Repair of DNA lesions induced by polycyclic aromatic hydrocarbons in human cell-free extracts:: involvement of two excision repair mechanisms in vitro

被引：107

作者：

Braithwaite, E ^{[1
]}

Wu, XH ^{[1
]}

Wang, ZG ^{[1
]}

机构：

[1] Univ Kentucky, Grad Ctr Toxicol, Lexington, KY 40536 USA

来源：

CARCINOGENESIS | 1998年 / 19卷 / 07期

关键词：

D O I：

10.1093/carcin/19.7.1239

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Polycyclic aromatic hydrocarbons (PAHs) are significant environmental pollutants representing an important risk factor in human cancers. DNA adducts formed by the ultimate carcinogens of PAHs are potentially toxic, mutagenic and carcinogenic. DNA repair represents an important defense system against these genotoxic insults, Using a human cell-free system we have examined repair of DNA lesions induced by several PAH dihydrodiol epoxides, including anti-(+/-)-benzo[a]pyrene-trans-7,8-dihydrodiol- 9,10-epoxide, anti-(+/-)-benz[a]anthracene-trans-3,4-dihydro- diol-1,2-epoxide, anti-(+/-)-benz[a]anthracene-trans-8,9-dihydro diol-10,11-epoxide, anti-(+/-)-benzo[b]fluoranthene-trans-9,10-dihydrodiol-11,12-epoxide and anti-(+/-)-chrysene-trans-1,2-dihydrodiol-3,4-epoxide. Effective repair of DNA damage induced by these five PAH metabolites was detected, Two distinct mechanisms of excision repair were observed. The major repair mechanism is nucleotide excision repair (NER), The other mechanism is independent of NER and correlated with the presence of apurinic/apyrimidinic sites in the damaged DNA, thus presumably reflecting base excision repair (BER). However, the contribution of BER to different PAH lesions varied in vitro, These results suggest the possibility that BER may also play an important role in repair of certain PAM-induced DNA lesions.

引用

页码：1239 / 1246

页数：8

共 36 条

[1] PREFERENTIAL MUTAGENESIS AT G.C BASE-PAIRS BY THE ANTI-3,4-DIHYDRODIOL 1,2-EPOXIDE OF 7-METHYLBENZ[A]ANTHRACENE
BIGGER, CAH
FLICKINGER, DJ
STJOHN, J
HARVEY, RG
DIPPLE, A
[J]. MOLECULAR CARCINOGENESIS, 1991, 4 (03) : 176 - 179
[2] MUTATIONAL SPECIFICITY OF THE ANTI 1,2-DIHYDRODIOL 3,4-EPOXIDE OF 5-METHYLCHRYSENE
BIGGER, CAH
FLICKINGER, DJ
STRANDBERG, J
PATAKI, J
HARVEY, RG
DIPPLE, A
[J]. CARCINOGENESIS, 1990, 11 (12) : 2263 - 2265
[3] THE ROLE OF EXCISION REPAIR IN THE REMOVAL OF TRANSIENT BENZO[A]PYRENE-INDUCED DNA LESIONS IN CHINESE HAMSTER OVARY CELLS
BLAKEY, DH
DOUGLAS, GR
[J]. MUTATION RESEARCH, 1990, 236 (01): : 35 - 41
[4] TUMORIGENICITY OF OPTICAL ENANTIOMERS OF DIASTEREOMERIC BENZO[A]PYRENE 7,8-DIOL-9,10-EPOXIDES IN NEWBORN MICE - EXCEPTIONAL ACTIVITY OF(+)-7-BETA, 8-ALPHA-DIHYDROXY-9-ALPHA, 10-ALPHA-EPOXY-7,8.9.10-TETRAHYDROBENZOL[A]PYRENE
BUENING, MK
WISLOCKI, PG
LEVIN, W
YAGI, H
THAKKER, DR
AKAGI, H
KOREEDA, M
JERINA, DM
CONNEY, AH
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1978, 75 (11) : 5358 - 5361
[5] CHANG RL, 1983, CANCER RES, V43, P192
[6] DNA ADDUCTS FROM CARCINOGENIC AND NONCARCINOGENIC ENANTIOMERS OF BENZO[A]PYRENE DIHYDRODIOL EPOXIDE
CHENG, SC
HILTON, BD
ROMAN, JM
DIPPLE, A
[J]. CHEMICAL RESEARCH IN TOXICOLOGY, 1989, 2 (05) : 334 - 340
[7] EXCISION REPAIR BY HUMAN FIBROBLASTS OF DNA DAMAGED BY R-7,T-8-DIHYDROXY -T-9,10-OXY-7,8,9,10-TETRAHYDROBENZO(A)PYRENE
DAY, RS
SCUDIERO, D
DIMATTINA, M
[J]. MUTATION RESEARCH, 1978, 50 (03): : 383 - 394
[8] THE ENZYMOLOGY OF APURINIC APYRIMIDINIC ENDONUCLEASES
DOETSCH, PW
CUNNINGHAM, RP
[J]. MUTATION RESEARCH, 1990, 236 (2-3): : 173 - 201
[9] ESTIMATION OF APURINIC-APYRIMIDINIC SITES AND PHOSPHOTRIESTERS IN DEOXYRIBONUCLEIC-ACID TREATED WITH ELECTROPHILIC CARCINOGENS AND MUTAGENS
DRINKWATER, NR
MILLER, EC
MILLER, JA
[J]. BIOCHEMISTRY, 1980, 19 (22) : 5087 - 5092
[10] FRIEDBERG EC, 1995, DNA REPAIR MUTAGENE

← 1 2 3 4 →