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Xenobiotica
the fate of foreign compounds in biological systems
Volume 39, 2009 - Issue 3
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Commentary

Drug–drug interaction studies in preclinical species: should metabolite(s) kinetics be studied?

Pages 193-196 | Received 06 Nov 2008, Accepted 28 Nov 2008, Published online: 01 Mar 2009
 

Abstract

  1. Drug–drug interaction studies are important building blocks in drug development to understand the perceived risk of a purported interaction due to the differing clinical pharmacology attributes of the co-administered drugs.

  2. Two case studies are presented that justify the importance of evaluating the metabolite kinetics data along with the parent in a preclinical model.

  3. Atorvastatin and verapamil have interesting clinical pharmacology attributes in that both agents are substrates and/or inhibitors of the dual cytochrome P450 (CYP) 3A4 and P-glycoprotein (Pgp) efflux transporter interplay.

  4. As articulated by the two case studies, the presence of metabolite kinetic data (i.e., norverapamil) provided unequivocal evidence in order to tease out the actual pathway responsible for the interaction between atorvastatin and verapamil.

  5. Therefore, consideration for metabolite kinetics, wherever feasible, appears to be prudent in defining the interaction liability between the two agents in a preclinical model.

Acknowledgements

Declaration of interest: The author reports no conflicts of interest.

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