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铁运输:在健康与疾病中的新作用

Iron transport: emerging roles in health and disease.

作者信息

Goswami Tapasree, Rolfs Andreas, Hediger Matthias A

机构信息

Renal Division, Brigham and Women's Hospital, Harvard Institutes of Medicine, Boston, MA 02115, USA.

出版信息

Biochem Cell Biol. 2002;80(5):679-89. doi: 10.1139/o02-159.

DOI:10.1139/o02-159
PMID:12440707
Abstract

In the theater of cellular life, iron plays an ambiguous and yet undoubted lead role. Iron is a ubiquitous core element of the earth and plays a central role in countless biochemical pathways. It is integral to the catalysis of the redox reactions of oxidative phosphorylation in the respiratory chain, and it provides a specific binding site for oxygen in the heme binding moiety of hemoglobin, which allows oxygen transport in the blood. Its biological utility depends upon its ability to readily accept or donate electrons, interconverting between its ferric (Fe3+) and ferrous (Fe2+) forms. In contrast to these beneficial features, free iron can assume a dangerous aspect catalyzing the formation of highly reactive compounds such as cytotoxic hydroxyl radicals that cause damage to the macromolecular components of cells, including DNA and proteins, and thereby cellular destruction. The handling of iron in the body must therefore be very carefully regulated. Most environmental iron is in the Fe3+ state, which is almost insoluble at neutral pH. To overcome the virtual insolubility and potential toxicity of iron, a myriad of specialized transport systems and associated proteins have evolved to mediate regulated acquisition, transport, and storage of iron in a soluble, biologically useful, non-toxic form. We are gradually beginning to understand how these proteins individually and in concert serve to maintain cellular and whole body homeostasis of this crucial yet potentially harmful metal ion. Furthermore, studies are increasingly implicating iron and its associated transport in specific pathologies of many organs. Investigation of the transport proteins and their functions is beginning to unravel the detailed mechanisms underlying the diseases associated with iron deficiency, iron overload, and other dysfunctions of iron metabolism.

摘要

在细胞生命的舞台上,铁扮演着一个模糊却又毋庸置疑的主角。铁是地球上普遍存在的核心元素,在无数生物化学途径中发挥着关键作用。它是呼吸链中氧化磷酸化氧化还原反应催化的必需元素,并且在血红蛋白的血红素结合部分为氧气提供了特定的结合位点,从而使氧气能够在血液中运输。其生物学效用取决于它易于接受或捐赠电子的能力,能够在其三价铁(Fe3+)和二价铁(Fe2+)形式之间相互转换。与这些有益特性形成对比的是,游离铁可能呈现出危险的一面,催化形成高活性化合物,如细胞毒性羟基自由基,这些自由基会对细胞的大分子成分(包括DNA和蛋白质)造成损害,进而导致细胞破坏。因此,体内铁的处理必须受到非常严格的调控。大多数环境中的铁处于Fe3+状态,在中性pH值下几乎不溶。为了克服铁的实际不溶性和潜在毒性,已经进化出了无数专门的运输系统和相关蛋白质,以介导铁以可溶、生物可用、无毒的形式进行调控获取、运输和储存。我们正逐渐开始了解这些蛋白质如何单独以及协同作用,以维持这种关键但可能有害的金属离子的细胞和全身稳态。此外,研究越来越多地表明铁及其相关运输与许多器官的特定病理状况有关。对运输蛋白及其功能的研究开始揭示与缺铁、铁过载和其他铁代谢功能障碍相关疾病的详细机制。

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