Coregulation of NADPH oxidase activation and phosphorylation of a 48-kD protein(s) by a cytosolic factor defective in autosomal recessive chronic granulomatous disease.

112

The enzyme NADPH oxidase is regulated by phospholipase D in intact neutrophils and is activated by phosphatidic acid (PA) plus diacylglycerol (DG) in cell-free systems. We showed previously that cell-free NADPH oxidase activation by these lipids involves both protein kinase-dependent and -independent pathways. Here we demonstrate that only the protein kinase-independent pathway is operative in a cell-free system of purified and recombinant NADPH oxidase components. Activation by PA ؉ DG was ATP-independent and unaffected by the protein kinase inhibitor staurosporine, indicating the lack of protein kinase involvement. Both PA and DG were required for optimal activation to occur. The drug R59949 reduced activation of NADPH oxidase by either arachidonic acid or PA ؉ DG, with IC 50 values of 46 and 25 M, respectively. The optimal concentration of arachidonic acid or PA ؉ DG for oxidase activation was shifted to the right with R59949, indicating interference of the drug with the interaction of lipid activators and enzyme components. R59949 inhibited the lipid-induced aggregation/sedimentation of oxidase components p47 phox and p67 phox , suggesting a disruption of the lipidmediated assembly process. The direct effects of R59949 on NADPH oxidase activation complicate its use as a "specific" inhibitor of DG kinase. We conclude that the protein kinase-independent pathway of NADPH oxidase activation by PA and DG involves direct interaction with NADPH oxidase components. Thus, NADPH oxidase proteins are functional targets for these lipid messengers in the neutrophil.The NADPH oxidase (the respiratory burst enzyme) in phagocytic cells produces superoxide (O 2 . ) 1 by catalyzing electron transfer from NADPH to molecular oxygen upon cell stimulation (1-3). This enzyme plays important roles in host defense against infection and in tissue damage due to inflammation (1-5). In addition, NADPH oxidase-like enzymes are present in a variety of other cell types, where the oxygen radicals formed may have signaling roles (5, 6). The enzyme in phagocytes consists of the membrane-bound heterodimeric flavocytochrome b 558 (gp91 phox and p22 phox ) and four cytosolic proteins (p47 phox , p67 phox , p40 phox , Rac1/2) (2-4, 7). Components must assemble in the membrane for the enzyme to become active (2-4, 7). The activation of NADPH oxidase is initiated by receptor-ligand interaction and involves complex intracellular signaling events. These include the activation of protein kinases to phosphorylate cellular proteins and NADPH oxidase components (2, 8) and the generation of various lipid second messengers (AA by phospholipase A 2 (9); DG by phospholipase C or PA phosphohydrolase; PA by phospholipase D or DG kinase (10, 11)). In cell-free systems, these lipids can induce activation of the enzyme (12-17). AA exerts its effect by directly acting on enzyme components (18 -22). PA has been shown to partially activate purified flavocytochrome b 558 (23), suggesting it interacts with this protein. It is not known whether DG has any direct effe...

Section: Methodsmentioning

confidence: 99%

Phosphatidic Acid and Diacylglycerol Directly Activate NADPH Oxidase by Interacting with Enzyme Components

Palicz

Foubert

Jesaitis

et al. 2001

112

“…Cells were resuspended (10 8 cells/ml) in sonication buffer (11% sucrose, 10 mM Pipes, pH 7.2, 5 mM EGTA, 5 mM EDTA, 130 mM NaCl, 1 M staurosporine, 5 mM Na 3 VO 4 , 1 M microcystin, 25 mM NaF, 1 mM p-nitrophenyl phosphate, 10 M benzamidine, 10 g/ml leupeptin, 10 M pepstatin, 1 g/ml aprotinin, and 1 M phenylmethylsulfonyl fluoride) and sonicated (41). The membrane and cytosol fractions were prepared by ultracentrifugation, using a 15/40% discontinuous sucrose gradient, as described previously (41).…”

Section: Methodsmentioning

confidence: 99%

“…The membrane and cytosol fractions were prepared by ultracentrifugation, using a 15/40% discontinuous sucrose gradient, as described previously (41). Membrane fractions were immediately solubilized with radioimmune precipitation buffer (see below) or stored at Ϫ70°C overnight for solubilization with n-octyl-␤-D-glucopyranoside.…”

Section: Methodsmentioning

confidence: 99%

Phosphorylation of p22 Is Mediated by Phospholipase D-dependent and -independent Mechanisms

Regier¹,

Greene²,

Sergeant³

et al. 2000

Human neutrophils participate in the host innate immune response, partly mediated by the multicomponent superoxide-generating enzyme NADPH oxidase. A correlation between phosphorylation of cytosolic NADPH oxidase components and enzyme activation has been identified but is not well understood. We previously showed that p22 phox , the small subunit of the membranebound oxidase component flavocytochrome b 558 , is an in vitro substrate for both a phosphatidic acid-activated kinase and conventional protein kinase C isoforms ( In intact neutrophils, several signaling mechanisms, initiated by receptor-ligand interactions, are involved in the regulation of NADPH oxidase (reviewed in Refs. 1 and 15). These events include activation of phospholipases, production of lipid second messengers, activation of protein kinases, and phosphorylation of neutrophil proteins and NADPH oxidase components. Activation of phospholipase A 2 and production of arachidonic acid is required for NADPH oxidase activity (16,17), although the role of arachidonic acid has not been identified. Phospholipase C also may be involved in NADPH oxidase activation (18 -20). Production of diacylglycerol by phospholipase C can induce activation of protein kinase C (PKC), which may mediate the phosphorylation of several NADPH oxidase components (see below) and is clearly an important regulator of NADPH oxidase activation (21, 22). Activation of phospholipase D (PLD), which cleaves phospholipids to form phosphatidic acid (PA), correlates with NADPH oxidase activation (23-30). The mechanism by which PA regulates NADPH oxidase has not been determined; however, a PA-activated protein kinase has been partially purified from neutrophil cytosol (31). phox , and p67 phox , 22-, 47, and 67-kDa phox component, respectively; dCB, dihydrocytochalasin B; fMLP, N-formyl-methionyl-leucyl-phenylalanine; OPZ, opsonized zymosan; PA, phosphatidic acid; PKC, protein kinase C; PLD, phospholipase D; PMA, phorbol 12-myristate 13-acetate; PVDF, polyvinylidene difluoride membrane; PAGE, polyacrylamide gel electrophoresis; GTP␥S, guanosine 5Ј-O-(3-thiotriphosphate); mAb, monoclonal antibody; Pipes, 1,4-piperazinediethanesulfonic acid.

“…The labeled bands were excised from the gel, and the radioactivity was measured by Č erenkov counting. The results (Table III) (3, 24 -29) and that the target serines for this phosphorylation lie between Ser-303 and Ser-379 in the C terminus of the protein (3)(4)(5)(6)(7). Direct evidence that the phosphorylation of p47…”

Section: Fig 5 In Vitro Phosphorylation Of Wt and Mutant Forms Of Rmentioning

confidence: 96%

Activation of p47 , a Cytosolic Subunit of the Leukocyte NADPH Oxidase

Johnson

Park²,

Benna³

et al. 1998

131