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小剂量皮下持续注射吗啡治疗重度癌痛

Treatment of severe cancer pain by low-dose continuous subcutaneous morphine.

作者信息

Drexel Heinz, Dzien Alexander, Spiegel Robert W, Lang Alois H, Breier Christoph, Abbrederis Klaus, Patsch Josef R, Braunsteiner Herbert

机构信息

Department of Medicine, Diabetes and Lipid Metabolism Division, University of Innsbruck, InnsbruckAustria Department of Medicine, City Hospital, DornbirnAustria.

出版信息

Pain. 1989 Feb;36(2):169-176. doi: 10.1016/0304-3959(89)90020-1.

Abstract

In a prospective and intraindividually controlled trial, we have compared the efficacy and safety of a continuous subcutaneous morphine infusion with conventional intermittent oral or subcutaneous morphine application. Twenty-eight in-patients with cancer pain received a short-term infusion lasting 2-42 days, and 8 out-patients underwent long-term infusion from 49 to 197 days during the terminal stage of their disease. Continuous subcutaneous morphine infusion significantly (P less than 0.001) improved both pain and quality of life when compared to conventional morphine application. With continuous infusion, 5-48 mg (median 19 mg) of morphine was required daily, significantly (P less than 0.001) less than the 10-90 mg (median 50 mg) necessary with conventional use. As a result of lower dosage, side effects under continuous infusion were infrequent and mild. Constipation occurred in 3 of the 36 patients and was always controlled by the addition of laxatives; no nausea, sedation or respiratory depression were observed. Signs of tolerance developed in 2 patients on long-term infusion, but the use of continuous subcutaneous methadone for 2 weeks reversed the tolerance. The study presented indicates that low-dose continuous subcutaneous morphine provides a valuable treatment modality for severe terminal cancer pain exhibiting a high degree of both efficacy and safety.

摘要

在一项前瞻性个体自身对照试验中,我们比较了持续皮下输注吗啡与传统口服或皮下间断应用吗啡的疗效和安全性。28例癌症疼痛住院患者接受了为期2 - 42天的短期输注,8例门诊患者在疾病终末期接受了为期49至197天的长期输注。与传统吗啡应用相比,持续皮下输注吗啡显著(P < 0.001)改善了疼痛和生活质量。持续输注时,每日所需吗啡剂量为5 - 48 mg(中位数19 mg),显著(P < 0.001)低于传统用法所需的10 - 90 mg(中位数50 mg)。由于剂量较低,持续输注时的副作用少见且轻微。36例患者中有3例出现便秘,均通过加用泻药得到控制;未观察到恶心、镇静或呼吸抑制。2例长期输注患者出现耐受迹象,但持续皮下应用美沙酮2周逆转了耐受。本研究表明,低剂量持续皮下输注吗啡为重度终末期癌症疼痛提供了一种疗效和安全性均高的有价值的治疗方式。

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