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Detection of Phenolic Metabolites of Styrene in Mouse Liver and Lung Microsomal IncubationsS⃞

机译:小鼠肝脏和肺中苯乙烯的酚类代谢产物的检测 微粒体培养

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摘要

Metabolic activation is considered to be a critical step for styrene-induced pulmonary toxicity. Styrene-7,8-oxide is a primary oxidative metabolite generated by vinyl epoxidation of styrene. In addition, urinary 4-vinylphenol (4-VP), a phenolic metabolite formed by aromatic hydroxylation, has been detected in workers and experimental animals after exposure to styrene. In the present study, new oxidative metabolites of styrene, including 2-vinylphenol (2-VP), 3-vinylphenol (3-VP), vinyl-1,4-hydroquinone, and 2-hydroxystyrene glycol were detected in mouse liver microsomal incubations. The production rates of 2-VP, 3-VP, 4-VP, and styrene glycol were 0.0527 ± 0.0045, 0.0019 ± 0.0006, 0.0053 ± 0.0002, and 4.42 ± 0.33 nmol/(min · mg protein) in mouse liver microsomes, respectively. Both disulfiram (100 μM) and 5-phenyl-1-pentyne (5 μM) significantly inhibited the formation of the VPs and styrene glycol. 2-VP, 3-VP, and 4-VP were metabolized in mouse liver microsomes at rates of 2.50 ± 0.30, 2.63 ± 0.13, and 3.45 ± 0.11 nmol/(min · mg protein), respectively. The three VPs were further metabolized to vinylcatechols and/or vinyl-1,4-hydroquinone and the corresponding glycols. Pulmonary toxicity of 2-VP, 3-VP, and 4-VP was evaluated in CD-1 mice, and 4-VP was found to be more toxic than 2-VP and 3-VP.
机译:代谢活化被认为是苯乙烯诱导的肺毒性的关键步骤。苯乙烯-7,8-氧化物是通过苯乙烯的乙烯基环氧化反应生成的主要氧化代谢物。此外,在工人和实验动物中,接触苯乙烯后,检出了由芳香族羟基化形成的酚类代谢产物尿4-乙烯基苯酚(4-VP)。在本研究中,在小鼠肝微粒体温育中检测到了苯乙烯的新氧化代谢产物,包括2-乙烯基苯酚(2-VP),3-乙烯基苯酚(3-VP),乙烯基-1,4-对苯二酚和2-羟基苯乙烯二醇。 。小鼠肝微粒体中2-VP,3-VP,4-VP和苯乙烯乙二醇的生产率分别为0.0527±0.0045、0.0019±0.0006、0.0053±0.0002和4.42±0.33 nmol /(min·mg蛋白) 。双硫仑(100μM)和5-苯基-1-戊炔(5μM)均显着抑制VP和苯乙烯乙二醇的形成。 2-VP,3-VP和4-VP在小鼠肝微粒体中的代谢速率分别为2.50±0.30、2.63±0.13和3.45±0.11 nmol /(min·mg蛋白)。三个VP进一步代谢为乙烯基邻苯二酚和/或乙烯基-1,4-氢醌和相应的二醇。在CD-1小鼠中评估了2-VP,3-VP和4-VP的肺毒性,发现4-VP比2-VP和3-VP毒性更高。

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