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Xenobiotica
the fate of foreign compounds in biological systems
Volume 30, 2000 - Issue 4
69
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Research Article

Metabolism of roquinimex in mouse and rat: an in vitro/in vivo comparison

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Pages 371-380 | Published online: 22 Sep 2008
 

Abstract

1.1. In vitro studies with roquinimex, animmuno-modulator, in liver microsomes from mouse and rat were conducted to evaluate the primary metabolism and compare the metabolite pattern as well as the rate of metabolismwith the in vivo pharmacokinetics of the compound in these two species. 2. In the presence ofNADPH, roquinimex wasmetabolized to six primary metabolites (R1-6) by liver microsomes from mouse and rat. The formation of these metabolites was qualitatively similar in both species, and was greatly enhanced by pretreatment with PCN, an inducer of cytochrome P4503A. 3. The identification of the R1-6 demonstratedthat roquinimex had been hydroxylated and demethylated. Hydroxylation at different sites of the quinoline moiety was the dominating reaction in both species. 4. Comparison of the resulting microsomal intrinsic clearance of 0.3 μmol mg−1 protein min−1 in mouse liver microsomes, versus 0.03 μmol mg−1 protein min−1 in rat liver microsomes demonstrated that the mouse possesses about a 10-fold greater metabolic capacity for roquinimex than the rat. 5. The in vivo pharmacokinetics of roquinimex demonstrated a 7-fold higher clearance in mouse than in the rat (82 ml h−1 kg−1 in mouse, 10.6 ml h−1 kg−1 in rat), which is in concordance with the in vitro findings.

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