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Unresolved questions in human copper pump mechanisms

机译:人体铜泵机制中尚未解决的问题

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Copper (Cu) is an essential transition metal providing activity to key enzymes in the human body. To regulate the levels and avoid toxicity, cells have developed elaborate systems for loading these enzymes with Cu. Most Cu-dependent enzymes obtain the metal from the membrane-bound Cu pumps ATP7A/B in the Golgi network. ATP7A/B receives Cu from the cytoplasmic Cu chaperone Atox1 that acts as the cytoplasmic shuttle between the cell membrane Cu importer, Ctr1 and ATP7A/B. Biological, genetic and structural efforts have provided a tremendous amount of information for how the proteins in this pathway work. Nonetheless, basic mechanistic-biophysical questions (such as how and where ATP7A/B receives Cu, how ATP7A/B conformational changes and domain-domain interactions facilitate Cu movement through the membrane, and, finally, how target polypeptides are loaded with Cu in the Golgi) remain elusive. In this perspective, unresolved inquiries regarding ATP7A/B mechanism will be highlighted. The answers are important from a fundamental view, since mechanistic aspects may be common to other metal transport systems, and for medical purposes, since many diseases appear related to Cu transport dysregulation.
机译:铜(Cu)是必不可少的过渡金属,可为人体中的关键酶提供活性。为了调节水平并避免毒性,细胞已开发出复杂的系统以将这些酶负载到Cu中。大多数依赖铜的酶从高尔基网络中与膜结合的铜泵ATP7A / B中获得金属。 ATP7A / B从细胞质Cu伴侣Atox1接收Cu,Cu伴侣Atox1充当细胞膜Cu导入物Ctr1和ATP7A / B之间的细胞质穿梭。生物,遗传和结构方面的努力为这种途径中的蛋白质如何工作提供了大量信息。但是,基本的机械生物物理问题(例如ATP7A / B如何以及在何处接收Cu,ATP7A / B构象变化和域-域相互作用如何促进Cu在膜中的移动,最后,靶多肽如何在Cu中负载铜高尔基)仍然难以捉摸。从这个角度来看,将突出显示有关ATP7A / B机制的未解决的询问。从根本上看,答案很重要,因为机械方面可能是其他金属运输系统所共有的,并且出于医学目的,因为许多疾病似乎都与铜运输失调有关。

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