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必需用于 D-环丝氨酸生物合成的 O-脲基-L-丝氨酸合酶的结构和突变分析。

The structural and mutational analyses of O-ureido-L-serine synthase necessary for D-cycloserine biosynthesis.

机构信息

Department of Molecular Microbiology and Biotechnology, Graduate School of Biomedical & Health Sciences, Hiroshima University, Japan.

出版信息

FEBS J. 2015 Oct;282(20):3929-44. doi: 10.1111/febs.13386. Epub 2015 Aug 18.

Abstract

UNLABELLED

We have recently been successful in cloning a gene cluster necessary for the biosynthesis of D-cycloserine (D-CS) from D-CS-producing Streptomyces lavendulae ATCC11924. Although dcsD, one of the ORFs located on the gene cluster, encodes a protein homologous to O-acetylserine sulfhydrylase that synthesizes L-cysteine using O-acetyl-L-serine together with sulfide, it functions to form O-ureido-L-serine as a D-CS biosynthetic intermediate, using O-acetyl-L-serine together with hydroxyurea (HU). In the present study, using crystallographic and mutational studies, three amino acid residues in DcsD that are important for the substrate preference toward HU were determined. We showed that two of the three residues are important for the binding of HU into the substrate-binding pocket. The other residue contributes to the formation of a loose hydrogen-bond network during the catalytic reaction. Information regarding the amino acid residues will be very useful in the design of a new catalyst for synthesizing the β-substituted-L-alanine derivatives.

DATABASE

The atomic coordinates and structure factors of wild-type DcsD and l-OUS-bound K43A mutant of DcsD have been deposited in the Protein Data Bank under accession codes 3X43 and 3X44, respectively.

摘要

未标记

我们最近成功地从生产 D-环丝氨酸(D-CS)的链霉菌属 lavendulae ATCC11924 中克隆出一个基因簇,该基因簇对于 D-CS 的生物合成是必需的。虽然位于基因簇上的 ORF 之一 dcsD 编码的蛋白与使用 O-乙酰-L-丝氨酸和硫化物合成 L-半胱氨酸的 O-乙酰丝氨酸硫代酶同源,但它的功能是使用 O-乙酰-L-丝氨酸和羟基脲(HU)形成 D-CS 生物合成中间体 O-脲基-L-丝氨酸。在本研究中,通过晶体学和突变研究,确定了 DcsD 中三个对 HU 底物偏好具有重要意义的氨基酸残基。我们表明,这三个残基中的两个对于 HU 结合到底物结合口袋中是重要的。另一个残基有助于在催化反应过程中形成松散的氢键网络。有关氨基酸残基的信息对于设计合成β取代-L-丙氨酸衍生物的新型催化剂将非常有用。

数据库

野生型 DcsD 和 DcsD 的 l-OUS 结合 K43A 突变体的原子坐标和结构因子已分别以 3X43 和 3X44 的登录号存入蛋白质数据库。

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