Dose-dependent mutation profile in the c-Ha-ras proto-oncogene of skin tumors in mice initiated with benzo[a]pyrene

doi:10.1093/carcin/20.9.1689

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Carcinogenesis, Vol. 20, No. 9, 1689-1696, September 1999
© 1999 Oxford University Press

Cancer Biology

Dose-dependent mutation profile in the c-Ha-ras proto-oncogene of skin tumors in mice initiated with benzo[a]pyrene

Shu-Jing Caroline Wei², Richard L. Chang, Kathleen A. Merkler, Mark Gwynne, Xiao Xing Cui, Bindu Murthy, Mou-Tuan Huang, Jian-Guo Xie, Yao-Ping Lu, You-Rong Lou, Donald M. Jerina¹ and Allan H. Conney

Laboratory for Cancer Research, Department of Chemical Biology, College of Pharmacy, Rutgers, The State University of New Jersey, 164 Frelinghuysen Road, Piscataway, NJ 08854-8020 and
¹ Section on Oxidation Mechanisms, Laboratory of Bioorganic Chemistry, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892, USA

Female CD-1 mice were treated topically with a low (25–50nmol) or high (800 nmol) dose of benzo[a]pyrene (BP) or acetonevehicle, followed by 5 nmol 12-O-tetradecanoylphorbol 13-acetate(TPA) twice a week for 26 weeks. Selective UV radiation fractionationfollowed by PCR methods were used to analyze histologicallydefined subsets of cells (~100–200 cells) on formalin-fixed,paraffin-embedded and H&E stained microscope sections. DNAsamples from normal-appearing, hyperplastic or tumor regionsfrom the skin of animals from each treatment group were isolatedand amplified by PCR with c-Ha-ras-specific primers. Single-strandconformation polymorphism (SSCP) analyses were performed onboth exon 1 and 2 products from each sample. DNA extracted fromeach aberrant band of SSCP analyses was amplified by PCR forfurther sequence analysis. The data indicate that c-Ha-ras mutationscan be detected in normal-looking and hyperplastic epidermalcells as well as in tumor cells obtained from mice initiatedwith BP and promoted with TPA. The frequencies of c-Ha-ras mutationsfor normal-looking, hyperplastic and tumor samples were 3/20(15%), 8/17 (47%) and 58/68 (85%), respectively, for the lowdose group and 8/18 (44%), 10/20 (50%) and 64/86 (74%), respectively,for the high dose group. These observations indicate that therewere no dose dependencies in the mutation frequencies for normal-looking,hyperplastic and tumor samples. For combined high dose and lowdose samples, differences in mutation frequencies of the c-Ha-rasgene between the normal-looking, hyperplastic and tumor sampleswere highly significant (P < 0.0001, Fisher's exact test).All mutations detected were located at codons 12, 13 and 61of the c-Ha-ras gene. With the numbers in parentheses indicatingthe nucleotide position in the coding sequence of the c-Ha-rasproto-oncogene, the distributions of mutations for G $->$ A (35),G $->$ T (35), G $->$ C (37), G $->$ T (38), C $->$ A (181), A $->$ T (182) and A $->$ G (182) inthe low dose tumors were 5, 2, 11, 74, 0, 7 and 2%, respectively,and the distribution of mutations in tumors from animals treatedwith a high dose of BP were 3, 7, 13, 61, 15, 1 and 0%, respectively.Differences in the global mutation spectra (site and kind ofall mutations) for the c-Ha-ras gene between the high and lowdose group tumors were statistically significant (P < 0.004,Fisher's exact test) and the major difference between thesetwo groups was C $->$ A (181) base substitutions. In summary, ourdata indicate that: (i) 79% of the BP/TPA skin tumors in CD-1mice had c-Ha-ras mutations for the combined data for high doseand low dose tumors; (ii) the major mutations detected in BP/TPAskin tumors were G $->$ T transversions; (iii) the global mutationprofile in the c-Ha-ras proto-oncogene in skin tumors obtainedafter initiation with a low dose of BP was different from thatobtained after initiation with a high dose of BP.

Abbreviations: BP, benzo[a]pyrene; BPDE, (+)-(7R,8S,9S,10R)-7,8-dihydroxy-9,10-epoxy-7,8,9,10-tetrahydrobenzo[a]pyrene; B[c]PhDE, (–)-(1R,2S, 3S,4R)-3,4-dihydroxy-1,2-epoxy-1,2,3,4-tetrahydrobenzo[c]phenanthrene; DB[a,l]P, dibenzo[a,l]pyrene; DMBA, 7,12-dimethylbenz[a]anthracene; hprt, hypoxanthine (guanine) phosphoribosyltransferase gene; H&E, hematoxylin and eosin; SSCP, single-strand conformation polymorphism; SURF, selective UV radiation fractionation; TPA, 12-O-tetradecanoylphorbol 13-acetate.

² To whom correspondence should be addressed Email: swei{at}rci.rutgers.edu

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