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Three unrelated sphingomyelin analogs spontaneously cluster into plasma membrane micrometric domains

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Tyteca, Donatienne [UCL] D'Auria, Ludovic [UCL] Van Der Smissen, Patrick [UCL] Medts, Thierry [UCL] Carpentier, Sarah [UCL] Monbaliu, Jean-Christophe [UCL] de Diesbach, Philippe [UCL] Courtoy, Pierre J. [UCL]

Micrometric lipid compartmentation at the plasma membrane is disputed. Using live confocal imaging, we found that three unrelated fluorescent sphingomyelin (SM) analogs spontaneously clustered at the outer leaflet into micrometric domains, contrasting with homogenous labelling by DiIC18 and TMA-DPH. In erythrocytes, these domains were round, randomly distributed, and reversibly coalesced under hypotonicity. BODIPY-SM and -glucosylceramide showed distinct temperature-dependence, in the same ranking as Tm for corresponding natural lipids, indicating phase behaviour. Scanning electron microscopy excluded micrometric surface structural features. In CHO cells, similar surface micrometric patches were produced by either direct BODIPY-SM insertion or intracellular processing from BODIPY-ceramide, ruling out aggregation artefacts. BODIPY-SM surface micrometric patches were refractory to endocytosis block or actin depolymerization and clustered upon cholesterol deprivation, indicating self-clustering at the plasma membrane. BODIPY-SM excimers further suggested clustering in ordered domains. Segregation of BODIPY-SM and -lactosylceramide micrometric domains showed coexistence of distinct phases. Consistent with micrometric domain boundaries, fluorescence recovery after photobleaching (FRAP) revealed restriction of BODIPY-SM lateral diffusion over long-range, but not short-range, contrasting with comparable high mobile fraction of BODPY-glucosylceramide in both ranges. Controlled perturbations of endogenous SM pool similarly affected BODIPY-SM domain size by confocal imaging and its mobile fraction by FRAP. The latter evidence supports the hypothesis that, as shown for BODIPY-SM, endogenous SM spontaneously clusters at the plasmalemma outer leaflet of living cells into ordered micrometric domains, defined in shape by liquid-phase coexistence and in size by membrane tension and cholesterol. This proposal remains speculative and calls for further investigations.

Type de document Article de périodique (Journal article) – Article de rechercheJournal Article, Research Support, Non-U.S. Gov't
Type d'accès Accès restreint
Année de publication 2010
Langue Anglais
Information sur le périodique "BBA - Biomembranes" - Vol. 1798, no. 5, p. 909-927 (2010)
Peer reviewed oui
Editeur Elsevier BV ((Netherlands) Amsterdam)
issn 0005-2736
Statut de la publication Publié
Affiliations UCL - SSS/DDUV - Institut de Duve
UCL - SSS/DDUV/CELL - Biologie cellulaire
UCL - SSS/IONS/CEMO - Pôle Cellulaire et moléculaire
UCL - (SLuc) Service de biochimie médicale
MESH Subject Sphingomyelins - chemistry ; Membrane Microdomains - chemistry - ultrastructure ; Membrane Lipids - chemistry - metabolism ; Humans ; Hela Cells ; Fluorescent Dyes - chemistry ; Fluorescence Recovery After Photobleaching ; Erythrocytes - cytology - metabolism ; Cricetulus ; Cricetinae ; Cholesterol - metabolism ; Ceramides - chemistry ; Cell Membrane - chemistry - ultrastructure ; CHO Cells ; Boron Compounds - chemistry ; Animals
Mots-clés Sphingomyelin ; Micrometric domain ; CHO plasma membrane ; Erythrocyte ; Lateral diffusion ; Phase coexistence
Liens
Référence bibliographique Tyteca, Donatienne ; D'Auria, Ludovic ; Van Der Smissen, Patrick ; Medts, Thierry ; Carpentier, Sarah ; et. al. Three unrelated sphingomyelin analogs spontaneously cluster into plasma membrane micrometric domains. In: BBA - Biomembranes, Vol. 1798, no. 5, p. 909-927 (2010)
Permalien http://hdl.handle.net/2078.1/29211