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首页> 外文期刊>The Journal of biological chemistry >Role of Glutaredoxin1 and Glutathione in Regulating the Activity of the Copper-transporting P-type ATPases, ATP7A and ATP7B
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Role of Glutaredoxin1 and Glutathione in Regulating the Activity of the Copper-transporting P-type ATPases, ATP7A and ATP7B

机译:谷氨酸毒素1和谷胱甘肽在调节铜传输P型ATP酶活性,ATP7A和ATP7B的活性方面的作用

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摘要

The copper-transporting P-type ATPases (Cu-ATPases), ATP7A and ATP7B, are essential for the regulation of intracellular copper homeostasis. In this report we describe new roles for glutathione (GSH) and glutaredoxin1 (GRX1) in Cu homeostasis through their regulation of Cu-ATPase activity. GRX1 is a thiol oxidoreductase that catalyzes the reversible reduction of GSH-mixed disulfides to their respective sulfhydryls (deglutathionylation). Here, we demonstrated that glutathionylation of the Cu-ATPases and their interaction with GRX1 were affected by alterations in Cu levels. The data support our hypothesis that the Cu-ATPases serve as substrates for Cu-dependent GRX1-mediated deglutathionylation. This in turn liberates the Cu-ATPase cysteinyl thiol groups for Cu binding and transport. GSH depletion experiments led to reversible inhibition of the Cu-ATPases that correlated with effects on intracellular Cu levels and GRX1 activity. Finally, knockdown of GRX1 expression resulted in an increase in intracellular Cu accumulation. Together, these data directly implicate GSH and GRX1 with important new roles in redox regulation of the Cu-ATPases, through modulation of Cu binding by the Cu-ATPase cysteine motifs.
机译:转运P型ATP酶(Cu-ATP酶),ATP7a和ATP7b对于细胞内铜稳态的调节至关重要。在本报告中,我们通过调节Cu-AtPase活性来描述Cu稳态中的谷胱甘肽(GSH)和谷胱甘肽和谷氨酸毒素1(GRX1)的新作用。 GRX1是硫醇氧化还原酶,其催化GSH-混合二硫化的可逆降低于它们各自的巯基(脱硫醚酰化)。在这里,我们证明了Cu-ATP酶的谷胱甘肽和它们与GRX1的相互作用受Cu水平的改变的影响。数据支持我们的假设,即Cu-ATP酶用作Cu依赖性GRX1介导的脱氮化的底物。这反过来释放出Cu结合和转运的Cu-Atpase Cysteinyl硫醇基团。 GSH耗尽实验导致与细胞内Cu水平和GRX1活性的影响相关的Cu-ATP酶的可逆抑制。最后,GRX1表达的敲低导致细胞内Cu积累的增加。这些数据在一起,通过Cu-Atpase半胱氨酸基序的Cu结合调节Cu-ATP酶的氧化铈调节中的重要性新作用,这些数据在一起直接致癌GSH和GRX1。

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