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SPRAVATO® (esketamine)

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Concomitant Use of SPRAVATO and Oral Antidepressants in Treatment-Resistant Depression Phase 3 Short-Term Trials with Adults Aged 18-64

Last Updated: 03/26/2024

SUMMARY

SPRAVATO should be administered in conjunction with an oral antidepressant (AD).¹^-³
In phase 3 clinical trials for treatment-resistant depression (TRD), a newly initiated, open-label, oral AD (one of a choice of 4 oral ADs; serotonin and norepinephrine reuptake inhibitors [SNRIs]: duloxetine, venlafaxine extended-release [XR]; selective serotonin reuptake inhibitors [SSRIs]: escitalopram, sertraline) was used concomitantly with SPRAVATO nasal spray.¹^-³
A post hoc pooled analysis of adults with TRD from the TRANSFORM-1² and TRANSFORM-2¹ studies showed no major differences in Montgomery-Åsberg Depression Rating Scale (MADRS) total score change from baseline to day 28 by the class of AD or individual AD. Response and remission rates were generally similar by AD class and individual AD. For individual AD, the response and remission rate of SPRAVATO + sertraline was lower than with other SPRAVATO+AD groups; however, the difference was not statistically significant.³
Based on the post hoc analysis, the rate of treatment-emergent adverse events (TEAEs) reported in ≥5% of patients in the SSRI and SNRI subgroups of the SPRAVATO+AD groups were 53.7% and 56.5%, respectively. The rate of TEAEs reported in ≥5% of patients in the SSRI and SNRI subgroups of the AD + placebo (PBO) groups were 22.9% and 23.0%, respectively. The incidence of TEAEs was generally similar among the individual ADs; however, higher rates of somnolence, increased blood pressure, and sedation were observed in the SPRAVATO + duloxetine vs other SPRAVATO+AD groups. While anxiety and nausea were reported at higher rates in the SPRAVATO + sertraline group compared with other SPRAVATO+AD groups, these data should be interpreted with caution due to the small sample receiving SPRAVATO + sertraline.³

BACKGROUND

Dosing of Oral Antidepressants

At the start of the double-blind induction phase, a newly initiated, open-label, oral AD was used concomitantly with SPRAVATO or PBO nasal spray. The oral AD was assigned by the investigator from four choices (duloxetine, escitalopram, sertraline, or venlafaxine XR).³

Doses of the oral AD were not to exceed the maximum doses defined in the titration schedule. If higher doses were not tolerated, a down-titration was permitted based on clinical judgment.

Oral Antidepressant Titration Schedule for Open-Label Induction Phase³

	Week 1 (Starting Day 1)	Week 2 (Starting Day 8)	Week 3 (Starting Day 15)	Week 4 (Starting Day 22)
Duloxetine	60 mg^a	60 mg	60 mg	60 mg
Escitalopram	10 mg	20 mg	20 mg	20 mg
Sertraline	50 mg	100 mg	150 mg	150 mg
Venlafaxine XR	75 mg	150 mg	225 mg	225 mg
^aSubjects that have in the past shown increased sensitivity towards selective serotonin reuptake inhibitors (SSRIs)/serotonin and norepinephrine reuptake inhibitors (SNRIs) can, at the discretion of the treating physician, be started on a 30-mg dose and up-titrated into the therapeutic range of 60 mg by the start of week 2.

At the end of the induction phase, the patients were receiving an oral AD to which they had been adherent at or above the minimum therapeutic dosage.¹

In a post hoc analysis of two short-term studies in TRD¹^,², the mean modal daily doses of each oral AD were: duloxetine, 59.6 mg; escitalopram, 17.1 mg; sertraline, 105.8 mg; and venlafaxine, 187.5 mg.³

Clinical data

Adigun et al (2019)³ conducted a post hoc, pooled analysis of two 4-week, double-blind, placebo-controlled studies¹^,² in TRD to examine the impact of individual AD (duloxetine, escitalopram, sertraline, and venlafaxine XR) and AD class (SSRI or SNRI) on the efficacy and safety of SPRAVATO+AD.

Efficacy - Pooled Short-Term Studies (TRD3001 and TRD3002)

MADRS

The SPRAVATO+AD group showed greater improvement from baseline to day 28 in mean MADRS total score compared with the AD+PBO group (-19.9 vs -16.4, respectively; P=0.002). Subgroup analyses in a pooled adult population with TRD from the TRANSFORM-2 (3002) and TRANSFORM-1 (3001) studies showed no significant differences in the change in MADRS total score from baseline to day 28 by the class of AD or individual AD (Figure: Montgomery-Åsberg Depression Rating Scale (MADRS) Total Score: Least Squares Mean Treatment Difference of Change from Baseline to Day 28 by [A] Treatment Group, [B] Antidepressant Class, and [C] Individual Antidepressant [Pooled Studies TRANSFORM-1 AND TRANSFORM-2]).³

Montgomery-Åsberg Depression Rating Scale (MADRS) Total Score: Least Squares Mean Treatment Difference of Change from Baseline to Day 28 by [A] Treatment Group, [B] Antidepressant Class, and [C] Individual Antidepressant [Pooled Studies TRANSFORM-1 AND TRANSFORM-2]³

Abbreviations: AD, antidepressant; BL, baseline; Dul, duloxetine; Esc, escitalopram; ESK, esketamine; LS, least squares; MADRS, Montgomery-Asberg Depression Rating Scale; PBO, placebo; SE, standard error; Sert, sertraline; SNRI, serotonin-norepinephrine reuptake inhibitors; SSRI, selective serotonin reuptake inhibitors; Ven XR, venlafaxine extended-release.

Response and Remission Rates

The proportion of patients who met the criteria for response (≥50% improvement in MADRS total score) at day 28 was greater in the SPRAVATO+AD group compared with the AD+PBO group (58.7% vs 45.2%, respectively; P<0.001). The response rates on day 28 were similar by AD class and individual AD. For individual AD, a lower response rate was observed with SPRAVATO + sertraline; however, the difference was not statistically significant (Figure: Response Rates at Day 28 by [A] Treatment Group, [B] Antidepressant Class, and [C] Individual Antidepressant).

Response Rates at Day 28 by [A] Treatment Group, [B] Antidepressant Class, and [C] Individual Antidepressant³

Abbreviations: AD, antidepressant; Dul, duloxetine; Esc, escitalopram; ESK, esketamine; PBO, placebo; Sert, sertraline; SNRI, serotonin-norepinephrine reuptake inhibitors; SSRI, selective serotonin reuptake inhibitors; Ven XR, venlafaxine extended-release.

Remission (MADRS total score ≤12) rates at day 28 was also greater in the SPRAVATO+AD group compared with the AD+PBO group (42.3% vs 30.8%, respectively; P=0.003). The remission rates at day 28 were similar by AD class and individual AD. For individual ADs, a lower remission rate was observed with SPRAVATO + sertraline; however, the difference was not statistically significant (Figure: Remission Rates at Day 28 by [A] Treatment Group, [B] Antidepressant Class, and [C] Individual Antidepressant).

Remission Rates at Day 28 by [A] Treatment Group, [B] Antidepressant Class, and [C] Individual Antidepressant³

Safety - Pooled Short-Term Studies (TRD3001 and TRD3002)

For the total SPRAVATO group, more patients received an SNRI (61%) compared with an SSRI (39%). The rate of TEAEs reported in ≥5% of patients from the SSRI and SNRI subgroups were 53.7% and 56.5%, respectively, in the SPRAVATO+AD group and 22.9% and 23.0%, respectively, in the AD+PBO group (Table: Most Frequently Reported Treatment-Emergent Adverse Events Reported in ≥5 Patients by Antidepressant Class).³

Most Frequently Reported Treatment-Emergent Adverse Events in ≥5% Patients by Antidepressant Class³

TEAE n (%)	SPRAVATO+AD		AD+PBO
TEAE n (%)	SSRI (n=134)	SNRI (n=209)	SSRI (n=134)	SNRI (n=134)
Nausea	43 (32.1)	54 (25.8)	9 (10.8)	10 (7.2)
Somnolence	18 (13.4)	42 (20.1)	8 (9.6)	12 (8.6)
Anxiety	20 (14.9)	10 (4.8)	3 (3.6)	9 (6.5)
Blood pressure increased	9 (6.7)	21 (10.1)	2 (2.4)	3 (2.2)
Sedation	4 (3.0)	15 (7.2)	1 (1.2)	1 (0.7)
Abbreviations: AD, antidepressant; PBO, placebo; SNRI, serotonin-norepinephrine reuptake inhibitor; SSRI, selective serotonin reuptake inhibitor; TEAE, treatment-emergent adverse event.

The only frequently reported TEAE (5%), which occurred at a higher rate in patients from the SNRI subgroup compared with patients from the SSRI subgroup (difference in incidence of 5%) was somnolence (20.1% vs 13.4%, respectively). Frequently reported TEAEs (5%) which occurred at a higher rate in patients from the SSRI subgroup compared with patients from the SNRI subgroup (difference in incidence of 5%) were nausea (32.1% vs 25.8%, respectively) and anxiety (14.9% vs 4.8%, respectively).

For individual AD, the rate of somnolence, increased blood pressure, and sedation were higher in the SPRAVATO + duloxetine vs other SPRAVATO+AD groups. The incidence of other TEAEs was generally similar among the individual ADs (Table: Most Frequently Reported Treatment-Emergent Adverse Events in 5% Patients by Individual Antidepressant). Anxiety and nausea were reported at higher rates in the SPRAVATO + sertraline group compared with other SPRAVATO+AD groups; however, these data should be interpreted with caution due to the small sample receiving SPRAVATO + sertraline (n=64).

Most Frequently Reported Treatment-Emergent Adverse Events in ≥5% Patients by Individual Antidepressant³

TEAE n (%)	SPRAVATO+AD				AD+PBO
TEAE n (%)	Esc (n=70)	Sert (n=64)	Dul (n=152)	Ven XR (n=57)	Esc (n=41)	Sert (n=41)	Dul (n=105)	Ven XR (n=35)
Nausea	20 (28.6)	23 (35.9)	41 (27.0)	13 (22.8)	5 (12.2)	3 (7.3)	11 (10.5)	0
Somnolence	11 (15.7)	7 (10.9)	34 (22.4)	8 (14.0)	3 (7.3)	5 (12.2)	9 (8.6)	3 (8.6)
Anxiety	6 (8.6)	14 (21.9)	5 (3.3)	5 (8.8)	2 (4.9)	1 (2.4)	6 (5.7)	3 (8.6)
Blood pressure increased	2 (2.9)	7 (10.9)	18 (11.8)	3 (5.3)	1 (2.4)	1 (2.4)	1 (1.0)	2 (5.7)
Sedation	1 (1.4)	3 (4.7)	14 (9.2)	1 (1.8)	0	1 (2.4)	1 (1.0)	0
Abbreviations: AD, antidepressant; Dul, duloxetine; Esc, escitalopram; PBO, placebo; Sert, sertraline; TEAE, treatment-emergent adverse event; Ven XR, venlafaxine extended-release.

Literature Search

A literature search of MEDLINE^®, Embase^®, BIOSIS Previews^®, and Derwent Drug File (and/or other resources, including internal/external databases) pertaining to this topic was conducted on 04 March 2024.

References

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1	Popova V, Daly EJ, Trivedi M, et al. Efficacy and safety of flexibly dosed esketamine nasal spray combined with a newly initiated oral antidepressant in treatment-resistant depression: a randomized double-blind active-controlled study. Am J Psychiatry. 2019;176(6):428-438.
2	Fedgchin M, Trivedi M, Daly EJ, et al. Efficacy and safety of fixed-dose esketamine nasal spray combined with a new oral antidepressant in treatment-resistant depression: results of a randomized, double-blind, active-controlled study (TRANSFORM-1). Int J Neuropsychopharmacol. 2019;22(10):616-630.
3	Adigun M, Sliwa JK, Turkoz I, et al. Impact of concomitant oral antidepressants on the efficacy and safety of esketamine nasal spray in patients with treatment-resistant depression. Poster presented at: US Psych Congress; October 3-6, 2019; San Diego, CA.