Exogenous Administration of Gangliosides Displaces GPI-anchored Proteins from Lipid Microdomains in Living Cells

Author:

Simons Mikael1,Friedrichson Tim2,Schulz Jörg B.1,Pitto Marina3,Masserini Massimo3,Kurzchalia Teymuras V.42

Affiliation:

1. Department of Neurology, University of Tübingen, D-77076 Tübingen, Germany;

2. Department of Cell Biology, Max-Delbrück Centre for Molecular Medicine, D-13092 Berlin-Buch, Germany

3. Department of Medical Chemistry and Biochemistry, University of Milan, 20133 Milan, Italy;

4. Max Planck Institute for Molecular Cell Biology and Genetics, Dresden, Germany; and

Abstract

Exogenous application of gangliosides to cells affects many cellular functions. We asked whether these effects could be attributed to the influence of gangliosides on the properties of sphingolipid–cholesterol microdomains on the plasma membrane, also termed rafts. The latter are envisaged as lateral assemblies of sphingolipids (including gangliosides), cholesterol, and a specific set of proteins. Rafts have been implicated in processes such as membrane trafficking, signal transduction, and cell adhesion. Recently, using a chemical cross-linking approach with Madin-Darby canine kidney (MDCK) cells permanently expressing a GPI-anchored form of growth hormone decay accelerating factor (GH-DAF) as a model system, we could show that GPI-anchored proteins are clustered in rafts in living cells. Moreover, this clustering was dependent on the level of cholesterol in the cell. Here we show that incubation of MDCK cells with gangliosides abolished subsequent chemical cross-linking of GH-DAF. Furthermore, insertion of gangliosides into the plasma membrane of MDCK GH-DAF cells renders GH-DAF soluble when subjected to extraction with Triton X-114 at 4°C. Our data suggest that exogenous application of gangliosides displaces GPI-anchored proteins from sphingolipid–cholesterol microdomains in living cells.

Publisher

American Society for Cell Biology (ASCB)

Subject

Cell Biology,Molecular Biology

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