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美他帕明的镇痛作用及关于内源性脑啡肽未参与三环类抗抑郁药所致镇痛作用的证据。

Analgesic effects of metapramine and evidence against the involvement of endogenous enkephalins in the analgesia induced by tricyclic antidepressants.

作者信息

Michael-Titus Adina, Costentin Jean

机构信息

Unité de Neuropsychopharmacologie expérimentale, UA 1170 CNRS U.E.R. de Médecine et Pharmacie, 76800 St. Etienne du RouvrayFrance.

出版信息

Pain. 1987 Dec;31(3):391-400. doi: 10.1016/0304-3959(87)90167-9.

Abstract

In several pain models, tricyclic antidepressants (TCAs) have been shown to reduce nociception. In the present study, we evaluated the antinociceptive effect of metapramine (META) in 4 nociception tests: (1) the hot plate test; (2) the phenylbenzoquinone-induced writhing; (3) the tail flick test; and (4) the test of electrical stimulation of the tail. We further analysed, using META and clomipramine (CLOM), the eventual role of endogenous opioids in analgesia induced by TCAs. The analgesic effects of META and CLOM in the hot plate test and in the test of electrical stimulation of the tail were reversed by naloxone. On the other hand, we failed to demonstrate a potentiation of META- or CLOM-induced analgesia by acetorphan, an inhibitor of 'enkephalinase.' We also failed to show a potentiation of Met5-enkephalin intracerebroventricularly injected by the two TCAs. Moreover, the administration of the enzymatic inhibitor or of Met5-enkephalin led to a slight decrease of the analgesic effect of the TCAs. These results (1) indicate that in our 4 pain tests, META clearly reduces nociception and (2) provide evidence that the involvement of endogenous enkephalins in the analgesia induced by TCAs is improbable.

摘要

在几种疼痛模型中,三环类抗抑郁药(TCAs)已被证明可减轻伤害感受。在本研究中,我们在4种伤害感受测试中评估了美他帕明(META)的抗伤害感受作用:(1)热板试验;(2)苯醌诱发的扭体反应;(3)甩尾试验;以及(4)尾部电刺激试验。我们进一步使用META和氯米帕明(CLOM)分析了内源性阿片类物质在TCAs诱导的镇痛中的最终作用。纳洛酮可逆转META和CLOM在热板试验和尾部电刺激试验中的镇痛作用。另一方面,我们未能证明“脑啡肽酶”抑制剂阿塞托芬可增强META或CLOM诱导的镇痛作用。我们也未能显示两种TCAs可增强脑室内注射的Met5-脑啡肽的作用。此外,给予酶抑制剂或Met5-脑啡肽会导致TCAs的镇痛作用略有降低。这些结果(1)表明在我们的4种疼痛测试中,META明显减轻了伤害感受,(2)提供了证据表明内源性脑啡肽不太可能参与TCAs诱导的镇痛作用。

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