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朊病毒蛋白八肽重复区以外的铜结合部位。

Copper binding extrinsic to the octarepeat region in the prion protein.

机构信息

Department of Chemistry & Biochemistry, University of California, Santa Cruz, Santa Cruz, CA 95064, USA.

出版信息

Curr Protein Pept Sci. 2009 Oct;10(5):529-35. doi: 10.2174/138920309789352056.

Abstract

Current research suggests that the function of the prion protein (PrP) is linked to its ability to bind copper. PrP is implicated in copper regulation, copper buffering and copper-dependent signaling. Moreover, in the development of prion disease, copper may modulate the rate of protein misfolding. PrP possesses a number of copper sites, each with distinct chemical characteristics. Most studies thus far have concentrated on elucidating chemical features of the octarepeat region (residues 60-91, hamster sequence), which can take up to four equivalents of copper, depending on the ratio of Cu2+ to protein. However, other sites have been proposed, including those at histidines 96 and 111, which are adjacent to the octarepeats, and also at histidines within PrP's folded C-terminal domain. Here, we review the literature of these copper sites extrinsic to the octarepeat region and add new findings and insights from recent experiments.

摘要

目前的研究表明,朊病毒蛋白(PrP)的功能与其结合铜的能力有关。PrP 参与铜的调节、铜缓冲和铜依赖性信号传递。此外,在朊病毒病的发展过程中,铜可能调节蛋白质错误折叠的速度。PrP 具有多个铜结合位点,每个位点都具有独特的化学特征。到目前为止,大多数研究都集中在阐明 octarepeat 区域(残基 60-91,仓鼠序列)的化学特征上,这取决于 Cu2+与蛋白质的比例,该区域可以结合多达四个当量的铜。然而,已经提出了其他位点,包括紧邻 octarepeats 的组氨酸 96 和 111 位点,以及位于 PrP 折叠 C 末端结构域内的组氨酸位点。在这里,我们综述了这些位于 octarepeat 区域之外的铜结合位点的文献,并添加了最近实验的新发现和见解。

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本文引用的文献

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