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脑啡肽酶抑制剂阿西托芬对实验性腹泻和急性腹泻的作用。

Effects of acetorphan, an enkephalinase inhibitor, on experimental and acute diarrhoea.

作者信息

Baumer P, Danquechin Dorval E, Bertrand J, Vetel J M, Schwartz J C, Lecomte J M

机构信息

Laboratoire Bioprojet, Marnes la Coquette, France.

出版信息

Gut. 1992 Jun;33(6):753-8. doi: 10.1136/gut.33.6.753.

Abstract

Acetorphan is an orally active inhibitor of enkephalinase (EC 3.4.24.11) with antidiarrhoeal activity in rodents apparently through protection of endogenous enkephalins and a purely antisecretory mechanism. Its antidiarrhoeal activity in man was assessed in an experimental model of cathartic induced secretory diarrhoea as well as in acute diarrhoea of presumed infectious origin. In six healthy volunteers receiving castor oil and pretreated with acetorphan or placebo in a crossover controlled trial, the drug significantly decreased the number and weight of stools passed during 24 hours. About 200 outpatients with severe acute diarrhoea (more than five stools per day) were included in a randomised double blind study of acetorphan against placebo. The significant antidiarrhoeal activity of acetorphan was established using a variety of criteria: (i) the duration of both diarrhoea and treatment were diminished; (ii) no acetorphan treated patient withdrew from the study whereas five dropped out because of worsening in the placebo group; (iii) the frequency of symptoms associated with diarrhoea--for example, abdominal pain or distension, nausea and anorexia--remaining after two weeks was nearly halved; (iv) using visual analogue scales acetorphan treatment was found more effective than placebo by both investigators and patients. There was statistically no significant difference between acetorphan and placebo in respect of side effects, particularly constipation, which often accompanies the antidiarrhoeal activity of mu opioid receptor agonists this difference is attributable to the lack of antipropulsive activity of acetorphan in man. The efficacy and tolerance of acetorphan suggest that enkephalinase inhibition may represent a novel therapeutic approach for the symptomatic management of acute secretory diarrhoea without impairing intestinal transit.

摘要

醋托芬是一种脑啡肽酶(EC 3.4.24.11)的口服活性抑制剂,在啮齿动物中具有止泻活性,显然是通过保护内源性脑啡肽以及一种纯粹的抗分泌机制实现的。在一种由泻药引起的分泌性腹泻的实验模型以及推测为感染性来源的急性腹泻中,对其在人体中的止泻活性进行了评估。在一项交叉对照试验中,六名接受蓖麻油并预先用醋托芬或安慰剂治疗的健康志愿者中,该药物显著减少了24小时内排出的粪便数量和重量。约200名患有严重急性腹泻(每天超过五次排便)的门诊患者被纳入一项醋托芬与安慰剂对比的随机双盲研究。使用多种标准确定了醋托芬具有显著的止泻活性:(i)腹泻持续时间和治疗时间均缩短;(ii)没有接受醋托芬治疗的患者退出研究,而安慰剂组有五名患者因病情恶化退出;(iii)两周后与腹泻相关的症状——例如腹痛或腹胀、恶心和厌食——的发生率几乎减半;(iv)使用视觉模拟量表,研究人员和患者均发现醋托芬治疗比安慰剂更有效。在副作用方面,醋托芬和安慰剂在统计学上没有显著差异,特别是便秘,而便秘常常伴随μ阿片受体激动剂的止泻活性,这种差异归因于醋托芬在人体中缺乏抗推进活性。醋托芬的疗效和耐受性表明,抑制脑啡肽酶可能代表一种治疗急性分泌性腹泻症状的新方法,且不会损害肠道运输功能。

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