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首页> 外文期刊>Chemico-biological interactions >Bioactivation of 1-chloro-2-hydroxy-3-butene, an in vitro metabolite of 1,3-butadiene, by rat liver microsomes
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Bioactivation of 1-chloro-2-hydroxy-3-butene, an in vitro metabolite of 1,3-butadiene, by rat liver microsomes

机译:1-氯-2-羟基-3-丁烯,1,3-丁二烯的体外代谢物的生物活化,通过大鼠肝微粒体

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Abstract 1-Chloro-2-hydroxy-3-butene (CHB) is an in vitro metabolite of 1,3-butadiene, a rodent/human carcinogen. To search for an approach detecting CHB in vivo, it is vital to obtain a full understanding of CHB metabolism. Previously, we demonstrated that CHB was bioactivated to 1-chloro-3-buten-2-one (CBO) by alcohol dehydrogenase. However, CHB metabolism by cytochrome P450s has not been reported. Thus, in the present study, CHB metabolism by rat liver microsomes was investigated. The results showed that CHB was converted to 1-chloro-3,4-epoxy-2-butanol (CEB) and CBO. 4-Methylpyrazole, a cytochrome P450 2E1-specific inhibitor, inhibited the formation of both CEB and CBO, while 1-benzylimidazole, a generic cytochrome P450 inhibitor, completely abolished the formation of CEB and CBO, suggesting that CHB metabolism was mediated by cytochrome P450s. Because the molecules have two chiral centers, CEB was detected as two stereoisomers, which were designated D-CEB and M-CEB, and were characterized as (2 S ,3 R )-/(2 R ,3 S )-CEB and (2 R ,3 R )-/(2 S ,3 S )-CEB, respectively. The amounts of M-CEB were more than those of D-CEB by 50–80%. The amounts of CEB and CBO increased linearly over time from 10 (or 20?min for CBO) to 50?min. CHB metabolism followed Michaelis-Menten kinetics; the K m and V max values were determined to be 6.4?±?0.7?mM and 0.10?±?0.01?nmol/min/mg protein for D-CEB, 4.2?±?0.5?mM and 0.16?±?0.01?nmol/min/mg protein for M-CEB, and 4.0?±?0.5?mM and 4.6?±?0.5?nmol/min/mg protein for CBO, respectively. Thus, CBO was the dominant product of CHB metabolism. Moreover, CEB was genotoxic at ≥ 50?μM as evaluated by the comet assay. Collectively, the data showed that CHB could be bioactivated to CEB and CBO by cytochrome P450s with CBO being the predominant product. Thus, the formation of CEB and CBO can be used as evidence of CHB production. The products may also play a role in toxicity of CHB. Graphical abstract Display Omitted Highlights ? 1-Chloro-2-hydroxy-3-butene could be metabolized by rat liver microsomes. ? Products were 1-chloro-3,4-epoxy-2-butanol (CEB) and 1-chloro-3-buten-2-one (CBO). ? Two CEB stereoisomers, (2 S ,3 R )-/(2 R ,3 S )-CEB and (2 R ,3 R )-/(2 S ,3 S )-CEB, were detected. ? CBO was the dominant product and all enzymatically kinetic constants were measured. ? Both CEB stereoisomers were genotoxic at?≥?50? μ M as examined by the comet assay.
机译:摘要1-氯-2-羟基-3-丁烯(CHB)是1,3-丁二烯,啮齿动物/人类致癌物质的体外代谢物。为了搜索在体内检测CHB的方法,对CHB新陈代谢充分了解至关重要。以前,我们证明CHB通过醇脱氢酶对1-氯-3-丁烯-2-一(CBO)生物活化。然而,尚未报告细胞色素P450的CHB代谢。因此,在本研究中,研究了大鼠肝微粒体的CHB代谢。结果表明,CHB转化为1-氯-3,4-环氧-2-丁醇(CEB)和CBO。 4-甲基吡唑,一种细胞色素P450 2E1特异性抑制剂,抑制了CEB和CBO的形成,而1-苄基咪唑,一种通用细胞色素P450抑制剂,完全废除了CEB和CBO的形成,表明CHB代谢由细胞色素P450介导。因为分子具有两个手性中心,所以将CEB检测为两个立体异构体,其被指定为D-CEB和M-CEB,并被表征为(2 S,3 R) - /(2R,3 S)-CEB和( 2 r,3 r) - /(2 s,3 s)-ceb。 M-CEB的量大于D-CEB的量50-80%。 CEB和CBO的量随时间的时间从10(或20μm)到50?min的时间增加。 CHB新陈代谢跟随Michaelis-Menten动力学;将K m和v max值确定为6.4?±0.7Ω·mm和0.10?±0.10?nmol / min / mg蛋白为D-CeB,4.2?±0.5?mm和0.16?±0.16?0.01?对于M-CEB的Nmol / min / mg蛋白,和4.0?±0.5Ω·mm和4.6?±0.5?Nmol / min / mg蛋白,分别用于CBO。因此,CBO是CHB新陈代谢的主要产物。此外,CEB的基因毒性为≥50Ωμm,如彗星测定评估的。统称,数据显示CHB可以通过CoCochrome P450S与COB和CBO进行生物活化,CON为主要产品。因此,CEB和CBO的形成可用作CHB生产的证据。产品也可能在CHB的毒性中起作用。图形抽象显示省略了亮点?可以通过大鼠肝微粒体代谢1-氯-2-羟基-3-丁烯。还产物是1-氯-3,4-环氧-2-丁醇(CEB)和1-氯-3-丁烯-2-一(CBO)。还检测到两个CEB立体异构体,(2S,3 r) - /(2 r,3 s)-ceb和(2 r,3 r) - /(2 s,3 s)-ceb。还CBO是主要产品,测量所有酶活性动力学常数。还CEB立体异构体都是遗传毒性的?≥≤50?由彗星测定检查μm。

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