鞘内注射吗啡与齐考诺肽联合应用的开放标签、多中心研究：在接受齐考诺肽治疗的严重慢性疼痛患者中添加吗啡。

Open-label, multicenter study of combined intrathecal morphine and ziconotide: addition of morphine in patients receiving ziconotide for severe chronic pain.

作者信息

Webster Lynn R, Fakata Keri L, Charapata Steven, Fisher Robert, MineHart Michael

机构信息

Lifetree Clinical Research and Pain Clinic, Salt Lake City, Utah, USA.

出版信息

Pain Med. 2008 Apr;9(3):282-90. doi: 10.1111/j.1526-4637.2007.00356.x.

DOI:10.1111/j.1526-4637.2007.00356.x

PMID:18366508

Abstract

OBJECTIVE

To assess the safety and efficacy of adding intrathecal morphine to intrathecal ziconotide in patients treated with stable ziconotide doses.

DESIGN

Multicenter, open-label study with a 4-week morphine titration phase during which ziconotide was held constant and an extension phase during which dosing of either drug could vary.

SETTING

Outpatient clinics.

PATIENTS

Patients with suboptimal pain relief receiving stable ziconotide doses (> or = 4.8 microg/day) in one of two ongoing ziconotide trials.

INTERVENTIONS

Ziconotide dosing remained constant during the titration phase; intrathecal morphine titration was based on each patient's daily systemic opioid dose at the study's start. During the extension phase, intrathecal ziconotide and morphine dosing were adjusted per investigator discretion.

OUTCOME MEASURES

Safety was assessed primarily via adverse events. Efficacy was analyzed via percentage change on the visual analog scale of pain intensity and in weekly systemic opioid consumption.

RESULTS

Twenty-five patients enrolled. The most common (> or = 10% of patients in either study phase) study drug-related (i.e., ziconotide/morphine combination [or ziconotide monotherapy in the extension phase only]) treatment-emergent adverse events included dizziness, peripheral edema, pruritus, and nausea. From the initial visit to week 4, visual analog scale of pain intensity scores improved by a mean of 26.3% (95% confidence interval: 15.6%-37.1%) but varied during the extension phase (mean percentage change from the initial visit ranged from -0.4% at week 16 to -35.0% at week 72). Mean percentage decrease in systemic opioid consumption from the initial visit was 49.1% at week 4 and 51.2% at week 56 of the extension phase.

CONCLUSIONS

Intrathecal morphine, combined with stable intrathecal ziconotide doses, reduced pain in patients with previously suboptimal pain relief on ziconotide monotherapy.

摘要

目的

评估在接受稳定剂量齐考诺肽治疗的患者中，鞘内注射吗啡联合鞘内注射齐考诺肽的安全性和有效性。

设计

多中心、开放标签研究，包括一个为期4周的吗啡滴定阶段（在此期间齐考诺肽剂量保持不变）和一个延长期（在此期间两种药物的剂量均可变化）。

地点

门诊诊所。

患者

在两项正在进行的齐考诺肽试验之一中，接受稳定剂量齐考诺肽（≥4.8微克/天）但疼痛缓解效果欠佳的患者。

干预措施

在滴定阶段，齐考诺肽剂量保持不变；鞘内注射吗啡的滴定基于研究开始时每位患者的每日全身性阿片类药物剂量。在延长期，鞘内注射齐考诺肽和吗啡的剂量由研究者自行决定调整。

观察指标

安全性主要通过不良事件进行评估。有效性通过疼痛强度视觉模拟量表上的变化百分比以及每周全身性阿片类药物消耗量进行分析。

结果

25名患者入组。最常见的（在任何一个研究阶段中≥10%的患者）与研究药物相关（即齐考诺肽/吗啡联合用药[或仅在延长期为齐考诺肽单药治疗]）的治疗中出现的不良事件包括头晕、外周水肿、瘙痒和恶心。从初次就诊到第4周，疼痛强度视觉模拟量表评分平均改善了26.3%（95%置信区间：15.6%-37.1%），但在延长期有所变化（从初次就诊起的平均变化百分比范围从第16周的-0.4%到第72周的-35.0%）。在延长期第4周时，全身性阿片类药物消耗量相对于初次就诊时平均减少了49.1%，在第56周时减少了51.2%。