阿片类药物引起的胃排空延迟：人类的一种外周机制。

Opioid-induced delay in gastric emptying: a peripheral mechanism in humans.

作者信息

Murphy D B, Sutton J A, Prescott L F, Murphy M B

机构信息

Cork University Hospital, Wilton, Cork City, Ireland.

出版信息

Anesthesiology. 1997 Oct;87(4):765-70. doi: 10.1097/00000542-199710000-00008.

DOI:10.1097/00000542-199710000-00008

PMID:9357876

Abstract

BACKGROUND

Opioids delay gastric emptying, which in turn may increase the risk of vomiting and pulmonary aspiration. Naloxone reverses this opiate action on gastric emptying, but it is not known whether this effect in humans is mediated by central or peripheral opiate antagonism. The importance of peripheral opioid receptor antagonism in modulating opioid-induced delay in gastric emptying was evaluated using methylnaltrexone, a quaternary derivative of the opiate antagonist naltrexone, which does not cross the blood-brain barrier.

METHODS

In a randomized, double-blind, crossover placebo-controlled study, 11 healthy volunteers were given either placebo (saline), 0.09 mg/kg morphine, or 0.09 mg/kg morphine plus 0.3 mg/kg methylnaltrexone on three separate occasions before ingesting 500 ml deionized water. The rate of gastric emptying was measured by two methods: a noninvasive epigastric bioimpedance technique and the acetaminophen absorption test.

RESULTS

The epigastric bioimpedance technique was sufficiently sensitive to detect opioid-induced changes in the rate of gastric emptying. The mean +/- SD time taken for the gastric volume to decrease to 50% (t0.5) after placebo was 5.5 +/- 2.1 min. Morphine prolonged gastric emptying to (t0.5) of 21 +/- 9.0 min (P < 0.03). Methylnaltrexone given concomitantly with morphine reversed the morphine-induced delay in gastric emptying to a t0.5 of 7.4 +/- 3.0 (P < 0.04). Maximum concentrations and area under the concentration curve from 0 to 90 min of serum acetaminophen concentrations after morphine were significantly different from placebo and morphine administered concomitantly with methylnaltrexone (P < 0.05). No difference in maximum concentration or area under the concentration curve from 0 to 90 min was noted between placebo and methylnaltrexone coadministered with morphine.

CONCLUSIONS

The attenuation of morphine-induced delay in gastric emptying by methylnaltrexone suggests that the opioid effect is mediated outside the central nervous system. Methylnaltrexone may have the potential to decrease the side effects of opioid medications, which are mediated peripherally, while maintaining the central analgesia effect of the opioid.

摘要

背景

阿片类药物会延迟胃排空，进而可能增加呕吐和肺误吸的风险。纳洛酮可逆转阿片类药物对胃排空的这种作用，但尚不清楚人类的这种效应是由中枢还是外周阿片类药物拮抗作用介导的。使用甲基纳曲酮评估外周阿片受体拮抗作用在调节阿片类药物引起的胃排空延迟中的重要性，甲基纳曲酮是阿片类拮抗剂纳曲酮的季铵衍生物，不能穿过血脑屏障。

方法

在一项随机、双盲、交叉安慰剂对照研究中，11名健康志愿者在摄入500毫升去离子水之前，分三次分别给予安慰剂（生理盐水）、0.09毫克/千克吗啡或0.09毫克/千克吗啡加0.3毫克/千克甲基纳曲酮。通过两种方法测量胃排空率：无创上腹部生物阻抗技术和对乙酰氨基酚吸收试验。

结果

上腹部生物阻抗技术对检测阿片类药物引起的胃排空率变化足够敏感。安慰剂组胃容积降至50%（t0.5）的平均±标准差时间为5.5±2.1分钟。吗啡使胃排空延长至（t0.5）21±9.0分钟（P<0.03）。与吗啡同时给予甲基纳曲酮可将吗啡引起的胃排空延迟逆转至t0.5为7.4±3.0（P<0.04）。吗啡后血清对乙酰氨基酚浓度在0至90分钟的最大浓度和浓度曲线下面积与安慰剂以及与甲基纳曲酮同时给予吗啡时显著不同（P<0.05）。在安慰剂与与吗啡共同给予甲基纳曲酮之间，0至90分钟的最大浓度或浓度曲线下面积未发现差异。