Biological Roles for the NOX Family NADPH Oxidases

Nauseef, William M.

doi:10.1074/jbc.r700045200

Cited by 283 publications

(237 citation statements)

References 52 publications

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“…Defective function of some of these proteins leads to serious pathologic conditions in humans [8,9]. However, numerous reports show that inappropriate activation of Nox proteins results in serious damage, mainly in the cardiovascular system [7,10]. Thus, strict spatiotemporal control of the activity of Nox family proteins is vitally important.…”

Section: Introductionmentioning

confidence: 99%

Role of Rac GTPase activating proteins in regulation of NADPH oxidase in human neutrophils

Lörincz

Szarvas

Smith

et al. 2014

Free Radical Biology and Medicine

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Precise spatiotemporal regulation of O2 •--generating NADPH oxidases (Nox) is a vital requirement. In the case of Nox1-3, which depend on the small GTPase Rac, acceleration of GTP hydrolysis by GTPase activating protein (GAP) could represent a feasible temporal control mechanism. Our goal was to investigate the molecular interactions between RacGAPs and phagocytic Nox2 in neutrophilic granulocytes. In structural studies we revealed that simultaneous interaction of Rac with its effector protein p67 phox and regulatory protein RacGAP was sterically possible. The effect of RacGAPs was experimentally investigated in a cell-free O2 •--generating system consisting of isolated membranes and recombinant p47 phox and p67 phox proteins. Addition of soluble RacGAPs decreased O2 •--production and there was no difference in the effect of four RacGAPs previously identified in neutrophils. Depletion of membrane-associated RacGAPs had selective effect: a decrease in ARHGAP1 or ARHGAP25 level increased O2 •--production but a depletion of ARHGAP35 had no effect.Only membrane-localized RacGAPs seem to be able to interact with Rac when it is assembled in the Nox2 complex. Thus, in neutrophils multiple RacGAPs are involved in the control of O2 •--production by Nox2, allowing selective regulation via different signaling pathways.

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Section: Introductionmentioning

confidence: 99%

Role of Rac GTPase activating proteins in regulation of NADPH oxidase in human neutrophils

Lörincz

Szarvas

Smith

et al. 2014

Free Radical Biology and Medicine

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“…5). Whereas the human NOX2 was discovered early on, other NOX (Nox1/3/4/5) as well as dual oxidase (DUOX) (Duox1/2) enzymes (displaying two domains: a NADPH oxidase domain and a peroxidase domain) have been found relatively recently in human cells.…”

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confidence: 99%

“…On the one hand, xanthine oxidase, an enzyme in the catabolism of purines, which catalyses the oxidation of hypoxanthine to xanthine and to uric acid, produces superoxide (4). On the other hand, NADPH oxidases (NOX) catalyze the production of superoxide from oxygen and NADPH (5).…”

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confidence: 99%

Yno1p/Aim14p, a NADPH-oxidase ortholog, controls extramitochondrial reactive oxygen species generation, apoptosis, and actin cable formation in yeast

Rinnerthaler

Büttner

Laun

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

130

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The large protein superfamily of NADPH oxidases (NOX enzymes) is found in members of all eukaryotic kingdoms: animals, plants, fungi, and protists. The physiological functions of these NOX enzymes range from defense to specialized oxidative biosynthesis and to signaling. In filamentous fungi, NOX enzymes are involved in signaling cell differentiation, in particular in the formation of fruiting bodies. On the basis of bioinformatics analysis, until now it was believed that the genomes of unicellular fungi like Saccharomyces cerevisiae and Schizosaccharomyces pombe do not harbor genes coding for NOX enzymes. Nevertheless, the genome of S. cerevisiae contains nine ORFs showing sequence similarity to the catalytic subunits of mammalian NOX enzymes, only some of which have been functionally assigned as ferric reductases involved in iron ion transport. Here we show that one of the nine ORFs (YGL160W, AIM14) encodes a genuine NADPH oxidase, which is located in the endoplasmic reticulum (ER) and produces superoxide in a NADPH-dependent fashion. We renamed this ORF YNO1 (yeast NADPH oxidase 1). Overexpression of YNO1 causes YCA1-dependent apoptosis, whereas deletion of the gene makes cells less sensitive to apoptotic stimuli. Several independent lines of evidence point to regulation of the actin cytoskeleton by reactive oxygen species (ROS) produced by Yno1p.cell cycle | integral membrane reductase | wiskostatin | latrunculin R eactive oxygen species (ROS) have multiple roles in physiology and pathophysiology, in particular during aging and induction of programmed cell death. This includes also nonmitochondrial sources, besides the long-studied mitochondrially generated ROS. These findings can be viewed as important additions to the classical "free radical theory of aging" (1) and theories developed thereafter (2, 3).In higher organisms, among others, at least two major sources of superoxide other than mitochondria are known. On the one hand, xanthine oxidase, an enzyme in the catabolism of purines, which catalyses the oxidation of hypoxanthine to xanthine and to uric acid, produces superoxide (4). On the other hand, NADPH oxidases (NOX) catalyze the production of superoxide from oxygen and NADPH (5).The NADPH oxidase superfamily of membrane-located enzymes of higher cells has been known for a decade (for review, ref. 5). Whereas the human NOX2 was discovered early on, other NOX (Nox1/3/4/5) as well as dual oxidase (DUOX) (Duox1/2) enzymes (displaying two domains: a NADPH oxidase domain and a peroxidase domain) have been found relatively recently in human cells. The human NOX2 was discovered as a defense enzyme of neutrophils and macrophages, which produce a burst of superoxide (O 2 · − ) as a first line of defense against invading microorganisms. Although X-ray or NMR structure determinations are not available, we know from indirect evidence and bioinformatics that the catalytic subunit of the macrophage enzyme contains six transmembrane helices, is located in the plasma membrane, and produces superoxide in a vectorial ...

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“…5 There are six homologues of Nox2 (namely Nox1, Nox3, Nox4, Nox5, Duox1 and Duox2); each has a specific pattern of expression, but their specific roles remain to be unravelled. 4 A few recent reports have described the relevance of NADPH oxidase ROS production in the differentiation of different kind of cells. 6,7 Therefore, it is tempting to speculate that NADPH ROS production might be a general mechanism common to all types of cell differentiation.…”

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confidence: 99%

“…The main non-mitochondrial sources of ROS are nicotinamide adenine dinucleotide phosphate (NADPH) oxidases (Nox). 4 These proteins are membrane-associated multi-protein complexes that produce superoxide (O 2 À ). The first complex to be described was the phagocyte NADPH oxidase, which produces huge amounts of superoxide and other ROS that are crucial for host defence.…”

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confidence: 99%

p22phox-dependent NADPH oxidase activity is required for megakaryocytic differentiation

et al. 2010

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Transient reactive oxygen species (ROS) production is currently proving to be an important mechanism in the regulation of intracellular signalling, but reports showing the involvement of ROS in important biological processes, such as cell differentiation, are scarce. In this study, we show for the first time that ROS production is required for megakaryocytic differentiation in K562 and HEL cell lines and also in human CD34 þ cells. ROS production is transiently activated during megakaryocytic differentiation, and such production is abolished by the addition of different antioxidants (such as N-acetyl cysteine, trolox, quercetin) or the nicotinamide adenine dinucleotide phosphate (NADPH) oxidase inhibitor diphenylene iodonium. The inhibition of ROS formation hinders differentiation. RNA interference experiments have shown that a p22 phoxdependent NADPH oxidase activity is responsible for ROS production. In addition, the activation of ERK, AKT and JAK2 is required for differentiation, but the activation of phosphatidylinositol 3-kinase and c-Jun N-terminal kinase seems to be less important. When ROS production is prevented, the activation of these signalling pathways is partly inhibited. Taken together, these results show that NADPH oxidase ROS production is essential for complete activation of the main signalling pathways involved in megakaryocytopoiesis to occur. We suggest that this might also be important for in vivo megakaryocytopoiesis.

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Biological Roles for the NOX Family NADPH Oxidases

Cited by 283 publications

References 52 publications

Role of Rac GTPase activating proteins in regulation of NADPH oxidase in human neutrophils

Role of Rac GTPase activating proteins in regulation of NADPH oxidase in human neutrophils

Yno1p/Aim14p, a NADPH-oxidase ortholog, controls extramitochondrial reactive oxygen species generation, apoptosis, and actin cable formation in yeast

p22phox-dependent NADPH oxidase activity is required for megakaryocytic differentiation

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