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铁代谢与IRE/IRP调节系统:最新进展

Iron metabolism and the IRE/IRP regulatory system: an update.

作者信息

Pantopoulos Kostas

机构信息

Lady Davis Institute for Medical Research, Sir Mortimer B. Davis Jewish General Hospital, and Department of Medicine, McGill University, Montreal, Quebec, Canada.

出版信息

Ann N Y Acad Sci. 2004 Mar;1012:1-13. doi: 10.1196/annals.1306.001.

Abstract

Cellular iron homeostasis is accomplished by the coordinated regulated expression of the transferrin receptor and ferritin, which mediate iron uptake and storage, respectively. The mechanism is posttranscriptional and involves two cytoplasmic iron regulatory proteins, IRP1 and IRP2. Under conditions of iron starvation, IRPs stabilize the transferrin receptor and inhibit the translation of ferritin mRNAs by binding to "iron responsive elements" (IREs) within their untranslated regions. The IRE/IRP system also controls the expression of additional IRE-containing mRNAs, encoding proteins of iron and energy metabolism. The activities of IRP1 and IRP2 are regulated by distinct posttranslational mechanisms in response to cellular iron levels. Thus, in iron-replete cells, IRP1 assembles a cubane iron-sulfur cluster, which prevents IRE binding, while IRP2 undergoes proteasomal degradation. IRP1 and IRP2 also respond, albeit differentially, to iron-independent signals, such as hydrogen peroxide, hypoxia, or nitric oxide. Basic principles of the IRE/IRP system and recent advances in understanding the regulation and the function of IRP1 and IRP2 are discussed.

摘要

细胞铁稳态是通过转铁蛋白受体和铁蛋白的协调调控表达来实现的,它们分别介导铁的摄取和储存。其机制是转录后调控,涉及两种细胞质铁调节蛋白,即铁调节蛋白1(IRP1)和铁调节蛋白2(IRP2)。在铁缺乏的情况下,IRP通过与转铁蛋白受体和铁蛋白mRNA非翻译区内的“铁反应元件”(IRE)结合,使转铁蛋白受体稳定并抑制铁蛋白mRNA的翻译。IRE/IRP系统还控制其他含IRE的mRNA的表达,这些mRNA编码铁和能量代谢相关的蛋白质。IRP1和IRP2的活性受不同的翻译后机制调控,以响应细胞内铁水平。因此,在铁充足的细胞中,IRP1组装一个八面体铁硫簇,阻止其与IRE结合,而IRP2则经历蛋白酶体降解。IRP1和IRP2对铁非依赖性信号(如过氧化氢、缺氧或一氧化氮)也有反应,只是反应方式不同。本文讨论了IRE/IRP系统的基本原理以及在理解IRP1和IRP2的调控和功能方面的最新进展。

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