞外间隙。此外,数据还表明内源性释放的促胰液素可以刺激胰岛素分泌。然而,免疫反应性促胰液素由盐酸介导产生的致胰岛素分泌作用太弱,无法影响外周免疫反应性胰岛素、葡萄糖和游离脂肪酸浓度。十二指肠内葡萄糖未能刺激促胰液素释放,这表明促胰液素不是胃肠道因葡萄糖而释放的胰岛素刺激因子。

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