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5-羟色胺对人体餐后结肠紧张性和阶段性反应的介导作用

Serotonergic mediation of postprandial colonic tonic and phasic responses in humans.

作者信息

von der Ohe M R, Hanson R B, Camilleri M

机构信息

Gastroenterology Research Unit, Mayo Clinic, Rochester, MN 55905.

出版信息

Gut. 1994 Apr;35(4):536-41. doi: 10.1136/gut.35.4.536.

Abstract

This study examined the hypothesis that 5HT3 mechanisms mediate the postprandial gastrocolonic response in humans. Fasting and postprandial colonic tone and motility were studied in 12 healthy volunteers and the effects of a selective 5HT3 antagonist, ondansetron assessed in a double blind, randomised, placebo controlled fashion. A manometry barostat assembly was positioned in the transverse or descending colon to quantitate contractile activity fasting, after drug infusion and postprandially after a 1000 kcal meal. Fasting colonic tone and motility indices were similar in the placebo and ondansetron groups; ondansetron did not affect fasting motility. The placebo group showed a significant reduction in barostat balloon volume (signifying increased tone) from 232 ml (median, interquartile range (IQR) 179-261) during fasting to 181 ml (median, IQR 128-208) (postprandially) (p = 0.02). In contrast, the ondansetron group did not have a tonic colonic response (median 248 ml (IQR 199-300) fasting to median, 226 ml (IQR 185-290) postprandially) after the meal. Phasic volume events measured by the barostat increased postprandially in both groups. Postprandial motor activity measured by manometry increased significantly in the placebo group, but not in the ondansetron group. In conclusion, a 5HT3 mechanism participates in the physiological contractile responses in the human transverse and descending colon after ingestion of a high energy meal.

摘要

本研究检验了5-羟色胺3(5HT3)机制介导人类餐后胃结肠反应的假说。对12名健康志愿者的空腹及餐后结肠张力和动力进行了研究,并以双盲、随机、安慰剂对照的方式评估了选择性5HT3拮抗剂昂丹司琼的作用。将压力传感器测压组件置于横结肠或降结肠以定量收缩活动,分别于空腹时、输注药物后以及摄入1000千卡餐后进行测量。安慰剂组和昂丹司琼组的空腹结肠张力和动力指数相似;昂丹司琼不影响空腹动力。安慰剂组压力传感器球囊体积(表示张力增加)从空腹时的232毫升(中位数,四分位间距(IQR)179 - 261)显著降至餐后的181毫升(中位数,IQR 128 - 208)(p = 0.02)。相比之下,昂丹司琼组餐后未出现结肠张力反应(空腹时中位数为248毫升(IQR 199 - 300),餐后中位数为226毫升(IQR 185 - 290))。两组中通过压力传感器测量的阶段性体积事件餐后均增加。通过测压法测量的餐后运动活性在安慰剂组显著增加,但在昂丹司琼组未增加。总之,5HT3机制参与了人类摄入高能餐后横结肠和降结肠的生理性收缩反应。

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