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细胞色素P-450加氧酶的内在多功能性。通过117位的单个氨基酸突变赋予细胞色素P-450 2a-4脱氢表雄酮羟化酶活性。

Inherent versatility of P-450 oxygenase. Conferring dehydroepiandrosterone hydroxylase activity to P-450 2a-4 by a single amino acid mutation at position 117.

作者信息

Iwasaki M, Darden T A, Parker C E, Tomer K B, Pedersen L G, Negishi M

机构信息

National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, North Carolina 27709.

出版信息

J Biol Chem. 1994 Mar 25;269(12):9079-83.

PMID:8132645
Abstract

Mouse steroid 15 alpha-hydroxylase P-450 2a-4 is restricted in its substrate specificity to the delta 4, 3-ketone steroids such as androstenedione. As a result, the P-450 exhibits little hydroxylase activity toward delta 5, 3-hydroxysteroids including dehydroepiandrosterone (DHEA). A single amino acid mutation of Ala at position 117 to Val, however, is enough to confer a high DHEA hydroxylase activity to P-450 2a-4 with 7 alpha-OH DHEA as one of the two major hydroxylated metabolites. Mouse coumarin 7-hydroxylase P-450 2a-5 contains Val at position 117, but it exhibits very low DHEA hydroxylase activity. P-450 2a-5 acquires high DHEA hydroxylase activity, however, by a mutation of Phe-209 to Asn. Moreover, the mutant P-450 2a-5 loses its activity when Val is replaced by Ala at position 117. The residue at position 117, therefore, plays the principal role in the determination of the DHEA hydroxylase activity of the P-450s. Conversely, mutations at residue 117 have little effect on the androstenedione hydroxylase activities of the P-450s. Further modeling of the DHEA binding orientation in the substrate-heme pocket of bacterial P-450cam (Iwasaki, M., Darden, T., Pedersen, L., Davis, D. G., Juvonen, R. O., Sueyoshi, T., and Negishi, M. (1993) J. Biol. Chem. 268, 759-762) provides support for the hypothesis that the type of residue at position 117 determines the steroid-substrate specificity of the P-450 depending on the substituent at the C3 position of steroid molecule.

摘要

小鼠甾体15α-羟化酶P-450 2a-4的底物特异性仅限于Δ4,3-酮甾体,如雄烯二酮。因此,该P-450对包括脱氢表雄酮(DHEA)在内的Δ5,3-羟基甾体几乎没有羟化酶活性。然而,第117位的丙氨酸单个氨基酸突变为缬氨酸,就足以赋予P-450 2a-4高DHEA羟化酶活性,7α-OH DHEA是两种主要羟化代谢产物之一。小鼠香豆素7-羟化酶P-450 2a-5在第117位含有缬氨酸,但它表现出非常低的DHEA羟化酶活性。然而,P-450 2a-5通过将苯丙氨酸-209突变为天冬酰胺而获得高DHEA羟化酶活性。此外,当第117位的缬氨酸被丙氨酸取代时,突变型P-450 2a-5失去其活性。因此,第117位的残基在决定P-450的DHEA羟化酶活性中起主要作用。相反,第117位残基的突变对P-450的雄烯二酮羟化酶活性影响很小。对细菌P-450cam底物-血红素口袋中DHEA结合方向的进一步建模(岩崎,M.,达登,T.,佩德森,L.,戴维斯,D.G.,尤沃宁,R.O.,末吉,T.,和根岸,M.(1993年)《生物化学杂志》268,759 - 762)为以下假设提供了支持:第117位残基的类型根据甾体分子C3位置的取代基决定P-450的甾体-底物特异性。

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1
Inherent versatility of P-450 oxygenase. Conferring dehydroepiandrosterone hydroxylase activity to P-450 2a-4 by a single amino acid mutation at position 117.细胞色素P-450加氧酶的内在多功能性。通过117位的单个氨基酸突变赋予细胞色素P-450 2a-4脱氢表雄酮羟化酶活性。
J Biol Chem. 1994 Mar 25;269(12):9079-83.
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Multiple steroid-binding orientations: alteration of regiospecificity of dehydroepiandrosterone 2- and 7-hydroxylase activities of cytochrome P-450 2a-5 by mutation of residue 209.多种类固醇结合方向:通过209位残基突变改变细胞色素P-450 2a-5的脱氢表雄酮2-羟化酶和7-羟化酶活性的区域特异性
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Role of residues 363 and 206 in conversion of cytochrome P450 2B1 from a steroid 16-hydroxylase to a 15 alpha-hydroxylase.残基363和206在细胞色素P450 2B1从类固醇16-羟化酶转变为15α-羟化酶过程中的作用。
Arch Biochem Biophys. 1994 Feb 15;309(1):52-7. doi: 10.1006/abbi.1994.1083.
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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.小鼠类固醇7α-羟化酶(细胞色素P-450(7)α)的定点诱变:209位残基在确定类固醇-细胞色素P-450相互作用中的作用。
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Engineering mouse P450coh to a novel corticosterone 15 alpha-hydroxylase and modeling steroid-binding orientation in the substrate pocket.将小鼠P450coh工程改造为一种新型的皮质酮15α-羟化酶,并对底物口袋中的类固醇结合取向进行建模。
J Biol Chem. 1993 Jan 15;268(2):759-62.
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Interconversion of the androstenedione hydroxylase specificities of cytochromes P450 2B4 and 2B5 upon simultaneous site-directed mutagenesis of four key substrate recognition residues.在对四个关键底物识别残基进行同时定点诱变时,细胞色素P450 2B4和2B5的雄烯二酮羟化酶特异性的相互转换
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Elucidation of amino acid residues critical for unique activities of rabbit cytochrome P450 2B5 using hybrid enzymes and reciprocal site-directed mutagenesis with rabbit cytochrome P450 2B4.利用杂交酶以及与兔细胞色素P450 2B4进行相互位点定向诱变,阐明对兔细胞色素P450 2B5独特活性至关重要的氨基酸残基。
Arch Biochem Biophys. 1996 Mar 15;327(2):308-18. doi: 10.1006/abbi.1996.0127.
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Reciprocal size-effect relationship of the key residues in determining regio- and stereospecificities of DHEA hydroxylase activity in P450 2a5.P450 2a5中决定脱氢表雄酮羟化酶活性区域和立体特异性的关键残基的相互尺寸效应关系。
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Role of residue 480 in substrate specificity of cytochrome P450 2B5 and 2B11.细胞色素P450 2B5和2B11底物特异性中480位残基的作用。
Arch Biochem Biophys. 1996 Mar 1;327(1):167-73. doi: 10.1006/abbi.1996.0105.

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