Mammary carcinogenesis and molecular analysis of in vivo cII gene mutations in the mammary tissue of female transgenic rats treated with the environmental pollutant 6-nitrochrysene

doi:10.1093/carcin/bgh040

Carcinogenesis Advance Access originally published online on December 4, 2003

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Carcinogenesis, Vol. 25, No. 4, 637-643, April 2004
Carcinogenesis vol.25 no.4 © Oxford University Press 2004; all rights reserved.

CARCINOGENESIS

Mammary carcinogenesis and molecular analysis of in vivo cII gene mutations in the mammary tissue of female transgenic rats treated with the environmental pollutant 6-nitrochrysene

Telih Boyiri¹, Joseph Guttenplan²^,3, Michael Khmelnitsky², Wieslawa Kosinska², Jyh-Ming Lin¹, Dhimant Desai¹, Shantu Amin¹, Brian Pittman¹ and Karam El-Bayoumy¹^,4

¹ American Health Foundation Cancer Center, Institute for Cancer Prevention, Valhalla, NY 10595, USA, ² Department of Basic Science, New York University Dental Center, New York, NY 10010, USA and ³ Department of Environmental Medicine, New York University, Medical Center, New York, NY 10016, USA

We determined the mutant fractions (MF) and mutational specificitiesin the cII gene in histologically confirmed normal, non-involvedand tumor mammary tissues of female transgenic (Big Blue F344x Sprague-Dawley)F₁ rats treated with the environmental pollutant6-nitrochrysene (6-NC). At 30 days of age, three groups wereset up for oral treatment with 6-NC dissolved in trioctanoin,or trioctanoin alone once a week for 8 weeks. Two dose levelsof 6-NC (100 and 200 µmol/rat) were selected on the basisof our previous carcinogenicity bioassays with CD rats. Therats were decapitated 32 weeks after the last carcinogen dose.Both incidence and multiplicity of mammary adenocarcinomas weresignificantly elevated in the high dose (36%, 0.57, P < 0.01)group but at the low dose these outcomes (16%, 0.23, P <0.1) were not significantly different from those of controlrats (3%, 0.03). The MF in normal, non-involved and tumor tissuesfrom the mammary glands of 6-NC-treated rats were comparable.At the high and low doses, respectively (4.8 ± 2.0, 3.2± 2.1) the MF of 6-NC-treated rats, were significantlyhigher (P < 0.05) than that observed in control rats (1.2± 0.6). Control mutants consisted primarily of GC $->$ ATtransitions, whereas 6-NC-induced mutants were comprised ofseveral major classes of mutations with GC $->$ TA, GC $->$ CG, AT $->$ GC and AT $->$ TA as the most prevalent. Further studies indicatedthat the structures of 6-NC–DNA adducts in the mammarytissue are consistent with the mutational specificities. Thisis the first report that defines the relationship between carcinogenesisand mutagenesis, as well as between structures of 6-NC–DNAadducts and mutation characteristics in the target organ invivo.

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This article has been cited by other articles:

J. B. Guttenplan, Z.-l. Zhao, W. Kosinska, R. G. Norman, J. Krzeminski, Y.-W. Sun, S. Amin, and K. El-Bayoumy
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