Efficacy and Safety of Intranasal Esketamine Adjunctive to Oral Antidepressant Therapy in Treatment-Resistant Depression: A Randomized Clinical Trial.
JAMA psychiatry
confidence
Key findings
Intranasal esketamine adjunctive to antidepressants produced rapid, dose-related improvement in TRD; effect sustained >2 months at lower dosing.
View source on PubMed (PMID 29282469) ↗
- Sample size
- 67 randomized; 60 completed double-blind; 126 screened
- Population
- Adults with major depressive disorder and treatment-resistant depression (inadequate response to ≥2 antidepressants)
- Dosing
- Esketamine 28 mg, 56 mg, or 84 mg twice weekly (double-blind), reduced to weekly then every 2 weeks (open-label)
- Duration
- Approximately 4 phases; double-blind days 1-15, open-label days 15-74, 8-week follow-up
- Route
- intranasal
- Blinding
- double_blind
- Controls
- placebo
- Drug class
- NMDA antagonist
Measured endpoints
- Change from baseline to day 8 in MADRS total score (esketamine 28 mg vs placebo)Improvedmental_healthsignificanteffect: -4.2 (SE 2.09)
- Change from baseline to day 8 in MADRS total score (esketamine 56 mg vs placebo)Improvedmental_healthsignificanteffect: -6.3 (SE 2.07)
- Change from baseline to day 8 in MADRS total score (esketamine 84 mg vs placebo)Improvedmental_healthsignificanteffect: -9.0 (SE 2.13)
- Dose-response relationship for MADRS improvementIncreasedmental_healthsignificanteffect: ascending dose-response
- Sustained improvement in depressive symptoms during open-label phaseImprovedmental_healthnot_reportedeffect: -7.2 (SE 1.84)
- Adverse events leading to discontinuation (syncope, headache, dissociative syndrome, ectopic pregnancy)Increasedsafetynot_reportedeffect: 3/56 (5%) esketamine double-blind; 1/57 (2%) open-label vs 0 placebo
Full abstract
Approximately one-third of patients with major depressive disorder (MDD) do not respond to available antidepressants. To assess the efficacy, safety, and dose-response of intranasal esketamine hydrochloride in patients with treatment-resistant depression (TRD). This phase 2, double-blind, doubly randomized, delayed-start, placebo-controlled study was conducted in multiple outpatient referral centers from January 28, 2014, to September 25, 2015. The study consisted of 4 phases: (1) screening, (2) double-blind treatment (days 1-15), composed of two 1-week periods, (3) optional open-label treatment (days 15-74), and (4) posttreatment follow-up (8 weeks). One hundred twenty-six adults with a DSM-IV-TR diagnosis of MDD and history of inadequate response to 2 or more antidepressants (ie, TRD) were screened, 67 were randomized, and 60 completed both double-blind periods. Intent-to-treat analysis was used in evaluation of the findings. In period 1, participants were randomized (3:1:1:1) to placebo (n = 33), esketamine 28 mg (n = 11), 56 mg (n = 11), or 84 mg (n = 12) twice weekly. In period 2, 28 placebo-treated participants with moderate-to-severe symptoms were rerandomized (1:1:1:1) to 1 of the 4 treatment arms; those with mild symptoms continued receiving placebo. Participants continued their existing antidepressant treatment during the study. During the open-label phase, dosing frequency was reduced from twice weekly to weekly, and then to every 2 weeks. The primary efficacy end point was change from baseline to day 8 (each period) in the Montgomery-Åsberg Depression Rating Scale (MADRS) total score. Sixty-seven participants (38 women, mean [SD] age, 44.7 [10.0] years) were included in the efficacy and safety analyses. Change (least squares mean [SE] difference vs placebo) in MADRS total score (both periods combined) in all 3 esketamine groups was superior to placebo (esketamine 28 mg: -4.2 [2.09], P = .02; 56 mg: -6.3 [2.07], P = .001; 84 mg: -9.0 [2.13], P < .001), with a significant ascending dose-response relationship (P < .001). Improvement in depressive symptoms appeared to be sustained (-7.2 [1.84]) despite reduced dosing frequency in the open-label phase. Three of 56 (5%) esketamine-treated participants during the double-blind phase vs none receiving placebo and 1 of 57 participants (2%) during the open-label phase had adverse events that led to study discontinuation (1 event each of syncope, headache, dissociative syndrome, and ectopic pregnancy). In this first clinical study to date of intranasal esketamine for TRD, antidepressant effect was rapid in onset and dose related. Response appeared to persist for more than 2 months with a lower dosing frequency. Results support further investigation in larger trials. clinicaltrials.gov identifier: NCT01998958.