Effects of Ketoconazole on the In Vivo Biotransformation and Hepatobiliary Transport of the Thrombin Inhibitor AZD0837 in Pigs

Effects of Ketoconazole on the In Vivo Biotransformation and Hepatobiliary Transport of the Thrombin Inhibitor AZD0837 in Pigs

Ketoconazole has been shown in clinical trials to increase the plasma exposure of the oral anticoagulant prodrug AZD0837 [(2S)-N-{4- [(Z)-amino(methoxyimino)methyl]benzyl}-1-{(2R)-2-[3-chloro-5-(difluoromethoxy)phenyl]-2-hydroxyethanoyl}-azetidine-2-carboxamide] and its active metabolite, AR-H067637...

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Veröffentlicht in:Drug metabolism and disposition 2011-02, Vol.39 (2), p.239-246
Hauptverfasser: MATSSON, Elin M, PALM, Johan E, ERIKSSON, Ulf G, BOTTNER, Pernilla, LUNDAHL, Anna, KNUTSON, Lars, LENNERNÄS, Hans
Format: Artikel
Sprache:eng
Schlagworte:
Amidines - administration & dosage
Amidines - blood
Amidines - pharmacokinetics
Amidines - pharmacology
Animals
Antithrombins - administration & dosage
Antithrombins - blood
Antithrombins - pharmacokinetics
Antithrombins - pharmacology
AZD0837
Azetidines - administration & dosage
Azetidines - blood
Azetidines - pharmacokinetics
Azetidines - pharmacology
Bile - metabolism
biliary clearance
Biological and medical sciences
Biological Transport - drug effects
Biotransformation
direct thrombin inhibitors
Drug Interactions
drug-drug interaction
FARMACI
hepatobiliary transport
Intestines - metabolism
ketoconazole
Ketoconazole - administration & dosage
Ketoconazole - pharmacology
Liver - metabolism
Male
Medical sciences
Molecular Structure
Perfusion
Pharmacology. Drug treatments
PHARMACY
Swine
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Zusammenfassung:Ketoconazole has been shown in clinical trials to increase the plasma exposure of the oral anticoagulant prodrug AZD0837 [(2S)-N-{4- [(Z)-amino(methoxyimino)methyl]benzyl}-1-{(2R)-2-[3-chloro-5-(difluoromethoxy)phenyl]-2-hydroxyethanoyl}-azetidine-2-carboxamide] and its active metabolite, AR-H067637 [(2S)-N-{4-[amino(imino)methyl]benzyl}-1-{(2R)-2-[3-chloro-5-(difluoromethoxy)phenyl]-2-hydroxyethanoyl}-azetidine-2-carboxamide]. To investigate the biotransformation of AZD0837 and the effect of ketoconazole on this process, we used an experimental model in pigs that allows repeated sampling from three blood vessels, the bile duct, and a perfused intestinal segment. The pigs received AZD0837 (500 mg) given enterally either alone (n = 5) or together with single-dose ketoconazole (600 mg) (n = 6). The prodrug (n = 2) and its active metabolite (n = 2) were also administered intravenously to provide reference doses. The plasma data revealed considerable interindividual variation in the exposure of the prodrug, intermediate metabolite, and active metabolite. However, AR-H067637 was detected at very high concentrations in the bile with low variability (Ae(bile) = 53 ± 6% of the enteral dose), showing that the compound had indeed been formed in all of the animals and efficiently transported into the bile canaliculi. Concomitant dosing with ketoconazole increased the area under the plasma concentration-time curve for AZD0837 (by 99%) and for AR-H067637 (by 51%). The effect on the prodrug most likely arose from inhibited CYP3A-mediated metabolism. Reduced metabolism also seemed to explain the increased plasma exposure of the active compound because ketoconazole prolonged the terminal half-life with no apparent effect on the extensive biliary excretion and biliary clearance. These in vivo results were supported by in vitro depletion experiments for AR-H067637 in pig liver microsomes with and without the addition of ketoconazole.
ISSN:0090-9556
1521-009X
1521-009X
DOI:10.1124/dmd.110.035022