阿戈美拉汀治疗广泛性焦虑症:一项活性对照和安慰剂对照研究。
Agomelatine in generalized anxiety disorder: an active comparator and placebo-controlled study.
作者信息
Stein Dan J, Ahokas Antti, Márquez Miguel S, Höschl Cyril, Oh Kang Seob, Jarema Marek, Avedisova Alla S, Albarran Cristina, Olivier Valérie
机构信息
University of Cape Town Department of Psychiatry, Groote Schuur Hospital, J-Block, Anzio Rd, Observatory, Cape Town 7925, South Africa
出版信息
J Clin Psychiatry. 2014 Apr;75(4):362-8. doi: 10.4088/JCP.13m08433.
BACKGROUND
Agomelatine was efficacious in reducing symptoms in a short-term placebo-controlled trial in generalized anxiety disorder (GAD) and in preventing relapse in a longer term placebo-controlled study. An additional short-term placebo-controlled study is required by regulatory agencies to confirm the efficacy of agomelatine in GAD.
METHOD
This 12-week, placebo-controlled, double-blind, randomized, parallel group, international, multicenter study was designed to confirm the efficacy of agomelatine 25-50 mg/d in the treatment of patients with a primary DSM-IV-TR diagnosis of GAD. The primary outcome measure was the Hamilton Anxiety Rating Scale (HARS) total score. Assay sensitivity was evaluated by including an escitalopram (10-20 mg/d) group.
SETTINGS
The study was undertaken in 45 clinical centers in Argentina, Czech Republic, Finland, South Korea, Poland, Russia, and Slovakia from April 2010 to July 2011.
RESULTS
One hundred thirty-nine outpatients were included in the agomelatine group, 131 in the placebo group, and 142 in the escitalopram group. Agomelatine significantly reduced mean (SD) HARS total score (agomelatine-placebo difference: 4.71 [1.03], P <.0001) and had significant effects on secondary outcome measures, including psychic and somatic HARS subscales, response rate (estimate [standard error]) (agomelatine-placebo difference: 27.4% [5.9%], P< .0001), remission on the HARS (agomelatine-placebo difference: 16.8% [5.4%], P = .002), Clinical Global Impressions-Severity of Illness scale (CGI-S) (P < .001), functional impairment (P < .0001), and sleep quality (P < .001). Findings were confirmed in the subset of more severely ill patients (HARS total score ≥ 25 with or without CGI-S ≥ 5 at baseline). Agomelatine was well tolerated by patients, with no more adverse events than placebo. Escitalopram was similarly efficacious but was accompanied by a higher incidence of adverse events compared to placebo.
CONCLUSIONS
In clinical practice, agomelatine has at least similar efficacy to that of escitalopram for the short-term treatment of GAD and is well tolerated.
TRIAL REGISTRATION
Controlled-Trials.com identifier: ISRCTN03554974.
背景
在一项针对广泛性焦虑症(GAD)的短期安慰剂对照试验中,阿戈美拉汀在减轻症状方面有效,并且在一项长期安慰剂对照研究中可预防复发。监管机构要求进行另一项短期安慰剂对照研究,以确认阿戈美拉汀在GAD中的疗效。
方法
这项为期12周、安慰剂对照、双盲、随机、平行组、国际多中心研究旨在确认25 - 50mg/d阿戈美拉汀治疗原发性DSM-IV-TR诊断为GAD患者的疗效。主要结局指标是汉密尔顿焦虑量表(HARS)总分。通过纳入艾司西酞普兰(10 - 20mg/d)组评估检测灵敏度。
设置
该研究于2010年4月至2011年7月在阿根廷、捷克共和国、芬兰、韩国、波兰、俄罗斯和斯洛伐克的45个临床中心进行。
结果
阿戈美拉汀组纳入139名门诊患者,安慰剂组131名,艾司西酞普兰组142名。阿戈美拉汀显著降低了HARS总分的均值(标准差)(阿戈美拉汀与安慰剂的差值:4.71[1.03],P <.0001),并且对次要结局指标有显著影响,包括HARS精神和躯体子量表、缓解率(估计值[标准误])(阿戈美拉汀与安慰剂的差值:27.4%[5.9%],P<.0001)、HARS缓解情况(阿戈美拉汀与安慰剂的差值:16.8%[5.4%],P =.002)、临床总体印象-疾病严重程度量表(CGI-S)(P <.001)、功能损害(P <.0001)和睡眠质量(P <.001)。在病情较重的患者亚组(基线时HARS总分≥25,无论CGI-S是否≥5)中也证实了这些结果。患者对阿戈美拉汀耐受性良好,不良事件不比安慰剂多。艾司西酞普兰同样有效,但与安慰剂相比不良事件发生率更高。
结论
在临床实践中,阿戈美拉汀在GAD的短期治疗中至少与艾司西酞普兰有相似的疗效,且耐受性良好。
试验注册
Controlled-Trials.com标识符:ISRCTN03554974。
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