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结核分枝杆菌磺基转移酶 STF9 的晶体结构。

Crystal structure of sulfotransferase STF9 from Mycobacterium avium.

机构信息

Department of Bioscience and Biotechnology, Graduate School of Bioresource and Bioenvironmental Sciences, Kyushu University, Higashi-ku, Fukuoka, Japan.

出版信息

Mol Cell Biochem. 2012 Feb;361(1-2):97-104. doi: 10.1007/s11010-011-1093-x. Epub 2011 Sep 30.

DOI:10.1007/s11010-011-1093-x
PMID:21959978
Abstract

Sulfotransferases catalyze the sulfate conjugation of a wide variety of endogenous and exogenous molecules. Human pathogenic mycobacteria produce numerous sulfated molecules including sulfolipids which are well related to the virulence of several strains. The genome of Mycobacterium avium encodes eight putative sulfotransferases (stf1, stf4-stf10). Among them, STF9 shows higher similarity to human heparan sulfate 3-O-sulfotransferase isoforms than to the bacterial STs. Here, we determined the crystal structure of sulfotransferase STF9 in complex with a sulfate ion and palmitic acid at a resolution of 2.6 Å. STF9 has a spherical structure utilizing the classical sulfotransferase fold. STF9 exclusively possesses three N-terminal α-helices (α1, α2, α3) parallel to the 3'-phosphoadenosine-5'-phosphosulfate (PAPS) binding motif. The sulfate ion binds to the PAPS binding structural motif and the palmitic acid molecule binds in the deep cleft of the predicted substrate binding site suggesting the nature of endogenous acceptor substrate of STF9 resembles palmitic acid. The substrate binding site is covered by a flexible loop which may have involvement in endogenous substrate recognition. Based on the mutational study (Hossain et al., Mol Cell Biochem 350:155-162; 2011) and structural resemblance of STF9-sulfate ion-palmitic acid complex to the hHS3OST3 complex with PAP (3'-phosphoadenosine-5'-phosphate) and an acceptor sugar chain, Glu170 and Arg96 are appeared to be catalytic residues in STF9 sulfuryl transfer mechanism.

摘要

磺基转移酶催化广泛的内源性和外源性分子的硫酸酯化共轭。人类致病性分枝杆菌产生许多硫酸化分子,包括与几种菌株的毒力密切相关的 sulfolipids。鸟分枝杆菌基因组编码八个推定的磺基转移酶(stf1、stf4-stf10)。其中,STF9 与人类肝素硫酸 3-O-磺基转移酶同工型的相似性高于细菌 STs。在这里,我们确定了磺基转移酶 STF9 与硫酸根离子和棕榈酸复合物的晶体结构,分辨率为 2.6Å。STF9 具有利用经典磺基转移酶折叠的球形结构。STF9 仅具有三个 N 端α-螺旋(α1、α2、α3)与 3'-磷酸腺苷-5'-磷酸硫酸(PAPS)结合基序平行。硫酸根离子结合到 PAPS 结合结构基序,棕榈酸分子结合在预测的底物结合位点的深裂缝中,表明 STF9 的内源性受体底物的性质类似于棕榈酸。底物结合位点被一个柔性环覆盖,该环可能参与内源性底物识别。基于突变研究(Hossain 等人,Mol Cell Biochem 350:155-162; 2011)和 STF9-硫酸根离子-棕榈酸复合物与 PAP(3'-磷酸腺苷-5'-磷酸)和受体糖链的 hHS3OST3 复合物的结构相似性,Glu170 和 Arg96 似乎是 STF9 硫酰基转移机制中的催化残基。

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