Lankford D Alan, Corser Bruce C, Zheng Yan-Ping, Li Zhengrong, Snavely Duane B, Lines Christopher R, Deacon Steve
Sleep Disorders Center of Georgia, Atlanta, GA 30342, USA.
Sleep. 2008 Oct;31(10):1359-70.
To evaluate the efficacy and tolerability of gaboxadol in the treatment of adult and elderly patients with primary insomnia.
Randomized, double-blind, placebo-controlled, multicenter, 30-night, polysomnography studies.
Sleep laboratory.
Primary insomnia, 18-64 y (adult study), or > or =65 y (elderly study).
Adult study: gaboxadol 15 mg (GBX15; N = 148), 10 mg (GBX10; N = 154), or placebo (N = 156); elderly study: GBX10 (N = 157), gaboxadol 5 mg (GBX5; N = 153), or placebo (N=176).
Primary endpoints were wake after sleep onset (WASO) and latency to persistent sleep (LPS). Slow wave sleep (SWS) was a secondary endpoint. Analyses were based on the change from baseline for the average of nights 1/2, and nights 29/30, and compared gaboxadol versus placebo. Exploratory endpoints included patient's subjective assessment of total sleep time (sTST), WASO (sWASO), time to sleep onset (sTSO), and number of awakenings (sNAW); these analyses were based on weekly means. 1) Adult study. GBX15 significantly (P < or = 0.05) improved WASO through nights 29/30 but had no significant effects on LPS. No significant differences were seen for GBX10 versus placebo on WASO or LPS. GBX15 and GBX10 enhanced SWS. GBX15 significantly improved sTST, sWASO, sTSO, and sNAW at weeks 1 and 4. 2) Elderly study. GBX10 significantly improved WASO through nights 29/30; a significant improvement was also seen for GBX5 at nights 1/2 but this was not maintained through nights 29/30. GBX10 significantly improved LPS at nights 1/2 but the improvement was not maintained through nights 29/30; no significant differences were seen for GBX5 versus placebo on LPS. GBX10 and GBX5 enhanced SWS. GBX10 significantly improved sTST at week 1, and sTST, sWASO, and sNAW at week 4. Gaboxadol was generally well tolerated in both studies.
The maximum studied doses of gaboxadol (GBX15 in adult patients and GBX10 in elderly patients) were effective at enhancing objective polysomnography measures of sleep maintenance and SWS, and also some subjective sleep measures, over 30 nights but had little or no effects on sleep onset. The clinical relevance of the enhancement of SWS by gaboxadol is unclear.
评估加波沙朵治疗成人及老年原发性失眠患者的疗效和耐受性。
随机、双盲、安慰剂对照、多中心、为期30晚的多导睡眠图研究。
睡眠实验室。
原发性失眠患者,年龄18 - 64岁(成人研究)或≥65岁(老年研究)。
成人研究:加波沙朵15毫克(GBX15;N = 148)、10毫克(GBX10;N = 154)或安慰剂(N = 156);老年研究:GBX10(N = 157)、加波沙朵5毫克(GBX5;N = 153)或安慰剂(N = 176)。
主要终点为睡眠起始后觉醒时间(WASO)和持续睡眠潜伏期(LPS)。慢波睡眠(SWS)为次要终点。分析基于第1/2晚和第29/30晚平均值相对于基线的变化,并比较加波沙朵与安慰剂。探索性终点包括患者对总睡眠时间(sTST)、WASO(sWASO)、入睡时间(sTSO)和觉醒次数(sNAW)的主观评估;这些分析基于每周平均值。1)成人研究。GBX15在第29/30晚显著(P≤0.05)改善了WASO,但对LPS无显著影响。GBX10与安慰剂在WASO或LPS方面无显著差异。GBX15和GBX10增强了SWS。GBX15在第1周和第4周显著改善了sTST、sWASO、sTSO和sNAW。2)老年研究。GBX10在第29/30晚显著改善了WASO;GBX5在第1/2晚也有显著改善,但在第29/30晚未维持。GBX10在第1/2晚显著改善了LPS,但在第29/30晚未维持;GBX5与安慰剂在LPS方面无显著差异。GBX10和GBX5增强了SWS。GBX10在第1周显著改善了sTST,在第4周显著改善了sTST、sWASO和sNAW。在两项研究中,加波沙朵总体耐受性良好。
加波沙朵的最大研究剂量(成人患者为GBX15,老年患者为GBX10)在30晚内有效增强了睡眠维持和SWS的客观多导睡眠图指标,以及一些主观睡眠指标,但对入睡几乎没有影响。加波沙朵增强SWS的临床相关性尚不清楚。
