Mutation frequency in the lacI gene of liver DNA from lambda/lacI transgenic mice following the interaction of PCBs with iron causing hepatic cancer and porphyria

doi:10.1093/mutage/15.5.379

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Mutagenesis, Vol. 15, No. 5, 379-383, September 2000
© 2000 UK Environmental Mutagen Society/Oxford University Press

Mutation frequency in the lacI gene of liver DNA from lambda/lacI transgenic mice following the interaction of PCBs with iron causing hepatic cancer and porphyria

Reginald Davies, Bruce Clothier and Andrew G. Smith¹

MRC Toxicology Unit, Hodgkin Building, Leicester University, Lancaster Road, Leicester LE1 9HN, UK

The synergistic interaction of iron overload, Ahr genotype andexposure to a mixture of polychlorinated biphenyls (PCBs) (Aroclor1254) in mice leads to hepatic porphyria, oxidative DNA damageand cancer. In humans, hepatocellular cancer is associated withiron overload and hepatic porphyria. Neither the mechanism ofhepatic carcinogenesis induced by PCBs in rodents nor hepatocellularcancer induced by iron and porphyria in humans are understood.To test the hypothesis that chronic interaction of iron andPCBs may induce mutagenesis in liver DNA, ${lambda}$ /lacI transgenicC57BL/6 mice were given iron dextran (600 mg iron/kg) and thenadministered Aroclor 1254 in the diet (0.01%) for 7 weeks. Hepaticiron, CYP1A activity and CYP1A1/1A2 protein were elevated >20-foldas a result of iron or Aroclor treatments, respectively, butporphyria with associated histological changes only developedin the combined iron/Aroclor treatment group. ${lambda}$ /lacI shuttlevectors were isolated from liver genomic DNA and the mutationalfrequency (MF) in the lacI gene determined. Both iron and Aroclortreatments alone caused significant small increases in MF (1.5-and 1.4-fold, respectively), however, the MF following the combinediron and Aroclor treatment (1.6-fold) was not greater than theadditive effects. In contrast, the MF was significantly elevated(4.7-fold) in liver DNA of mice 2 weeks following five dailydoses of N-nitrosodimethylamine (4 mg/kg). These studies demonstratethat neither PCBs nor iron overload caused marked point mutationseven in a combination regime that leads to oxidative damageand cancer. There was also no strong evidence either that porphyrinsor chronic CYP1A1 expression induced by the PCBs after thisperiod caused marked point mutagens or simple deletions. Hence,to understand the PCBs–iron synergism more complex scenariosthan point mutations or simple deletions must be invoked.

¹ To whom correspondence should be addressed. Tel: +44 116 2525617; Fax: +44 116 252 5616; Email: ags5{at}le.ac.uk

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