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首页> 外文期刊>Applied and Environmental Microbiology >Metabolism of 6-nitrochrysene by intestinal microflora.
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Metabolism of 6-nitrochrysene by intestinal microflora.

机译:肠道菌群代谢6-硝基丙烯。

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摘要

Since bacterial nitroreduction may play a critical role in the activation of nitropolycyclic aromatic hydrocarbons, we have used batch and semicontinuous culture systems to determine the ability of intestinal microflora to metabolize the carcinogen 6-nitrochrysene (6-NC). 6-NC was metabolized by the intestinal microflora present in the semicontinuous culture system to 6-aminochrysene (6-AC), N-formyl-6-aminochrysene (6-FAC), and 6-nitrosochrysene (6-NOC). These metabolites were isolated and identified by high-performance liquid chromatography, mass spectrometry, and UV-visible spectrophotometry and compared with authentic compounds. Almost all of the 6-NC was metabolized after 10 days. Nitroreduction of 6-NC to 6-AC was rapid; the 6-AC concentration reached a maximum at 48 h. The ratio of the formation of 6-AC to 6-FAC to 6-NOC at 48 h was 93.4:6.3:0.3. Interestingly, compared with results in the semicontinuous culture system, the only metabolite detected in the batch studies was 6-AC. The rate of nitroreduction differed among human, rat, and mouse intestinal microflora, with human intestinal microflora metabolizing 6-NC to the greatest extent. Since 6-AC has been shown to be carcinogenic in mice and since nitroso derivatives of other nitropolycyclic aromatic hydrocarbons are biologically active, our results suggest that the intestinal microflora has the enzymatic capacity to generate genotoxic compounds and may play an important role in the carcinogenicity of 6-NC.
机译:由于细菌的硝基还原作用可能在硝基多环芳烃的活化中起关键作用,因此我们使用分批和半连续培养系统来确定肠道菌群代谢致癌物6-硝基丙烯(6-NC)的能力。半连续培养系统中的肠道菌群将6-NC代谢为6-氨基amino(6-AC),N-甲酰基-6-氨基ch(6-FAC)和6-亚硝基och(6-NOC)。这些代谢物通过高效液相色谱,质谱和紫外可见分光光度法进行分离和鉴定,并与真实化合物进行比较。 10天后几乎所有6-NC都被代谢。 6-NC硝基还原为6-AC的速度很快。 6-AC浓度在48 h达到最大值。在48小时时6-AC至6-FAC至6-NOC的形成比例为93.4:6.3:0.3。有趣的是,与半连续培养系统的结果相比,分批研究中唯一检测到的代谢产物是6-AC。人,大鼠和小鼠肠道菌群的硝化还原速率不同,其中人类肠道菌群最大程度地代谢6-NC。由于6-AC已被证明对小鼠具有致癌作用,并且由于其他硝基多环芳烃的亚硝基衍生物具有生物活性,因此我们的结果表明,肠道菌群具有产生遗传毒性化合物的酶促能力,并且可能在小鼠的致癌性中发挥重要作用。 6-NC。

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