口服甲基纳曲酮对阿片类药物引起的便秘和慢性非癌性疼痛患者的镇痛效果没有负面影响。
Oral methylnaltrexone does not negatively impact analgesia in patients with opioid-induced constipation and chronic noncancer pain.
作者信息
Webster Lynn R, Israel Robert J
机构信息
PRA Health Sciences, Salt Lake City, UT, USA.
Clinical and Medical Affairs, Salix Pharmaceuticals, Bridgewater, NJ, USA,
出版信息
J Pain Res. 2018 Aug 13;11:1503-1510. doi: 10.2147/JPR.S160488. eCollection 2018.
PURPOSE
An oral formulation of methylnaltrexone has been developed for treating opioid-induced constipation (OIC). This manuscript examines the impact of oral methylnaltrexone, a peripherally acting µ-opioid receptor antagonist, on opioid analgesia.
METHODS
This Phase III, randomized, double-blind, placebo-controlled trial, evaluated changes in pain intensity scores (0= no pain to 10= worst possible pain) and opioid use in adults with chronic noncancer pain. Patients taking ≥50 mg/day oral morphine equivalent dose (MED) for ≥14 days before screening with less than three rescue-free bowel movements/week received oral methylnaltrexone 150 mg/day (n=201), 300 mg/day (n=201), 450 mg/day (n=200), or placebo (n=201) once daily for 4 weeks followed by 8 weeks of oral methylnaltrexone as needed.
RESULTS
The primary condition requiring opioid use was back pain (68.2% of 803 patients). Baseline pain intensity scores were similar among treatment groups (mean range, 6.2-6.4) and remained stable throughout the 4-week double-blind (mean range, 6.1-6.5) and 8-week as needed (mean range, 6.3-6.5) periods. Baseline mean MED was comparable between oral methylnaltrexone 150 mg (200.0 mg/day), methylnaltrexone 450 mg (218.0 mg/day), and placebo (209.7 mg/day), but was slightly higher in the oral methylnaltrexone 300-mg group (252.6 mg/day). Nonsignificant, minimal changes in mean MED were observed after 4 weeks of treatment (214.5-235.6 mg/day) and at the end of the as needed phase (202.3-234.9 mg/day). The percentage of patients who initiated new opioid medications during the 4-week, once-daily dosing period was generally similar among the oral methylnaltrexone 150-mg, 300-mg, and 450-mg groups (44.8%, 43.3%, and 35.0%, respectively), the oral methylnaltrexone combined group (41.0%), and the placebo group (39.8%). The most common newly initiated opioid medications during this once-daily period were oxycodone (oral methylnaltrexone groups combined, 14.6%; placebo, 12.4%) and morphine (oral methylnaltrexone combined, 10.1%; placebo, 7.0%).
CONCLUSION
Oral methylnaltrexone does not elicit opioid withdrawal or interfere with opioid analgesia.
目的
已研发出甲基纳曲酮口服制剂用于治疗阿片类药物引起的便秘(OIC)。本手稿研究了外周作用的μ-阿片受体拮抗剂口服甲基纳曲酮对阿片类药物镇痛效果的影响。
方法
这项III期随机双盲安慰剂对照试验,评估了慢性非癌性疼痛成人患者的疼痛强度评分(0 = 无疼痛至10 = 可能的最严重疼痛)和阿片类药物使用情况的变化。在筛选前服用≥50mg/天口服吗啡等效剂量(MED)≥14天且每周排便少于三次且无需救援的患者,接受150mg/天(n = 201)、300mg/天(n = 201)、450mg/天(n = 200)的口服甲基纳曲酮或安慰剂(n = 201),每日一次,持续4周,随后根据需要进行8周的口服甲基纳曲酮治疗。
结果
需要使用阿片类药物的主要病症是背痛(803例患者中的68.2%)。各治疗组的基线疼痛强度评分相似(平均范围为6.2 - 6.4),在4周双盲期(平均范围为6.1 - 6.5)和8周按需治疗期(平均范围为6.3 - 6.5)内均保持稳定。口服甲基纳曲酮150mg(200.0mg/天)、甲基纳曲酮450mg(218.0mg/天)和安慰剂(209.7mg/天)组的基线平均MED相当,但口服甲基纳曲酮300mg组(252.6mg/天)略高。治疗4周后(214.5 - 235.6mg/天)和按需治疗阶段结束时(202.3 - 234.9mg/天),观察到平均MED的变化无统计学意义且极小。在4周每日一次给药期内开始使用新阿片类药物的患者百分比在口服甲基纳曲酮150mg、300mg和450mg组(分别为44.8%、43.3%和35.0%)、口服甲基纳曲酮联合组(41.0%)和安慰剂组(39.8%)中总体相似。在此每日一次给药期内最常见的新开始使用的阿片类药物是羟考酮(口服甲基纳曲酮组合并,14.6%;安慰剂,12.4%)和吗啡(口服甲基纳曲酮合并组,10.1%;安慰剂,7.0%)。
结论
口服甲基纳曲酮不会引起阿片类药物戒断或干扰阿片类药物镇痛效果。
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