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阿片肽能系统在抗抑郁化合物的抗伤害感受作用机制中的参与。

The involvement of the opioidergic system in the antinociceptive mechanism of action of antidepressant compounds.

作者信息

Gray A M, Spencer P S, Sewell R D

机构信息

Division of Pharmacology, The Welsh School of Pharmacy, UWC, Cardiff, Wales.

出版信息

Br J Pharmacol. 1998 Jun;124(4):669-74. doi: 10.1038/sj.bjp.0701882.

Abstract
  1. Debate exists as to the nature of antidepressant-induced antinociception. It is unclear whether antidepressants are inherently antinociceptive, are able to potentiate opioid antinociception or both. We have used the acetic acid induced abdominal constriction assay in mice to investigate antidepressant-induced antinociception. 2. All the antidepressants tested (s.c.) produced dose-dependent protection against acetic acid-induced abdominal constriction. Similarly, morphine and aspirin were also effective antinociceptive agents in this nociceptive assay. 3. Opioid antagonists, naloxone (0.5 mg kg(-1), s.c.) and naltrindole (1 mg kg(-1), s.c.), shifted the dose-response relationships to the right for each of the antidepressant agents (dothiepin, amitriptyline, sibutramine, (+)-oxaprotiline and paroxetine). In this context the naloxone dose-ratios were 1.95, 3.90, 2.32, 4.50 and 2.65, with naltrindole dose-ratios of 4.36, 17.00, 4.28, 11.48 and 2.65 were obtained, respectively. Naloxone also shifted the morphine dose-response relationship to the right, by a factor of 2.62, whilst naltrindole had no effect upon morphine antinociception. Aspirin antinociception remained unaffected by both opioid antagonists. 4. The enkephalin catabolism inhibitor acetorphan, by itself, produced no activity in this test at a dose of 10 mg kg(-1) (s.c.). However, at higher doses, acetorphan produced a linear dose-response relationship against acetic acid-induced abdominal constriction. 5. When acetorphan was administered before either the antidepressants or morphine, there was a clear potentiation of the antidepressant- or morphine-induced antinociception. However, acetorphan had no effect on aspirin antinociception. 6. Since neither of the opioid antagonists were able to attenuate, nor was acetorphan able to potentiate, aspirin antinociception, we concluded that the mechanism of antidepressant-induced antinociception is different from that of the non-steroidal anti-inflammatory drugs. 7. These data are consistent with the view that antidepressants may induce endogenous opioid peptide release, as shown by the acetorphan study. In this context, the ability of naltrindole to displace the antidepressant dose-response relationship to the right without affecting morphine antinociception, implicates the delta-opioid receptor and endogenous opioid peptides in antidepressant-induced antinociception.
摘要
  1. 关于抗抑郁药诱导的抗伤害感受的本质存在争议。目前尚不清楚抗抑郁药本身是否具有抗伤害感受作用,是否能够增强阿片类药物的抗伤害感受作用,或者两者兼具。我们利用醋酸诱导的小鼠腹部收缩试验来研究抗抑郁药诱导的抗伤害感受作用。2. 所有测试的抗抑郁药(皮下注射)对醋酸诱导的腹部收缩均产生剂量依赖性保护作用。同样,吗啡和阿司匹林在该伤害感受试验中也是有效的抗伤害感受剂。3. 阿片类拮抗剂纳洛酮(0.5mg/kg,皮下注射)和纳曲吲哚(1mg/kg,皮下注射)使每种抗抑郁药(多塞平、阿米替林、西布曲明、(+)-奥沙普替林和帕罗西汀)的剂量 - 反应关系向右移动。在此情况下,纳洛酮的剂量比分别为1.95、3.90、2.32、4.50和2.65,纳曲吲哚的剂量比分别为4.36、17.00、4.28、11.48和2.65。纳洛酮也使吗啡的剂量 - 反应关系向右移动,移动系数为2.62,而纳曲吲哚对吗啡的抗伤害感受作用没有影响。阿司匹林的抗伤害感受作用不受两种阿片类拮抗剂的影响。4. 脑啡肽分解代谢抑制剂醋托芬本身在剂量为10mg/kg(皮下注射)时在该试验中无活性。然而,在更高剂量时,醋托芬对醋酸诱导的腹部收缩产生线性剂量 - 反应关系。5. 在抗抑郁药或吗啡给药前给予醋托芬时,抗抑郁药或吗啡诱导的抗伤害感受作用明显增强。然而,醋托芬对阿司匹林的抗伤害感受作用没有影响。6. 由于两种阿片类拮抗剂均不能减弱,醋托芬也不能增强阿司匹林的抗伤害感受作用,我们得出结论,抗抑郁药诱导的抗伤害感受机制与非甾体抗炎药不同。7. 这些数据与抗抑郁药可能诱导内源性阿片肽释放的观点一致,如醋托芬研究所示。在此情况下,纳曲吲哚在不影响吗啡抗伤害感受作用的情况下使抗抑郁药剂量 - 反应关系向右移动,这表明δ - 阿片受体和内源性阿片肽参与了抗抑郁药诱导的抗伤害感受作用。

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