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Query: EC:1.6.3.1 (
NADPH oxidase
)
11,281
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Tumor necrosis factor alpha (TNF-alpha) receptor-associated factors (TRAFs) play important roles in TNF-alpha signaling by interacting with downstream signaling molecules, e.g., mitogen-activated protein kinases (MAPKs). However, TNF-alpha also signals through reactive oxygen species (ROS)-dependent pathways. The interrelationship between these pathways is unclear; however, a recent study suggested that
TRAF4
could bind to the
NADPH oxidase
subunit p47phox. Here, we investigated the potential interaction between p47phox phosphorylation and
TRAF4
binding and their relative roles in acute TNF-alpha signaling. Exposure of human microvascular endothelial cells (HMEC-1) to TNF-alpha (100 U/ml; 1 to 60 min) induced rapid (within 5 min) p47phox phosphorylation. This was paralleled by a 2.7- +/- 0.5-fold increase in p47phox-
TRAF4
association, membrane translocation of p47phox-
TRAF4
, a 2.3- +/- 0.4-fold increase in p47phox-p22phox complex formation, and a 3.2- +/- 0.2-fold increase in NADPH-dependent O2- production (all P < 0.05).
TRAF4
-p47phox binding was accompanied by a progressive increase in extracellular signal-regulated kinases 1 and 2 (ERK1/2) and p38(MAPK) activation, which was inhibited by an O2- scavenger, tiron.
TRAF4
predominantly bound the phosphorylated form of p47phox, in a protein kinase C-dependent process. Knockdown of
TRAF4
expression using siRNA had no effect on p47phox phosphorylation or binding to p22phox but inhibited TNF-alpha-induced ERK1/2 activation. In coronary microvascular EC from p47phox-/- mice, TNF-alpha-induced
NADPH oxidase
activation, ERK1/2 activation, and cell surface intercellular adhesion molecule 1 (ICAM-1) expression were all inhibited. Thus, both p47phox phosphorylation and
TRAF4
are required for acute TNF-alpha signaling. The increased binding between p47phox and
TRAF4
that occurs after p47phox phosphorylation could serve to spatially confine ROS generation from
NADPH oxidase
and subsequent MAPK activation and cell surface ICAM-1 expression in EC.
...
PMID:Acute tumor necrosis factor alpha signaling via NADPH oxidase in microvascular endothelial cells: role of p47phox phosphorylation and binding to TRAF4. 1574 27
Toll-like receptors (TLR) and nicotinamide adenine dinucleotide phosphate (NADPH) oxidase play an essential role in intracellular eradication of engulfed pathogens. Here, we demonstrate the physical and functional association between components of the cytosolic
NADPH oxidase
and TLR-mediated signaling molecules. Cytosolic components of
NADPH oxidase
suppressed TLR-mediated NF-kappaB activation as well as IFN-beta promoter activation. We demonstrate that TNF-associated factor (TRAF) 4 associates with p47(phox), a component of cytosolic
NADPH oxidase
, and physically interacts and functionally counteracts with TRAF6 and Toll-IL-1 receptor (TIR) domain-containing adaptor-inducing IFN-beta (TRIF) molecules that critically regulate TLR-mediated signaling.
TRAF4
mRNA expression was elicited in RPMI 8226 cells following LPS or CpG DNA treatment. These results suggest that
TRAF4
participates in the molecular mechanism underlying silencing of TLR-mediated signaling through the interaction with molecules harboring phagosome/endosome membrane.
...
PMID:TRAF4 acts as a silencer in TLR-mediated signaling through the association with TRAF6 and TRIF. 1605 31
Endogenous oxidants participate in endothelial cell migration, suggesting that the enzymatic source of oxidants, like other proteins controlling cell migration, requires precise subcellular localization for spatial confinement of signaling effects. We found that the nicotinamide adenine dinucleotide phosphate reduced (NADPH) oxidase adaptor p47(phox) and its binding partner
TRAF4
were sequestered within nascent, focal complexlike structures in the lamellae of motile endothelial cells.
TRAF4
directly associated with the focal contact scaffold Hic-5, and the knockdown of either protein, disruption of the complex, or oxidant scavenging blocked cell migration. An active mutant of
TRAF4
activated the
NADPH oxidase
downstream of the Rho GTPases and p21-activated kinase 1 (PAK1) and oxidatively modified the focal contact phosphatase PTP-PEST. The oxidase also functioned upstream of Rac1 activation, suggesting its participation in a positive feedback loop. Active
TRAF4
initiated robust membrane ruffling through Rac1, PAK1, and the oxidase, whereas the knockdown of PTP-PEST increased ruffling independent of oxidase activation. Our data suggest that
TRAF4
specifies a molecular address within focal complexes that is targeted for oxidative modification during cell migration.
...
PMID:Subcellular targeting of oxidants during endothelial cell migration. 1633 Jul 15
Reactive oxygen species (ROS) function as signaling molecules to mediate various biological responses, including cell migration, growth, and gene expression. ROS are diffusible and short-lived molecules. Thus, localizing the ROS signal at the specific subcellular compartment is essential for activating redox signaling events after receptor activation. NADPH (nicotinamide adenine dinucleotide phosphate) oxidase is one of the major sources of ROS in vasculature; it consists of a catalytic subunit (Nox1, Nox2, Nox3, Nox4, or Nox5), p22phox, p47phox, p67phox, and the small guanosine triphosphatase Rac1. Targeting of
NADPH oxidase
to focal complexes in lamellipodia and membrane ruffles through the interaction of p47phox with the scaffold proteins
TRAF4
and WAVE1 provides a mechanism for achieving localized ROS production, which is required for directed cell migration. ROS are believed to inactivate protein tyrosine phosphatases, which concentrate in specific subcellular compartments, thereby establishing a positive feedback system that activates redox signaling pathways to promote cell movement. Additionally, ROS production may be localized through interactions of
NADPH oxidase
with signaling platforms associated with lipid rafts and caveolae, as well as with endosomes. There is also evidence that
NADPH oxidase
is found in the nucleus, indicating its involvement in redox-responsive gene expression. This review focuses on targeting of
NADPH oxidase
to discrete subcellular compartments as a mechanism of localizing ROS and activation of downstream redox signaling events that mediate various cell functions.
...
PMID:Localizing NADPH oxidase-derived ROS. 1692 63
