首页> 外文期刊>American Journal of Physiology >Inhibition of human pancreatic and biliary output but not intestinal motility by physiological intraileal lipid loads.
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Inhibition of human pancreatic and biliary output but not intestinal motility by physiological intraileal lipid loads.

机译:通过生理性回肠内脂质负荷抑制人胰腺和胆道输出,但不抑制肠道蠕动。

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摘要

Lipid perfusion into the distal ileal lumen at supraphysiological loads inhibits pancreatic exocrine secretion and gastrointestinal motility in humans. In the present study, we sought to determine the effects of physiological postprandial intraileal lipid concentrations on endogenously stimulated pancreaticobiliary secretion, intestinal motility, and release of regulatory mediators. Eight healthy volunteers were intubated with an oroileal multilumen tube for continuous duodenal perfusion of essential amino acids (450 mumol/min), ileal perfusion of graded doses of lipids (0, 50 and 100 mg/min, each dose for 90-120 min), aspiration of duodenal and ileal chyme, and intestinal manometry. Venous blood samples were obtained for measurement of GLP-1 and PYY. Ileal lipid perfusion dose dependently decreased endogenously stimulated trypsin 262 +/- 59 vs. 154 +/- 42 vs. 92 +/- 20 U/min (P 0.84; P < 0.05), whereas the motility index did not. Physiological postprandial ileal lipid concentrations dose dependently inhibited human digestive pancreatic protease and bile acid output, but not intestinal motor activity. Thus physiological postprandial ileal nutrient exposure may be of importance for the termination of digestive secretory responses. Ileocolonic release of GLP-1 and PYY appears to participate in mediating these effects.
机译:脂质在超生理负荷下灌注到回肠远端管腔中会抑制人体胰腺外分泌和胃肠蠕动。在本研究中,我们试图确定生理性餐后餐后回肠内脂质浓度对内源性刺激的胰胆分泌、肠蠕动和调节介质释放的影响。8 名健康志愿者用口回多腔管插管进行十二指肠连续灌注必需氨基酸 (450 mumol/min)、回肠灌注分级剂量的脂质(0、50 和 100 mg/min,每次剂量 90-120 分钟)、十二指肠和回肠食糜抽吸和肠道测压。采集静脉血样以测量 GLP-1 和 PYY。回肠脂质灌注剂量依赖性地降低内源性刺激的胰蛋白酶 [262 +/- 59 vs. 154 +/- 42 vs. 92 +/- 20 U/min (P 0.84;P<0.05),而运动指数则没有。生理性餐后回肠脂质浓度剂量依赖性抑制人消化胰腺蛋白酶和胆汁酸输出,但不抑制肠道运动活动。因此,生理性餐后回肠营养物质暴露对于终止消化分泌反应可能很重要。GLP-1 和 PYY 的回结肠释放似乎参与介导这些作用。

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