The metabolism of the 5HT3 antagonists, ondansetron, alosetron and GR87442 II: Investigation into the in vitro methods used to predict the in vivo hepatic clearance of ondansetron, alosetron and GR87442 in the rat, dog and human

G. I. Somers, M. K. Bayliss, J. B. Houston

    Research output: Contribution to journalArticlepeer-review

    Abstract

    The in vitro clearances of the 5HT3 antagonists, ondansetron, alosetron and GR87442 were investigated. Intrinsic clearances using either metabolite formation or substrate depletion methods were equivalent (R 2 = 0.95). Hepatocytes from preclinical species were superior to microsomes for the prediction of hepatic clearance (CLH), whereas the predictions from human microsomes and hepatocytes were similar. Using a non-restrictive model, seven of the nine CLH predictions using hepatocytes were within 2-fold of the in vivo CLH values. If the unbound fraction was included, the clearance of the compounds was generally under-predicted by both in vitro models. However, for the most metabolically stable compound, GR87442, the non-restrictive model over-predicted CLp. This and the possibility of extrahepatic metabolism indicate that the restrictive model is more appropriate for prediction of CLH. The rank order of metabolic stability correlated with that in vivo. All three compounds were more metabolically stable in human than in the preclinical animal species examined. © 2007 Informa UK Ltd.
    Original languageEnglish
    Pages (from-to)855-869
    Number of pages14
    JournalXenobiotica
    Volume37
    Issue number8
    DOIs
    Publication statusPublished - Aug 2007

    Keywords

    • 5-HT3 Antagonists
    • Hepatic clearance
    • Hepatocytes
    • Microsomes

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