Abstract
In intact neutrophils, phorbol ester treatment activates the respiratory burst oxidase, the enzyme responsible for O 2-production by phagocytes. This effect is thought to be dependent on protein kinase C and on the phosphorylation of p47 phox . In this paper, we report that protein kinase C activates the respiratory burst oxidase in a cell-free system consisting of isolated neutrophil cytosol and membrane. Oxidase activation required a highly active protein kinase C, recombinant p47 phox and ATP, and was inhibited by the protein kinase C inhibitors H-7 and GF-109203X. Partial depletion of cytosolic ATP by dialysis reduced oxidase activation by over 50%. In contrast, neither protein kinase C inhibitors nor ATP depletion affected oxidase activation by SDS. These findings strongly suggest that in the cell-free system, the oxidase can be activated by the phosphorylation of p47 phox .
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