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Evidence for endogenous formation of the hepatocarcinogen N-nitrosodihydrouracil in rats treated with dihydrouracil and sodium nitrite: A potential source of human hepatic DNA carboxyethylation

机译:用二氢尿嘧啶和亚硝酸钠治疗的大鼠中肝致癌物N-亚硝基二氢尿嘧啶的内源性形成的证据:人肝DNA羧乙基化的潜在来源

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An earlier study demonstrated that hydrolysates of all human liver DNA samples analyzed contain the DNA adduct 7-(2'-carboxyethyl)guanine (7-CEGua) with an average level of 74.6 adducts per 109 nucleotides. One possible source of this DNA adduct would be endogenous nitrosation of the normal pyrimidine metabolites dihydrouracil (DHU) and β-ureidopropionic acid (β-UPA), yielding the corresponding nitroso compounds N-nitrosodihydrouracil, a potent hepatocarcinogen, and N-nitroso-β-ureidopropionic acid. Another potential source would be reaction of endogenously formed acrylic acid with DNA. We tested these hypotheses in a study in which rats were treated with NaNO2 in the drinking water, alone, or in combination with dietary DHU or β-UPA, or with acrylic acid in the drinking water, for either 2 or 4weeks. Hepatic DNA from these rats was analyzed for 7-CEGua, using liquid chromatography-tandem mass spectrometry-selected reaction monitoring with confirmation by high resolution mass spectrometry. The results demonstrated consistent statistically significant increases of 7-CEGua in hepatic DNA of the rats treated with the combination of NaNO2 and DHU compared to the corresponding controls, while the other treatments gave variable results. These results support the hypothesis that endogenous nitrosation of DHU could be a major source of 7-CEGua in human hepatic DNA. Development of methodology for analysis of 7-CEGua in human leukocyte DNA is also reported, which will allow testing of this hypothesis in epidemiologic and clinical studies.
机译:较早的一项研究表明,分析的所有人类肝脏DNA样品的水解产物均含有DNA加合物7-(2'-羧乙基)鸟嘌呤(7-CEGua),平均每109个核苷酸有74.6个加合物。该DNA加合物的一种可能来源是正常嘧啶代谢物二氢尿嘧啶(DHU)和β-脲基丙酸(β-UPA)的内源亚硝化作用,产生相应的亚硝基化合物N-亚硝基二氢尿嘧啶,强力肝癌和N-亚硝基-脲基丙酸。另一个潜在的来源是内源形成的丙烯酸与DNA的反应。我们在一项研究中检验了这些假设,在该研究中,大鼠在饮用水中单独使用NaNO2或与饮食DHU或β-UPA联合使用,或在饮用水中用丙烯酸处理2周或4周。使用液相色谱-串联质谱-选择的反应监测方法对这些大鼠的肝DNA进行7-CEGua分析,并通过高分辨率质谱法进行确认。结果表明,与相应的对照组相比,用NaNO2和DHU组合治疗的大鼠肝DNA中7-CEGua的统计学一致性一直具有统计学显着性提高,而其他治疗则产生了不同的结果。这些结果支持这样的假说,即DHU的内源性亚硝化可能是人肝DNA中7-CEGua的主要来源。还报道了开发用于分析人类白细胞DNA中7-CEGua方法的方法,这将有助于在流行病学和临床研究中验证这一假设。

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