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醚磷脂的前体是通过黄素酶通过共价催化合成的。

Precursor of ether phospholipids is synthesized by a flavoenzyme through covalent catalysis.

机构信息

Department of Biology and Biotechnology, University of Pavia, 27100 Pavia, Italy.

出版信息

Proc Natl Acad Sci U S A. 2012 Nov 13;109(46):18791-6. doi: 10.1073/pnas.1215128109. Epub 2012 Oct 29.

Abstract

The precursor of the essential ether phospholipids is synthesized by a peroxisomal enzyme that uses a flavin cofactor to catalyze a reaction that does not alter the redox state of the substrates. The enzyme crystal structure reveals a V-shaped active site with a narrow constriction in front of the prosthetic group. Mutations causing inborn ether phospholipid deficiency, a very severe genetic disease, target residues that are part of the catalytic center. Biochemical analysis using substrate and flavin analogs, absorbance spectroscopy, mutagenesis, and mass spectrometry provide compelling evidence supporting an unusual mechanism of covalent catalysis. The flavin functions as a chemical trap that promotes exchange of an acyl with an alkyl group, generating the characteristic ether bond. Structural comparisons show that the covalent versus noncovalent mechanistic distinction in flavoenzyme catalysis and evolution relies on subtle factors rather than on gross modifications of the cofactor environment.

摘要

必需醚磷脂的前体是由过氧化物酶体酶合成的,该酶使用黄素辅因子来催化不改变底物氧化还原状态的反应。该酶的晶体结构揭示了一个 V 形活性位点,在辅基前面有一个狭窄的收缩。导致先天性醚磷脂缺乏的基因突变,这是一种非常严重的遗传疾病,靶向的残基是催化中心的一部分。使用底物和黄素类似物、吸收光谱、突变和质谱的生化分析提供了令人信服的证据,支持共价催化的不寻常机制。黄素作为一种化学陷阱,促进酰基与烷基的交换,生成特征性的醚键。结构比较表明,黄素酶催化和进化中的共价与非共价机制区别依赖于微妙的因素,而不是辅因子环境的重大改变。

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