不同胆盐单独或联合十二指肠内应用对人外分泌胰腺及血浆中胆囊收缩素、胰多肽和生长抑素的影响。

R L Riepl, F Fiedler, C Kowalski, J Teufel, P Lehnert
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引用次数: 0

摘要

胆盐是十二指肠内刺激胰腺基底分泌的物质。本研究旨在揭示人胆汁的三种主要胆盐对胰腺分泌的作用是否存在差异,联合使用后是相互增强还是相互抑制。此外,还评估了对胃肠胰肽释放的影响。12名受试者采用胃十二指肠双腔管。等摩尔剂量(0.6 mmol)的牛磺酸胆酸盐(322 mg),牛磺酸去氧胆酸盐(313 mg),以及两种刺激的组合在十二指肠内给予。另外12名受试者服用牛磺胆酸盐(313毫克)代替牛磺胆酸盐。十二指肠抽吸液中测定体积、碳酸氢盐、胰蛋白酶和脂肪酶。用放射免疫法测定血浆样品中的胆囊收缩素、胰多肽和生长抑素。所有胆汁盐及其组合均具有显著的水动力学和促排卵作用。与牛磺胆酸盐和牛磺胆酸盐相比,复合刺激的水动力学反应明显更高。就促排卵反应而言,只有胰蛋白酶的输出量与牛磺酸脱氧胆酸盐相比有显著差异。血浆胆囊收缩素仅在联合刺激后才显著升高。除牛磺胆酸刺激后胰腺多肽和生长抑素显著升高外,其他刺激均显著升高。联合使用增强了单一胆盐的水动力学和促凝作用。因此,胆囊收缩素可能作为促排卵作用的中介。胰腺多肽释放表明胆碱能机制是进一步的介质。正如生长抑素释放所证明的那样,十二指肠内胆汁盐也会触发反调节机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Exocrine pancreatic secretion and plasma levels of cholecystokinin, pancreatic polypeptide, and somatostatin after single and combined intraduodenal application of different bile salts in man.

Bile salts are intraduodenal stimulants of basal pancreatic secretion. This study aims to show whether the three main bile salts of human bile differ in their action on pancreatic secretion, and whether they enhance or inhibit each other after combined use. Furthermore, the effect on gastroenteropancreatic peptide release is evaluated. Twelve subjects were provided with a gastroduodenal double-lumen tube. Equimolar doses (0.6 mmol) of taurocholate (322 mg), taurodeoxycholate (313 mg), and a combination of both stimuli were given intraduodenally. Another 12 subjects received taurochenodeoxycholate (313 mg) instead of taurocholate. Volume, bicarbonate, trypsin, and lipase were determined in duodenal aspirates. Cholecystokinin, pancreatic polypeptide, and somatostatin were measured radioimmunologically in plasma samples. All bile salts and combinations exerted a significant hydrokinetic and ecbolic effect. The hydrokinetic response of the combined stimuli was significantly higher as compared with taurocholate and taurochenodeoxycholate, respectively. As far as concerns the ecbolic response, the difference was significant only for trypsin output as compared with taurochenodeoxycholate. Plasma cholecystokinin rose significantly only after the combined stimuli. Pancreatic polypeptide and somatostatin increased significantly after all stimuli, except pancreatic polypeptide after taurocholate. Combined use enhances the hydrokinetic and ecbolic effects of single bile salts. Cholecystokinin may, hereby, be involved as a mediator of the ecbolic effect. Pancreatic polypeptide release indicates cholinergic mechanisms as further mediators. As demonstrated by somatostatin release, counter-regulatory mechanisms are also triggered by intraduodenal bile salts.

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