| Literature DB >> 25034009 |
Theodore R Johnson1, Weiwei Tan, Lance Goulet, Evan B Smith, Shinji Yamazaki, Gregory S Walker, Melissa T O'Gorman, Gabriella Bedarida, Helen Y Zou, James G Christensen, Leslie N Nguyen, Zhongzhou Shen, Deepak Dalvie, Akintunde Bello, Bill J Smith.
Abstract
1. Crizotinib (XALKORI®), an oral inhibitor of anaplastic lymphoma kinase (ALK) and mesenchymal-epithelial transition factor kinase (c-Met), is currently approved for the treatment of patients with non-small cell lung cancer that is ALK-positive. 2. The metabolism, excretion and pharmacokinetics of crizotinib were investigated following administration of a single oral dose of 250 mg/100 µCi [(14)C]crizotinib to six healthy male subjects. 3. Mean recovery of [(14)C]crizotinib-related radioactivity in excreta samples was 85% of the dose (63% in feces and 22% in urine). 4. Crizotinib and its metabolite, crizotinib lactam, were the major components circulating in plasma, accounting for 33% and 10%, respectively, of the 0-96 h plasma radioactivity. Unchanged crizotinib was the major excreted component in feces (∼ 53% of the dose). In urine, crizotinib and O-desalkyl crizotinib lactam accounted for ∼ 2% and 5% of the dose, respectively. Collectively, these data indicate that the primary clearance pathway for crizotinib in humans is oxidative metabolism/hepatic elimination. 5. Based on plasma exposure in healthy subjects following a single dose of crizotinib and in vitro potency against ALK and c-Met, the crizotinib lactam diastereomers are not anticipated to contribute significantly to in vivo activity; however, additional assessment in cancer patients is warranted.Entities:
Keywords: Crizotinib; excretion; human; metabolism; oncology; pharmacokinetics
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Year: 2014 PMID: 25034009 DOI: 10.3109/00498254.2014.941964
Source DB: PubMed Journal: Xenobiotica ISSN: 0049-8254 Impact factor: 1.908