| Literature DB >> 27180975 |
Peter N Morcos1, Li Yu1, Katrijn Bogman2, Mika Sato3, Hisakazu Katsuki4, Kosuke Kawashima3, David J Moore1, Matt Whayman5, Keith Nieforth6, Katja Heinig2, Elena Guerini2, Dieter Muri2, Meret Martin-Facklam2, Alex Phipps5.
Abstract
1. Alectinib is a highly selective, central nervous system-active small molecule anaplastic lymphoma kinase inhibitor. 2. The absolute bioavailability, metabolism, excretion and pharmacokinetics of alectinib were studied in a two-period single-sequence crossover study. A 50 μg radiolabelled intravenous microdose of alectinib was co-administered with a single 600 mg oral dose of alectinib in the first period, and a single 600 mg/67 μCi oral dose of radiolabelled alectinib was administered in the second period to six healthy male subjects. 3. The absolute bioavailability of alectinib was moderate at 36.9%. Geometric mean clearance was 34.5 L/h, volume of distribution was 475 L and the hepatic extraction ratio was low (0.14). 4. Near-complete recovery of administered radioactivity was achieved within 168 h post-dose (98.2%) with excretion predominantly in faeces (97.8%) and negligible excretion in urine (0.456%). Alectinib and its major active metabolite, M4, were the main components in plasma, accounting for 76% of total plasma radioactivity. In faeces, 84% of dose was excreted as unchanged alectinib with metabolites M4, M1a/b and M6 contributing to 5.8%, 7.2% and 0.2% of dose, respectively. 5. This novel study design characterised the full absorption, distribution, metabolism and excretion properties in each subject, providing insight into alectinib absorption and disposition in humans.Entities:
Keywords: Intravenous; metabolites; microtracer; pharmacokinetics; radiolabelled alectinib
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Year: 2016 PMID: 27180975 DOI: 10.1080/00498254.2016.1179821
Source DB: PubMed Journal: Xenobiotica ISSN: 0049-8254 Impact factor: 1.908