CPS Research, Glasgow, UK.
BMC Med. 2010 Aug 16;8:51. doi: 10.1186/1741-7015-8-51.
Melatonin is extensively used in the USA in a non-regulated manner for sleep disorders. Prolonged release melatonin (PRM) is licensed in Europe and other countries for the short term treatment of primary insomnia in patients aged 55 years and over. However, a clear definition of the target patient population and well-controlled studies of long-term efficacy and safety are lacking. It is known that melatonin production declines with age. Some young insomnia patients also may have low melatonin levels. The study investigated whether older age or low melatonin excretion is a better predictor of response to PRM, whether the efficacy observed in short-term studies is sustained during continued treatment and the long term safety of such treatment.
Adult outpatients (791, aged 18-80 years) with primary insomnia, were treated with placebo (2 weeks) and then randomized, double-blind to 3 weeks with PRM or placebo nightly. PRM patients continued whereas placebo completers were re-randomized 1:1 to PRM or placebo for 26 weeks with 2 weeks of single-blind placebo run-out. Main outcome measures were sleep latency derived from a sleep diary, Pittsburgh Sleep Quality Index (PSQI), Quality of Life (World Health Organzaton-5) Clinical Global Impression of Improvement (CGI-I) and adverse effects and vital signs recorded at each visit.
On the primary efficacy variable, sleep latency, the effects of PRM (3 weeks) in patients with low endogenous melatonin (6-sulphatoxymelatonin [6-SMT] <or=8 microg/night) regardless of age did not differ from the placebo, whereas PRM significantly reduced sleep latency compared to the placebo in elderly patients regardless of melatonin levels (-19.1 versus -1.7 min; P = 0.002). The effects on sleep latency and additional sleep and daytime parameters that improved with PRM were maintained or enhanced over the 6-month period with no signs of tolerance. Most adverse events were mild in severity with no clinically relevant differences between PRM and placebo for any safety outcome.
The results demonstrate short- and long-term efficacy and safety of PRM in elderly insomnia patients. Low melatonin production regardless of age is not useful in predicting responses to melatonin therapy in insomnia. The age cut-off for response warrants further investigation.
褪黑素在美国被广泛用于治疗睡眠障碍,但未受监管。在欧洲和其他国家,延长释放型褪黑素(PRM)被批准用于治疗年龄在 55 岁及以上的原发性失眠症患者,疗程较短。然而,缺乏对目标患者人群的明确定义以及对长期疗效和安全性的充分对照研究。众所周知,褪黑素的产生随年龄增长而下降。一些年轻的失眠症患者也可能存在褪黑素水平低的情况。本研究旨在探讨年龄较大或褪黑素排泄量较低是否是对 PRM 反应的更好预测指标,以及在短期研究中观察到的疗效是否在持续治疗期间得到维持,以及这种治疗的长期安全性。
患有原发性失眠的成年门诊患者(791 人,年龄 18-80 岁)先接受安慰剂(2 周)治疗,然后随机、双盲接受 PRM 或安慰剂每晚治疗 3 周。PRM 患者继续治疗,而安慰剂完成者则以 1:1 的比例重新随机分为 PRM 或安慰剂治疗 26 周,同时进行 2 周的单盲安慰剂洗脱期。主要疗效指标为睡眠潜伏期,由睡眠日记得出,匹兹堡睡眠质量指数(PSQI)、生活质量(世界卫生组织-5)、临床总体印象改善(CGI-I)和不良反应以及每次就诊时的生命体征。
在主要疗效变量睡眠潜伏期方面,无论年龄大小,内源性褪黑素水平较低(6-硫酸褪黑素[6-SMT]≤8μg/夜)的 PRM 患者的疗效与安慰剂无差异,而褪黑素水平较低的老年患者的 PRM 治疗显著降低了睡眠潜伏期(-19.1 分钟与-1.7 分钟;P=0.002)。与安慰剂相比,PRM 改善了睡眠潜伏期和其他睡眠及日间参数的效果在 6 个月的治疗期间得以维持或增强,且无耐受迹象。大多数不良反应的严重程度为轻度,PRM 与安慰剂之间在任何安全性结果方面均无临床相关差异。
这些结果表明 PRM 对老年失眠症患者具有短期和长期疗效和安全性。无论年龄大小,褪黑素产量较低都不能用于预测失眠症患者对褪黑素治疗的反应。对反应的年龄截止值需要进一步研究。
