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Metabolism of aflatoxin B1 by rat hepatic microsomes induced by polyhalogenated biphenyl congeners.

机译:多卤代联苯同源物诱导的大鼠肝微粒体代谢黄曲霉毒素B1。

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The metabolism of aflatoxin B1 to aflatoxins M1 and Q1 by rat liver microsomes from animals pretreated with polychlorinated or polybrominated biphenyl congeners depended on the structure of the halogenated biphenyl inducers. Microsomes from rats treated with phenobarbital (PB) or halogenated biphenyls that exhibit PB-type activity preferentially enhanced the conversion of aflatoxin B1 to aflatoxin Q1. In contrast, microsomes from rats treated with 3-methylcholanthrene (MC) or halogenated biphenyls that exhibit MC-type induction activity increased the metabolism of aflatoxin B1 to aflatoxin M1. The coadministration of PB and MC produced microsomes that exhibited both types of induction activity (mixed type) in catalyzing the oxidative metabolism of diverse xenobiotic agents. However, PB-plus-MC-induced hepatic microsomes from immature male Wistar rats preferentially increased the metabolism of aflatoxin B1 to aflatoxin M1 but did not enhance the conversion of aflatoxin B1 to aflatoxin Q1. Comparable results were observed with microsomes from rats pretreated with halogenated biphenyls classified as mixed-type inducers; moreover, in some cases there was a significant decrease in the conversion of aflatoxin B1 to aflatoxin Q1 (compared with that of controls treated with corn oil).
机译:用多氯或多溴联苯同源物预处理的动物的大鼠肝脏微粒体将黄曲霉毒素B1代谢为黄曲霉毒素M1和Q1取决于卤代联苯诱导物的结构。用苯巴比妥(PB)或表现出PB型活性的卤代联苯处理的大鼠微粒体优先增强了黄曲霉毒素B1向黄曲霉毒素Q1的转化。相比之下,来自老鼠的微粒体经3-甲基胆固醇(MC)或卤代联苯处理后表现出MC型诱导活性,从而增加了黄曲霉毒素B1向黄曲霉毒素M1的代谢。 PB和MC的共同给药产生的微粒体在催化多种异源生物试剂的氧化代谢中均表现出两种诱导活性(混合型)。但是,未成熟雄性Wistar大鼠的PB-plus-MC诱导的肝微粒体优先增加了黄曲霉毒素B1向黄曲霉毒素M1的代谢,但并未增强黄曲霉毒素B1向黄曲霉毒素Q1的转化。用分类为混合型诱导剂的卤代联苯预处理的大鼠微粒体观察到了可比的结果。此外,在某些情况下,黄曲霉毒素B1向黄曲霉毒素Q1的转化率显着下降(与用玉米油处理的对照相比)。

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