Zemlan Frank P, Mulchahey J Jeffery, Scharf Martin B, Mayleben David W, Rosenberg Russell, Lankford Alan
Phase 2 Discovery, Inc., Cincinnati, OH 45219, USA.
J Clin Psychiatry. 2005 Mar;66(3):384-90. doi: 10.4088/jcp.v66n0316.
While melatonin agonists are known to regulate circadian sleep rhythms, it is not clear whether melatonin agonists have a direct soporific effect. It has been suggested that melatonin's soporific effect is secondary to its ability to induce hypothermia. beta-Methyl-6-chloromelatonin is a high-affinity melatonin receptor agonist that is not associated with hypothermia. The purpose of the present study was to determine if the melatonin agonist beta-methyl-6-chloromelatonin has a direct soporific effect in subjects with primary insomnia.
A double-blind, placebo-controlled, crossover safety and efficacy study of 20 mg, 50 mg, and 100 mg of beta-methyl-6-chloromelatonin and placebo was conducted in subjects with DSM-IV-TR primary insomnia. Of 84 subjects screened, 40 progressed to randomly receive each of 3 beta-methyl-6-chloromelatonin doses or placebo on each of 2 consecutive nights with 5-day washout periods between treatments. The effect of treatment on both polysomnographic and subjectively measured sleep parameters, next-morning psychomotor performance, and safety measures was determined. The primary outcome measure was latency to persistent sleep measured by polysomnography.
A significant effect of beta-methyl-6-chloromelatonin on the primary efficacy variable, latency to persistent sleep, was observed (p = .0003). The 20-mg dose resulted in a significant 31% improvement in sleep latency compared with placebo, while significant 32% and 41% improvements were observed at the 50-mg and 100-mg doses, respectively (20 mg, p = .0082; 50 mg, p = .0062; 100 mg, p < .0001). Similarly, a significant effect of beta-methyl-6-chloromelatonin on subjective measures of time to fall asleep occurred (p = .0050), with significant improvement observed at both the 50-mg and 100-mg doses (p = .0350 and .0198, respectively) and a trend toward improvement observed at the 20-mg dose (p = .0582). Adverse events were mild to moderate in severity and did not differ in frequency between beta-methyl-6-chloromelatonin and placebo treatments.
beta-Methyl-6-chloromelatonin significantly decreases both objective and subjective measures of sleep latency in subjects with primary insomnia. Thus, these data suggest that mel-atonin agonists may exert a direct soporific effect, as previous research indicates that beta-methyl-6-chloromelatonin is not associated with changes in body temperature, heart rate, or blood pressure.
虽然已知褪黑素激动剂可调节昼夜睡眠节律,但尚不清楚褪黑素激动剂是否具有直接的催眠作用。有人认为褪黑素的催眠作用是其诱导体温过低能力的继发效应。β-甲基-6-氯褪黑素是一种高亲和力的褪黑素受体激动剂,与体温过低无关。本研究的目的是确定褪黑素激动剂β-甲基-6-氯褪黑素对原发性失眠患者是否具有直接的催眠作用。
对符合《精神疾病诊断与统计手册》第四版修订版(DSM-IV-TR)原发性失眠标准的受试者进行了一项双盲、安慰剂对照、交叉安全性和有效性研究,给予20毫克、50毫克和100毫克的β-甲基-6-氯褪黑素及安慰剂。在84名筛查的受试者中,40名受试者随机接受3种β-甲基-6-氯褪黑素剂量或安慰剂中的每一种,连续两晚各服用一次,每次治疗之间有5天的洗脱期。确定治疗对多导睡眠图和主观测量的睡眠参数、次晨精神运动表现及安全指标的影响。主要结局指标是通过多导睡眠图测量的持续睡眠潜伏期。
观察到β-甲基-6-氯褪黑素对主要疗效变量即持续睡眠潜伏期有显著影响(p = .0003)。与安慰剂相比,20毫克剂量使睡眠潜伏期显著改善31%,而50毫克和100毫克剂量分别使睡眠潜伏期显著改善32%和41%(20毫克,p = .0082;50毫克,p = .0062;100毫克,p < .0001)。同样,β-甲基-6-氯褪黑素对入睡时间的主观测量指标有显著影响(p = .0050),50毫克和100毫克剂量均有显著改善(分别为p = .0350和.0198),20毫克剂量有改善趋势(p = .0582)。不良事件严重程度为轻度至中度,β-甲基-6-氯褪黑素治疗组和安慰剂治疗组在发生频率上无差异。
β-甲基-6-氯褪黑素可显著降低原发性失眠患者睡眠潜伏期的客观和主观测量指标。因此,这些数据表明褪黑素激动剂可能发挥直接的催眠作用,因为先前的研究表明β-甲基-6-氯褪黑素与体温、心率或血压的变化无关。
