Abstract
Despite the role of sphingolipid/cholesterol rafts as signaling platforms for Fcgamma receptor II (FcgammaRII), the mechanism governing translocation of an activated receptor toward the rafts is unknown. We show that at the onset of FcgammaRII 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 onset of FcgammaRII cross-linking. The time course of ceramide production preceded the recruitment of FcgammaRII to rafts and the receptor phosphorylation. Exogenous C(16)-ceramide facilitated clustering of FcgammaRII and its association with rafts. In contrast, inhibition of acid sphingomyelinase diminished both the ceramide generation and clustering of cross-linked FcgammaRII. Under these conditions, tyrosine phosphorylation of FcgammaRII and receptor-accompanying proteins was also reduced. All the inhibitory effects were bypassed by treatment of cells with exogenous ceramide. These data provide evidence that the generation of cell surface ceramide is a prerequisite for fusion of cross-linked FcgammaRII and rafts, which triggers the receptor tyrosine phosphorylation and signaling.
Highlights
Fc␥ receptors IIA and IIC (Fc␥RII1 A/C) are single chain, 40-kDa members of the Fc␥R family that are expressed exclusively in human cells of the immunodefense system
1 The abbreviations used are: Fc␥RII, Fc␥ receptor II; ASMase, acid sphingomyelinase; BHK-FcIIA, BHK cells stably transfected with Fc␥RIIA; CDX, -cyclodextrin; ConA, concanavalin A; CRD/⌬KSR-GST, cysteine-rich domain of kinase suppressor of RAS fused with glutathione S-transferase; Fc⑀RI, Fc⑀ receptor I; Hepesbuffered saline (HBS), Hepes-buffered saline; lysenin-His, lysenin fused with polyhistidine; neutral SMase (NSMase), neutral sphingomyelinase; SM, sphingomyelin; SMase, sphingomyelinase; T cell receptors (TCR), T cell receptor; TfR, transferrin receptor; TNF, tumor necrosis factor; MES, 4-morpholineethanesulfonic acid; PBS, phosphate-buffered saline; FITC, fluorescein isothiocyanate
The ceramide visualized in the cells after 5 min of Fc␥RII cross-linking formed abundant small dots dispersed in the plane of the plasma membrane and occasionally fused into large clusters (Fig. 1, compare D and E)
Summary
Fc␥RII, Fc␥ receptor II; ASMase, acid sphingomyelinase; BHK-FcIIA, BHK cells stably transfected with Fc␥RIIA; CDX, -cyclodextrin; ConA, concanavalin A; CRD/⌬KSR-GST, cysteine-rich domain of kinase suppressor of RAS fused with glutathione S-transferase; Fc⑀RI, Fc⑀ receptor I; HBS, Hepes-buffered saline; lysenin-His, lysenin fused with polyhistidine; NSMase, neutral sphingomyelinase; SM, sphingomyelin; SMase, sphingomyelinase; TCR, T cell receptor; TfR, transferrin receptor; TNF, tumor necrosis factor; MES, 4-morpholineethanesulfonic acid; PBS, phosphate-buffered saline; FITC, fluorescein isothiocyanate. Lyzing enzyme, acid SMase (ASMase), has been shown recently to generate ceramide in the extracellular leaflet of the plasma membrane. This cell surface-oriented ASMase was found to be activated in T cells upon stimulation of the CD95/Fas receptor, another member of the TNF receptor family. An involvement of ASMase, but not NSMase, in ceramide generation in response to interleukin 1 was suggested by an early report coupling the enzyme activity to caveolae [22] These data were not supported, by recent studies [18, 23] showing an enrichment of NSMase relative to ASMase activity in these structures. Our data indicate that ceramide, released at the onset of Fc␥RII activation, can control efficient receptor clustering and its association with rafts, required for Fc␥RII phosphorylation and generation of signaling cascades
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