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CYP109E1 对维生素 D2 的高度区域和立体选择性羟化。

Highly regio- and stereoselective hydroxylation of vitamin D2 by CYP109E1.

机构信息

Institute of Biochemistry, Saarland University, D-66123, Saarbruecken, Germany.

Endotherm Life Science Molecules, D-66123, Saarbruecken, Germany.

出版信息

Biochem Biophys Res Commun. 2020 Apr 2;524(2):295-300. doi: 10.1016/j.bbrc.2020.01.091. Epub 2020 Jan 25.

Abstract

Vitamin D2 is a form of vitamin D derived from mushrooms and plants which is structurally modified in the body due to the action of several enzymes. The resulting metabolites represent important compounds with potential bioactive properties. However, they are poorly studied and their availability is mostly limited. In order to identify new enzymes capable of producing vitamin D2 metabolites, we investigated a bacterial P450 monooxygenase, CYP109E1, which was previously shown to be a vitamin D3 hydroxylase. It was found that CYP109E1 catalyzes a vitamin D2 two-step hydroxylation at positions C24 and C25 resulting in the generation of 24(R),25-diOH VD2. Interestingly, the enzyme showed high selectivity towards vitamin D2, whereas it showed an unselective product pattern for the structurally similar vitamin D3. Our docking results for vitamin D2 and D3 revealed favorable hydroxylation positions for both substrates and suggested an explanation for the high selectivity of CYP109E1 towards vitamin D2. In addition, we established a whole-cell biocatalyst expressing CYP109E1 in Bacillus megaterium to produce 24(R),25-diOH VD2 and a production yield of 12.3 ± 1.2 mg/L was obtained after 48 h. To the best of our knowledge, this is the first report on the generation of 24(R),25-diOH VD2 by a microbial biocatalyst allowing a low-cost and eco-friendly production of this pharmaceutically interesting and expensive metabolite from the relatively cheap substrate, VD2.

摘要

维生素 D2 是一种从蘑菇和植物中提取的维生素 D 形式,由于几种酶的作用,在体内结构发生了修饰。由此产生的代谢物是具有潜在生物活性的重要化合物。然而,它们的研究还很有限,其可用性大多受到限制。为了鉴定能够产生维生素 D2 代谢物的新酶,我们研究了一种细菌 P450 单加氧酶 CYP109E1,该酶先前被证明是维生素 D3 羟化酶。结果发现,CYP109E1 能够催化维生素 D2 在 C24 和 C25 位的两步羟化反应,生成 24(R),25-二羟维生素 D2。有趣的是,该酶对维生素 D2 具有很高的选择性,而对结构相似的维生素 D3 则表现出非选择性的产物模式。我们对维生素 D2 和 D3 的对接结果表明,两种底物都具有有利的羟化位置,并为 CYP109E1 对维生素 D2 的高选择性提供了解释。此外,我们在巨大芽孢杆菌中建立了表达 CYP109E1 的全细胞生物催化剂,以生产 24(R),25-二羟维生素 D2,经过 48 小时后,获得了 12.3±1.2 mg/L 的产量。据我们所知,这是首次报道微生物生物催化剂生成 24(R),25-二羟维生素 D2,允许从相对廉价的底物维生素 D2 以低成本和环保的方式生产这种具有药用价值且昂贵的代谢物。

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