Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment: a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7)

K Martiny; E R Larsen; R W Licht; C T Nielsen; P Damkier; E Refsgaard; M Lunde; B Straasø; E M Christensen; A Lolk; J Holmskov; C H Sørensen; I Brødsgaard; S Z Eftekhari; B B Bendsen; R Klysner; I M Terp; J K Larsen; P Vestergaard; P E Buchholtz; L F Gram; P Bech; Danish University Antidepressant Group (DUAG*)

doi:10.1055/s-0035-1565063

Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment: a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7)

K Martiny, E R Larsen, R W Licht, C T Nielsen, P Damkier, E Refsgaard, M Lunde, B Straasø, E M Christensen, A Lolk, J Holmskov, C H Sørensen, I Brødsgaard, S Z Eftekhari, B B Bendsen, R Klysner, I M Terp, J K Larsen, P Vestergaard, P E BuchholtzL F Gram, P Bech, Danish University Antidepressant Group (DUAG*)

Institut for Klinisk Medicin

5 Citationer (Scopus)

Abstract

Introduction: Electroconvulsive treatment (ECT) is an effective treatment for severe depression but carries a risk of relapse in the following months. Methods: Major depressive disorder patients in a current episode attaining remission from ECT (17-item Hamilton Depression Rating Scale (HAM-D₁₇) score≤9) received randomly escitalopram 10 mg, 20 mg, 30 mg or nortriptyline 100 mg as monotherapies and were followed for 6 months in a multicentre double-blind set-up. Primary endpoint was relapse (HAM-D₁₇≥16). Results: As inclusion rate was low the study was prematurely stopped with only 47 patients randomised (20% of the planned sample size). No statistically significant between-group differences could be detected. When all patients receiving escitalopram were compared with those receiving nortriptyline, a marginal superiority of nortriptyline was found (p=0.08). One third of patients relapsed during the study period, and one third completed. Discussion: Due to small sample size, no valid efficacy inferences could be made. The outcome was poor, probably due to tapering off of non-study psychotropic drugs after randomisation; this has implications for future study designs. ClinicalTrials.gov

Originalsprog	Engelsk
Tidsskrift	Pharmacopsychiatry
Vol/bind	48
Udgave nummer	7
Sider (fra-til)	274-8
Antal sider	5
ISSN	0176-3679
DOI	https://doi.org/10.1055/s-0035-1565063
Status	Udgivet - 3 nov. 2015

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10.1055/s-0035-1565063

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Citationsformater

Martiny, K., Larsen, E. R., Licht, R. W., Nielsen, C. T., Damkier, P., Refsgaard, E., Lunde, M., Straasø, B., Christensen, E. M., Lolk, A., Holmskov, J., Sørensen, C. H., Brødsgaard, I., Eftekhari, S. Z., Bendsen, B. B., Klysner, R., Terp, I. M., Larsen, J. K., Vestergaard, P., ... Danish University Antidepressant Group (DUAG*) (2015). Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment: a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7). Pharmacopsychiatry, 48(7), 274-8. https://doi.org/10.1055/s-0035-1565063

Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment : a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7). / Martiny, K; Larsen, E R; Licht, R W et al.

I: Pharmacopsychiatry, Bind 48, Nr. 7, 03.11.2015, s. 274-8.

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

Martiny, K, Larsen, ER, Licht, RW, Nielsen, CT, Damkier, P, Refsgaard, E, Lunde, M, Straasø, B, Christensen, EM, Lolk, A, Holmskov, J, Sørensen, CH, Brødsgaard, I, Eftekhari, SZ, Bendsen, BB, Klysner, R, Terp, IM, Larsen, JK, Vestergaard, P, Buchholtz, PE, Gram, LF, Bech, P & Danish University Antidepressant Group (DUAG*) 2015, 'Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment: a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7)', Pharmacopsychiatry, bind 48, nr. 7, s. 274-8. https://doi.org/10.1055/s-0035-1565063

Martiny K, Larsen ER, Licht RW, Nielsen CT, Damkier P, Refsgaard E et al. Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment: a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7). Pharmacopsychiatry. 2015 nov. 3;48(7):274-8. doi: 10.1055/s-0035-1565063

Martiny, K ; Larsen, E R ; Licht, R W et al. / Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment : a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7). I: Pharmacopsychiatry. 2015 ; Bind 48, Nr. 7. s. 274-8.

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title = "Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment: a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7)",

abstract = "Introduction: Electroconvulsive treatment (ECT) is an effective treatment for severe depression but carries a risk of relapse in the following months. Methods: Major depressive disorder patients in a current episode attaining remission from ECT (17-item Hamilton Depression Rating Scale (HAM-D17) score≤9) received randomly escitalopram 10 mg, 20 mg, 30 mg or nortriptyline 100 mg as monotherapies and were followed for 6 months in a multicentre double-blind set-up. Primary endpoint was relapse (HAM-D17≥16). Results: As inclusion rate was low the study was prematurely stopped with only 47 patients randomised (20% of the planned sample size). No statistically significant between-group differences could be detected. When all patients receiving escitalopram were compared with those receiving nortriptyline, a marginal superiority of nortriptyline was found (p=0.08). One third of patients relapsed during the study period, and one third completed. Discussion: Due to small sample size, no valid efficacy inferences could be made. The outcome was poor, probably due to tapering off of non-study psychotropic drugs after randomisation; this has implications for future study designs. ClinicalTrials.gov",

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T1 - Relapse Prevention in Major Depressive Disorder After Successful Acute Electroconvulsive Treatment

T2 - a 6-month Double-blind Comparison of Three Fixed Dosages of Escitalopram and a Fixed Dose of Nortriptyline - Lessons from a Failed Randomised Trial of the Danish University Antidepressant Group (DUAG-7)

AU - Martiny, K

AU - Larsen, E R

AU - Licht, R W

AU - Nielsen, C T

AU - Damkier, P

AU - Refsgaard, E

AU - Lunde, M

AU - Straasø, B

AU - Christensen, E M

AU - Lolk, A

AU - Holmskov, J

AU - Sørensen, C H

AU - Brødsgaard, I

AU - Eftekhari, S Z

AU - Bendsen, B B

AU - Klysner, R

AU - Terp, I M

AU - Larsen, J K

AU - Vestergaard, P

AU - Buchholtz, P E

AU - Gram, L F

AU - Bech, P

AU - Danish University Antidepressant Group (DUAG)

PY - 2015/11/3

Y1 - 2015/11/3

N2 - Introduction: Electroconvulsive treatment (ECT) is an effective treatment for severe depression but carries a risk of relapse in the following months. Methods: Major depressive disorder patients in a current episode attaining remission from ECT (17-item Hamilton Depression Rating Scale (HAM-D17) score≤9) received randomly escitalopram 10 mg, 20 mg, 30 mg or nortriptyline 100 mg as monotherapies and were followed for 6 months in a multicentre double-blind set-up. Primary endpoint was relapse (HAM-D17≥16). Results: As inclusion rate was low the study was prematurely stopped with only 47 patients randomised (20% of the planned sample size). No statistically significant between-group differences could be detected. When all patients receiving escitalopram were compared with those receiving nortriptyline, a marginal superiority of nortriptyline was found (p=0.08). One third of patients relapsed during the study period, and one third completed. Discussion: Due to small sample size, no valid efficacy inferences could be made. The outcome was poor, probably due to tapering off of non-study psychotropic drugs after randomisation; this has implications for future study designs. ClinicalTrials.gov

AB - Introduction: Electroconvulsive treatment (ECT) is an effective treatment for severe depression but carries a risk of relapse in the following months. Methods: Major depressive disorder patients in a current episode attaining remission from ECT (17-item Hamilton Depression Rating Scale (HAM-D17) score≤9) received randomly escitalopram 10 mg, 20 mg, 30 mg or nortriptyline 100 mg as monotherapies and were followed for 6 months in a multicentre double-blind set-up. Primary endpoint was relapse (HAM-D17≥16). Results: As inclusion rate was low the study was prematurely stopped with only 47 patients randomised (20% of the planned sample size). No statistically significant between-group differences could be detected. When all patients receiving escitalopram were compared with those receiving nortriptyline, a marginal superiority of nortriptyline was found (p=0.08). One third of patients relapsed during the study period, and one third completed. Discussion: Due to small sample size, no valid efficacy inferences could be made. The outcome was poor, probably due to tapering off of non-study psychotropic drugs after randomisation; this has implications for future study designs. ClinicalTrials.gov

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DO - 10.1055/s-0035-1565063

M3 - Journal article

C2 - 26529118

SN - 0176-3679

VL - 48

SP - 274

EP - 278

JO - Pharmacopsychiatry

JF - Pharmacopsychiatry

IS - 7

ER -