Kamimura Hidetaka, Ito Satoshi, Nozawa Kohei, Nakamura Shota, Chijiwa Hiroyuki, Nagatsuka Shin-ichiro, Kuronuma Miyuki, Ohnishi Yasuyuki, Suemizu Hiroshi, Ninomiya Shin-ichi
ADME & Tox. Research Institute, Sekisui Medical Co., Ltd., Tokyo, Japan (H.K., S.I., K.N., S.Nak., H.C., S.Nag., S.Ni); and Central Institute for Experimental Animals, Kawasaki, Kanagawa, Japan (M.K., Y.O., H.S.)
ADME & Tox. Research Institute, Sekisui Medical Co., Ltd., Tokyo, Japan (H.K., S.I., K.N., S.Nak., H.C., S.Nag., S.Ni); and Central Institute for Experimental Animals, Kawasaki, Kanagawa, Japan (M.K., Y.O., H.S.).
Drug Metab Dispos. 2015 Mar;43(3):309-16. doi: 10.1124/dmd.114.061689. Epub 2014 Dec 11.
3'-Hydroxy-4'-methoxydiclofenac (VI) is a human-specific metabolite known to accumulate in the plasma of patients after repeated administration of diclofenac sodium. Diclofenac also produces glutathione-conjugated metabolites, some of which are human-specific. In the present study, we investigated whether these metabolites could be generated in humanized chimeric mice produced from TK-NOG mice. After a single oral administration of diclofenac to humanized mice, the unchanged drug in plasma peaked at 0.25 hour and then declined with a half-life (t1/2) of 2.4 hours. 4'-Hydroxydiclofenac (II) and 3'-hydroxydiclofenac also peaked at 0.25 hour and were undetectable within 24 hours. However, VI peaked at 8 hours and declined with a t1/2 of 13 hours. When diclofenac was given once per day, peak and trough levels of VI reached plateau within 3 days. Studies with administration of II suggested VI was generated via II as an intermediate. Among six reported glutathione-conjugated metabolites of diclofenac, M1 (5-hydroxy-4-(glutathion-S-yl)diclofenac) to M6 (2'-(glutathion-S-yl)monoclofenac), we found three dichlorinated conjugates [M1, M2 (4'-hydroxy-3'-(glutathion-S-yl)diclofenac), and M3 (5-hydroxy-6-(glutathion-S-yl)diclofenac)], and a single monochlorinated conjugate [M4 (2'-hydroxy-3'-(glutathion-S-yl)monoclofenac) or M5 (4'-hydroxy-2'-(glutathion-S-yl)monoclofenac)], in the bile of humanized chimeric mice. M4 and M5 are positional isomers and have been previously reported as human-specific in vitro metabolites likely generated via arene oxide and quinone imine-type intermediates, respectively. The biliary monochlorinated metabolite exhibited the same mass spectrum as those of M4 and M5, and we discuss whether this conjugate corresponded to M4 or M5. Overall, humanized TK-NOG chimeric mice were considered to be a functional tool for the study of drug metabolism of diclofenac in humans.
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