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纳洛酮肠溶制剂对服用可待因的志愿者肠道转运的影响。

Effect of an enteric-release formulation of naloxone on intestinal transit in volunteers taking codeine.

作者信息

Hawkes N D, Richardson C, Evans B K, Rhodes J, Lewis S J, Thomas G A

机构信息

Department of Gastroenterology, University Hospital of Wales, Cardiff, UK.

出版信息

Aliment Pharmacol Ther. 2001 May;15(5):625-30. doi: 10.1046/j.1365-2036.2001.00970.x.

Abstract

INTRODUCTION

Constipation is a common side-effect of opioid therapy; in addition to their analgesic effect, opioids reduce intestinal secretion and motility with an increase in whole-gut transit time. Naloxone, a specific opioid antagonist, reverses these effects but may also cause symptoms of opioid withdrawal in patients on long-term therapy.

AIM

To use an enteric-release formulation, designed to produce a topical effect in the gut, with minimum systemic effects.

METHODS

Naloxone 10 mg b.d. and codeine 30 mg b.d. were used with identical placebo capsules in four sets of studies; 12 male volunteers were given the drugs alone and in combination, with a control study involving double placebo, during each of four study periods. Whole-gut transit time was calculated and compared for each treatment period.

RESULTS

Naloxone, both alone and with codeine, significantly shortened the mean whole-gut transit time compared with the control period, respectively, from 53.1 to 42.1 h (P=0.005) and to 40.7 h (P=0.024). Urgency to defecate was reported by two volunteers on naloxone alone and by three on combination therapy.

CONCLUSIONS

The results show that the naloxone formulation counteracts the effect of codeine on intestinal transit, suggesting that it may have useful clinical applications.

摘要

引言

便秘是阿片类药物治疗常见的副作用;除了止痛作用外,阿片类药物还会减少肠道分泌和蠕动,增加全肠道转运时间。纳洛酮是一种特异性阿片类拮抗剂,可逆转这些作用,但对于长期接受治疗的患者,它也可能引发阿片类药物戒断症状。

目的

使用一种肠溶制剂,该制剂旨在在肠道产生局部作用,同时使全身作用最小化。

方法

在四组研究中,使用10毫克每日两次的纳洛酮和30毫克每日两次的可待因,并搭配相同的安慰剂胶囊;在四个研究阶段的每个阶段,12名男性志愿者单独服用药物以及联合服用药物,并进行一项涉及双安慰剂的对照研究。计算并比较每个治疗阶段的全肠道转运时间。

结果

与对照阶段相比,单独使用纳洛酮以及纳洛酮与可待因联合使用时,平均全肠道转运时间均显著缩短,分别从53.1小时缩短至42.1小时(P = 0.005)以及缩短至40.7小时(P = 0.024)。单独使用纳洛酮时有两名志愿者、联合治疗时有三名志愿者报告有排便紧迫感。

结论

结果表明,纳洛酮制剂可抵消可待因对肠道转运的影响,提示其可能具有有益的临床应用价值。

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