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Am J Physiol Renal Physiol 278: F13-F28, 2000;
0363-6127/00 $5.00
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Vol. 278, Issue 1, F13-F28, January 2000

INVITED REVIEW
Structure and function of aquaporin water channels

A. S. Verkman1 and Alok K. Mitra2

1 Departments of Medicine and Physiology, Cardiovascular Research Institute, University of California, San Francisco 94143-0521; and 2 Department of Cell Biology, the Scripps Research Institute, La Jolla, California 92037

The aquaporins (AQPs) are a family of small membrane-spanning proteins (monomer size ~30 kDa) that are expressed at plasma membranes in many cells types involved in fluid transport. This review is focused on the molecular structure and function of mammalian aquaporins. Basic features of aquaporin structure have been defined using mutagenesis, epitope tagging, and spectroscopic and freeze-fracture electron microscopy methods. Aquaporins appear to assemble in membranes as homotetramers in which each monomer, consisting of six membrane-spanning alpha -helical domains with cytoplasmically oriented amino and carboxy termini, contains a distinct water pore. Medium-resolution structural analysis by electron cryocrystallography indicated that the six tilted helical segments form a barrel surrounding a central pore-like region that contains additional protein density. Several of the mammalian aquaporins (e.g., AQP1, AQP2, AQP4, and AQP5) appear to be highly selective for the passage of water, whereas others (recently termed aquaglyceroporins) also transport glycerol (e.g., AQP3 and AQP8) and even larger solutes (AQP9). Evidence for possible movement of ions and carbon dioxide through the aquaporins is reviewed here, as well as evidence for direct regulation of aquaporin function by posttranslational modification such as phosphorylation. Important unresolved issues include definition of the molecular pathway through which water and solutes move, the nature of monomer-monomer interactions, and the physiological significance of aquaporin-mediated solute movement. Recent results from knockout mice implicating multiple physiological roles of aquaporins suggest that the aquaporins may be suitable targets for drug discovery by structure-based and/or high-throughput screening strategies.

water transport; protein structure; electron microscopy; crystallography; water permeability


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