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铜毒性不只是氧化损伤:锌系统与威尔逊病的启示

Copper Toxicity Is Not Just Oxidative Damage: Zinc Systems and Insight from Wilson Disease.

作者信息

Barber R G, Grenier Zoey A, Burkhead Jason L

机构信息

Department of Biological Sciences, University of Alaska Anchorage, 3211 Providence Dr., Anchorage, AK 99058, USA.

出版信息

Biomedicines. 2021 Mar 20;9(3):316. doi: 10.3390/biomedicines9030316.

Abstract

Essential metals such as copper (Cu) and zinc (Zn) are important cofactors in diverse cellular processes, while metal imbalance may impact or be altered by disease state. Cu is essential for aerobic life with significant functions in oxidation-reduction catalysis. This redox reactivity requires precise intracellular handling and molecular-to-organismal levels of homeostatic control. As the central organ of Cu homeostasis in vertebrates, the liver has long been associated with Cu storage disorders including Wilson Disease (WD) (heritable human Cu toxicosis), Idiopathic Copper Toxicosis and Endemic Tyrolean Infantile Cirrhosis. Cu imbalance is also associated with chronic liver diseases that arise from hepatitis viral infection or other liver injury. The labile redox characteristic of Cu is often discussed as a primary mechanism of Cu toxicity. However, work emerging largely from the study of WD models suggests that Cu toxicity may have specific biochemical consequences that are not directly attributable to redox activity. This work reviews Cu toxicity with a focus on the liver and proposes that Cu accumulation specifically impacts Zn-dependent processes. The prospect that Cu toxicity has specific biochemical impacts that are not entirely attributable to redox may promote further inquiry into Cu toxicity in WD and other Cu-associated disorders.

摘要

铜(Cu)和锌(Zn)等必需金属是多种细胞过程中的重要辅助因子,而金属失衡可能会受到疾病状态的影响或发生改变。铜对于有氧生命至关重要,在氧化还原催化中具有重要功能。这种氧化还原反应性需要精确的细胞内处理以及从分子到生物体水平的稳态控制。作为脊椎动物铜稳态的中心器官,肝脏长期以来一直与铜储存障碍有关,包括威尔逊病(WD)(遗传性人类铜中毒)、特发性铜中毒和地方性蒂罗尔婴儿肝硬化。铜失衡还与由病毒感染或其他肝损伤引起的慢性肝病有关。铜不稳定的氧化还原特性常被认为是铜毒性的主要机制。然而,主要来自WD模型研究的工作表明,铜毒性可能具有并非直接归因于氧化还原活性的特定生化后果。本文综述了以肝脏为重点的铜毒性,并提出铜积累会特别影响依赖锌的过程。铜毒性具有并非完全归因于氧化还原的特定生化影响这一前景,可能会促进对WD和其他与铜相关疾病中铜毒性的进一步研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7481/8003939/7538eaa3e618/biomedicines-09-00316-g001.jpg

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