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吗啡、芬太尼、曲马多及其联合应用对吗啡耐受小鼠的镇痛作用。

Antinociceptive effects of morphine, fentanyl, tramadol and their combination, in morphine-tolerant mice.

机构信息

Department of Anesthesiology, Hospital del Mar. Physiopatholology and Pain Management Research Group, Institut Municipal d'Investigació Mèdica (IMIM), Universitat Autònoma de Barcelona, Spain.

出版信息

Pharmacol Biochem Behav. 2010 Dec;97(2):363-9. doi: 10.1016/j.pbb.2010.09.005. Epub 2010 Sep 16.

Abstract

The development of morphine-tolerance after chronic administration, reduces analgesic efficacy and is a significant clinical problem in some patients; may be managed clinically by increasing the doses of morphine and/or the administration of a second mu-opioid agonist. In morphine-tolerant mice, we investigated the presence of an interaction when two opioids are administered simultaneously. We determined the antinociceptive effects of morphine (M), fentanyl (FEN), and tramadol (TRM) individually and combined in a 1:1 proportion, based on their potency. Nociceptive thresholds were evaluated in CD1 mice using the hot plate test. Morphine tolerance was induced by the subcutaneous implantation of a 75mg morphine pellet, whereas control animals received a placebo pellet; the experiments were performed three days later. In both (placebo and morphine pellets), dose-response curves for M, FEN and TRM, individually and combined were obtained, and the doses that produced 50% inhibition (ED(50)) were determined. Sustained exposure to morphine induced a significant decrease in antinociceptive potency to acute M or FEN administration (tolerance), which was of a lesser magnitude after acute TRM; in these experiments the analysis of the interaction between chronic morphine and each opioid, demonstrated functional antagonism. The simultaneous administration of two opioids in morphine-tolerant mice, demonstrated antagonism for the M:FEN combination, whereas the effects of TRM combined with M or FEN, remained additive. The results suggest that during morphine-tolerance, TRM could be a useful drug to induce effective analgesia when combined with FEN or M.

摘要

在慢性给予吗啡后,会产生吗啡耐受,从而降低镇痛效果,这在一些患者中是一个重大的临床问题;临床上可以通过增加吗啡剂量和/或给予第二种μ阿片激动剂来管理。在吗啡耐受的小鼠中,我们研究了当同时给予两种阿片类药物时是否存在相互作用。我们根据它们的效力,单独和联合使用 1:1 比例的吗啡(M)、芬太尼(FEN)和曲马多(TRM),确定其镇痛作用。使用热板试验在 CD1 小鼠中评估镇痛阈值。通过皮下植入 75mg 吗啡丸来诱导吗啡耐受,而对照动物则接受安慰剂丸;实验在三天后进行。在(安慰剂和吗啡丸)中,单独和联合使用 M、FEN 和 TRM 获得了剂量反应曲线,并确定了产生 50%抑制(ED(50))的剂量。持续暴露于吗啡可导致急性 M 或 FEN 给药的镇痛效力显著降低(耐受),而急性 TRM 后则降低程度较小;在这些实验中,慢性吗啡和每种阿片类药物之间相互作用的分析表明存在功能拮抗。在吗啡耐受的小鼠中同时给予两种阿片类药物,M:FEN 联合显示拮抗作用,而 TRM 与 M 或 FEN 联合的效果仍然是相加的。结果表明,在吗啡耐受期间,当与 FEN 或 M 联合使用时,TRM 可能是一种有用的药物,可以诱导有效的镇痛。

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