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动态铜导航的协调 - 新的和缺失的部分。

Orchestration of dynamic copper navigation - new and missing pieces.

机构信息

Medical Biochemistry and Microbiology, Uppsala University, Sweden.

出版信息

Metallomics. 2017 Sep 20;9(9):1204-1229. doi: 10.1039/c7mt00010c.

Abstract

A general principle in all cells in the body is that an essential metal - here copper - is taken up at the plasma membrane, directed through cellular compartments for use in specific enzymes and pathways, stored in specific scavenging molecules if in surplus, and finally expelled from the cells. Here we attempt to provide a critical view on key concepts involved in copper transfer across membranes and through compartments in the human body. The focus of this review is on the influence of bioinorganic and thermodynamic rules on the flow in cellular copper networks. Transition of copper from one oxidation state to another will often lead to errant electrons that are highly reactive and prone to form radicals and reactive oxygen or nitrogen species (ROS and RNS). Strict control of potentially toxic oxidative species is an important part of understanding the edge of human copper metabolism. The present review critically covers translocation across simple and complex membranes as well as extracellular and intracellular copper routing. We discuss in depth four tissues with polarized cell barriers - the gut, liver, kidneys, and brain - to illustrate the similarities and differences in transcellular transfer. Copper chaperoning, buffering and binding dynamics to guide the metal to different sites are also covered, while individual molecular interaction kinetics are not detailed. Sorting and targeting mechanisms and principles crucial for correct localisation will also be touched upon.

摘要

在体内所有细胞中都存在一个普遍原则,即一种必需的金属——此处为铜——会在质膜处被摄取,在细胞内被定向用于特定的酶和途径,如果有剩余则储存在特定的清除分子中,最后被排出细胞。在此,我们试图批判性地审视铜在人体跨膜和穿过隔室转运过程中的关键概念。本综述的重点是生物无机和热力学规则对细胞内铜网络流动的影响。铜从一种氧化态向另一种氧化态的转变通常会导致错误的电子,这些电子具有很高的反应性,容易形成自由基和活性氧或氮物质(ROS 和 RNS)。严格控制潜在的毒性氧化物质是理解人类铜代谢边缘的重要部分。本综述批判性地涵盖了简单和复杂膜以及细胞外和细胞内铜路由的转运。我们深入讨论了具有极化细胞屏障的四个组织——肠道、肝脏、肾脏和大脑——以说明细胞间转运的相似性和差异性。铜伴侣蛋白、缓冲和结合动力学将金属引导至不同的部位也得到了涵盖,而个别分子相互作用的动力学细节则未详细描述。对正确定位至关重要的分拣和靶向机制和原则也将被提及。

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