Species-Specific Kinetics and Zonation of Hepatic DNA Synthesis Induced by Ligands of PPAR{alpha}

doi:10.1093/toxsci/kfn062

ToxSci Advance Access originally published online on March 28, 2008
Toxicological Sciences 2008 104(1):74-85; doi:10.1093/toxsci/kfn062

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Species-Specific Kinetics and Zonation of Hepatic DNA Synthesis Induced by Ligands of PPAR ${alpha}$

Abdullah Al Kholaifi^*, Abeer Amer^*, Brett Jeffery^*, Tim J. B. Gray, Ruth A. Roberts and David R. Bell^*^,1

^* School of Biology, University of Nottingham, University Park, Nottingham NG7 2RD, UK Sanofi-Aventis, Willowburn Avenue, Alnwick, Northumberland NE66 2JH, UK AstraZeneca Pharmaceuticals plc, Alderley Park, Macclesfield, Cheshire SK10 4TJ, UK

¹ To whom correspondence should be addressed. Fax: +44-115-9513251. E-mail david.bell{at}nottingham.ac.uk.

Received February 13, 2008; accepted March 14, 2008

Abstract

Peroxisome proliferator–activated receptor ${alpha}$ (PPAR ${alpha}$ ) ligandsevoke a profound mitogenic response in rodent liver, and theaim of this study was to characterize the kinetics of inductionof DNA synthesis. The CAR ligand, 1,4-bis[2-(3,5-dichoropyridyloxy)]benzene,caused induction of hepatocyte DNA synthesis within 48 h in129S4/SvJae mice, but the potent PPAR ${alpha}$ ligand, ciprofibrate,induced hepatocyte DNA synthesis only after 3 or 4 days dosing;higher or lower doses did not hasten the DNA synthesis response.This contrasted with the rapid induction (24 h) reported byStyles et al., 1988, Carcinogenesis 9, 1647–1655. C57BL/6and DBA/2J mice showed significant induction of DNA synthesisafter 4, but not 2, days ciprofibrate treatment. Alderley Parkand 129S4/SvJae mice dosed with methylclofenapate induced hepatocyteDNA synthesis at 4, but not 2, days after dosing and provedthat inconsistency with prior work was not due to a differencein mouse strain or PPAR ${alpha}$ ligand. Ciprofibrate-induced liver DNAsynthesis and growth was absent in PPAR ${alpha}$ -null mice and are PPAR ${alpha}$ dependent. In the Fisher344 rat, hepatocyte DNA synthesis wasinduced at 24 h after dosing, with a second peak at 48 h. Lobularlocalization of hepatocyte DNA synthesis showed preferentialperiportal induction of DNA synthesis in rat but panlobularzonation of hepatocyte DNA synthesis in mouse. These resultscharacterize a markedly later hepatic induction of panlobularDNA synthesis by PPAR ${alpha}$ ligands in mouse, compared to rapid inductionof periportal DNA synthesis in rat.

Key Words: liver growth; hepatocyte; PPAR; peroxisome proliferation; DNA synthesis.

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