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Site-directed mutagenesis of mouse steroid 7 alpha-hydroxylase (cytochrome P-450(7) alpha): role of residue-209 in determining steroid-cytochrome P-450 interaction.

机译：小鼠类固醇7α-羟化酶（细胞色素P-450（7）α）的定点诱变：残基209在确定类固醇与细胞色素P-450相互作用中的作用。

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摘要

We have cloned a cDNA encoding mouse steroid 7 alpha-hydroxylase P450(7) alpha (cytochrome P-450(7) alpha) and expressed it in Saccharomyces cerevisiae. Mouse P450(7) alpha is 70% identical in its amino acid sequence with the mouse steroid 15 alpha-hydroxylase P450(15) alpha (2A4). The Leu at position 209 of P450(15) alpha is the most important residue to determine the steroid hydroxylase activity of the P450 [Lindberg and Negishi (1989) Nature (London) 339, 632-634]. The P450(7) alpha contains Asn at the position corresponding to the Leu-209 of P450(15) alpha, although both P450s hydroxylate testosterone. The CO-reduced P450(7) alpha complex is unstable, so that it is quickly converted into the inactive P420, whereas the P450(15) alpha is very stable. The P450(7) alpha, however, is stabilized either by addition of testosterone or by a mutation of Asn-209 to Leu. The mutant P450(7) alpha displays a 17-fold lower Vmax. value than the wild-type enzyme. Unexpectedly, it also has 3-fold lower Km and Kd values. Residue 209 in P450(7) alpha, therefore, appears to be located at a critical site of the haem-substrate-binding pocket. Corticosterone inhibits the testosterone 7 alpha-hydroxylase activity of the wild-type P450(7) alpha, whereas it does not inhibit the mutant P450(7) alpha. Conversely, the P450(15) alpha activity becomes inhibited by corticosterone upon the replacement of Leu-209 by Asn. In addition, this mutation increases the corticosterone 15 alpha-hydroxylase activity of P450(15) alpha at least 20-fold. Whereas the inhibition by corticosterone depends on the presence of Asn at position 209, deoxycorticosterone inhibits the activities of the P450s regardless of the type of residue at 209. The results indicate, therefore, that the identity of residue 209 determines the affinity as well as specificity of steroid binding to both P450(7) alpha and P450(15) alpha.

机译：我们已经克隆了编码小鼠类固醇7α-羟化酶P450（7）α（细胞色素P-450（7）α）的cDNA，并在酿酒酵母中表达了它。小鼠P450（7）alpha在氨基酸序列上与小鼠类固醇15α-羟化酶P450（15）alpha（2A4）相同。 P450（15）α位置209处的亮氨酸是确定P450甾类羟化酶活性的最重要残基[Lindberg and Negishi（1989）Nature（London）339，632-634]。尽管两个P450均羟基化了睾丸激素，但P450（7）α在对应于P450（15）alpha的Leu-209的位置含有Asn。 CO还原的P450（7）α络合物不稳定，因此可以迅速转化为非活性P420，而P450（15）α则非常稳定。然而，P450（7）α通过添加睾丸激素或Asu-209突变至Leu得以稳定。突变体P450（7）α的Vmax降低了17倍。价值比野生型酶高。出乎意料的是，它的Km和Kd值也降低了3倍。因此，P450（7）alpha中的残基209似乎位于血红素与底物结合的口袋的关键部位。皮质酮抑制野生型P450（7）α的睾丸激素7α-羟化酶活性，而它不抑制突变体P450（7）α。相反，当Asn取代Leu-209时，皮质酮会抑制P450（15）α的活性。此外，此突变将P450（15）α的皮质酮15α-羟化酶活性提高至少20倍。皮质类固醇的抑制作用取决于位置209处Asn的存在，而脱氧皮质酮则抑制P450的活性，而与209位残基的类型无关。因此，结果表明，残基209的身份决定了亲和力和特异性类固醇与P450（7）alpha和P450（15）alpha结合的作用。

著录项

期刊名称 Biochemical Journal
作者
M Iwasaki; R L Lindberg; R O Juvonen; M Negishi;
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年(卷),期 1993(291),Pt 2
年度 1993
页码 569–573
总页数 5
原文格式 PDF
正文语种
中图分类分子生物学;
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专利

1. Site-directed mutagenesis of mouse steroid 7α-hydroxylase (cytochrome P-4507α): role of residue-209 in determining steroid-cytochrome P-450 interaction [J] . M Iwasaki, M Negishi, R L P Lindberg, The biochemical journal . 1993,第2期

机译：小鼠类固醇7α-羟化酶（细胞色素P-4507α）的定点诱变：残基209在确定类固醇与细胞色素P-450相互作用中的作用
2. Use of the steroid derivative RPR 106541 in combination with site-directed mutagenesis for enhanced cytochrome P-450 3A4 structure/function analysis. [J] . Stevens JC, Domanski TL, Harlow GR, The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics . 1999,第2期

机译：类固醇衍生物RPR 106541与定点诱变结合用于增强细胞色素P-450 3A4结构/功能分析的用途。
3. Use of chimeric enzymes and site-directed mutagenesis for identification of three key residues responsible for differences in steroid hydroxylation between canine cytochromes P-450 3A12 and 3A26. [J] . Fraser DJ, He YQ, Harlow GR, Molecular pharmacology. . 1999,第2期

机译：嵌合酶和定点诱变的用途，用于鉴定造成犬细胞色素P-450 3A12和3A26之间甾体羟基化差异的三个关键残基。
4. Regulation of cytochrome P-450 dependent steroid hydroxylase activity in Manduca sexta: Effects of the juvenoids hydroprene and methoprene on ecdysone 20-monooxygenase activity. [D] . Crooks, John Richard. 1993

机译：调节六倍体曼荼罗中细胞色素P-450依赖的甾体羟化酶活性：少年类异戊二烯和异戊二烯对蜕皮激素20-单加氧酶活性的影响。
5. Sex-dependent expression of mouse testosterone 16 alpha-hydroxylase (cytochrome P-450(16) alpha): cDNA cloning and pretranslational regulation. [O] . N Harada, M Negishi 1985

机译：小鼠睾丸激素16α-羟化酶（细胞色素P-450（16）α）的性别依赖性表达：cDNA克隆和翻译前调控。
6. Site-directed mutagenesis of mouse steroid 7α-hydroxylase (cytochrome P-4507α): role of residue-209 in determining steroid-cytochrome P-450 interaction [O] . M Iwasaki, R L P Lindberg, R O Juvonen, 1993

机译：小鼠类固醇7α-羟化酶（细胞色素P-4507α）的诱变诱变：残留物-209在确定类固醇 - 细胞色素P-450相互作用时的作用
7. Inhibition of Aromatase Cytochrome P-450 (Estrogen Synthetase) by Derivatives of alpha-Naphthoflavone [R] . Kellis, J. T. , Nesnow, S. , Vickery, L. E. 1986

机译：α-萘黄酮衍生物对芳香化酶细胞色素p-450（雌激素合成酶）的抑制作用

Site-directed mutagenesis of mouse steroid 7 alpha-hydroxylase (cytochrome P-450(7) alpha): role of residue-209 in determining steroid-cytochrome P-450 interaction.

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