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多铜氧化酶与人类铁代谢。

Multi-copper oxidases and human iron metabolism.

机构信息

Department of Cellular and Physiological Sciences, University of British Columbia, 2350 Health Sciences Mall, Vancouver, BC V6T1Z3, Canada.

出版信息

Nutrients. 2013 Jun 27;5(7):2289-313. doi: 10.3390/nu5072289.

Abstract

Multi-copper oxidases (MCOs) are a small group of enzymes that oxidize their substrate with the concomitant reduction of dioxygen to two water molecules. Generally, multi-copper oxidases are promiscuous with regards to their reducing substrates and are capable of performing various functions in different species. To date, three multi-copper oxidases have been detected in humans--ceruloplasmin, hephaestin and zyklopen. Each of these enzymes has a high specificity towards iron with the resulting ferroxidase activity being associated with ferroportin, the only known iron exporter protein in humans. Ferroportin exports iron as Fe(2+), but transferrin, the major iron transporter protein of blood, can bind only Fe(3+) effectively. Iron oxidation in enterocytes is mediated mainly by hephaestin thus allowing dietary iron to enter the bloodstream. Zyklopen is involved in iron efflux from placental trophoblasts during iron transfer from mother to fetus. Release of iron from the liver relies on ferroportin and the ferroxidase activity of ceruloplasmin which is found in blood in a soluble form. Ceruloplasmin, hephaestin and zyklopen show distinctive expression patterns and have unique mechanisms for regulating their expression. These features of human multi-copper ferroxidases can serve as a basis for the precise control of iron efflux in different tissues. In this manuscript, we review the biochemical and biological properties of the three human MCOs and discuss their potential roles in human iron homeostasis.

摘要

多铜氧化酶(MCOs)是一小类酶,它们在将底物氧化的同时将分子氧还原为两个水分子。通常,多铜氧化酶对于其还原底物具有混杂性,并且能够在不同物种中执行各种功能。迄今为止,人类已检测到三种多铜氧化酶--铜蓝蛋白、亚铁氧化酶和yklopen。这些酶中的每一种对铁都具有很高的特异性,由此产生的亚铁氧化酶活性与铁蛋白(ferroportin)有关,铁蛋白是人类唯一已知的铁输出蛋白。铁蛋白将铁输出为 Fe(2+),而血液中主要的铁转运蛋白转铁蛋白只能有效地结合 Fe(3+)。肠细胞中的铁氧化主要由亚铁氧化酶介导,从而允许膳食铁进入血液。yklopen 参与铁从胎盘滋养层向胎儿的铁转移过程中从胎盘滋养层的铁外排。肝脏中铁的释放依赖于铁蛋白和铜蓝蛋白的亚铁氧化酶活性,铜蓝蛋白以可溶性形式存在于血液中。铜蓝蛋白、亚铁氧化酶和 yklopen 表现出独特的表达模式,并具有独特的调节其表达的机制。这些人类多铜亚铁氧化酶的特征可以作为不同组织中铁外排的精确控制的基础。在本文中,我们综述了三种人类 MCO 的生化和生物学特性,并讨论了它们在人类铁稳态中的潜在作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1008/3738974/cbf58a0a1ed0/nutrients-05-02289-g001.jpg

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