Bull Janet, Wellman Charles V, Israel Robert J, Barrett Andrew C, Paterson Craig, Forbes William P
1 Four Seasons , Flat Rock, North Carolina.
2 Hospice of the Western Reserve , Cleveland, Ohio.
J Palliat Med. 2015 Jul;18(7):593-600. doi: 10.1089/jpm.2014.0362. Epub 2015 May 14.
Subcutaneous methylnaltrexone (MNTX), dosed based on body weight, is efficacious and well tolerated in inducing bowel movements in patients with advanced illness and opioid-induced constipation (OIC); however, fixed-dose administration of MNTX may improve ease of administration.
The study objective was to assess safety and efficacy of fixed-dose MNTX in two phase 4 trials.
In a double-blind, randomized, placebo-controlled trial (RCT), patients with advanced illness and OIC received MNTX (8 mg or 12 mg by body weight [38 kg to <62 kg or ≥62 kg, respectively]) or placebo every other day (QOD) for two weeks. Patients completing the RCT could enroll in an open-label extension (OLE) study with MNTX administered as needed (PRN). The primary endpoint was percentage of patients with a rescue-free bowel movement (RFBM) within four hours after ≥2 of the first 4 doses in the first week.
In the RCT, 116 and 114 patients received MNTX and placebo, respectively, and 149 patients continued to the OLE study. The percentage of patients achieving primary endpoint was 62.9% and 9.6% for MNTX and placebo groups, respectively (p<0.0001). Median time to RFBM after the first dose was 0.8 hour and 23.6 hours in MNTX and placebo groups, respectively (p<0.0001). Efficacy results during the OLE study were consistent with the RCT. MNTX demonstrated a favorable safety profile in the RCT and OLE study.
Fixed-dose MNTX administered QOD in the RCT and PRN in the OLE study demonstrated robust efficacy and was well tolerated in treating OIC in patients with advanced illness.
皮下注射甲基纳曲酮(MNTX),根据体重给药,在晚期疾病和阿片类药物引起的便秘(OIC)患者中诱导排便有效且耐受性良好;然而,MNTX固定剂量给药可能会提高给药的便利性。
本研究目的是在两项4期试验中评估固定剂量MNTX的安全性和有效性。
在一项双盲、随机、安慰剂对照试验(RCT)中,晚期疾病和OIC患者每隔一天接受MNTX(根据体重分别为8mg或12mg [分别适用于体重38kg至<62kg或≥62kg的患者])或安慰剂,持续两周。完成RCT的患者可参加开放标签扩展(OLE)研究,根据需要(PRN)给予MNTX。主要终点是在第一周前4剂中≥2剂后4小时内无补救性排便(RFBM)的患者百分比。
在RCT中,分别有116例和114例患者接受了MNTX和安慰剂,149例患者继续参加OLE研究。MNTX组和安慰剂组达到主要终点的患者百分比分别为62.9%和9.6%(p<0.0001)。MNTX组和安慰剂组首次给药后至RFBM的中位时间分别为0.8小时和23.6小时(p<0.0001)。OLE研究期间的疗效结果与RCT一致。MNTX在RCT和OLE研究中显示出良好的安全性。
在RCT中每隔一天给药以及在OLE研究中根据需要给药的固定剂量MNTX在治疗晚期疾病患者的OIC方面显示出强大的疗效且耐受性良好。
