Troglitazone-Induced Hepatic Necrosis in an Animal Model of Silent Genetic Mitochondrial Abnormalities

doi:10.1093/toxsci/kfl180

ToxSci Advance Access originally published online on December 5, 2006
Toxicological Sciences 2007 97(1):205-213; doi:10.1093/toxsci/kfl180

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© The Author 2006. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournals.org

HIGHLIGHTED ARTICLE

Troglitazone-Induced Hepatic Necrosis in an Animal Model of Silent Genetic Mitochondrial Abnormalities

Michie M.K. Ong^*, Calivarathan Latchoumycandane^* and Urs A. Boelsterli^*^,^,1

^* Department of Pharmacology, Yong Loo Lin School of Medicine Department of Pharmacy, Faculty of Science, National University of Singapore, Singapore 117 597

¹ To whom correspondence should be addressed at Molecular Toxicology Lab, Department of Pharmacology, National University of Singapore, MD2, 18 Medical Drive, Singapore 117 597. Fax: +65-6873-7690. E-mail: phcbua{at}nus.edu.sg.

Received September 6, 2006; accepted November 29, 2006

Abstract

Troglitazone, a first-generation thiazolidinedione antidiabeticdrug, was withdrawn from the market due to an unacceptable riskof idiosyncratic hepatotoxicity. Troglitazone does not causehepatotoxicity in normal healthy rodents, but it produces mitochondrialinjury in vitro at high concentrations. The aim of this studywas to explore whether genetic mitochondrial abnormalities mightsensitize mice to hepatic adverse effects of troglitazone. Weused heterozygous superoxide dismutase 2 (Sod2^+/–) miceas a model of clinically silent mitochondrial stress. Troglitazonewas daily administered for 4 weeks (0, 10 or 30 mg/kg/day, ip).We found that troglitazone caused overt liver injury in thehigh-dose group, manifested by increased serum alanine aminotransferaseactivity (> twofold) and midzonal areas of hepatic necrosis,in Sod2^+/– but not in wild-type mice. No signs of hepatotoxicitywere apparent at 2 weeks of treatment. Hepatic mitochondriaisolated from troglitazone-treated mice exhibited decreasedactivities of aconitase (by 45%) and complex I (by 46%) andincreased (by 58%) protein carbonyls, indicative of enhancedmitochondrial oxidant stress. This was paralleled by compensatoryincreases in mitochondrial glutathione levels. Finally, in hepatocytesisolated from untreated Sod2^+/–, but not wild-type mice,troglitazone caused a concentration-dependent increase in superoxideanion levels as demonstrated with a selective mitochondria-targetingfluorescent probe. In conclusion, prolonged administration oftroglitazone can superimpose oxidant stress, potentiate mitochondrialdamage, and induce delayed hepatic necrosis in mice with geneticallycompromised mitochondrial function. These data are consistentwith our hypothesis that inherited or acquired mitochondrialabnormalities may be one of the contributing determinants ofsusceptibility to troglitazone-induced idiosyncratic liver injury.

Key Words: drug-induced liver injury (DILI); idiosyncratic drug toxicity; oxidative stress; mitochondria; determinants of susceptibility; hepatotoxicity; superoxide dismutase.

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