Controlled Comparison of Milnacipran and Fluoxetine in Major Depression

[en] The efficacy and the tolerance of milnacipran (100 mg/day), a second generation antidepressant which equipotently inhibits both noradrenaline and serotonin reuptake, was compared to fluoxetine (20 mg/day), a selective serotonin reuptake inhibitor, in two parallel groups of, respectively, 97 and 93 major depressive outpatients. The duration of the study was 6 weeks, with assessments every 2 weeks by means of the Montgomery and Asberg depression scale (MADRS), the Hamilton depression scale, the clinical global impressions (CGI), and a checklist of symptoms and side-effects. Results showed significant superiority of fluoxetine over milnacipran on most rating instruments: MADRS (P = 0.01) including five individual items, Hamilton depression scale (P = 0.002) including ten individual items, CGI of severity (P = 0.01) and therapeutical index (P = 0.002). On visual analogue scales assessing the clinical profile of the compounds, fluoxetine was rated as exhibiting more psychostimulating activity than milnacipran (P = 0.0008). The tolerance of the two antidepressants was very similar, with the exception of symptoms of dizziness which were more frequently reported with milnacipran (P = 0.01). These differences in efficacy favoring fluoxetine could result from the selection of a dose of milnacipran below the optimal therapeutic dose for this type of psychiatric patients or to the administration of the compounds in single daily intakes, whereas milnacipran possesses a plasma elimination half-life of only 7 h.

Disciplines :

Treatment & clinical psychology
Psychiatry

Author, co-author :

Ansseau, Marc ; Université de Liège - ULiège > Département des sciences cliniques > Psychiatrie et psychologie médicale

Papart, Patrick ; Université de Liège - ULiège > Département des sciences cliniques > Psycho. quantitative - Psychiatrie légale et sociale

Troisfontaines, Benoît ; Université de Liège - ULiège

Bartholome, F.

Bataille, Michel

Charles, G.

Schittecatte, M.

Darimont, Philippe

Devoitille, J. M.

De Wilde, J.

Language :

English

Title :

Controlled Comparison of Milnacipran and Fluoxetine in Major Depression

Publication date :

February 1994

Journal title :

Psychopharmacology

ISSN :

0033-3158

eISSN :

1432-2072

Publisher :

Springer, Germany

Volume :

114

Issue :

Pages :

131-7

Peer reviewed :

Peer Reviewed verified by ORBi

Available on ORBi :

since 15 December 2020

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Bibliography

.
Ansseau M. (1992) The Atlantic gap: clinical trials in Europe and the United States. Biol Psychiatry 31:109-111.
Ansseau M., Diricq, Bataille M., Breulet M., Cerfontaine J.L., Collard J., Coûteaux F., Dufrasne M., Fraipont J., Gernay P., Troisfontaines B., Bobon D. (1985) Une physionomie comparée originale de l'activité clinique des antidépresseurs. Acta Psychiatr Belg 85:644-661.
Ansseau M., Bataille M., Bobon D., Cerfontaine J.L., Charles G., Coûteaux F., Diricq, Fraipont J., Gernay P., Troisfontaines B. (1988) Evaluation de l'activité clinique de la fluoxétine (Prozac) selon “les étoiles de Liège”. Acta Psychiatr Belg 88:127-137.
Ansseau M., von Frenckell R., Mertens C., De Wilde J., Botte L., Devoitille J.M., Evrard J.L., De Nayer A., Darimont P., Dejaiffe G., Mirel J., Meurice E., Parent M., Couzinier J.P., Demarez J.P., Serre C. (1989) Controlled comparison of two doses of milnacipran (F 2207) and amitriptyline in major depressive inpatients. Psychopharmacology 98:163-168.
Ansseau M., von Frenckell R., Papart P., Mertens C., De Wilde J., Botte L., Devoitille J.M., Evrard J.L., De Nayer A., Koch-Bourdouxhe S., Darimont P., Lecoq A., Mirel J., Couzinier J.P., Demarez J.P., Serre C. (1989) Controlled comparison of milnacipran (F 2207) 200 mg and amitriptyline in endogenous depressive inpatients. Hum Psychopharmacol 4:221-227.
Ansseau M., von Frenckell R., Gérard M.A., Mertens C., De Wilde J., Botte L., Devoitille J.M., Evrard J.L., De Nayer A., Darimont P., Mirel J., Troisfontaines B., Toussaint C., Couzinier J.P., Demarez J.P., Serre C. (1991) Interest of a loading dose of milnacipran in endogenous depressive inpatients: comparison with the standard regimen and with fluvoxamine. Eur Neuropsychopharmacol 1:113-121.
Benfield P., Ward A. (1986) Fluvoxamine: a review of its pharmacodynamic and pharmacokinetic properties, and therapeutic eficacy in depressive illness. Drugs 32:313-334.
Benfield P., Heel R.C., Lewis S.P. (1986) Fluoxetine: a review of its pharmacodynamic and pharmacokinetic properties, and therapeutic efficacy in depressive illness. Drugs 32:481-508.
Clerc G., Pagot R., Bouchard J.M., Oules J., Guibert M., Amicot M., Guillard A., Cottin M., Dachary J.M., Bezoury J.P., Parmentier G., Gresle P., von Frenckell R., Serre C. (1990) Intérêt thérapeutique du milnacipran et de la clomipramine au cours d'un traitement de 3 mois: résultats d'un essai comparatif. Psychiatr Psychobiol 5:137-146.
Covi L., Lipman R., McNair D.M., Czerlinski T. (1979) Symptomatic volunteers in multicenter drug trials. Prog Neuropsychopharmacol 3:521-533.
ECDEU Assessment manual for psychopharmacology (revised), W., Guy, National Institute of Mental Health, Psychopharmacology Research Branch, Rockville, MD; 1976.
Hamilton M. (1960) A rating scale for depression. J Neurol Neurosurg Psychiatry 12:56-62.
Macher J.P., Sichel J.P., Serre C., von Frenckell R., Huck J.C., Demarez J.P. (1989) Double-blind placebo-controlled study of milnacipran in hospitalized patients with major depressive disorders. Neuropsychobiology 22:77-82.
Mathieu M. New drug development: a regulatory overview, Parexel, Cambridge, MA; 1990.
.
Montgomery A., Asberg M. (1979) A new depression scale designed to be sensitive to change. Br J Psychiatry 134:382-389.
Moret C., Charveron M., Finberg J.P.M., Couzinier J.P., Briley M. (1985) Biochemical profile of midlacipran (F 2207), 1-phenyl-1-diethyl-aminocarbonyl-2-aminomethyl-cyclopropane (Z) hydrochloride, a potential fourth generation antidepressant drug. Neuropharmacology 24:1211-1219.
Puozzo C., Filaquier C., Briley M. (1985) Plasma levels of F 2207, midalcipran, a novel antidepressant, after single oral administration in volunteers. Br J Clin Pharmacol 20:291-292.
Raskin A., Schulterbrandt J., Reatig N., Rice C.E. (1967) Factors of psychopathology in interview, ward behavior and self-report ratings of hospitalized depressions. J Consult Psychol 31:270-278.
Schwartz D. L'essai thérapeutique chez l'homme, Flammarion, Paris; 1970.
Solles A., Serre C., Sutet P., Briley M. (1991) Milnacipran: a potent antidepressant with combined NA and 5-HT mechanism of action. Biological markers of depression: state of the art , M., Ansseau, R., von Frenckell, G., Franck, Excerpta Medica, Amsterdam; 197-202.
Van Praag H.M. (1980) Central monoamine metabolism in depressions. I. Serotonin and related compounds. Compr Psychiatry 21:30-43.
Van Praag H.M. (1980) Central monoamine metabolism in depressions. ll. Catecholamines and related compounds. Compr Psychiatry 21:44-54.
Van Praag H.M. (1984) Studies in the mechanism of action of serotonin precursors in depression. Psychopharmacol Bull 20:599-602.
von Frenckell R., Ansseau M., Serre C., Sutet P. (1990) Pooling two controlled comparisons of milnacipran (F 2207) and amitriptyline in endogenous inpatients. Int Clin Psychopharmacol 5:49-56.
.