Evidence that a burst of DNA depurination in SENCAR mouse skin induces error-prone repair and forms mutations in the H-ras gene

Dhrubajyoti Chakravarti, Paula C. Mailander, Kai Ming Li, Sheila Higginbotham, Henry L. Zhang, Michael L. Gross, Jane L. Meza, Ercole L. Cavalieri, Eleanor G. Rogan

Research output: Contribution to journalArticlepeer-review

174 Scopus citations

Abstract

Treatment of SENCAR mouse skin with dibenzo[a, l]pyrene results in abundant formation of abasic sites that undergo error-prone excision repair, forming oncogenic H-ras mutations in the early preneoplastic period. To examine whether the abundance of abasic sites causes repair infidelity, we treated SENCAR mouse skin with estradiol-3, 4-quinone (E2-3, 4-Q) and determined adduct leveis 1 h after treatment, as well as mutation spectra in the H-ras gene between 6 h and 3 days after treatment. E2-3, 4-Q formed predominantly (≥99%) the rapidly-depurinating 4-hydroxy estradiol (4-OHE2)-1-N3Ade adduct and the slower-depurinating 4-OHE2-1-N7Gua adduct. Between 6 h and 3 days, E2-3, 4-Q induced abundant A to G mutations in H-ras DNA, frequently in the context of a 3′-G residue. Using a T.G-DNA glycosylase (TDG)-PCR assay, we determined that the early A to G mutations (6 and 12 h) were in the form of G.T heteroduplexes, suggesting misrepair at A-specific depurination sites. Since G-specific mutations were infrequent in the spectra, it appears that the slow rate of depurination of the N7Gua adducts during active repair may not generate a threshold level of G-specific abasic sites to affect repair fidelity. These results also suggest that E2-3, 4-Q, a suspected endogenous carcinogen, is a genotoxic compound and could cause mutations.

Original languageEnglish (US)
Pages (from-to)7945-7953
Number of pages9
JournalOncogene
Volume20
Issue number55
DOIs
StatePublished - Nov 29 2001

Keywords

  • Abasic sites
  • DNA repair
  • Depurinating adducts
  • Estradiol-3, 4-quinone
  • H-ras mutation in SENCAR mouse skin
  • Mismatched heteroduplex

ASJC Scopus subject areas

  • Molecular Biology
  • Genetics
  • Cancer Research

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