Function and Regulation of Human Copper-Transporting ATPases

ATP7A型 门克斯病 ATP酶 细胞生物学 胞浆 生物 型三磷酸腺脢 平衡 生物化学 细胞内 分泌物 化学 转运蛋白 铜代谢 有机化学
作者
Svetlana Lutsenko,Natalie Barnes,Mee Y. Bartee,Oleg Y. Dmitriev
出处
期刊:Physiological Reviews [American Physiological Society]
卷期号:87 (3): 1011-1046 被引量:844
标识
DOI:10.1152/physrev.00004.2006
摘要

Copper-transporting ATPases (Cu-ATPases) ATP7A and ATP7B are evolutionarily conserved polytopic membrane proteins with essential roles in human physiology. The Cu-ATPases are expressed in most tissues, and their transport activity is crucial for central nervous system development, liver function, connective tissue formation, and many other physiological processes. The loss of ATP7A or ATP7B function is associated with severe metabolic disorders, Menkes disease, and Wilson disease. In cells, the Cu-ATPases maintain intracellular copper concentration by transporting copper from the cytosol across cellular membranes. They also contribute to protein biosynthesis by delivering copper into the lumen of the secretory pathway where metal ion is incorporated into copper-dependent enzymes. The biosynthetic and homeostatic functions of Cu-ATPases are performed in different cell compartments; targeting to these compartments and the functional activity of Cu-ATPase are both regulated by copper. In recent years, significant progress has been made in understanding the structure, function, and regulation of these essential transporters. These studies raised many new questions related to specific physiological roles of Cu-ATPases in various tissues and complex mechanisms that control the Cu-ATPase function. This review summarizes current data on the structural organization and functional properties of ATP7A and ATP7B as well as their localization and functions in various tissues, and discusses the current models of regulated trafficking of human Cu-ATPases.
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