CPS Research, Glasgow, UK.
Curr Med Res Opin. 2011 Jan;27(1):87-98. doi: 10.1185/03007995.2010.537317. Epub 2010 Nov 24.
The authors recently reported on efficacy and safety of prolonged-release melatonin formulation (PRM; Circadin 2 mg) in elderly insomnia patients. The age cut-off for response to PRM and the long-term maintenance of efficacy and safety were further evaluated by looking at the total cohort (age 18-80 years) from that study and subsets of patients aged 18-54 and 55-80 years (for whom the drug is currently indicated).
Randomised, double-blind, placebo controlled trial.
Multicentre, outpatients, primary care setting.
A total of 930 males and females aged 18-80 years with primary insomnia who reported mean nightly sleep latency (SL) >20 min were enrolled and 791 entered the active phase of the study. The study comprised a 2-week, single-blind placebo run-in period followed by 3 week's double-blind treatment with PRM or placebo, one tablet per day at 2 hours before bedtime. PRM patients continued whereas placebo completers were re-randomised 1:1 to PRM or placebo for 26 weeks followed by 2-weeks run-out on placebo.
SL and other sleep variables derived from sleep diary, Pittsburgh Sleep Quality Index (PSQI), Quality of life (WHO-5), Clinical Global Impression of Improvement (CGI-I) and adverse effects, recorded each visit, withdrawal and rebound effects during run-out.
In all, 746 patients completed the 3-week and 555 (421 PRM, 134 placebo) completed the 6-month period. The principal reason for drop-out was patient decision. At 3 weeks, significant differences in SL (diary, primary variable) in favour of PRM vs. placebo treatment were found for the 55-80-year group (-15.4 vs. -5.5 min, p = 0.014) but not the 18-80-year cut-off which included younger patients. Other variables (SL-PSQI, PSQI, WHO-5, CGI-I scores) improved significantly with PRM in the 18-80-year population, more so than in the 55-80-year age group. Improvements were maintained or enhanced over the 6-month period with no signs of tolerance. No withdrawal symptoms or rebound insomnia were detected. Most adverse events were mild with no significant differences between PRM and placebo groups in any safety outcome.
The results demonstrate short- and long-term efficacy of PRM in insomnia patients aged 18-80 years, particularly those aged 55 and over. PRM was well-tolerated over the entire 6-month period with no rebound or withdrawal symptoms following discontinuation. Study Registry No: ClinicalTrials.gov ID: NCT00397189.
作者最近报道了延长释放褪黑素制剂(PRM;Circadin 2mg)在老年失眠患者中的疗效和安全性。通过研究该研究的总队列(年龄 18-80 岁)和年龄在 18-54 岁和 55-80 岁的患者亚组(目前该药物适用),进一步评估了对 PRM 的反应和长期疗效及安全性的年龄界限。
随机、双盲、安慰剂对照试验。
多中心、门诊、初级保健环境。
共纳入 930 名年龄在 18-80 岁之间、原发性失眠、每晚平均睡眠潜伏期(SL)>20 分钟的男性和女性,其中 791 名进入研究的主动治疗阶段。该研究包括 2 周的单盲安慰剂导入期,随后进行 3 周的 PRM 或安慰剂双盲治疗,每天睡前 2 小时服用 1 片。PRM 组继续治疗,而安慰剂组完成者以 1:1 的比例重新随机分配至 PRM 或安慰剂组,随后进行 26 周的治疗,然后进行 2 周的安慰剂洗脱期。
从睡眠日记、匹兹堡睡眠质量指数(PSQI)、生活质量(WHO-5)、临床总体印象改善(CGI-I)和不良反应中得出的 SL 和其他睡眠变量,每次就诊时记录,洗脱期和反弹效应。
共有 746 名患者完成了 3 周的治疗,555 名患者(421 名 PRM,134 名安慰剂)完成了 6 个月的治疗。退出的主要原因是患者决定。在 3 周时,与安慰剂治疗相比,PRM 在 55-80 岁组的 SL(日记,主要变量)有显著改善(-15.4 分钟对-5.5 分钟,p=0.014),但在包括年轻患者的 18-80 岁截止值中则无差异。其他变量(SL-PSQI、PSQI、WHO-5、CGI-I 评分)在 18-80 岁人群中均有显著改善,在 55-80 岁年龄组中的改善更为显著。在 6 个月的治疗期间,改善情况得以维持或增强,且未出现耐受迹象。未发现停药症状或反弹性失眠。大多数不良事件为轻度,PRM 和安慰剂组在任何安全性结果方面均无显著差异。
结果表明,PRM 对 18-80 岁失眠患者,特别是 55 岁及以上患者的短期和长期疗效均有显著疗效。PRM 在整个 6 个月的治疗期间耐受性良好,停药后无反弹或停药症状。研究注册号:ClinicalTrials.gov 注册号:NCT00397189。
