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Etoxazole is Metabolized Enantioselectively in Liver Microsomes of Rat and Human <i>in Vitro</i>
22
Citations
25
References
2016
Year
Molecular PharmacologyPharmacological StudyBiochemistryChitin BiosynthesisMedicineLiver PhysiologyEtoxazole EnantiomersToxicologyPharmacotherapyLiver MicrosomesAcaricide Etoxazole BelongsExperimental PharmacologyHepatotoxicityExperimental ToxicologyPharmacologyDrug-induced Liver InjuryPharmacokineticsDrug Discovery
Acaricide etoxazole belongs to the ovicides/miticides diphenyloxazole class, affecting adults to lay sterile eggs by inhibiting chitin biosynthesis possibly. The reverse-phase HPLC-MS/MS method was used to determine the etoxazole enantiomers. The enantioselective degradation behavior of rac-etoxazole in liver microsomes of rat and human in vitro with NADPH was dramatically different. The t1/2 of (R)-etoxazole was 15.23 min in rat liver microsomes and 30.54 min in human liver microsomes, while 21.73 and 23.50 min were obtained for (S)-etoxazole, respectively. The Vmax of (R)-etoxazole was almost 5-fold of (S)-etoxazole in liver microsomes of rat in vitro. However, the Vmax of (S)-etoxazole was almost 2-fold of (R)-etoxazole in liver microsomes of human in vitro. The CLint of etoxazole was also shown the enantioselectivity on the contrary in liver microsomes of rat and human. These results indicated that the metabolism of two etoxazole enantiomers was selective in liver microsomes of rat and human in vitro, and enantioselectivity in the two kinds of liver microsomes was in the difference in degradation performance. The reason might be related to the composition and content involved in the enzyme system.
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