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首页> 外文期刊>Acta crystallographica. Section F, Structural biology communications >Structural and functional insights into the stationary-phase survival protein SurE, an important virulence factor of Brucella abortus
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Structural and functional insights into the stationary-phase survival protein SurE, an important virulence factor of Brucella abortus

机译:结构和功能见解静止相存蛋白肯定,这是布鲁氏菌的重要毒力因子

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摘要

The stationary-phase survival protein SurE from Brucella abortus (BaSurE) is a metal-dependent phosphatase that is essential for the survival of this bacterium in the stationary phase of its life cycle. Here, BaSurE has been biochemically characterized and its crystal structure has been determined to a resolution of 1.9 angstrom. BaSurE was found to be a robust enzyme, showing activity over wide ranges of temperature and pH and with various phosphoester substrates. The active biomolecule is a tetramer and each monomer was found to consist of two domains: an N-terminal domain, which forms an approximate alpha + beta fold, and a C-terminal domain that belongs to the alpha/beta class. The active site lies at the junction of these two domains and was identified by the presence of conserved negatively charged residues and a bound Mg2+ ion. Comparisons of BaSurE with its homologues have revealed both common features and differences in this class of enzymes. The number and arrangement of some of the equivalent secondary structures, which are seen to differ between BaSurE and its homologues, are responsible for a difference in the size of the active-site area and the overall oligomeric state of this enzyme in other organisms. As it is absent in mammals, it has the potential to be a drug target.
机译:静止相存活蛋白肯定来自Brucella abortus(碱基)是一种金属依赖性磷酸酶,对于其生命周期的固定阶段,该细菌的存活至关重要。这里,碱基已经生物化学特征,并且其晶体结构已被确定为1.9埃的分辨率。发现碱基是一种稳健的酶,在宽的温度和pH范围内显示出具有各种磷酸酯基材的活性。活性生物分子是四聚体,发现每个单体由两个结构域组成:n末端结构域,其形成α+β折叠的近似α+β折叠,以及属于α/β类的C末端结构域。活性位点位于这两个结构域的结处,并通过存在保守的带负电荷残基和结合的Mg 2 +离子来鉴定。碱性与其同源物的比较揭示了这类酶的常见特征和差异。一些等同的二级结构的数量和布置在碱基和其同源物之间观察到不同,这是对其他生物中该酶的典型和整体低聚状态的差异。因为它不存在于哺乳动物中,它有可能成为药物目标。

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