Signaling events mediating activation of brain ethanolamine plasmalogen hydrolysis by ceramide

Abstract: Ceramide is a lipid second messenger that acts on multiple-target enzymes, some of which are involved in other signal-transduction systems. We have previously demonstrated that endogenous ceramide modifies the metabolism of brain ethanolamine plasmalogens. The mechanism involved was studied. On the basis of measurements of breakdown products, specific inhibitor effects, and previous findings, we suggest that a plasmalogen-selective phospholipase A 2 is the ceramide target. Arachidonaterich pools of the diacylp… Show more

“…Other glycosphingolipids, such as cerebrosides and sulfatides, have no effect. However, ceramide markedly stimulates PlsEtn-PLA 2 activity in a time-and dose-dependent manner (Latorre et al, 2003). Treatment of rat brain slices with Staphylococcus aureus sphingomyelinase or C2-ceramide produces a marked decrease in PlsEtn levels, suggesting stimulation of PlsEtn-PLA 2 activity.…”

“…Treatment of rat brain slices with Staphylococcus aureus sphingomyelinase or C2-ceramide produces a marked decrease in PlsEtn levels, suggesting stimulation of PlsEtn-PLA 2 activity. Bromoenol lactone, a potent inhibitor of iPLA 2 , does not affect this stimulation, but quinacrine and gangliosides, nonspecific inhibitors of PlsEtn-PLA 2 , completely block it (Latorre et al, 2003;Yang et al, 1994a,b). These studies have led to the suggestion that the degradation of plasmalogen by PlsEtn-PLA 2 is a receptormediated process Farooqui et al, 2003a;Latorre et al, 2003) and may involve an interaction between plasmalogen metabolism and sphingolipid metabolism.…”

Inhibitors of Brain Phospholipase A₂Activity: Their Neuropharmacological Effects and Therapeutic Importance for the Treatment of Neurologic Disorders

“…Other glycosphingolipids, such as cerebrosides and sulfatides, have no effect. However, ceramide markedly stimulates PlsEtn-PLA 2 activity in a time-and dose-dependent manner (Latorre et al, 2003). Treatment of rat brain slices with Staphylococcus aureus sphingomyelinase or C2-ceramide produces a marked decrease in PlsEtn levels, suggesting stimulation of PlsEtn-PLA 2 activity.…”

“…Treatment of rat brain slices with Staphylococcus aureus sphingomyelinase or C2-ceramide produces a marked decrease in PlsEtn levels, suggesting stimulation of PlsEtn-PLA 2 activity. Bromoenol lactone, a potent inhibitor of iPLA 2 , does not affect this stimulation, but quinacrine and gangliosides, nonspecific inhibitors of PlsEtn-PLA 2 , completely block it (Latorre et al, 2003;Yang et al, 1994a,b). These studies have led to the suggestion that the degradation of plasmalogen by PlsEtn-PLA 2 is a receptormediated process Farooqui et al, 2003a;Latorre et al, 2003) and may involve an interaction between plasmalogen metabolism and sphingolipid metabolism.…”

Inhibitors of Brain Phospholipase A₂Activity: Their Neuropharmacological Effects and Therapeutic Importance for the Treatment of Neurologic Disorders

“…The P2X7 purinergic receptor affects levels of several lipid messengers including arachidonic acid, diacylglycerol, phosphatidic acid, and ceramide via modulation of phospholipases A 2 , C, D, and N-SMase [79]. Sphingomyelinase and ceramide decrease the levels of plasmalogen, a vinylether group containing phospholipid, which acts as an antioxidant through the action of plasmalogenselective PLA 2 (iPLA 2 ) [80,81]. Decrease in plasmalogens induced by sphingomyelinase or ceramide is inhibited by quinacrine and bromoenol lactone, which are inhibitors of iPLA 2 [81,82].…”

Role of sphingomyelinases in neurological disorders

“…The cause of the increased PlsEtn-PLA 2 activity is not fully understood. However, it is becoming increasingly evident that ceramide, a lipid mediator of sphingolipid metabolism, stimulates PlsEtn-PLA 2 activity in a dose-dependent manner [13]. So increase in PlsEtn-PLA 2 activity may be due to the accumulation of ceramide in brain from AD patients [14,15].…”

Studies on Plasmalogen-Selective Phospholipase A2 in Brain