TY - JOUR
T1 - Sex differences in the pharmacokinetics and bioequivalence of the delayed-release combination of doxylamine succinate-pyridoxine hydrochloride; Implications for pharmacotherapy in pregnancy
AU - Koren, Gideon
AU - Vranderick, Manon
AU - Gill, Simerpal K.
AU - Macleod, Stuart
PY - 2013/12
Y1 - 2013/12
N2 - Most bioequivalence (BE) studies are conducted in males with the assumption that variability in pharmacokinetics is similar between the sexes. The purpose of this single]center, reference replicate study was to determine the effect of sex on the pharmacokinetics and BE of doxylamine.pyridoxine 10 mg.10 mg delayed-release tablets. Healthy males (n.12) and non-pregnant females (n.12) were administered two tablets, and blood sampling was conducted from 1 hour pre-dose until 72 hours post-dose. After 21 days, dose administration and blood sampling were re-conducted. All analytes were measured using liquid chromatography-tandem mass-spectrometry. Pharmacokinetic parameters were calculated for each study period using standard, non-compartmental methods, and differences were assessed using ANOVA. BE testing was conducted using the relative 90% confidence interval for the AUC0t for each analyte. Females had significantly larger AUC0t for doxylamine, 1,550 ng h/mL (coefficient of variance [CV=19%]) versus 1,272 ng h/ mL (CV=21%; P≤.05), and pyridoxine, 35 ng h/mL, (CV=43%) versus 25 ng h/mL (CV=31%; P≤.05) compared to males. A higher Cmax for doxylamine was observed in females, 107 ng/mL (CV=16%), compared to males, 86 ng/mL (CV=15%) (P≤.05). BE testing did not demonstrate bioequivalence between males and females. Pharmacokinetic differences observed between the sexes have implications for future BE studies using doxylamine.pyridoxine.
AB - Most bioequivalence (BE) studies are conducted in males with the assumption that variability in pharmacokinetics is similar between the sexes. The purpose of this single]center, reference replicate study was to determine the effect of sex on the pharmacokinetics and BE of doxylamine.pyridoxine 10 mg.10 mg delayed-release tablets. Healthy males (n.12) and non-pregnant females (n.12) were administered two tablets, and blood sampling was conducted from 1 hour pre-dose until 72 hours post-dose. After 21 days, dose administration and blood sampling were re-conducted. All analytes were measured using liquid chromatography-tandem mass-spectrometry. Pharmacokinetic parameters were calculated for each study period using standard, non-compartmental methods, and differences were assessed using ANOVA. BE testing was conducted using the relative 90% confidence interval for the AUC0t for each analyte. Females had significantly larger AUC0t for doxylamine, 1,550 ng h/mL (coefficient of variance [CV=19%]) versus 1,272 ng h/ mL (CV=21%; P≤.05), and pyridoxine, 35 ng h/mL, (CV=43%) versus 25 ng h/mL (CV=31%; P≤.05) compared to males. A higher Cmax for doxylamine was observed in females, 107 ng/mL (CV=16%), compared to males, 86 ng/mL (CV=15%) (P≤.05). BE testing did not demonstrate bioequivalence between males and females. Pharmacokinetic differences observed between the sexes have implications for future BE studies using doxylamine.pyridoxine.
KW - Bioequivalence
KW - Diclegis
KW - Doxylamine succinate
KW - Gender differences
KW - Pyridoxal-50 -phosphate
KW - Pyridoxine hydrochloride
UR - http://www.scopus.com/inward/record.url?scp=84892968196&partnerID=8YFLogxK
U2 - 10.1002/jcph.184
DO - 10.1002/jcph.184
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C2 - 24123059
AN - SCOPUS:84892968196
SN - 0091-2700
VL - 53
SP - 1268
EP - 1276
JO - Journal of Clinical Pharmacology
JF - Journal of Clinical Pharmacology
IS - 12
ER -