Role of G->T transversions in the mutagenicity of alkylperoxyl radicals: Induction of alkali-labile sites in bacteriophage M13mp19

被引：17

作者：

Harkin, LA ^{[1
]}

Butler, LM ^{[1
]}

Burcham, PC ^{[1
]}

机构：

[1] UNIV ADELAIDE, DEPT CLIN & EXPT PHARMACOL, ADELAIDE, SA 5005, AUSTRALIA

来源：

CHEMICAL RESEARCH IN TOXICOLOGY | 1997年 / 10卷 / 05期

关键词：

D O I：

10.1021/tx9602022

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

The mutagenicity of peroxyl radicals, ubiquitous products of lipid peroxidation, was assessed using an in vitro M13 forward mutational assay. Single-stranded M13mp19 plasmids were incubated with a range of concentrations of the azo initiator 2,2'-azobis(2-amidinopropane) hydrochloride, and then transfected into competent, SOS-induced Escherichia coli JM105 cells. Incubation with peroxyl radicals produced a concentration-dependent decrease in phage survival, with a 500 mu M concentration of the azo initiator reducing the transfection efficiency by more than 90% while inducing a corresponding B-fold increase in lacZ(alpha), mutation frequencies. Peroxyl radical-induced mutagenesis was completely prevented by the peroxyl radical scavenger Trolox. Automated DNA sequence analysis of the lacZ(alpha), gene of 100 peroxyl radical-induced mutants revealed that the most frequent sequence changes were base pair substitutions (92/95), with G-->T transversions predominating (73/92). Alkaline treatment prior to transfection diminished the mutagenicity of damaged plasmids to a level resembling that of unmodified DNA. While abasic sites might account for the sensitivity to alkaline cleavage, the possibility that unidentified nonabasic alkaline-labile lesions also contribute to peroxyl radical mutagenesis cannot be excluded. Collectively, these findings raise the possibility that DNA damage caused by a major class of endogenous radicals contributes to one of the most common spontaneous mutational events, the G-->T transversion.

引用

页码：575 / 581

页数：7

共 64 条

[1] INACTIVATION OF TRANSFORMING ACTIVITY OF PLASMID DNA BY LIPID-PEROXIDATION [J].

AKASAKA, S .

BIOCHIMICA ET BIOPHYSICA ACTA, 1986, 867 (04) :201-208

[2] MUTAGENESIS RESULTING FROM DNA-DAMAGE BY LIPID-PEROXIDATION IN THE SUPF GENE OF ESCHERICHIA-COLI [J].

AKASAKA, S ;

YAMAMOTO, K .

MUTATION RESEARCH-DNA REPAIR, 1994, 315 (02) :105-112

[3] THE CAUSES AND PREVENTION OF CANCER [J].

AMES, BN ;

GOLD, LS ;

WILLETT, WC .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (12) :5258-5265

[4] ENDOGENOUS DNA DAMAGE AS RELATED TO CANCER AND AGING [J].

AMES, BN .

MUTATION RESEARCH, 1989, 214 (01) :41-46

[5] SPECIFICITY OF IONIZING RADIATION-INDUCED MUTAGENESIS IN THE LAC REGION OF SINGLE-STRANDED PHAGE-M13 MP10 DNA [J].

AYAKI, H ;

HIGO, K ;

YAMAMOTO, O .

NUCLEIC ACIDS RESEARCH, 1986, 14 (12) :5013-5018

[6] INDUCTION OF MUTATIONS BY REPLICATION OF MALONDIALDEHYDE-MODIFIED M13 DNA IN ESCHERICHIA-COLI - DETERMINATION OF THE EXTENT OF DNA MODIFICATION, GENETIC REQUIREMENTS FOR MUTAGENESIS, AND TYPES OF MUTATIONS INDUCED [J].

BENAMIRA, M ;

JOHNSON, K ;

CHAUDHARY, A ;

BRUNER, K ;

TIBBETTS, C ;

MARNETT, LJ .

CARCINOGENESIS, 1995, 16 (01) :93-99

[7]

BURCHAM PC, 1994, J BIOL CHEM, V269, P28844

[8] EVIDENCE THAT LIPID-PEROXIDATION PRODUCTS BIND TO DNA IN LIVER-CELLS [J].

CAO, EH ;

LIU, XQ ;

WANG, LG ;

WANG, JJ ;

XU, NF .

BIOCHIMICA ET BIOPHYSICA ACTA-LIPIDS AND LIPID METABOLISM, 1995, 1259 (02) :187-191

[9]

CHAMULITRAT W, 1989, J BIOL CHEM, V264, P20968

[10] MECHANISMS AND EFFECTS OF LIPID-PEROXIDATION [J].

CHEESEMAN, KH .

MOLECULAR ASPECTS OF MEDICINE, 1993, 14 (03) :191-197

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