Gangliosides GM1 and GM3 in the Living Cell Membrane Form Clusters Susceptible to Cholesterol Depletion and Chilling

Akikazu Fujita,* Jinglei Cheng,* Minako Hirakawa, ${dagger}$ Koichi Furukawa, ${ddagger}$ Susumu Kusunoki, ${dagger}$ and Toyoshi Fujimoto*

Departments of ^*Anatomy and Molecular Cell Biology and Biochemistry II, Nagoya University Graduate School of Medicine, Nagoya 466-8550, Japan; Department of Neurology, Kinki University School of Medicine, Osaka 589-8511, Japan

Monitoring Editor: Jean Gruenberg

Presence of microdomains hasbeen postulated in the cell membrane, but two-dimensional distributionof lipid molecules has been difficult to determine in the submicrometerscale. In the present paper, we examined the distribution ofgangliosides GM1 and GM3, putative raft molecules in the cellmembrane, by immunoelectron microscopy using quick-frozen andfreeze-fractured specimens. This method physically immobilizedmolecules in situ and thus minimized the possibility of artifactualperturbation. By point pattern analysis of immunogold labeling,GM1 was shown to make clusters of <100 nm in diameter innormal mouse fibroblasts. GM1-null fibroblasts were not labeled,but developed a similar clustered pattern when GM1 was administered.On cholesterol depletion or chilling, the clustering of bothendogenous and exogenously-loaded GM1 decreased significantly,but the distribution showed marked regional heterogeneity inthe cells. GM3 also showed cholesterol-dependent clustering,and although clusters of GM1 and GM3 were found to occasionallycoincide, these aggregates were separated in most cases, suggestingthe presence of heterogeneous microdomains. The present methodenabled to capture the molecular distribution of lipids in thecell membrane, and demonstrated that GM1 and GM3 form clustersthat are susceptible to cholesterol depletion and chilling.

Address correspondence to: Toyoshi Fujimoto (tfujimot{at}med.nagoya-u.ac.jp)

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