Toxic Effects of Fumonisin in Mouse Liver Are Independent of the Peroxisome Proliferator-Activated Receptor {alpha}

doi:10.1093/toxsci/kfj019

ToxSci Advance Access originally published online on October 12, 2005
Toxicological Sciences 2006 89(1):108-119; doi:10.1093/toxsci/kfj019

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Published by Oxford University Press 2005.

Toxic Effects of Fumonisin in Mouse Liver Are Independent of the Peroxisome Proliferator-Activated Receptor ${alpha}$

Kenneth A. Voss^*^,1, Jie Liu, Steven P. Anderson^,2, Corrie Dunn, J. David Miller^¶, Joy R. Owen^*, Ronald T. Riley^*, Charles W. Bacon^* and J. Christopher Corton^||^,3

^* Toxicology & Mycotoxin Research Unit, USDA-Agricultural Research Service, Athens, Georgia 30604–5677; Inorganic Carcinogenesis, LCC, NCI at NIEHS, Research Triangle Park, North Carolina 27709; GlaxoSmithKline, Research Triangle Park, North Carolina 27709; CIIT Centers for Health Research, Research Triangle Park, North Carolina 27709; ^¶ Department of Chemistry, Carleton University, Ottawa, Ontario, Canada K1S 5B6; and ^|| ToxicoGenomics, Chapel Hill, North Carolina 27514

Received May 16, 2005; accepted October 6, 2005

Fumonisin mycotoxins occur worldwide in corn and corn-basedfoods. Fumonisin B₁ (FB₁) is a rodent liver carcinogen and suspectedhuman carcinogen. It inhibits ceramide synthase and increasestissue sphinganine (Sa) and sphingosine (So) concentrations.Events linking disruption of sphingolipid metabolism and fumonisintoxicity are not fully understood; however, Sa and So were shownto bind mouse recombinant peroxisome proliferator-activatedreceptor ${alpha}$ (PPAR ${alpha}$ ) in vitro. To investigate the role of PPAR ${alpha}$ infumonisin hepatotoxicity in vivo, wild-type (WT) and PPAR ${alpha}$ -nullmice were fed control diets or diets containing 300 ppm FB₁,Fusarium verticillioides culture material (CM) providing 300ppm FB₁, or 500 ppm of the peroxisome proliferator WY-14,643(WY) for 1 week. WY-fed WT mice exhibited hepatomegaly, an effectnot found in WY-fed PPAR ${alpha}$ -null mice, and WY did not change liversphingoid base concentrations in either strain. Hepatotoxicityfound in FB₁- and CM-fed WT and PPAR ${alpha}$ -null mice was similar,qualitatively different from that found in WY-treated animals,and characterized by increased Sa concentration, apoptosis,and cell proliferation. Transcript profiling using oligonucleotidearrays showed that CM and FB₁ elicited similar expression patternsof genes involved in cell proliferation, signal transduction,and glutathione metabolism that were different from that alteredby WY. Real-time RT-PCR analysis of gene expression demonstratedPPAR ${alpha}$ -dependence of lipid metabolism gene expression in WY-treatedmice, whereas PPAR ${alpha}$ -independent alterations of genes in lipidmetabolism, and other categories, were found in CM- and FB₁-fedmice. Together, these findings demonstrate that FB₁- and CM-inducedhepatotoxicity in mice does not require PPAR ${alpha}$ .

Key Words: fumonisin; peroxisome proliferator-activated receptor ${alpha}$ ; hepatotoxicity.

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