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中脑导水管周围灰质抑制作用的激活介导了安乃近的中枢镇痛作用。

Activation of inhibition from the periaqueductal grey matter mediates central analgesic effect of metamizol (dipyrone).

作者信息

Carlsson Karl-Heinz, Helmreich Julika, Jurna Ilmar

机构信息

Institut für Pharmakologie und Toxikologie, Universität des Saarlandes, D-6650 Homburg/SaarF.R.G.

出版信息

Pain. 1986 Dec;27(3):373-390. doi: 10.1016/0304-3959(86)90161-2.

Abstract

The pyrazolone derivative, metamizol (dipyrone), possesses analgesic, antipyretic, anti-inflammatory and spasmolytic properties. It is often classified as peripherally acting. To test the possibility that a central action of the drug contributes to its antinociceptive and analgesic effects, experiments were carried out in which the tail-flick response to radiant heat, flexor reflex activity in the tibialis anterior muscle and activity in ascending spinal axons evoked by stimulation of afferent C fibres in the sural nerve, and activity of neurones in the periaqueductal grey matter and the substantia nigra were assessed in rats. Metamizol administered by intraperitoneal (i.p.; 10, 20 and 40 mg/kg) or intrathecal (i.t.; 50 to 400 micrograms) injection to intact rats dose-dependently prolonged the tail-flick latency. Administration by i.t. injection to spinal rats was without effect. Intravenous (i.v.) injection of metamizol (140 mg/kg) reduced flexor reflex activity in intact animals, while an i.t. injection to spinal rats was ineffective at a low dose (100 micrograms) or enhanced the reflex activity at a higher dose (400 micrograms). Activity in ascending axons responding to afferent C fibre stimulation was mostly depressed by i.t. injection of metamizol (40, 80 and 140 mg/kg) in rats with an intact spinal cord. Ascending activity was increased by i.t. injection of the drug (100 and 200 micrograms) to spinal rats. Metamizol (140 mg/kg) i.v. increased the activity of neurones in the PAG and reduced that of neurones in the substantia nigra. Metamizol administered by microinjection into the PAG prolonged the tail-flick latency (15-100 micrograms) and depressed C fibre-evoked activity in ascending axons (100 micrograms). The results suggest that a central action is involved in the analgesic effect of metamizol and that this central action manifests itself by an activation of inhibition originating in the PAG.

摘要

吡唑酮衍生物安乃近(二氢吡喃酮)具有镇痛、解热、抗炎和解痉特性。它常被归类为外周作用药物。为了检验该药物的中枢作用是否有助于其抗伤害感受和镇痛效果,进行了相关实验,在实验中评估了大鼠对辐射热的甩尾反应、胫前肌的屈肌反射活动、由刺激腓肠神经传入C纤维诱发的脊髓上行轴突活动,以及中脑导水管周围灰质和黑质中神经元的活动。对完整大鼠腹腔注射(i.p.;10、20和40mg/kg)或鞘内注射(i.t.;50至400μg)安乃近,剂量依赖性地延长了甩尾潜伏期。对脊髓大鼠进行鞘内注射则无效果。静脉注射(i.v.)安乃近(140mg/kg)可降低完整动物的屈肌反射活动,而对脊髓大鼠进行鞘内注射,低剂量(100μg)时无效,高剂量(400μg)时则增强反射活动。在脊髓完整的大鼠中,鞘内注射安乃近(40、80和140mg/kg)大多会抑制对传入C纤维刺激产生反应的上行轴突活动。对脊髓大鼠进行鞘内注射该药物(100和200μg)可增加上行活动。静脉注射安乃近(140mg/kg)可增加中脑导水管周围灰质中神经元的活动,并降低黑质中神经元的活动。向中脑导水管周围灰质微量注射安乃近可延长甩尾潜伏期(15 - 100μg),并抑制上行轴突中C纤维诱发的活动(100μg)。结果表明,中枢作用参与了安乃近的镇痛效果,且这种中枢作用通过激活源自中脑导水管周围灰质的抑制作用而表现出来。

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