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非甾体抗炎药(NSAIDs)与右美沙芬联合口服给药对大鼠关节炎性疼痛行为症状的影响。

Effects of the combined oral administration of NSAIDs and dextromethorphan on behavioral symptoms indicative of arthritic pain in rats.

作者信息

Price D D, Mao J, Lu J, Caruso F S, Frenk H, Mayer D J

机构信息

Department of Anesthesiology, Medical College of Virginia, Virginia Commonwealth University, Richmond 23298, USA.

出版信息

Pain. 1996 Nov;68(1):119-27.

PMID:9252006
Abstract

The effects of combined single oral treatments with non-steroidal anti-inflammatory drugs (NSAIDs) and the non-competitive N-methyl-D-aspartate (NMDA) receptor antagonist dextromethorphan (DM) on arthritic pain were examined in a rat model of adjuvant-induced arthritis. Although 12.5-100 mg/kg doses of DM alone produced no reliable effects, treatments with ibuprofen (IB, 50 and 100 mg/kg but not 12.5 or 25 mg/kg) produced mild analgesia in arthritic rats as determined using the Randall-Sellito test. IB showed a dose-response relationship which appeared to plateau at doses of 50 and 100 mg/kg. Adding 50 mg/kg DM to each IB dose resulted in significantly greater analgesic activity than IB alone at doses of 25, 50 and 100 mg/kg. A similar interaction between 50 mg/kg DM and 50 mg/kg IB occurred with respect to spontaneous pain behavior. Adding 25 mg/kg DM to 25 mg/kg IB likewise increased analgesia as measured by both the Randall-Sellito and spontaneous pain behavior tests (both P < 0.05). Five more NSAIDs were evaluated using the Randall-Sellito test, which included naproxen (NP), piroxicam (PIR), etodolac (ET), diclofenac (DC), and ketorolac (KE). For all six NSAIDS, the addition of 50 mg/kg DM reliably increased their analgesic potency, as indicated by reliable increases in previously effective NSAID doses (all six NSAIDs) as well as previously ineffective NSAID doses (IB, NP, DC, and PIR). These data demonstrate that DM greatly potentiates the analgesic activity of IB, DC, NP, PIR, ET, and KT and increases the peak effect over the NSAIDs alone. Similiar to DM's previously demonstrated enhancement of opioid analgesia in acute pain, the combination of DM and an NSAID may represent a novel analgesic approach to improved management of arthritic pain.

摘要

在佐剂诱导的关节炎大鼠模型中,研究了非甾体抗炎药(NSAIDs)与非竞争性N-甲基-D-天冬氨酸(NMDA)受体拮抗剂右美沙芬(DM)联合单次口服治疗对关节炎疼痛的影响。尽管单独使用12.5 - 100 mg/kg剂量的DM未产生可靠效果,但使用布洛芬(IB,50和100 mg/kg,而非12.5或25 mg/kg)治疗可使关节炎大鼠产生轻度镇痛作用,这是通过兰德尔-塞利托试验确定的。IB呈现剂量反应关系,在50和100 mg/kg剂量时似乎达到平台期。在每个IB剂量中添加50 mg/kg DM,在25、50和100 mg/kg剂量时产生的镇痛活性明显高于单独使用IB。在自发疼痛行为方面,50 mg/kg DM与50 mg/kg IB之间也出现了类似的相互作用。在25 mg/kg IB中添加25 mg/kg DM同样增加了镇痛效果,这通过兰德尔-塞利托试验和自发疼痛行为试验均得到验证(两者P < 0.05)。使用兰德尔-塞利托试验评估了另外五种NSAIDs,包括萘普生(NP)、吡罗昔康(PIR)、依托度酸(ET)、双氯芬酸(DC)和酮咯酸(KE)。对于所有六种NSAIDs,添加50 mg/kg DM均可靠地提高了它们的镇痛效力,这表现为先前有效NSAID剂量(所有六种NSAIDs)以及先前无效NSAID剂量(IB、NP、DC和PIR)的可靠增加。这些数据表明,DM极大地增强了IB、DC、NP、PIR、ET和KT的镇痛活性,并使峰值效应超过单独使用NSAIDs。与DM先前在急性疼痛中增强阿片类镇痛作用类似,DM与NSAID的联合可能代表一种改善关节炎疼痛管理的新型镇痛方法。

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