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分析人体尿液中4-(甲基亚硝胺基)-1-(3-吡啶基)-1-丁酮(一种烟草特异性肺癌致癌物)的吡啶-N-氧化物代谢产物。

Analysis of human urine for pyridine-N-oxide metabolites of 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone, a tobacco-specific lung carcinogen.

作者信息

Carmella S G, Borukhova A, Akerkar S A, Hecht S S

机构信息

American Health Foundation, Valhalla, New York 10595, USA.

出版信息

Cancer Epidemiol Biomarkers Prev. 1997 Feb;6(2):113-20.

PMID:9037562
Abstract

4-(Methylnitrosamino)-1-(3-pyridyl)-1-butanone (NNK) is a potent pulmonary carcinogen in rodents and is believed to be a causative factor for lung cancer in smokers. NNK also may be involved in oral cancer etiology in users of smokeless tobacco products. Pyridine-N-oxidation of NNK and its major metabolite, 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanol (NNAL), produces NNK-N-oxide and NNAL-N-oxide, respectively, which are detoxification products of NNK metabolism and are excreted in the urine of rodents and primates. Our goal is to develop a panel of urinary biomarkers to assess the metabolic activation and detoxification of NNK in humans. In this study, we developed methodology to analyze human urine for NNK-N-oxide and NNAL-N-oxide. The key step in the method was conversion of the N-oxides to NNK and NNAL by treatment with Proteus mirabilis. The resulting samples were then analyzed essentially by methods that we have described previously. 4-(Methylnitrosamino)-4-(3-pyridyl-N-oxide)-1-butanol (iso-NNAL-N-oxide) was used as internal standard. Levels of NNAL-N-oxide in smokers' urine ranged from 0.06 to 1.4 pmol/mg creatinine, mean +/- SD 0.53 +/- 0.36 pmol/mg creatinine. Its presence was confirmed by high performance liquid chromatography-electrospray ionization-tandem mass spectrometry. NNK-N-oxide was not detected in smokers' urine. Levels of NNAL-N-oxide in the urine of smokeless tobacco users ranged from 0.02 to 1.2 pmol/mg creatinine, mean +/- SD 0.41 +/- 0.35 pmol/mg creatinine. The amounts of NNAL-N-oxide in urine were less than 20% of those of [4-(methylnitrosamino)-1-(3-pyridyl)but-1-yl]-beta-O-D-glucosiduronic acid (NNAL-Gluc) and were approximately 50% as great as those of free NNAL. These results demonstrate that pyridine-N-oxidation is a relatively minor detoxification pathway of NNK and NNAL in humans. The method was applied to analysis of urine from 11 smokers who consumed a diet containing watercress. In an earlier study (S.S. Hecht et al., Cancer Epidemiol., Biomarkers & Prev., 4: 877-884, 1995), we showed that consumption of watercress, a source of phenethyl isothiocyanate (PEITC), caused an increase in urinary excretion of NNAL plus NNAL-Gluc. This was attributed to inhibition of alpha-hydroxylation of NNK by PEITC, as seen in rodents in which PEITC also inhibits the pulmonary carcinogenicity of NNK. However, PEITC also could have inhibited pyridine-N-oxidation of NNK and NNAL. The urine of these smokers was analyzed for NNAL-N-oxide. The results demonstrated that watercress consumption had no effect on levels of NNAL-N-oxide in urine, supporting the conclusion that PEITC does inhibit the metabolic activation of NNK in humans.

摘要

4-(甲基亚硝基氨基)-1-(3-吡啶基)-1-丁酮(NNK)是一种在啮齿动物中具有强致癌性的肺部致癌物,被认为是吸烟者患肺癌的一个致病因素。NNK也可能与无烟烟草产品使用者的口腔癌病因有关。NNK及其主要代谢产物4-(甲基亚硝基氨基)-1-(3-吡啶基)-1-丁醇(NNAL)发生吡啶-N-氧化反应,分别生成NNK-N-氧化物和NNAL-N-氧化物,它们是NNK代谢的解毒产物,通过啮齿动物和灵长类动物的尿液排出。我们的目标是开发一组尿液生物标志物,以评估人类体内NNK的代谢活化和解毒情况。在本研究中,我们开发了分析人尿液中NNK-N-氧化物和NNAL-N-氧化物的方法。该方法的关键步骤是通过奇异变形杆菌处理将N-氧化物转化为NNK和NNAL。然后,基本上按照我们之前描述的方法对所得样品进行分析。4-(甲基亚硝基氨基)-4-(3-吡啶基-N-氧化物)-1-丁醇(异-NNAL-N-氧化物)用作内标。吸烟者尿液中NNAL-N-氧化物的水平范围为0.06至1.4皮摩尔/毫克肌酐,平均值±标准差为0.53±0.36皮摩尔/毫克肌酐。通过高效液相色谱-电喷雾电离-串联质谱法确认了其存在。在吸烟者尿液中未检测到NNK-N-氧化物。无烟烟草使用者尿液中NNAL-N-氧化物的水平范围为0.02至1.2皮摩尔/毫克肌酐,平均值±标准差为0.41±0.35皮摩尔/毫克肌酐。尿液中NNAL-N-氧化物的量不到[4-(甲基亚硝基氨基)-1-(3-吡啶基)丁-1-基]-β-O-D-葡萄糖醛酸(NNAL-Gluc)的20%,约为游离NNAL的50%。这些结果表明,吡啶-N-氧化是人类体内NNK和NNAL相对次要的解毒途径。该方法应用于分析11名食用含豆瓣菜饮食的吸烟者的尿液。在早期研究(S.S.赫克特等人,《癌症流行病学、生物标志物与预防》,4:877 - 884,1995)中,我们表明食用作为苯乙基异硫氰酸酯(PEITC)来源的豆瓣菜会导致NNAL加NNAL-Gluc的尿排泄增加。这归因于PEITC对NNK的α-羟基化的抑制作用,正如在啮齿动物中所见,其中PEITC也抑制NNK的肺部致癌性。然而,PEITC也可能抑制了NNK和NNAL的吡啶-N-氧化反应。对这些吸烟者的尿液进行NNAL-N-氧化物分析。结果表明,食用豆瓣菜对尿液中NNAL-N-氧化物的水平没有影响,支持了PEITC确实抑制人类体内NNK代谢活化的结论。

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