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(-)反式-7,8-二羟基-7,8-二氢苯并[a]芘代谢产物与细胞色素P-450 LM2和LM4以及NADPH-细胞色素P-450还原酶的共价结合研究。

Studies on covalent binding of (-)trans-7,8-dihydroxy-7,8-dihydrobenzo[a]pyrene metabolites to cytochromes P-450 LM2 and LM4 and NADPH-cytochrome P-450 reductase.

作者信息

Deutsch J, Vatsis K P, Leutz J C, Coon M J, Gelboin H V

机构信息

Laboratory of Molecular Carcinogenesis, National Cancer Institute, Bethesda, Maryland 20892.

出版信息

Xenobiotica. 1989 Dec;19(12):1421-35. doi: 10.3109/00498258909043193.

DOI:10.3109/00498258909043193
PMID:2515665
Abstract
  1. Metabolism of 14C-labelled benzo[a]pyrene (-)trans-7,8-dihydrodiol to protein- and DNA-binding products in a reconstituted enzyme system proceeds 5 to 10 times faster with rabbit cytochrome P-450 LM4 than with LM2. 2. Either cytochrome converts the substrate to ethyl acetate- and water-soluble metabolites, identified by h.p.l.c. Water-soluble metabolites comprise 78% of the total products with cytochrome P-450 LM2, but only 50% of those formed by LM4. The relative proportion of the two types of metabolites is differentially affected by certain modifiers such as 7,8-benzoflavone. 3. Half of the radioactivity in the aqueous phase of reaction mixtures containing cytochrome P-450 LM4 represents (-)trans-7,8-diol metabolites in complex primarily with NADPH and phosphate. The remaining water-soluble products are bound covalently to proteins in the reconstituted system. 4. Polyacrylamide gel electrophoresis, autoradiography, and measurement of the radioactivity in individual bands indicate that a larger fraction of metabolites is bound to cytochrome P-450 LM4 than to NADPH-cytochrome P-450 reductase, and only marginal binding to cytochrome P-450 LM2 is seen. Metabolite binding to added DNA is likewise substantially greater in magnitude when cytochrome P-450 LM4, as opposed to LM2, catalyses (-)trans-7,8-diol oxygenation. Thus, the degree of metabolite binding to monoxygenase proteins and to DNA correlates well with the catalytic activity of cytochrome P-450 LM4 and LM2 towards (-)trans-7,8-diol. 5. DNA causes a dramatic enhancement in the activity of cytochrome P-450 LM4 with (-)trans-7,8-diol, indicating that the cytochrome and/or the reductase may be functionally impaired by metabolites of this substrate. Such an effect may alter the balance between detoxication and activation of the carcinogenic benzo[a]pyrene.
摘要
  1. 在重组酶系统中,14C标记的苯并[a]芘(-)反式-7,8-二氢二醇代谢生成与蛋白质和DNA结合产物的过程,兔细胞色素P-450 LM4比LM2快5至10倍。2. 两种细胞色素都将底物转化为乙酸乙酯和水溶性代谢产物,通过高效液相色谱法鉴定。水溶性代谢产物在细胞色素P-450 LM2生成的总产物中占78%,但在LM4生成的产物中仅占50%。两种代谢产物的相对比例受到某些修饰剂如7,8-苯并黄酮的不同影响。3. 含有细胞色素P-450 LM4的反应混合物水相中的放射性有一半代表主要与NADPH和磷酸盐结合的(-)反式-7,8-二醇代谢产物。其余水溶性产物在重组系统中与蛋白质共价结合。4. 聚丙烯酰胺凝胶电泳、放射自显影以及对各条带放射性的测量表明,与NADPH-细胞色素P-450还原酶相比,更多比例的代谢产物与细胞色素P-450 LM4结合,而与细胞色素P-450 LM2的结合仅为微量。当细胞色素P-450 LM4而非LM2催化(-)反式-7,8-二醇氧化时,代谢产物与添加的DNA的结合量同样显著更高。因此,代谢产物与单加氧酶蛋白和DNA的结合程度与细胞色素P-450 LM4和LM2对(-)反式-7,8-二醇的催化活性密切相关。5. DNA使细胞色素P-450 LM4对(-)反式-7,8-二醇的活性显著增强,表明该细胞色素和/或还原酶可能受到该底物代谢产物的功能损害。这种效应可能会改变致癌性苯并[a]芘解毒与活化之间的平衡。

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1
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Xenobiotica. 1989 Dec;19(12):1421-35. doi: 10.3109/00498258909043193.
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