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首页> 外文期刊>Plant Science: An International Journal of Experimental Plant Biology >Evolutionary relationship and substrate specificity of Arabidopsis thaliana fatty acid omega-hydroxylase
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Evolutionary relationship and substrate specificity of Arabidopsis thaliana fatty acid omega-hydroxylase

机译:拟南芥脂肪酸ω-羟化酶的进化关系和底物特异性

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On the basis of a phylogenic tree constructed using the available Arabidopsis thaliana genomic sequence, new fatty acid (FA) omegahydroxylases were cloned and expressed in yeast. Several uncharacterized cytochrome P450s (CYP, P450), comprising a phylogenic sub-cluster (CYP86A, 94B, 94C, 96A, 704A, 97B and 711 A) demonstrated FA omega-hydroxylase activities towards saturated FAs with medium chain length. While CYP96A4 showed the highest catalytic activity among the enzymes characterized in this study, other CYP96A subfamily members did not display any potent activity. In addition, CYP704A2 and CYP711A1, which are phylogenetically distant to both CYP86 and CYP94 with FA omega-hydroxylase activities, did not show any metabolic conversion of FAs. As we have studied omega-hydroxylation of FAs catalyzed by a series of CYP94 isoforms, active site models were produced to compare inactive CYP704A2 and CYP711A1 to active CYP94C1. The modeled structures revealed that the hydrophobicity in the heme binding site is very different between active and inactive isoforms. CYP94C1 contains highly hydrophobic residues while CYP704A2 and C-YP711A1 do not. Our study provides evidence that substrate specificity is conserved in phylogenetically related isoforms and suggests specific residues in the active site pocket that play a key role in determining substrate specificity. (c) 2005 Elsevier Ireland Ltd. All rights reserved.
机译:基于使用可获得的拟南芥基因组序列构建的系统树,克隆了新的脂肪酸(FA)ω-羟化酶并在酵母中表达。包含系统发育亚簇(CYP86A,94B,94C,96A,704A,97B和711A)的几种未表征的细胞色素P450(CYP,P450)表现出FAω-羟化酶活性对具有中等链长的饱和FA的活性。尽管在本研究中表征的酶中CYP96A4表现出最高的催化活性,但其他CYP96A亚家族成员未显示任何有效活性。此外,CYP704A2和CYP711A1在系统发育上与具有FAω-羟化酶活性的CYP86和CYP94距离较远,但未显示FA的任何代谢转化。由于我们研究了由一系列CYP94同工型催化的FA的ω-羟基化反应,因此建立了活性位点模型以比较非活性CYP704A2和CYP711A1与活性CYP94C1。建模的结构表明,血红素结合位点的疏水性在有活性和无活性同工型之间非常不同。 CYP94C1含有高度疏水的残基,而CYP704A2和C-YP711A1不含有。我们的研究提供了证据,表明在系统发育相关的亚型中底物特异性是保守的,并提示了活性位点袋中的特定残基在决定底物特异性中起着关键作用。 (c)2005 Elsevier Ireland Ltd.保留所有权利。

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