Which bioequivalence study for a racemic drug? Application to milnacipran

Which bioequivalence study for a racemic drug? Application to milnacipran

Milnacipran, a new non tricyclic antidepressant drug, is a racemic mixture (F2207) composed of two enantiomers: F2695 and F2696, both demonstrated to be active. A randomized open label, single-dose latin square study was undertaken in 24 healthy volunteers to compare, based on racemate data, the rel...

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Veröffentlicht in:European journal of drug metabolism and pharmacokinetics 1998-04, Vol.23 (2), p.166-171
Hauptverfasser: DEPREZ, D, CHASSARD D, D, BAILLE P, P, MIGNOT, A, UNG, H. L, PUOZZO, C
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Sprache:eng
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Adult
Antidepressive Agents - pharmacokinetics
Area Under Curve
Biological and medical sciences
Chemistry, Pharmaceutical
Cross-Over Studies
Cyclopropanes - pharmacokinetics
Humans
Male
Medical sciences
Neuropharmacology
Pharmacology. Drug treatments
Psychoanaleptics: cns stimulant, antidepressant agent, nootropic agent, mood stabilizer..., (alzheimer disease)
Psychology. Psychoanalysis. Psychiatry
Psychopharmacology
Stereoisomerism
Therapeutic Equivalency
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container_end_page 171
container_issue 2
container_start_page 166
container_title European journal of drug metabolism and pharmacokinetics
container_volume 23
creator DEPREZ, D
CHASSARD D, D
BAILLE P, P
MIGNOT, A
UNG, H. L
PUOZZO, C
description Milnacipran, a new non tricyclic antidepressant drug, is a racemic mixture (F2207) composed of two enantiomers: F2695 and F2696, both demonstrated to be active. A randomized open label, single-dose latin square study was undertaken in 24 healthy volunteers to compare, based on racemate data, the relative bioavailability of two new formulations to that of a reference formulation. Later on, as suggested by actual regulatory trend, analysis was carried out on enantiomer data, although in a supportive way. Bioequivalence was assessed on calculation of 90% confidence intervals for log-transformed Cmax and AUC(0-infinity) and on Wilcoxon test for Tmax with a 5% level of significance. Based on racemate data, both test formulations were demonstrated to be equivalent to the reference capsule in terms of Cmax and AUC-(0-infinity). Differences in Tmax reached statistical significance, although their mean magnitude was small, and probably not relevant when related to antidepressant long-term therapy. When considering the test capsule - reference capsule comparison, the equivalence demonstrated for the racemate reflect that of each enantiomer. On the contrary, equivalence between the test tablet and the reference capsule demonstrated for the racemate, is not supported by both enantiomers as Cmax of F2696 fails to reach bioequivalence criteria, making more uncertain the conclusion of bioequivalence. From this experience, it seems than when equivalence is demonstrated close to the limits for the racemate, it is difficult, especially for a low variability drug such as milnacipran, to comply with equivalence criteria for both enantiomers.
doi_str_mv 10.1007/BF03189334
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source MEDLINE; SpringerLink Journals - AutoHoldings
subjects Adult
Antidepressive Agents - pharmacokinetics
Area Under Curve
Biological and medical sciences
Chemistry, Pharmaceutical
Cross-Over Studies
Cyclopropanes - pharmacokinetics
Humans
Male
Medical sciences
Neuropharmacology
Pharmacology. Drug treatments
Psychoanaleptics: cns stimulant, antidepressant agent, nootropic agent, mood stabilizer..., (alzheimer disease)
Psychology. Psychoanalysis. Psychiatry
Psychopharmacology
Stereoisomerism
Therapeutic Equivalency
title Which bioequivalence study for a racemic drug? Application to milnacipran
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