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铁稳态和氧代谢之间的密切对话受缺氧诱导因子 (HIFs) 调节。

An intimate crosstalk between iron homeostasis and oxygen metabolism regulated by the hypoxia-inducible factors (HIFs).

机构信息

Department of Human Stress Response Science, Institute of Biomedical Science, Kansai Medical University, Hirakata, Japan.

出版信息

Free Radic Biol Med. 2019 Mar;133:118-129. doi: 10.1016/j.freeradbiomed.2018.07.018. Epub 2018 Jul 24.

DOI:10.1016/j.freeradbiomed.2018.07.018
PMID:30053508
Abstract

Oxygen and iron are among the most abundant elements and have significant roles in human biology. Iron is essential for oxygen transport and is a component of molecular O-carrying proteins, such as hemoglobin and myoglobin. Iron is also a constituent of redox enzymes and can occupy multiple oxidation states. An elaborate system has evolved to stringently regulate the concentrations of both, free iron and oxygen, in various sites of the body. The final destination for iron and oxygen in the cells is the mitochondria. The mitochondria require substantial amounts of iron for heme synthesis and maturation of iron-sulfur clusters, and oxygen, as the electron acceptor in oxidative phosphorylation. Therefore, the balance between the control of iron availability and the physiology of hypoxic responses is critical for maintaining cell homeostasis. Several lines of study have clearly demonstrated that the transcription factors, hypoxia-inducible factors (HIFs), play a central role in cellular adaptation to critically low oxygen levels in both normal and compromised tissues. It has also been shown that several target genes of HIFs are involved in iron homeostasis, reflecting the molecular links between oxygen homeostasis and iron metabolism. Furthermore, HIF activation is modulated by intracellular iron, through regulation of hydroxylase activity, which requires iron as a cofactor. In addition, HIF-2α translation is controlled by iron regulatory protein (IRP) activity, providing another level of interdependence between iron and oxygen homeostasis.

摘要

氧和铁是最丰富的元素之一,在人类生物学中具有重要作用。铁是氧气运输所必需的,是分子携氧蛋白(如血红蛋白和肌红蛋白)的组成部分。铁也是氧化还原酶的组成部分,可以占据多个氧化态。已经进化出一个精细的系统来严格调节体内各个部位的自由铁和氧的浓度。铁和氧在细胞中的最终目的地是线粒体。线粒体需要大量的铁来合成血红素和成熟铁硫簇,以及氧作为氧化磷酸化中的电子受体。因此,控制铁的可用性和缺氧反应的生理学之间的平衡对于维持细胞内稳态至关重要。多项研究清楚地表明,转录因子缺氧诱导因子 (HIFs) 在正常和受损组织中细胞对极低氧水平的适应中起着核心作用。还表明,HIF 的几个靶基因参与铁稳态,反映了氧稳态和铁代谢之间的分子联系。此外,HIF 激活受细胞内铁的调节,通过调节需要铁作为辅助因子的羟化酶活性。此外,HIF-2α 的翻译受铁调节蛋白 (IRP) 活性的控制,为铁和氧稳态之间的另一个相互依赖水平提供了证据。

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