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Mass balance study of [¹⁴C]eribulin in patients with advanced solid tumors.

Anne-Charlotte Dubbelman ,
Hilde Rosing ,
Robert S Jansen ,
Marja Mergui-Roelvink ,
Alwin D R Huitema ,
Barbara Koetz ,
Margarita Lymboura ,
Larisa Reyderman ,
Arturo Lopez-Anaya ,
Jan H M Schellens ,
Jos H Beijnen

Abstract

This mass balance study investigated the metabolism and excretion of eribulin, a nontaxane microtubule dynamics inhibitor with a novel mechanism of action, in patients with advanced solid tumors. A single approximately 2 mg (approximately 80 μCi) dose of [¹⁴C]eribulin acetate was administered as a 2 to 5 min bolus injection to six patients on day 1. Blood, urine, and fecal samples were collected at specified time points on days 1 to 8 or until sample radioactivity was ≤1% of the administered dose. Mean plasma eribulin exposure (627 ng · h/ml) was comparable with that of total radioactivity (568 ng Eq · h/ml). Time-matched concentration ratios of eribulin to total radioactivity approached unity in blood and plasma, indicating that unchanged parent compound constituted almost all of the eribulin-derived radioactivity. Only minor metabolites were detected in plasma samples up to 60 min postdose, pooled across patients, each metabolite representing ≤0.6% of eribulin. Elimination half-lives for eribulin (45.6 h) and total radioactivity (42.3 h) were comparable. Eribulin-derived radioactivity excreted in feces was 81.5%, and that of unchanged eribulin was 61.9%. Renal clearance (0.301 l/h) was a minor component of total eribulin clearance (3.93 l/h). Eribulin-derived radioactivity excreted in urine (8.9%) was comparable with that of unchanged eribulin (8.1%), indicating minimal excretion of metabolite(s) in urine. Total recovery of the radioactive dose was 90.4% in urine and feces. Overall, no major metabolites of eribulin were detected in plasma. Eribulin is eliminated primarily unchanged in feces, whereas urine constitutes a minor route of elimination.

More about this publication

Drug metabolism and disposition: the biological fate of chemicals

Volume 40
Issue nr. 2
Pages 313-21
Publication date 01-02-2012

Full text links

Publisher website (DOI) 10.1124/dmd.111.042762
Europe PubMed Central 22041109
Pubmed 22041109

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