Case report of extensive metabolism by aldehyde oxidase in humans: pharmacokinetics and metabolite profile of FK3453 in rats, dogs, and humans

Takafumi Akabane; Kohichiro Tanaka; Megumi Irie; Shigeyuki Terashita; Toshio Teramura

doi:10.3109/00498254.2010.549970

Case report of extensive metabolism by aldehyde oxidase in humans: pharmacokinetics and metabolite profile of FK3453 in rats, dogs, and humans

Xenobiotica. 2011 May;41(5):372-84. doi: 10.3109/00498254.2010.549970. Epub 2011 Mar 9.

Authors

Takafumi Akabane¹, Kohichiro Tanaka, Megumi Irie, Shigeyuki Terashita, Toshio Teramura

Affiliation

¹ Analysis & Pharmacokinetics Research Labs, Discovery Drug Metabolism & Pharmacokinetics, Astellas Pharma Inc., 21 Miyukigaoka, Tsukuba City, Ibaraki, Japan. takafumi.akabane@us.astellas.com

PMID: 21385103
DOI: 10.3109/00498254.2010.549970

Abstract

We describe the preclinical and clinical pharmacokinetic profiles of FK3453 [6-(2-amino-4-phenylpyrimidin-5-yl)-2-isopropylpyridazin-3(2H)-one] and the mechanism responsible for poor oral exposure of FK3453 in humans. FK3453 showed favourable profiles in preclinical pharmacokinetic studies, including satisfactory absolute bioavailability and total body clearance in animals (30.5%-41.4%, 54.7%-68.2%, and 71.3%-93.4% and 10.8-17.6, 1.9-17.1, and 5.0 mL/min/kg in male rats, female rats, and dogs, respectively), and good metabolic stability in liver microsomes (42.3, 14.5, and 1.1 mL/min/kg in male rats, dogs, and humans, respectively). However, despite these promising preclinical findings, plasma concentrations of FK3453 in humans were extremely low, with the oxidative metabolite of the aminopyrimidine moiety (M4) identified as a major metabolite. Given that aldehyde oxidase (AO) and xanthine oxidase (XO) were presumed to be the enzymes responsible for M4 formation, we investigated the mechanism of M4 formation using human liver subcellular fractions. M4 was detected in the incubation mixture with S9 and cytosol but not with microsomes, and M4 formation was inhibited by AO inhibitors (menadione, isovanillin) but not by cytochrome P-450 inhibitor (1-aminobenzotiazole) or XO inhibitor (allopurinol). These results suggest M4 formation is catalyzed by AO, and therefore, its poor exposure in humans was attributed to extensive AO metabolism.

Publication types

Clinical Trial, Phase I

MeSH terms

Administration, Oral
Adult
Aldehyde Oxidase / metabolism*
Animals
Biological Availability
Chromatography, High Pressure Liquid
Cytosol / enzymology
Dogs
Female
Humans
Injections, Intravenous
Liver / metabolism
Male
Metabolic Networks and Pathways
Metabolome*
Protein Binding
Pyridazines / administration & dosage
Pyridazines / metabolism*
Pyridazines / pharmacokinetics*
Pyrimidines / administration & dosage
Pyrimidines / chemistry
Pyrimidines / metabolism*
Pyrimidines / pharmacokinetics*
Rats
Rats, Sprague-Dawley
Subcellular Fractions / metabolism
Time Factors
Young Adult

Substances

FK3453
Pyridazines
Pyrimidines
Aldehyde Oxidase