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强直性疼痛与发作性疼痛:酮洛芬的剂量相关效应

Tonic versus phasic pain: dose-related effects of ketoprofen.

作者信息

Hummel T, Huber H, Menzel S, Kobal G

机构信息

Department of Experimental and Clinical Pharmacology and Toxicology, University of Erlangen-Nürnberg, Germany.

出版信息

Eur J Clin Pharmacol. 1995;49(1-2):7-14. doi: 10.1007/BF00192351.

Abstract

Only recently has a new experimental technique been developed which combines tonic and phasic painful stimulation. By means of this technique the non-steroidal anti-inflammatory drug (NSAID) ibuprofen has been shown to produce a dose-related decrease in heterotopically applied phasic and tonic pain. The present study aimed to investigate the dose-related effects of the NSAID ketoprofen (50, 100, and 150 mg i.v.) when tonic and phasic stimuli were applied homotopically. Eighteen healthy volunteers participated in the double-blind, randomized, placebo-controlled study. After an initial training session subjects took part in four experiments, each of which was divided into three sessions (before, 30, and 120 min after drug administration). During each session 45 painful phasic CO2 stimuli of three concentrations were presented to the left nostril in randomized order (duration 200 ms; interval 40 s; 45%, 52%, and 59% v/v CO2). The left nostril was additionally stimulated with a constant stream of dry air, which produced a tonic painful sensation described as dull and burning. Subjects rated the intensity of the painful stimuli by means of visual analogue scales. Chemosomatosensory event-related potentials (CSSERPs) were recorded in response to phasic painful CO2 stimuli. Ketoprofen reduced the subjects' estimates of tonic pain in a dose-related manner. In contrast, given the special conditions of homotopic application of tonic and phasic painful stimuli, estimates of phasic pain increased significantly, corresponding to a significant increase in CSSERP amplitudes. An explanation of this inverse effect of the drug on responses to tonic and phasic pain may be a lateralized interaction between both C-fiber and A delta-fiber systems at a spinal or peripheral level.

摘要

直到最近才开发出一种新的实验技术,该技术结合了持续性和阶段性疼痛刺激。通过这种技术,已证明非甾体抗炎药(NSAID)布洛芬能使异位施加的阶段性和持续性疼痛产生剂量相关的减轻。本研究旨在调查当持续性和阶段性刺激在同位点施加时,NSAID酮洛芬(静脉注射50、100和150毫克)的剂量相关效应。18名健康志愿者参与了这项双盲、随机、安慰剂对照研究。在初始训练阶段后,受试者参加了四项实验,每项实验分为三个阶段(给药前、给药后30分钟和120分钟)。在每个阶段,以随机顺序向左侧鼻孔呈现三种浓度的45次阶段性疼痛性二氧化碳刺激(持续时间200毫秒;间隔40秒;45%、52%和59%体积/体积的二氧化碳)。左侧鼻孔还受到持续的干燥气流刺激,产生一种被描述为钝痛和灼痛的持续性疼痛感觉。受试者通过视觉模拟量表对疼痛刺激的强度进行评分。记录了对阶段性疼痛性二氧化碳刺激的化学体感事件相关电位(CSSERP)。酮洛芬以剂量相关的方式降低了受试者对持续性疼痛的估计。相比之下,鉴于持续性和阶段性疼痛刺激同位点施加的特殊条件,对阶段性疼痛的估计显著增加,这与CSSERP振幅的显著增加相对应。药物对持续性和阶段性疼痛反应的这种相反作用的一种解释可能是C纤维和Aδ纤维系统在脊髓或外周水平的侧化相互作用。

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