Efficacy and Safety of Intranasal Esketamine for the Rapid Reduction of Symptoms of Depression and Suicidality in Patients at Imminent Risk for Suicide: Results of a Double-Blind, Randomized, Placebo-Controlled Study.
The American journal of psychiatry
confidence
Key findings
Intranasal esketamine plus standard-of-care produced rapid improvement in depression and suicidal ideation at 4 and 24 hours, but not at day 25.
View source on PubMed (PMID 29656663) ↗
- Sample size
- 68 participants
- Population
- Depressed patients at imminent risk for suicide
- Dosing
- 84 mg twice weekly
- Duration
- 4 weeks (assessed through day 25)
- Route
- intranasal
- Blinding
- double_blind
- Controls
- placebo
- Drug class
- NMDA antagonist
Measured endpoints
- Change in MADRS score from baseline at 4 hoursImprovedmental_healthsignificanteffect: 0.61 (LS mean difference=-5.3, SE=2.10)
- Change in MADRS score from baseline at 24 hoursImprovedmental_healthsignificanteffect: 0.65 (LS mean difference=-7.2, SE=2.85)
- Change in MADRS score from baseline at day 25No changemental_healthnot_significanteffect: 0.35 (LS mean difference=-4.5, SE=3.14)
- MADRS suicidal thoughts item score at 4 hoursImprovedmental_healthsignificanteffect: 0.67
- MADRS suicidal thoughts item score at 24 hoursNo changemental_healthnot_significanteffect: 0.35
- MADRS suicidal thoughts item score at day 25No changemental_healthnot_significanteffect: 0.29
- Clinician global judgment of suicide riskNo changemental_healthnot_significant
- Adverse events (nausea, dizziness, dissociation, unpleasant taste, headache)Increasedsafetynot_reported
Full abstract
The authors compared the efficacy of standard-of-care treatment plus intranasal esketamine or placebo for rapid reduction of symptoms of major depression, including suicidality, among individuals at imminent suicide risk. In a double-blind, multicenter, proof-of-concept study, 68 participants were randomly assigned to receive esketamine (84 mg) or placebo twice weekly for 4 weeks, in addition to comprehensive standard-of-care treatment. The primary efficacy endpoint was change in score from baseline to 4 hours after initial dose on the Montgomery-Åsberg Depression Rating Scale (MADRS). Clinician global judgment of suicide risk (from the Suicide Ideation and Behavior Assessment Tool) was also assessed. Secondary endpoints included these measures at 24 hours and double-blind endpoint at day 25. A significantly greater improvement in MADRS score was observed in the esketamine group compared with the placebo group at 4 hours (least-square mean difference=-5.3, SE=2.10; effect size=0.61) and at ∼24 hours (least-square mean difference=-7.2, SE=2.85; effect size=0.65), but not at day 25 (least-square mean difference=-4.5, SE=3.14; effect size=0.35). Significantly greater improvement was also observed in the esketamine group on the MADRS suicidal thoughts item score at 4 hours (effect size=0.67), but not at 24 hours (effect size=0.35) or at day 25 (effect size=0.29). Between-group reductions in clinician global judgment of suicide risk scores were not statistically different at any time point. The most common adverse events among participants in the esketamine group were nausea, dizziness, dissociation, unpleasant taste, and headache. These preliminary findings indicate that intranasal esketamine compared with placebo, given in addition to comprehensive standard-of-care treatment, may result in significantly rapid improvement in depressive symptoms, including some measures of suicidal ideation, among depressed patients at imminent risk for suicide.