Statements in which the resource exists as a subject.
PredicateObject
rdf:type
lifeskim:mentions
pubmed:issue
8
pubmed:dateCreated
2009-7-20
pubmed:abstractText
The metabolism and disposition of [(14)C]apixaban, a potent, reversible, and direct inhibitor of coagulation factor Xa, were investigated in mice, rats, rabbits, dogs, and humans after a single oral administration and in incubations with hepatocytes. In plasma, the parent compound was the major circulating component in mice, rats, dogs, and humans. O-Demethyl apixaban sulfate (M1) represented approximately 25% of the parent area under the time curve in human plasma. This sulfate metabolite was present, but in lower amounts relative to the parent, in plasma from mice, rats, and dogs. Rabbits showed a plasma metabolite profile distinct from that of other species with apixaban as a minor component and M2 (O-demethyl apixaban) and M14 (O-demethyl apixaban glucuronide) as prominent components. The fecal route was a major elimination pathway, accounting for >54% of the dose in animals and >46% in humans. The urinary route accounted for <15% of the dose in animals and 25 to 28% in humans. Apixaban was the major component in feces of every species and in urine of all species except rabbit. M1 and M2 were common prominent metabolites in urine and feces of all species as well as in bile of rats and humans. In vivo metabolite profiles showed quantitative differences between species and from in vitro metabolite profiles, but all human metabolites were found in animal species. After intravenous administration of [(14)C]apixaban to bile duct-cannulated rats, the significant portion (approximately 22%) of the dose was recovered as parent drug in the feces, suggesting direct excretion of the drug from gastrointestinal tracts of rats. Overall, apixaban was effectively eliminated via multiple elimination pathways in animals and humans, including oxidative metabolism, and direct renal and intestinal excretion.
pubmed:language
eng
pubmed:journal
pubmed:citationSubset
IM
pubmed:chemical
pubmed:status
MEDLINE
pubmed:month
Aug
pubmed:issn
1521-009X
pubmed:author
pubmed:issnType
Electronic
pubmed:volume
37
pubmed:owner
NLM
pubmed:authorsComplete
Y
pubmed:pagination
1738-48
pubmed:meshHeading
pubmed-meshheading:19420130-Administration, Oral, pubmed-meshheading:19420130-Adolescent, pubmed-meshheading:19420130-Adult, pubmed-meshheading:19420130-Animals, pubmed-meshheading:19420130-Area Under Curve, pubmed-meshheading:19420130-Bile, pubmed-meshheading:19420130-Biotransformation, pubmed-meshheading:19420130-Carbon Radioisotopes, pubmed-meshheading:19420130-Dealkylation, pubmed-meshheading:19420130-Dogs, pubmed-meshheading:19420130-Factor Xa, pubmed-meshheading:19420130-Feces, pubmed-meshheading:19420130-Female, pubmed-meshheading:19420130-Fibrinolytic Agents, pubmed-meshheading:19420130-Glucuronides, pubmed-meshheading:19420130-Hepatocytes, pubmed-meshheading:19420130-Humans, pubmed-meshheading:19420130-Infusions, Intravenous, pubmed-meshheading:19420130-Macaca fascicularis, pubmed-meshheading:19420130-Male, pubmed-meshheading:19420130-Metabolomics, pubmed-meshheading:19420130-Mice, pubmed-meshheading:19420130-Mice, Inbred ICR, pubmed-meshheading:19420130-Middle Aged, pubmed-meshheading:19420130-Oxidation-Reduction, pubmed-meshheading:19420130-Pyrazoles, pubmed-meshheading:19420130-Pyridones, pubmed-meshheading:19420130-Rabbits, pubmed-meshheading:19420130-Rats, pubmed-meshheading:19420130-Rats, Sprague-Dawley, pubmed-meshheading:19420130-Species Specificity, pubmed-meshheading:19420130-Young Adult
pubmed:year
2009
pubmed:articleTitle
Comparative metabolism of 14C-labeled apixaban in mice, rats, rabbits, dogs, and humans.
pubmed:affiliation
Pharmaceutical Candidate Optimization, Bristol-Myers Squibb Research and Development, Princeton, NJ 08543-4000, USA. donglu.zhang@bms.com
pubmed:publicationType
Journal Article, Clinical Trial, Comparative Study