PPAR alpha, more than PPAR delta, Mediates the Hepatic and Skeletal Muscle Alterations Induced by the PPAR Agonist GW0742

doi:10.1093/toxsci/kfn130

ToxSci Advance Access originally published online on June 30, 2008
Toxicological Sciences 2008 105(2):384-394; doi:10.1093/toxsci/kfn130

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PPAR alpha, more than PPAR delta, Mediates the Hepatic and Skeletal Muscle Alterations Induced by the PPAR Agonist GW0742

Brenda Faiola^*^,1, James Greg Falls^*, Richard A. Peterson^*, Nancy R. Bordelon^*^,, Thomas A. Brodie^*^,, Connie A. Cummings^*, Elizabeth H. Romach^* and Richard T. Miller^*

^* Safety Assessment Department, GlaxoSmithKline, Research Triangle Park, North Carolina 27709 Department of Toxicology, Alcon Research Labs, Fort Worth, Texas 76134 Safety Assessment Department, GlaxoSmithKline, The Frythe, UK

¹ To whom correspondence should be addressed at GSK, PO Box 13398, 5 Moore Dr., Research Triangle Park, NC 27709. Fax: (919) 483-6858. E-mail: Brenda.x.Faiola{at}gsk.com.

Received April 1, 2008; accepted June 23, 2008

Abstract

Therapeutic use of certain peroxisome proliferator–activatedreceptor (PPAR) alpha agonists (fibrates) for the treatmentof dyslipidemia has infrequently been associated with the untowardside effect of myopathy. With interest in PPAR- ${delta}$ as a therapeutictarget, this study assessed whether a PPAR- ${delta}$ agonist inducedsimilar hepatic and skeletal muscle alterations as noted withsome fibrates. PPAR- ${alpha}$ null (KO) and corresponding wild-type (WT)mice were administered toxicological dosages of a potent PPAR- ${delta}$ agonist tool ligand (GW0742; which also has weak PPAR- ${alpha}$ agonistactivity) or a potent PPAR- ${alpha}$ agonist (WY-14,643) for 10 days.Increases in liver weights and clinical chemistry indicatorsof skeletal muscle damage and/or liver injury were more pronouncedin WT mice compared with KO mice administered the PPAR- ${delta}$ agonist.Likewise, the incidence and severity of skeletal myopathy weregreater in WT mice given GW0742 compared with KO mice. Ultrastructuraland immunohistochemical analyses revealed significant peroxisomeproliferation in muscle and liver of WT mice treated with eachagonist; however, KO animals showed little or no evidence ofhepatic and muscle peroxisome proliferation. PMP-70 proteinexpression in liver was consistent with these results. The hepatomegaly,hepatic and skeletal muscle peroxisome proliferation, and skeletalmyopathy induced by this PPAR- ${delta}$ ligand was predominantly mediatedby its cross-activation of PPAR- ${alpha}$ , though PPAR- ${delta}$ agonism contributedslightly to these effects.

Key Words: peroxisome proliferator–activated receptor; myopathy; mice.

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