2004
DOI: 10.1074/jbc.m402170200
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Cell Surface Ceramide Generation Precedes and Controls FcγRII Clustering and Phosphorylation in Rafts

Abstract: Despite the role of sphingolipid/cholesterol rafts as signaling platforms for Fc␥ receptor II (Fc␥RII), the mechanism governing translocation of an activated receptor toward the rafts is unknown. We show that at the onset of Fc␥RII cross-linking acid sphingomyelinase is rapidly activated. This enzyme is extruded from intracellular compartments to the cell surface, and concomitantly, exofacially oriented ceramide is produced. Both non-raft and, to a lesser extent, raft sphingomyelin pools were hydrolyzed at the… Show more

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Cited by 99 publications
(31 citation statements)
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“…In 2001, Grassmé and coworkers demonstrated for the first time that ASM activation is linked to translocation of the enzyme to the plasma membrane upon CD95 stimulation (Grassmé et al, 2001a). Since then, a large number of studies have analyzed the regulation of lysosomal ASM with respect to ASM translocation in combination with ASM activation in response to different stimuli (e.g., Grassmé et al, 2002; Abdel Shakor et al, 2004; Lacour et al, 2004; Rotolo et al, 2005; Dumitru and Gulbins, 2006; Zeidan and Hannun, 2007; Zhang et al, 2007; Perrotta et al, 2010; Edelmann et al, 2011; Li et al, 2012, 2013), but only a few studies have addressed the secreted form of the enzyme (Schissel et al, 1996, 1998; Wong et al, 2000; Jenkins et al, 2009) and these studies have been limited to cell models, plasma, or serum (Mühle et al, 2013). …”
Section: Acid Sphingomyelinasementioning
confidence: 99%
“…In 2001, Grassmé and coworkers demonstrated for the first time that ASM activation is linked to translocation of the enzyme to the plasma membrane upon CD95 stimulation (Grassmé et al, 2001a). Since then, a large number of studies have analyzed the regulation of lysosomal ASM with respect to ASM translocation in combination with ASM activation in response to different stimuli (e.g., Grassmé et al, 2002; Abdel Shakor et al, 2004; Lacour et al, 2004; Rotolo et al, 2005; Dumitru and Gulbins, 2006; Zeidan and Hannun, 2007; Zhang et al, 2007; Perrotta et al, 2010; Edelmann et al, 2011; Li et al, 2012, 2013), but only a few studies have addressed the secreted form of the enzyme (Schissel et al, 1996, 1998; Wong et al, 2000; Jenkins et al, 2009) and these studies have been limited to cell models, plasma, or serum (Mühle et al, 2013). …”
Section: Acid Sphingomyelinasementioning
confidence: 99%
“…Ceramide molecules self-associate to small ceramide-enriched membrane microdomains, which have the tendency to spontaneously fuse to large ceramide-enriched membrane domains [36-38]. The formation of ceramide-enriched membrane domains was shown to occur in cells after stimulation via a variety of stimuli including CD95 [39-41], CD40 [42], DR5 [43], FcγRII [44], the PAF-receptor [45], but also after infection with P. aeruginosa [19], Neisseriae gonorrhoeae [46] , Rhinovirus [47], application of stress stimuli such as UV-light [48], cisplatin [49] or Cu 2+ -treatment [50]. The great variety of stimuli that trigger the formation of ceramide-enriched membrane platforms suggests that these membrane domains facilitate signal transduction, but are very likely not part of the specific signal transduction pathway elicited by the these stimuli.…”
Section: Ceramidementioning
confidence: 99%
“…The cholesterol effect can be attributed to the changes of sphingomyelin topology in the membrane yielding local concentration of sphingomyelin into discrete microdomains [14,16]. Accordingly, lysenin was applied for identification of sphingomyelin-rich domains in the plasma membrane [17].…”
Section: Introductionmentioning
confidence: 99%