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Structure and Kinetic Analysis of H2S Production by Human Mercaptopyruvate Sulfurtransferase

机译:H2S生产的结构和动力学分析硫磺酸硫磺酸硫酸盐硫磺酸盐酶

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Mercaptopyruvate sulfurtransferase (MST) is a source of endogenous H2S, a gaseous signaling molecule implicated in a wide range of physiological processes. The contribution of MST versus the other two H2S generators, cystathionine β-synthase and γ-cystathionase, has been difficult to evaluate because many studies on MST have been conducted at high pH and have used varied reaction conditions. In this study, we have expressed, purified, and crystallized human MST in the presence of the substrate 3-mercaptopyruvate (3-MP). The kinetics of H2S production by MST from 3-MP was studied at pH 7.4 in the presence of various physiological persulfide acceptors: cysteine, dihydrolipoic acid, glutathione, homocysteine, and thioredoxin, and in the presence of cyanide. The crystal structure of MST reveals a mixture of the product complex containing pyruvate and an active site cysteine persulfide (Cys248-SSH) and a nonproductive intermediate in which 3-MP is covalently linked via a disulfide bond to an active site cysteine. The crystal structure analysis allows us to propose a detailed mechanism for MST in which an Asp-His-Ser catalytic triad is positioned to activate the nucleophilic cysteine residue and participate in general acid-base chemistry, whereas our kinetic analysis indicates that thioredoxin is likely to be the major physiological persulfide acceptor for MST.
机译:巯基吡喃磺酸硫酸硫磺酸硫磺酸酯(MST)是内源H2S的源,一种气态信号传导分子涉及各种生理过程。 MST与其他两个H2S发生器,胱硫脲β-合酶和γ-胱硫代胱芹硫酶的贡献难以评估,因为许多关于MST的研究已经在高pH下进行并且使用了不同的反应条件。在该研究中,我们在底物3-巯基吡合他分(3mP)存在下表达,纯化和结晶的人MST。在各种生理过硫化物受体的存在下,在pH 7.4中研究了MST从3-MP产生的H2S产生的动力学:半胱氨酸,二氢丙烯酸,谷胱甘肽,同型半胱氨酸和硫氧胺,以及在氰化物存在下。 MST的晶体结构揭示了含有丙酮酸的产物络合物和活性位点半胱氨酸过硫化物(Cys248-SSH)的混合物和非培养中间体,其中3-MP通过二硫键与活性位点半胱氨酸共价连接。晶体结构分析使我们能够提出用于MST的详细机制,其中ASP-HIS-SER催化三合会定位以激活亲核半胱氨酸残基并参与一般酸碱化学,而我们的动力学分析表明患者可能是肺毒素是MST的主要生理过敏受体。

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