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双氯芬酸在癌痛中的吗啡节省效应。

Morphine-sparing effect of diclofenac in cancer pain.

作者信息

Björkman R, Ullman A, Hedner J

机构信息

Department of Clinical Pharmacology, Sahlgrenska Hospital, Gothenburg, Sweden.

出版信息

Eur J Clin Pharmacol. 1993;44(1):1-5. doi: 10.1007/BF00315271.

Abstract

The effectiveness of diclofenac 50 mg t.i.d. as additive treatment to parenteral patient-controlled administration therapy (PCAT) with morphine in cancer pain has been investigated in a double-blind study. In the fifteen patients who completed the study, morphine i.v. was titrated to optimal pain relief over 5 days. The mean total morphine consumption was significantly reduced during diclofenac administration (82.8 mg morphine per day) compared to placebo (95.0 mg morphine per day). The reduction in mean morphine consumption during active treatment with diclofenac was independent of the initial dose of self-titrated morphine. Pain, self-assessed according to VAS, tended to be lower during the diclofenac period, although the difference did not reach statistical significance. No adverse events were recorded among the 15 patients who completed the study. The present findings show that a non-steroidal anti-inflammatory agent, such as diclofenac, has a morphine-sparing effect in morphine-treated patients with cancer pain.

摘要

在一项双盲研究中,对双氯芬酸50毫克每日三次作为吗啡静脉自控镇痛疗法(PCAT)治疗癌症疼痛的辅助治疗效果进行了研究。在完成研究的15名患者中,静脉注射吗啡在5天内滴定至最佳疼痛缓解。与安慰剂(每天95.0毫克吗啡)相比,双氯芬酸给药期间平均吗啡总消耗量显著降低(每天82.8毫克吗啡)。双氯芬酸积极治疗期间平均吗啡消耗量的减少与自行滴定吗啡的初始剂量无关。根据视觉模拟评分法(VAS)自我评估的疼痛在双氯芬酸治疗期间往往较低,尽管差异未达到统计学意义。在完成研究的15名患者中未记录到不良事件。目前的研究结果表明,非甾体抗炎药如双氯芬酸在接受吗啡治疗的癌症疼痛患者中具有吗啡节省作用。

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