雌激素农药甲氧氯和滴滴涕对大鼠肝脏CYP2B和CYP3A酶的诱导作用。对甲氧氯代谢的影响。

Journal of biochemical toxicology Pub Date : 1995-02-01
H C Li, S S Dehal, D Kupfer
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引用次数: 0

摘要

在早期的研究中,甲氧基氯处理并没有引起大鼠肝脏P450单加氧酶的诱导,这显然是由于甲氧基氯在体内的半衰期短。目前的研究表明,雌性大鼠每日多次服用甲氧氯可显著诱导肝微粒体P450 2B1/2B2和3A蛋白的表达。CYP1A1和CYP2E1蛋白均未增加,表明甲氧氯诱导具有选择性。同样,甲氧氯类似物滴滴涕(DDT)可以增加CYP2B和3A蛋白,但对CYP1A1和2E1没有影响。甲氧基氯适度提高CYP2B和3A催化的酶活性。在未成熟大鼠中,只有较高剂量的甲氧基氯(300 mg/kg)在16 α位置(主要产物)产生睾酮羟基化升高,这具有统计学意义,表明CYP2B1/2B2的催化作用增强。低剂量(150 mg/kg)和高剂量(300 mg/kg)甲氧基氯均增加了睾酮的6 β羟化(主要产物)和2 β和15 β羟化(次要产物),表明CYP3A的催化作用增强。在成熟雌性大鼠中,甲氧基氯和滴滴涕处理均可提高16 α和6 β羟基化和雄烯二酮的形成。甲氧基氯和ddt介导的CYP2B酶活性在成熟和未成熟大鼠中诱导的另一个适应症是甲氧基氯环羟基化的增加,这种活性归因于CYP2B。这些发现表明,甲氧氯和滴滴涕属于苯巴比妥型诱导剂,暴露于甲氧氯可影响其自身代谢。甲氧基氯介导的CYP2B和3A蛋白的增加明显大于相应酶活性的增加。本文讨论了P450水平与其酶活性之间缺乏相关性的可能原因,以及甲氧氯诱导其代谢和毒性的潜在相关性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Induction of the hepatic CYP2B and CYP3A enzymes by the proestrogenic pesticide methoxychlor and by DDT in the rat. Effects on methoxychlor metabolism.

In earlier investigations, methoxychlor treatment did not elicit induction of hepatic P450 monooxygenases in rats, apparently due to the short half-life of methoxychlor in vivo. The current study demonstrates that multiple bidaily doses of methoxychlor to female rats produce a marked induction of the hepatic microsomal P450 2B1/2B2 and 3A proteins. There was no increase in CYP1A1 or CYP2E1 proteins, demonstrating selectivity of induction by methoxychlor. Similarly, treatment with DDT, a methoxychlor analog, increased CYP2B and 3A proteins but had no effect on CYP1A1 and 2E1. Methoxychlor moderately elevated the enzymatic activity corresponding to CYP2B and 3A catalysis. In immature rats, only the higher dose of methoxychlor (300 mg/kg), produced elevation of testosterone hydroxylation at the 16 alpha position (major product) that was statistically significant, indicative of increased catalysis by CYP2B1/2B2. Both the low (150 mg/kg) and high dose (300 mg/kg) of methoxychlor increased the 6 beta hydroxylation (major product) and 2 beta and 15 beta hydroxylation (minor products) of testosterone, indicative of increased catalysis by CYP3A. In mature female rats, both methoxychlor and DDT treatment elevated the 16 alpha and 6 beta hydroxylation and androstenedione formation. Additional indication of methoxychlor- and DDT-mediated induction of CYP2B enzymatic activity in mature and immature rats was evident from increased ring hydroxylation of methoxychlor, an activity attributed to CYP2B. These findings indicate that methoxychlor and DDT belong to the phenobarbital type of inducers and that exposure to methoxychlor can affect its own metabolism. The methoxychlor-mediated increase in CYP2B and 3A proteins was considerably larger than the increase in the corresponding enzymatic activities. The possible reasons for the lack of correlation between P450 levels and their enzymatic activities and the potential relevance of induction by methoxychlor to its metabolism and toxicity are discussed.

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