Sphingomyelin organization is required for vesicle biogenesis at the Golgi complex

Sphingomyelin and cholesterol can assemble into domains and segregate from other lipids in the membranes. These domains are reported to function as platforms for protein transport and signalling. Do similar domains exist in the Golgi membranes and are they required for protein secretion? We tested t...

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Veröffentlicht in:The EMBO journal 2012-12, Vol.31 (24), p.4535-4546
Hauptverfasser: Duran, Juan M, Campelo, Felix, van Galen, Josse, Sachsenheimer, Timo, Sot, Jesús, Egorov, Mikhail V, Rentero, Carles, Enrich, Carlos, Polishchuk, Roman S, Goñi, Félix M, Brügger, Britta, Wieland, Felix, Malhotra, Vivek
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Sprache:eng
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Zusammenfassung:Sphingomyelin and cholesterol can assemble into domains and segregate from other lipids in the membranes. These domains are reported to function as platforms for protein transport and signalling. Do similar domains exist in the Golgi membranes and are they required for protein secretion? We tested this hypothesis by using D ‐ceramide‐C6 to manipulate lipid homeostasis of the Golgi membranes. Lipidomics of the Golgi membranes isolated from D ‐ceramide‐C6‐treated HeLa cells revealed an increase in the levels of C6‐sphingomyelin, C6‐glucosylceramide, and diacylglycerol. D ‐ceramide‐C6 treatment in HeLa cells inhibited transport carrier formation at the Golgi membranes without affecting the fusion of incoming carriers. The defect in protein secretion as a result of D ‐ceramide‐C6 treatment was alleviated by knockdown of the sphingomyelin synthases 1 and 2. C6‐sphingomyelin prevented liquid‐ordered domain formation in giant unilamellar vesicles and reduced the lipid order in the Golgi membranes of HeLa cells. These findings highlight the importance of a regulated production and organization of sphingomyelin in the biogenesis of transport carriers at the Golgi membranes. Lipid‐raft domains enriched in sphingomyelin and cholesterol in the Golgi membranes are required for the biogenesis of transport carriers leaving the Golgi, but not for the fusion of incoming carriers from the endoplasmic reticulum.
ISSN:0261-4189
1460-2075
DOI:10.1038/emboj.2012.317