1,N-6-ETHENODEOXYADENOSINE AND 3,N-4-ETHENODEOXYCYTIDINE IN LIVER DNA FROM HUMANS AND UNTREATED RODENTS DETECTED BY IMMUNOAFFINITY P-32 POSTLABELING

被引:218
作者
NAIR, J [1 ]
BARBIN, A [1 ]
GUICHARD, Y [1 ]
BARTSCH, H [1 ]
机构
[1] INT AGCY RES CANC,F-69372 LYON 08,FRANCE
关键词
D O I
10.1093/carcin/16.3.613
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The etheno-bridged exocyclic DNA adducts 1,N-6-ethenodeoxyadenosine (epsilon dA) and epsilon,N-4-ethenadeoxycytine (epsilon dC) can be formed by several structurally diverse carcinogens and mutagens that include vinyl chloride and urethane. In order to investigate the occurrence and persistence of these adducts in rodents exposed to such DNA-damaging agents, an ultra-sensitive detection method has been developed. It is based on immunoaffinity purification of the etheno adducts and subsequent P-32-postlabelling followed by separation as 5'-monophosphates on polyethyleneimine-cellulose-coated thin-layer plates. Normal nucleotides in the DNA samples were quantitated by HPLC. Optimal conditions for enzymatic hydrolysis of DNA are described: deoxyuridine 3'-monophosphate was used as internal standard to correct for labelling efficiency of the etheno adducts. The method had a detection limit of 25 amol of epsilon dA and epsilon dC for a 50 mu g DNA sample. Using this technique, analysis of liver DNA from humans with unknown exposure revealed the presence of epsilon dA and epsilon dC residues in the range of 0-27 adducts per 10(9) parent bases. Liver DNA obtained from untreated mice and rats was also shown to contain similar low but variable levels of these etheno adducts. In vitro studies indicated that these promutagenic DNA lesions could arise from endogenously formed lipid peroxidation products.
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页码:613 / 617
页数:5
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