Duodenal Cytochrome b (DCYTB) in Iron Metabolism: An Update on Function and Regulation

新陈代谢 细胞色素 功能(生物学) 生物 化学 生物化学 生理学 内科学 医学 遗传学
作者
Darius J.R. Lane,Dong-Hun Bae,Angelica M. Merlot,Sumit Sahni,Des R. Richardson
出处
期刊:Nutrients [Multidisciplinary Digital Publishing Institute]
卷期号:7 (4): 2274-2296 被引量:119
标识
DOI:10.3390/nu7042274
摘要

Iron and ascorbate are vital cellular constituents in mammalian systems. The bulk-requirement for iron is during erythropoiesis leading to the generation of hemoglobin-containing erythrocytes. Additionally; both iron and ascorbate are required as co-factors in numerous metabolic reactions. Iron homeostasis is controlled at the level of uptake; rather than excretion. Accumulating evidence strongly suggests that in addition to the known ability of dietary ascorbate to enhance non-heme iron absorption in the gut; ascorbate regulates iron homeostasis. The involvement of ascorbate in dietary iron absorption extends beyond the direct chemical reduction of non-heme iron by dietary ascorbate. Among other activities; intra-enterocyte ascorbate appears to be involved in the provision of electrons to a family of trans-membrane redox enzymes; namely those of the cytochrome b561 class. These hemoproteins oxidize a pool of ascorbate on one side of the membrane in order to reduce an electron acceptor (e.g., non-heme iron) on the opposite side of the membrane. One member of this family; duodenal cytochrome b (DCYTB); may play an important role in ascorbate-dependent reduction of non-heme iron in the gut prior to uptake by ferrous-iron transporters. This review discusses the emerging relationship between cellular iron homeostasis; the emergent “IRP1-HIF2α axis”; DCYTB and ascorbate in relation to iron metabolism.

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