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奈福泮与酮洛芬在啮齿动物抗伤害感受模型中的协同作用。

Nefopam and ketoprofen synergy in rodent models of antinociception.

作者信息

Girard Philippe, Verniers Danielle, Coppé Marie-Claude, Pansart Yannick, Gillardin Jean-Marie

机构信息

Biocodex, Service de Pharmacologie, Zac de Mercières 60200 Compiègne, France.

出版信息

Eur J Pharmacol. 2008 Apr 28;584(2-3):263-71. doi: 10.1016/j.ejphar.2008.02.012. Epub 2008 Feb 14.

Abstract

Combinations of analgesics with different mechanisms of action offer the possibility of efficient analgesia with a decrease in side effects as a result of reduced dosages of one or both compounds. Based on a clinical observation of synergism between nefopam, a centrally acting non-opioid that inhibits monoamines reuptake, and ketoprofen, a non-steroidal anti-inflammatory drug, the objective of this study was to further explore this antinociceptive synergy in four distinct animal models of pain (both drugs were administered subcutaneously). Strong antinociceptive properties were observed in the mouse writhing abdominal test with ED50 values of 2.56+/-0.38 and 1.41+/-0.41 mg/kg for nefopam and ketoprofen, respectively. In the inflammatory phase of the mouse formalin test, both compounds significantly inhibited the licking time of the injected hind-paw with ED50 of 4.32+/-0.17 mg/kg for nefopam and 49.56+/-15.81 mg/kg for ketoprofen. Isobolographic analysis revealed that this drug combination is synergistic in the formalin test and additive in the writhing test. In rat carrageenan-induced tactile allodynia, single administration of nefopam or ketoprofen only partially reduced allodynia. Combination of low analgesic doses of nefopam (10 or 30 mg/kg) with low analgesic doses of ketoprofen (30 or 100 mg/kg) significantly reduced or reversed allodynia, with a more pronounced anti-allodynic effect and a longer duration efficacy. In a rat model of postoperative thermal hyperalgesia induced by incision, co-administration of nefopam at a low analgesic dose (10 mg/kg) with ketoprofen at non-analgesic doses (30 or 100 mg/kg) showed the appearance of a strong anti-hyperalgesic effect, maintained during at least 3 h. In conclusion, co-administration of nefopam with ketoprofen is synergistic, and should allow either to increase their analgesic efficacy and/or to reduce their side effects.

摘要

作用机制不同的镇痛药联合使用,有可能在减少一种或两种药物剂量的情况下实现有效镇痛并降低副作用。基于对奈福泮(一种抑制单胺再摄取的中枢性非阿片类药物)与酮洛芬(一种非甾体抗炎药)之间协同作用的临床观察,本研究的目的是在四种不同的疼痛动物模型中进一步探究这种镇痛协同作用(两种药物均皮下给药)。在小鼠扭体腹部试验中观察到了强大的镇痛特性,奈福泮和酮洛芬的半数有效量(ED50)值分别为2.56±0.38和1.41±0.41mg/kg。在小鼠福尔马林试验的炎症期,两种化合物均显著抑制注射后足的舔舐时间,奈福泮的ED50为4.32±0.17mg/kg,酮洛芬的ED50为49.56±15.81mg/kg。等效应线图分析表明,该药物组合在福尔马林试验中具有协同作用,在扭体试验中具有相加作用。在大鼠角叉菜胶诱导的触觉异常性疼痛中,单独给予奈福泮或酮洛芬仅部分减轻了异常性疼痛。低镇痛剂量的奈福泮(10或30mg/kg)与低镇痛剂量的酮洛芬(30或100mg/kg)联合使用可显著减轻或逆转异常性疼痛,具有更明显的抗异常性疼痛作用和更长的疗效持续时间。在大鼠切口诱导的术后热痛觉过敏模型中,低镇痛剂量(10mg/kg)的奈福泮与非镇痛剂量(30或100mg/kg)的酮洛芬联合给药显示出强大的抗痛觉过敏作用,至少持续3小时。总之,奈福泮与酮洛芬联合给药具有协同作用,应能提高它们的镇痛效果和/或减少它们的副作用。

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