Horoszok Lucy, Baleeiro Thais, D'Aniello Fabiana, Gropper Savion, Santos Benjamin, Guglietta Antonio, Roth Thomas
R&D Centre, Ferrer Internacional S.A., Barcelona, Spain.
Hum Psychopharmacol. 2014 May;29(3):266-73. doi: 10.1002/hup.2395.
A 5-h phase advance model of insomnia was used to evaluate the efficacy of lorediplon, a new non-benzodiazepine hypnotic.
Thirty-five male, healthy subjects were included in a five-way randomized cross-over study. During each of the periods, sleep was recorded, and residual effects were measured. All subjects received lorediplon 1, 5, and 10 mg, placebo, and zolpidem 10 mg (i.e., active control).
Polysomnographic evaluation revealed that lorediplon (5 and 10 mg) significantly decreased wake after sleep onset (WASO) and increased total sleep time. Analysis by quarters of the night showed a progressive increasing effectiveness of lorediplon 10 mg across the first three quarters. Lorediplon increased non-rapid eye movement slow wave sleep and stage N2 sleep in the second and third quarters. The magnitude of these effects was dose related, with minimal effects seen with 1 mg. No residual effects were observed 13 h post dose.
Lorediplon demonstrated a dose-dependent improvement in sleep, whereas zolpidem showed a more sustained WASO effect. No next-day hangover effects were observed. These sleep effects are also consistent with the pharmacokinetic profile of lorediplon. These results warrant clinical trials in patients with insomnia.
采用失眠的5小时相位提前模型来评估新型非苯二氮䓬类催眠药洛雷地普隆的疗效。
35名健康男性受试者纳入一项五组随机交叉研究。在每个阶段记录睡眠情况,并测量残留效应。所有受试者接受洛雷地普隆1毫克、5毫克和10毫克、安慰剂以及唑吡坦10毫克(即活性对照)。
多导睡眠图评估显示,洛雷地普隆(5毫克和10毫克)显著减少睡眠起始后觉醒时间(WASO)并增加总睡眠时间。按夜间四个时段分析显示,在前三个时段洛雷地普隆10毫克的有效性逐渐增加。洛雷地普隆在第二和第三时段增加非快速眼动慢波睡眠和N2期睡眠。这些效应的程度与剂量相关,1毫克时效应最小。给药后13小时未观察到残留效应。
洛雷地普隆显示出剂量依赖性的睡眠改善,而唑吡坦显示出更持久的WASO效应。未观察到次日宿醉效应。这些睡眠效应也与洛雷地普隆的药代动力学特征一致。这些结果值得在失眠患者中进行临床试验。
