A randomized, crossover comparison of ketamine and electroconvulsive therapy for treatment of major depressive episodes: a Canadian biomarker integration network in depression (CAN-BIND) study protocol.
Biomarkers
Bipolar disorder
Clinical trial
Depression
Electroconvulsive therapy
Genomics
Intravenous ketamine
Major depressive disorder
Neuroimaging
Journal
BMC psychiatry
ISSN: 1471-244X
Titre abrégé: BMC Psychiatry
Pays: England
ID NLM: 100968559
Informations de publication
Date de publication:
02 06 2020
02 06 2020
Historique:
received:
19
12
2019
accepted:
18
05
2020
entrez:
4
6
2020
pubmed:
4
6
2020
medline:
3
11
2020
Statut:
epublish
Résumé
Recent evidence underscores the utility of rapid-acting antidepressant interventions, such as ketamine, in alleviating symptoms of major depressive episodes (MDE). However, to date, there have been limited head-to-head comparisons of intravenous (IV) ketamine infusions with other antidepressant treatment strategies in large randomized trials. This study protocol describes an ongoing multi-centre, prospective, randomized, crossover, non-inferiority trial comparing acute treatment of individuals meeting diagnostic criteria for a major depressive episode (MDE) with ketamine and electroconvulsive therapy (ECT) on efficacy, speed of therapeutic effects, side effects, and health care resource utilization. A secondary aim is to compare a 6-month maintenance strategy for ketamine responders to standard of care ECT maintenance. Finally, through the measurement of clinical, cognitive, neuroimaging, and molecular markers we aim to establish predictors and moderators of treatment response as well as treatment-elicited effects on these outcomes. Across four participating Canadian institutions, 240 patients with major depressive disorder or bipolar disorder experiencing a MDE are randomized (1:1) to a course of ECT or racemic IV ketamine (0.5 mg/kg) administered 3 times/week for 3 or 4 weeks. Non-responders (< 50% improvement in Montgomery-Åsberg Depression Rating Scale [MADRS] scores) crossover to receive the alternate treatment. Responders during the randomization or crossover phases then enter the 6-month maintenance phase during which time they receive clinical assessments at identical intervals regardless of treatment arm. ECT maintenance follows standard of care while ketamine maintenance involves: weekly infusions for 1 month, then bi-weekly infusions for 2 months, and finally monthly infusions for 3 months (returning to bi-weekly in case of relapse). The primary outcome measure is change in MADRS scores after randomized treatment as assessed by raters blind to treatment modality. This multi-centre study will help identify molecular, imaging, and clinical characteristics of patients with treatment-resistant and/or severe MDEs who would benefit most from either type of therapeutic strategy. In addition to informing clinical practice and influencing health care delivery, this trial will add to the robust platform and database of CAN-BIND studies for future research and biomarker discovery. ClinicalTrials.gov identifier NCT03674671. Registered September 17, 2018.
Sections du résumé
BACKGROUND
Recent evidence underscores the utility of rapid-acting antidepressant interventions, such as ketamine, in alleviating symptoms of major depressive episodes (MDE). However, to date, there have been limited head-to-head comparisons of intravenous (IV) ketamine infusions with other antidepressant treatment strategies in large randomized trials. This study protocol describes an ongoing multi-centre, prospective, randomized, crossover, non-inferiority trial comparing acute treatment of individuals meeting diagnostic criteria for a major depressive episode (MDE) with ketamine and electroconvulsive therapy (ECT) on efficacy, speed of therapeutic effects, side effects, and health care resource utilization. A secondary aim is to compare a 6-month maintenance strategy for ketamine responders to standard of care ECT maintenance. Finally, through the measurement of clinical, cognitive, neuroimaging, and molecular markers we aim to establish predictors and moderators of treatment response as well as treatment-elicited effects on these outcomes.
METHODS
Across four participating Canadian institutions, 240 patients with major depressive disorder or bipolar disorder experiencing a MDE are randomized (1:1) to a course of ECT or racemic IV ketamine (0.5 mg/kg) administered 3 times/week for 3 or 4 weeks. Non-responders (< 50% improvement in Montgomery-Åsberg Depression Rating Scale [MADRS] scores) crossover to receive the alternate treatment. Responders during the randomization or crossover phases then enter the 6-month maintenance phase during which time they receive clinical assessments at identical intervals regardless of treatment arm. ECT maintenance follows standard of care while ketamine maintenance involves: weekly infusions for 1 month, then bi-weekly infusions for 2 months, and finally monthly infusions for 3 months (returning to bi-weekly in case of relapse). The primary outcome measure is change in MADRS scores after randomized treatment as assessed by raters blind to treatment modality.
DISCUSSION
This multi-centre study will help identify molecular, imaging, and clinical characteristics of patients with treatment-resistant and/or severe MDEs who would benefit most from either type of therapeutic strategy. In addition to informing clinical practice and influencing health care delivery, this trial will add to the robust platform and database of CAN-BIND studies for future research and biomarker discovery.
TRIAL REGISTRATION
ClinicalTrials.gov identifier NCT03674671. Registered September 17, 2018.
Identifiants
pubmed: 32487236
doi: 10.1186/s12888-020-02672-3
pii: 10.1186/s12888-020-02672-3
pmc: PMC7265624
doi:
Substances chimiques
Biomarkers
0
Ketamine
690G0D6V8H
Banques de données
ClinicalTrials.gov
['NCT03674671']
Types de publication
Clinical Trial Protocol
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
268Subventions
Organisme : Ontario Brain Institute
ID : NA
Pays : International
Références
J Clin Psychiatry. 1998;59 Suppl 20:22-33;quiz 34-57
pubmed: 9881538
Br J Psychiatry. 2008 Jan;192(1):52-8
pubmed: 18174510
Schizophr Bull. 2009 Jan;35(1):15-8
pubmed: 19023124
Am J Geriatr Psychiatry. 2012 Jan;20(1):5-17
pubmed: 22183009
Eur J Clin Pharmacol. 2012 Jun;68(6):979-86
pubmed: 22286159
Arch Gen Psychiatry. 2003 Mar;60(3):261-9
pubmed: 12622659
Br J Psychiatry. 1979 Apr;134:382-9
pubmed: 444788
Arch Ital Biol. 2010 Sep;148(3):207-17
pubmed: 21175009
Pharmacol Rev. 2018 Jul;70(3):621-660
pubmed: 29945898
Am J Psychiatry. 2015 Oct;172(10):950-66
pubmed: 26423481
Psychiatry Res. 2014 Feb 28;215(2):355-61
pubmed: 24374115
Aust J Physiother. 2007;53(3):208
pubmed: 17899676
JAMA Psychiatry. 2019 Jun 5;:
pubmed: 31166571
Biol Psychiatry. 2012 Jun 1;71(11):939-46
pubmed: 22297150
J Psychiatry Neurosci. 2019 Oct 01;44(6):384-385
pubmed: 31573153
Contemp Clin Trials. 2019 Feb;77:19-26
pubmed: 30572160
J Biomed Inform. 2009 Apr;42(2):377-81
pubmed: 18929686
Arch Intern Med. 2006 May 22;166(10):1092-7
pubmed: 16717171
Arch Gen Psychiatry. 2002 Jun;59(6):530-7
pubmed: 12044195
J Clin Psychiatry. 2001;62 Suppl 16:10-7
pubmed: 11480879
Transl Psychiatry. 2019 Apr 3;9(1):127
pubmed: 30944309
Appl Neuropsychol. 2009 Oct;16(4):254-61
pubmed: 20183180
Am J Psychiatry. 2011 Dec;168(12):1266-77
pubmed: 22193671
Curr Pharm Des. 2012;18(36):5976-89
pubmed: 22681173
Can J Psychiatry. 2002 Mar;47(2):174-80
pubmed: 11926080
Biol Psychiatry. 2013 Aug 15;74(4):250-6
pubmed: 22840761
Am J Psychiatry. 2019 May 1;176(5):401-409
pubmed: 30922101
Psychol Med. 2016 May;46(7):1459-72
pubmed: 26867988
Adv Biomed Res. 2019 Apr 10;8:25
pubmed: 31123668
BMC Bioinformatics. 2011 Mar 09;12:71
pubmed: 21385461
J Clin Psychiatry. 2015 Oct;76(10):1374-84
pubmed: 26528644
J Psychiatr Res. 2018 Nov;106:61-68
pubmed: 30278319
Br J Psychiatry. 1978 Nov;133:429-35
pubmed: 728692
Neuropsychopharmacology. 2020 Mar;45(4):606-612
pubmed: 31759333
Occup Med (Lond). 2015 Dec;65(9):764-5
pubmed: 26644445
J Clin Psychiatry. 2019 Feb 5;80(2):
pubmed: 30840787
J Psychiatry Neurosci. 2019 Mar 06;44(4):223-236
pubmed: 30840428
J Affect Disord. 2014 Feb;155:123-9
pubmed: 24268616
Psychopharmacol Bull. 1993;29(2):321-6
pubmed: 8290681
Science. 2012 Oct 5;338(6103):68-72
pubmed: 23042884
Am J Psychiatry. 2016 Nov 1;173(11):1101-1109
pubmed: 27418379
Am J Psychiatry. 2006 Jan;163(1):28-40
pubmed: 16390886
J Clin Psychopharmacol. 2015 Jun;35(3):334-6
pubmed: 25928701
Neuropsychobiology. 2011;64(3):129-40
pubmed: 21811083
Biol Psychiatry. 2000 Feb 15;47(4):351-4
pubmed: 10686270
J Magn Reson Imaging. 2012 Jul;36(1):39-54
pubmed: 22314879
Can J Psychiatry. 2016 Sep;61(9):561-75
pubmed: 27486154
J Gen Intern Med. 2001 Sep;16(9):606-13
pubmed: 11556941
Psychiatry Res. 2015 Sep 30;229(1-2):109-19
pubmed: 26250147
BMC Psychiatry. 2016 Apr 16;16:105
pubmed: 27084692