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首页> 外文期刊>Structure >Structural Views along the Mycobacterium tuberculosis MenD Reaction Pathway Illuminate Key Aspects of Thiamin Diphosphate-Dependent Enzyme Mechanisms
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Structural Views along the Mycobacterium tuberculosis MenD Reaction Pathway Illuminate Key Aspects of Thiamin Diphosphate-Dependent Enzyme Mechanisms

机译:结核分枝杆菌MenD反应途径沿结构的观点阐明了硫胺素二磷酸依赖性酶机制的关键方面

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Menaquinone (MQ) is an essential component of the respiratory chains of many pathogenic organisms, including Mycobacterium tuberculosis (Mtb). The first committed step in MQ biosynthesis is catalyzed by 2-succinyl-5-enolpyruvyl-6-hydroxy-3-cyclohexadiene-1-carboxylate synthase (MenD), a thiamin diphosphate (ThDP)-dependent enzyme. Catalysis proceeds through two covalent intermediates as the substrates 2-oxoglutarate and isochorismate are successively added to the cofactor before final cleavage of the product. We have determined a series of crystal structures of Mtb-MenD that map the binding of both substrates, visualizing each step in the MenD catalytic cycle, including both intermediates. ThDP binding induces a marked asymmetry between the coupled active sites of each dimer, and possible mechanisms of communication can be identified. The crystal structures also reveal conformational features of the two intermediates that facilitate reaction but prevent premature product release. These data fully map chemical space to inform early-stage drug discovery targeting MenD.
机译:甲萘醌(MQ)是许多致病生物(包括结核分枝杆菌(Mtb))的呼吸链的重要组成部分。 MQ生物合成的第一步是通过2-琥珀酰二磷酸酯(ThDP)依赖性酶2-琥珀酰-5-烯醇丙酮酰6-羟基-3-环己二烯-1-羧酸合酶(MenD)催化的。催化作用通过两个共价中间体进行,因为在最终裂解产物之前,先将底物2-氧戊二酸酯和异辛酸酯添加到辅因子中。我们已经确定了一系列Mtb-MenD的晶体结构,这些结构绘制了两种底物的结合图,可视化了MenD催化循环中的每个步骤,包括两个中间体。 ThDP结合在每个二聚体的偶联的活性位点之间引起明显的不对称性,并且可以确定可能的通信机制。晶体结构还显示出两种中间体的构象特征,这些构象特征有助于反应但防止产物过早释放。这些数据完整地映射了化学空间,为靶向MenD的早期药物发现提供了信息。

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