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lüll Endocytosis of glycosylphosphatidylinositol-anchored proteins Lakhan SE; Sabharanjak S; De AJ Biomed Sci 2009[Oct]; 16 (1): 93Glycosylphosphatidylinositol-anchored proteins (GPI-APs) represent an interesting amalgamation of the three basic kinds of cellular macromolecules viz. proteins, carbohydrates and lipids. An unusually hybrid moiety, the GPI-anchor is expressed in a diverse range of organisms from parasites to mammalian cells and serves to anchor a large number of functionally diverse proteins and has been the center of attention in scientific debate for some time now. Membrane organization of GPI-APs into laterally-organized cholesterol-sphingolipid ordered membrane domains or "rafts" and endocytosis of GPI-APs has been intensely debated. Inclusion into or exclusion from these membrane domains seems to be the critical factor in determining the endocytic mechanisms and intracellular destinations of GPI-APs. The intracellular signaling as well as endocytic trafficking of GPI-APs is critically dependent upon the cell surface organization of GPI-APs, and the associations with these lipid rafts play a vital role during these processes. The mechanism of endocytosis for GPI-APs may differ from other cellular endocytic pathways, such as those mediated by clathrin-coated pits (caveolae), and is necessary for unique biological functions. Numerous intracellular factors are involved in and regulate the endocytosis of GPI-APs, and these may be variably dependent on cell-type. The central focus of this article is to describe the significance of the endocytosis of GPI-APs on a multitude of biological processes, ranging from nutrient-uptake to more complex immune responses. Ultimately, a thorough elucidation of GPI-AP mediated signaling pathways and their regulatory elements will enhance our understanding of essential biological processes and benefit as components of disease intervention strategies.|*Endocytosis[MESH]|Animals[MESH]|Cell Membrane/metabolism[MESH]|Clathrin/chemistry[MESH]|Glycosylphosphatidylinositols/*chemistry[MESH]|Humans[MESH]|Lipids/chemistry[MESH]|Membrane Microdomains/*chemistry[MESH]|Models, Biological[MESH]|Mutation[MESH]|Prions/metabolism[MESH]|Proteins/chemistry[MESH]|Signal Transduction[MESH]|Sphingolipids/chemistry[MESH] |