Duke University School of Medicine, Durham, NC 27710, USA.
Sleep. 2010 Nov;33(11):1553-61. doi: 10.1093/sleep/33.11.1553.
to evaluate the efficacy and safety of doxepin 1 mg and 3 mg in elderly subjects with chronic primary insomnia.
the study was a randomized, double-blind, parallel-group, placebo-controlled trial. Subjects meeting DSM-IV-TR criteria for primary insomnia were randomized to 12 weeks of nightly treatment with doxepin (DXP) 1 mg (n = 77) or 3 mg (n = 82), or placebo (PBO; n = 81). Efficacy was assessed using polysomnography (PSG), patient reports, and clinician ratings. Objective efficacy data are reported for Nights (N) 1, 29, and 85; subjective efficacy data during Weeks 1, 4, and 12; and Clinical Global Impression (CGI) scale and Patient Global Impression (PGI) scale data after Weeks 2, 4, and 12 of treatment. Safety assessments were conducted throughout the study.
DXP 3 mg led to significant improvement versus PBO on N1 in wake time after sleep onset (WASO; P < 0.0001; primary endpoint), total sleep time (TST; P < 0.0001), overall sleep efficiency (SE; P < 0.0001), SE in the last quarter of the night (P < 0.0001), and SE in Hour 8 (P < 0.0001). These improvements were sustained at N85 for all variables, with significance maintained for WASO, TST, overall SE, and SE in the last quarter of the night. DXP 3 mg significantly improved patient-reported latency to sleep onset (Weeks 1, 4, and 12), subjective TST (Weeks 1, 4, and 12), and sleep quality (Weeks 1, 4, and 12). Several global outcome-related variables were significantly improved, including the severity and improvement items of the CGI (Weeks 2, 4, and 12), and all 5 items of the PGI (Week 12; 4 items after Weeks 2 and 4). Significant improvements were observed for DXP 1 mg for several measures including WASO, TST, overall SE, and SE in the last quarter of the night at several time points. Rates of discontinuation were low, and the safety profiles were comparable across the 3 treatment groups. There were no significant next-day residual effects; additionally, there were no reports of memory impairment, complex sleep behaviors, anticholinergic effects, weight gain, or increased appetite.
DXP 1 mg and 3 mg administered nightly to elderly chronic insomnia patients for 12 weeks resulted in significant and sustained improvements in most endpoints. These improvements were not accompanied by evidence of next-day residual sedation or other significant adverse effects. DXP also demonstrated improvements in both patient- and physician-based ratings of global insomnia outcome. The efficacy of DXP at the doses used in this study is noteworthy with respect to sleep maintenance and early morning awakenings given that these are the primary sleep complaints of the elderly. This study, the longest placebo-controlled, double-blind, polysomnographic trial of nightly pharmacotherapy for insomnia in the elderly, provides the best evidence to date of the sustained efficacy and safety of an insomnia medication in older adults.
评估多塞平 1mg 和 3mg 在患有慢性原发性失眠的老年患者中的疗效和安全性。
这是一项随机、双盲、平行组、安慰剂对照试验。符合 DSM-IV-TR 原发性失眠标准的受试者被随机分配至每晚接受多塞平(DXP)1mg(n=77)或 3mg(n=82)或安慰剂(PBO;n=81)治疗 12 周。使用多导睡眠图(PSG)、患者报告和临床医生评分评估疗效。客观疗效数据报告了第 1、29 和 85 夜;主观疗效数据在第 1、4 和 12 周;以及治疗后第 2、4 和 12 周的临床总体印象(CGI)量表和患者总体印象(PGI)量表数据。在整个研究过程中进行安全性评估。
与 PBO 相比,DXP 3mg 在第 1 夜的睡眠潜伏期后觉醒时间(WASO;P<0.0001;主要终点)、总睡眠时间(TST;P<0.0001)、总睡眠效率(SE;P<0.0001)、夜间最后四分之一时间的 SE(P<0.0001)和第 8 小时的 SE(P<0.0001)方面均有显著改善。在第 85 夜,所有变量均保持持续改善,WASO、TST、总 SE 和夜间最后四分之一时间的 SE 均保持显著。DXP 3mg 显著改善了患者报告的入睡潜伏期(第 1、4 和 12 周)、主观 TST(第 1、4 和 12 周)和睡眠质量(第 1、4 和 12 周)。几个与整体结果相关的变量也得到显著改善,包括 CGI 的严重程度和改善项目(第 2、4 和 12 周)以及 PGI 的所有 5 个项目(第 12 周;第 2 和 4 周后 4 个项目)。DXP 1mg 在几个指标上也观察到了显著改善,包括 WASO、TST、总 SE 和夜间最后四分之一时间的 SE,这些指标在几个时间点均有改善。停药率较低,3 个治疗组的安全性特征相似。无明显次日残留效应;此外,无记忆障碍、复杂睡眠行为、抗胆碱能作用、体重增加或食欲增加的报告。
多塞平 1mg 和 3mg 每晚一次给予老年慢性失眠症患者 12 周,可显著且持续改善大多数终点。这些改善没有伴随次日残留镇静或其他显著不良反应的证据。DXP 还改善了基于患者和医生的整体失眠症结果评估。鉴于老年人的主要睡眠抱怨是维持睡眠和清晨早醒,因此在这项研究中,使用的剂量的多塞平的疗效在睡眠维持和清晨早醒方面值得关注。这项最长时间的安慰剂对照、双盲、多导睡眠图试验为老年人失眠症的夜间药物治疗提供了迄今为止最好的证据,证明了老年人群中失眠药物的持续疗效和安全性。
