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Time course of DNA adduct formation in peripheral blood granulocytes and lymphocytes after drinking alcohol

机译:饮酒后外周血粒细胞和淋巴细胞中DNA加合物形成的时程

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Alcohol consumption is an established risk factor for cancers of the head and neck, colorectum, liver and female breast. Acetaldehyde, the primary metabolite of ethanol, is suspected to play a major role in alcohol-related carcinogenesis. Acetaldehyde binds to DNA resulting in formation of adducts. DNA adducts are involved in mutagenesis and carcinogenesis. N 2- Ethylidenedeoxyguanosine (N 2-ethylidene-dGuo) is the major adduct formed in this reaction. Studies have shown an association between alcohol drinking and levels of this DNA adduct, suggesting its potential use as a biomarker for studying alcohol-related carcinogenesis. However, there are no reports on the kinetics of formation and repair of N 2-ethylidene-dGuo after alcohol consumption. Therefore, we investigated levels of N 2-ethylidene-dGuo in DNA from human peripheral blood cells at several time points after consumption of increasing doses of alcohol. Ten healthy non-smokers were recruited and asked to abstain from alcohol consumption except for the study doses. The subjects were given measured doses of alcohol once a week for 3 weeks, targeting increasing blood alcohol levels. Blood was collected at several time points before and after each dose, DNA was isolated from granulocytes and lymphocytes and N 2-ethylidene-dGuo was quantified as its NaBH 3CN reduction product N 2-ethyldeoxyguanosine by liquid chromatography-electrospray ionisation-tandem mass spectrometry. Significant increases in N 2-ethylidene-dGuo were observed after all doses and in both cell types. However, there was substantial intraindividual variability, indicating that there are other important sources of this adduct in peripheral blood DNA. Further studies are needed to better understand the origins of N 2-ethylidene-dGuo in blood cells, the exposures it reflects, and thus its potential use as a marker of alcohol's genotoxic effects.
机译:饮酒是确定的头颈癌,结肠直肠癌,肝癌和女性乳腺癌的危险因素。乙醛是乙醇的主要代谢产物,被怀疑在与酒精有关的癌变过程中起主要作用。乙醛与DNA结合,形成加合物。 DNA加合物参与诱变和致癌作用。 N 2-乙二氧基鸟苷(N 2-亚乙基-dGuo)是该反应中形成的主要加合物。研究表明,饮酒与该DNA加合物的水平之间存在关联,表明其潜在用途可作为研究与酒精相关的癌变的生物标记。但是,没有关于饮酒后N 2-亚乙基-dGuo形成和修复动力学的报道。因此,我们研究了在饮酒剂量增加后的几个时间点,人类外周血细胞DNA中N 2-亚乙基-dGuo的水平。招募了十名健康的非吸烟者,要求除研究剂量外戒酒。受试者每周3次每周接受一次测定剂量的酒精,以提高血液中的酒精含量为目标。在每次给药之前和之后的几个时间点收集血液,通过液相色谱-电喷雾电离串联质谱法从粒细胞和淋巴细胞中分离DNA,并将N 2-亚乙基-dGuo定量为其NaBH 3CN还原产物N 2-乙基脱氧鸟苷。在所有剂量和两种细胞类型中均观察到N 2-亚乙基-dGuo的显着增加。然而,个体间存在很大的个体差异,表明外周血DNA中该加合物还有其他重要来源。需要进一步研究以更好地了解血细胞中N 2-亚乙基-dGuo的起源,其所反映的暴露程度,并因此有可能将其用作酒精遗传毒性作用的标志。

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