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DJ-1 Is a Copper Chaperone Acting on SOD1 Activation

机译:DJ-1是一种用于SOD1活化的铜伴侣

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Lack of oxidative stress control is a common and often prime feature observed in many neurodegenerative diseases. Both DJ-1 and SOD1, proteins involved in familial Parkinson disease and amyotrophic lateral sclerosis, respectively, play a protective role against oxidative stress. Impaired activity and modified expression of both proteins have been observed in different neurodegenerative diseases. A potential cooperative action of DJ-1 and SOD1 in the same oxidative stress response pathway may be suggested based on a copper-mediated interaction between the two proteins reported here. To investigate the mechanisms underlying the antioxidative function of DJ-1 in relation to SOD1 activity, we investigated the ability of DJ-1 to bind copper ions. We structurally characterized a novel copper binding site involving Cys-106, and we investigated, using different techniques, the kinetics of DJ-1 binding to copper ions. The copper transfer between the two proteins was also examined using both fluorescence spectroscopy and specific biochemical assays for SOD1 activity. The structural and functional analysis of the novel DJ-1 copper binding site led us to identify a putative role for DJ-1 as a copper chaperone. Alteration of the coordination geometry of the copper ion in DJ-1 may be correlated to the physiological role of the protein, to a potential failure in metal transfer to SOD1, and to successive implications in neurodegenerative etiopathogenesis.
机译:缺乏氧化应激控制是在许多神经变性疾病中观察到的常见且通常的主要特征。 DJ-1和SOD1均分别参与家族帕金森病和肌营养的侧筒状菌病,分别对氧化应激发挥保护作用。在不同的神经变性疾病中观察到两种蛋白质的活性和修饰的两种蛋白质的表达。可以基于此处报告的两种蛋白质之间的铜介导的相互作用来提示在相同氧化应激响应途径中的DJ-1和SOD1的潜在合作作用。为了研究DJ-1关于SOD1活性的抗氧化功能的机制,我们研究了DJ-1结合铜离子的能力。我们在结构上表征了一种新型铜结合位点,涉及Cys-106,我们使用不同的技术研究了DJ-1与铜离子的动力学。还使用荧光光谱和SOD1活性的特异性生物化学测定检查两种蛋白质之间的铜转移。新型DJ-1铜结合位点的结构和功能分析LED指导了DJ-1作为铜伴侣的推定作用。 DJ-1中铜离子的协调几何形状的改变可以与蛋白质的生理作用相关,以对SOD1的金属转移的潜在失败,以及在神经退行性病因发生的连续影响。

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