Publication | Open Access
Leukotriene C promotes prostacyclin synthesis by human endothelial cells.
88
Citations
30
References
1983
Year
Endothelial CellsLipid PeroxidationImmunologyCulture MediumCellular PhysiologyOxidative StressInflammationLeukotriene CClinical ChemistryCultured Endothelial CellsEndothelial Cell PathobiologyOxysterolBiochemistryVascular BiologyReactive Oxygen SpecieMetabolomicsPharmacologyCell BiologyCytokinePhysiologyEndothelial DysfunctionMetabolismMedicine
Cultured endothelial cells from human umbilical vein were labelled with [3H]arachidonic acid for 16 hr. The radiolabel was localized primarily in phospholipids (93%) and 73% was distributed equally between phosphatidylcholine and phosphatidylethanolamine. Leukotriene C (10-1,000 nM) promoted a dose-dependent release of radiolabel into the culture medium. This response was 3.3 times control values at 100 nM. The major arachidonic acid metabolite synthesized was prostacyclin, which was 33% of the total released radiolabel. Endothelial cells also released small amounts of prostaglandin F2 alpha (6.1%), unidentified lipoxygenase products (14.8%), and unreacted arachidonic acid (33%). The 30-min time course of release was independent of the leukotriene C concentration used. Leukotriene D at similar concentrations also promoted endothelial cells to release primarily prostacyclin and unreacted arachidonic acid. The release of prostacyclin, a potent vasodilator agent, may be an important mediator in slow reacting substance effects on the vasculature.
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