Agomelatine in pediatric patients with moderate to severe major depressive disorder: an open-label extension study.

IF 6 2区医学 Q1 PEDIATRICS

European Child & Adolescent Psychiatry Pub Date : 2024-10-10 DOI:10.1007/s00787-024-02587-4

Celso Arango, Joerg M Fegert, Françoise Picarel-Blanchot, Ute Marx, Lucie Truffaut-Chalet, Pierre-François Pénélaud, Jan Buitelaar

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Abstract

Major depressive disorder (MDD) in young people is a common psychiatric disorder, but treatment options are limited. Agomelatine has demonstrated short-term efficacy and safety in pediatric patients. We report here the results of a 92-week open-label extension (OLE). The international, multicenter, double-blind, study randomized 400 patients (80 children, 320 adolescents) with moderate-to-severe MDD to one of four treatment groups: agomelatine 10 mg (n = 102), agomelatine 25 mg (n = 95), placebo (n = 103), and fluoxetine 10-20 mg (n = 100). After 12 weeks, patients who could benefit from treatment continuation were offered entry into an optional OLE during which they received agomelatine 10 or 25 mg for a further 92 weeks. A total of 339 patients (271 adolescents) entered the OLE. Treatment groups considered for the OLE analysis reflected those received in the double-blind and OLE periods: agomelatine (10 or 25 mg) in both (ago/ago, n = 170); placebo then agomelatine 10-25 mg (pcb/ago, n = 85); or fluoxetine then agomelatine 10-25 mg (fluox/ago, n = 84). Mean age (± SD) at entry into the double-blind phase (Week 0) was 13.6 ± 2.7 years and 61.9% were female. Mean changes in Children's Depression Rating Scale revised (CDRS-R) raw total score from Week 12 to last post-Week 12 value in the three groups were - 16.3 ± 12.2 (ago/ago), - 18.9 ± 16.1 (pcb/ago), and - 16.1 ± 15.5 (fluox/ago), reflecting the difference in efficacy between treatments during the double-blind period, and heterogeneity at W12 between the treatment groups. Adverse events considered related to treatment occurred in 14.5% of patients: 15.3% ago/ago, 16.5% pcb/ago, and 10.7% fluox/ago. Three patients (all adolescents) experienced treatment-related severe adverse events: two treated with ago/ago and one treated with pcb/ago. Among the adolescents, one treatment-related severe adverse event in a patient in the pcb/ago group led to study withdrawal. Agomelatine was associated with continuous improvement in depressive symptoms without unexpected safety signals. These findings support the safe use of agomelatine in a pediatric population with moderate-to-severe MDD for up to 104 weeks.Trial registration No: EUDRACT No. 2015-002181-23.

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阿戈美拉汀治疗中度至重度重度抑郁症儿科患者：一项开放标签延伸研究。

青少年重度抑郁障碍（MDD）是一种常见的精神疾病，但治疗方法有限。阿戈美拉汀对儿童患者具有短期疗效和安全性。我们在此报告一项为期 92 周的开放标签延长治疗（OLE）的结果。这项国际多中心双盲研究将 400 名中重度 MDD 患者（80 名儿童、320 名青少年）随机分为四组：阿戈美拉汀 10 毫克组（102 人）、阿戈美拉汀 25 毫克组（95 人）、安慰剂组（103 人）和氟西汀 10-20 毫克组（100 人）。12 周后，可从继续治疗中获益的患者可选择参加 OLE，在此期间接受 10 或 25 毫克阿戈美拉汀治疗，为期 92 周。共有 339 名患者（271 名青少年）参加了 OLE。OLE分析所考虑的治疗组反映了在双盲期和OLE期接受的治疗：阿戈美拉汀（10或25毫克）在双盲期和OLE期均接受治疗（前/后，n = 170）；先接受安慰剂治疗，再接受阿戈美拉汀10-25毫克治疗（pcb/后，n = 85）；或先接受氟西汀治疗，再接受阿戈美拉汀10-25毫克治疗（fluox/后，n = 84）。进入双盲阶段（第0周）时的平均年龄（± SD）为13.6±2.7岁，61.9%为女性。儿童抑郁量表修订版（CDRS-R）原始总分从第12周到第12周后最后一次评分的平均变化为- 16.3 ± 12.2（ago/ago）、- 18.9 ± 16.1（pcb/ago）和- 16.1 ± 15.5（fluox/ago），反映了双盲期不同治疗方法之间的疗效差异，以及治疗组之间在第12周时的异质性。14.5%的患者出现了与治疗相关的不良反应：15.3%的患者为前药/前药，16.5%的患者为PCB/前药，10.7%的患者为Fluox/前药。三名患者（均为青少年）出现了与治疗相关的严重不良事件：两名患者接受了ago/ago治疗，一名患者接受了pcb/ago治疗。在青少年患者中，pcb/ago组的一名患者因治疗相关的严重不良事件而退出研究。阿戈美拉汀可持续改善抑郁症状，且无意外安全信号。这些研究结果支持阿戈美拉汀在中重度MDD儿科人群中安全使用长达104周。

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来源期刊

European Child & Adolescent Psychiatry 医学-精神病学

CiteScore

12.80

自引率

4.70%

发文量

186

审稿时长

6-12 weeks

期刊介绍： European Child and Adolescent Psychiatry is Europe''s only peer-reviewed journal entirely devoted to child and adolescent psychiatry. It aims to further a broad understanding of psychopathology in children and adolescents. Empirical research is its foundation, and clinical relevance is its hallmark. European Child and Adolescent Psychiatry welcomes in particular papers covering neuropsychiatry, cognitive neuroscience, genetics, neuroimaging, pharmacology, and related fields of interest. Contributions are encouraged from all around the world.