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小鼠中二苯并[a,j]吖啶DNA加合物的32P后标记分析:初始遗传毒性代谢物的初步测定及其对生物标志物水平的影响

32P-postlabeling analysis of dibenz[a,j]acridine DNA adducts in mice: preliminary determination of initial genotoxic metabolites and their effect on biomarker levels.

作者信息

Roh J, Schamer M, Reilman R, Xue W, Warshawsky D, Talaska G

机构信息

Dept. of Preventive Medicine and Public Health, Yonsei University College of Medicine, Seoul, Korea.

出版信息

Int Arch Occup Environ Health. 1993;65(1 Suppl):S99-102. doi: 10.1007/BF00381316.

Abstract

N-Heterocyclic aromatics (NHA) are widely occurring environmental pollutants formed during the pyrolysis of nitrogen-containing organic chemicals. NHA are found in significant amounts in tobacco condensates, synthetic fuels, gasoline engine exhaust, and effluents from the heating of coal. Dibenz[a,j]acridine (DBA) is an example of NHA. The potency of many carcinogenic compounds is related, at least in part, to the efficiency of their biological activation. We undertook studies to determine which initial metabolites of DBA lead to the formation of high levels of carcinogen-DNA adducts in vivo. DBA and its metabolites, trans-DBA-1,2-dihydrodiol (DBA-1,2-DHD), trans-DBA-3,4-dihydrodiol (DBA-3,4-DHD), and trans-DBA-5,6-dihydrodiol (DBA-5,6-DHD), were applied to the skin of mice. DNA was isolated using enzyme-solvent extraction method. DNA was 32P-postlabeled under conditions of limiting [32P]ATP. In skin, DBA produced two distinct adducts. The same two adducts were seen when DBA-3,4-DHD was applied. In addition the total adduct level elicited by DBA-3,4-DHD was higher than that of parent compound. Two adducts were seen when DBA-5,6DHD was applied, but these were very different from adducts seen with DBA. These results suggested that activation of DBA to DNA-binding compounds in skin includes initial formation of DBA-3,4-DHD. The data support development of biomarkers for the exposure and effect of this compound, and also suggest that specific metabolic susceptibility markers might be able to predict populations at increased risk.

摘要

N-杂环芳烃(NHA)是含氮有机化学品热解过程中广泛产生的环境污染物。在烟草冷凝物、合成燃料、汽油发动机尾气以及煤炭燃烧产生的废水中都大量存在NHA。二苯并[a,j]吖啶(DBA)就是NHA的一个例子。许多致癌化合物的致癌性至少部分与它们的生物活化效率有关。我们开展研究以确定DBA的哪些初始代谢产物会在体内导致高水平致癌物-DNA加合物的形成。将DBA及其代谢产物反式-DBA-1,2-二氢二醇(DBA-1,2-DHD)、反式-DBA-3,4-二氢二醇(DBA-3,4-DHD)和反式-DBA-5,6-二氢二醇(DBA-5,6-DHD)涂抹于小鼠皮肤。采用酶-溶剂萃取法分离DNA。在[32P]ATP受限的条件下对DNA进行32P后标记。在皮肤中,DBA产生两种不同的加合物。涂抹DBA-3,4-DHD时也观察到同样的两种加合物。此外,DBA-3,4-DHD引发的总加合物水平高于母体化合物。涂抹DBA-5,6-DHD时观察到两种加合物,但这些加合物与DBA产生的加合物非常不同。这些结果表明,DBA在皮肤中活化为DNA结合化合物的过程包括DBA-3,4-DHD的初始形成。这些数据支持开发该化合物暴露和效应的生物标志物,也表明特定的代谢易感性标志物或许能够预测风险增加的人群。

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