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铁调节蛋白与哺乳动物铁代谢的分子调控

Iron regulatory proteins and the molecular control of mammalian iron metabolism.

作者信息

Eisenstein R S

机构信息

Department of Nutritional Sciences, University of Wisconsin, Madison, Wisconsin 53706, USA.

出版信息

Annu Rev Nutr. 2000;20:627-62. doi: 10.1146/annurev.nutr.20.1.627.

Abstract

Mammalian iron homeostasis is maintained through the concerted action of sensory and regulatory networks that modulate the expression of proteins of iron metabolism at the transcriptional and/or post-transcriptional levels. Regulation of gene transcription provides critical developmental, cell cycle, and cell-type-specific controls on iron metabolism. Post-transcriptional control through the action of iron regulatory protein 1 (IRP1) and IRP2 coordinate the use of messenger RNA-encoding proteins that are involved in the uptake, storage, and use of iron in all cells of the body. IRPs may also provide a link between iron availability and cellular citrate use. Multiple factors, including iron, nitric oxide, oxidative stress, phosphorylation, and hypoxia/reoxygenation, influence IRP function. Recent evidence indicates that there is diversity in the function of the IRP system with respect to the response of specific IRPs to the same effector, as well as the selectivity with which IRPs modulate the use of specific messenger RNA.

摘要

哺乳动物的铁稳态是通过感觉和调节网络的协同作用来维持的,这些网络在转录和/或转录后水平上调节铁代谢蛋白的表达。基因转录调控对铁代谢提供关键的发育、细胞周期和细胞类型特异性控制。通过铁调节蛋白1(IRP1)和IRP2的作用进行的转录后控制,协调了参与体内所有细胞中铁摄取、储存和利用的信使RNA编码蛋白的使用。IRP还可能在铁的可用性和细胞对柠檬酸的利用之间提供联系。多种因素,包括铁、一氧化氮、氧化应激、磷酸化以及缺氧/复氧,都会影响IRP的功能。最近的证据表明,IRP系统的功能存在多样性,体现在特定IRP对相同效应物的反应,以及IRP调节特定信使RNA使用的选择性方面。

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