Department of Biology and Biological Engineering, Chalmers University of Technology, 41296 Gothenburg, Sweden.
Essays Biochem. 2022 Dec 16;66(7):977-986. doi: 10.1042/EBC20220043.
Copper (Cu) ion dys-homeostasis and α-synclein amyloid deposits are two hallmarks of Parkinson's disease (PD). Here, I will discuss the connections between these features, with a major focus on the role of Cu in the α-synuclein (aS) amyloid formation process. The structurally disordered aS monomer can bind to both redox states of Cu (i.e., oxidized Cu(II) and reduced Cu(I)) with high affinity in vitro. Notably, the presence of Cu(II) (in absence of aS N-terminal acetylation) and Cu(I) (when in complex with the copper chaperone Atox1) modulate aS assembly into β-structured amyloids in opposite directions in vitro. Albeit the link to biological relevance is not fully unraveled, existing observations clearly emphasize the need for more knowledge on this interplay and its consequences to eventually combat destructive reactions that promote PD.
铜(Cu)离子动态平衡失调和α-突触核蛋白淀粉样沉积是帕金森病(PD)的两个标志。在这里,我将讨论这两个特征之间的联系,主要关注 Cu 在α-突触核蛋白(aS)淀粉样形成过程中的作用。结构无序的 aS 单体在体外与 Cu 的两种氧化还原态(即氧化态 Cu(II)和还原态 Cu(I))具有高亲和力结合。值得注意的是,Cu(II)的存在(在没有 aS N 端乙酰化的情况下)和 Cu(I)(当与铜伴侣蛋白 Atox1 形成复合物时)在体外以相反的方向调节 aS 组装成β-结构淀粉样。尽管与生物学相关性的联系尚未完全阐明,但现有观察结果清楚地强调了需要更多地了解这种相互作用及其后果,以最终对抗促进 PD 的破坏性反应。
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