| Literature DB >> 29320949 |
Zeen Tong1, Christian Atsriku1, Usha Yerramilli1, Xiaomin Wang1, Yan Li2, Josephine Reyes2, Bin Fan3, Hua Yang3, Matthew Hoffmann1, Sekhar Surapaneni1.
Abstract
1. The absorption, distribution, metabolism and excretion of enasidenib were studied following a single oral dose of [14C]enasidenib to rats (10 mg/kg; 100 μCi/kg) and healthy volunteers (100 mg; 318 nCi). 2. Enasidenib was readily absorbed, extensively metabolized and primarily eliminated via the hepatobiliary pathway. Enasidenib-derived radioactivity was widely distributed in rats. Excretion of radioactivity was approximately 95-99% of the dose from rats in 168 h post-dose and 82.4% from human volunteers in 504 h post-dose. In rat bile, approximately 35-42% of the administered dose was recovered, with less than 5% of the dose excreted as the parent drug. Renal elimination was a minor pathway, with <12% of the dose excreted in rat urine and <10% of the dose excreted in human urine. 3. Enasidenib was the prominent radioactive component in rat and human systemic circulation. Enasidenib was extensively metabolized in rats and human volunteers through N-dealkylation, oxidation, direct glucuronidation and combinations of these pathways. Glucuronidation was the major metabolic pathway in rats while N-dealkylation was the prominent metabolic pathway in human volunteers. All human metabolites were detected in rats.Entities:
Keywords: Absorption; accelerator mass spectrometry; distribution; isocitrate dehydrogenase inhibitor; metabolism and excretion; species comparison
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Year: 2018 PMID: 29320949 DOI: 10.1080/00498254.2018.1425511
Source DB: PubMed Journal: Xenobiotica ISSN: 0049-8254 Impact factor: 1.908