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

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

Publication date: Oct 10, 2024

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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Concepts Keywords
12weeks Adolescent
Female Agomelatine
Fluoxetine Children
Psychiatry Major depressive disorder
Open-label extension
Pediatric

Semantics

Type Source Name
drug DRUGBANK Agomelatine
disease MESH major depressive disorder
disease MESH psychiatric disorder
drug DRUGBANK Fluoxetine
disease MESH Depression
drug DRUGBANK Coenzyme M
disease MESH anxiety disorders
disease MESH Suicide
disease MESH death
disease MESH anxiety
disease MESH COVID 19 pandemic
drug DRUGBANK Sertraline
drug DRUGBANK Escitalopram
drug DRUGBANK Methylenedioxyethamphetamine
drug DRUGBANK Melatonin
drug DRUGBANK Serotonin
disease MESH treatment resistant depression
drug DRUGBANK Trestolone
drug DRUGBANK Aspartame
disease MESH Relapse
drug DRUGBANK Adenosine
disease MESH underweight
disease MESH overweight
disease MESH mood disorders
disease MESH somnolence
disease MESH hypotension
disease MESH suicidal ideations
disease MESH suicide attempt
disease MESH weight gain
disease MESH Nervous system disorders
disease MESH Gastrointestinal disorders
drug DRUGBANK Vilazodone
drug DRUGBANK Somatotropin
disease MESH abnormalities
disease MESH complications
drug DRUGBANK Indoleacetic acid
drug DRUGBANK Ademetionine
disease MESH Autism
disease MESH privacy
drug DRUGBANK Naproxen
drug DRUGBANK Sulfasalazine
disease MESH depressive disorder
disease MESH attention deficit hyperactivity disorder
disease MESH syndrome

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