A new role of Pro-73 of p47phox in the activation of neutrophil NADPH oxidase

A new role of Pro-73 of p47phox in the activation of neutrophil NADPH oxidase

The PX domain of p47phox is thought to be involved in autoinhibition. However, when the domain was deleted, the ability to activate the phagocyte NADPH oxidase was markedly diminished. We have mutated the proline-rich region of the PX domain and examined the mutants for the ability to activate. Subs...

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Veröffentlicht in:Archives of biochemistry and biophysics 2003-08, Vol.416 (1), p.92-100
Hauptverfasser: Nagasawa, Teruaki, Ebisu, Kentaro, Inoue, Yasuyuki, Miyano, Kei, Tamura, Minoru
Format: Artikel
Sprache:eng
Schlagworte:
Amino Acid Motifs
Cells, Cultured
Circular Dichroism
Cytochrome b Group - metabolism
Enzyme Activation - physiology
Humans
Kinetics
Mutation
NADPH Oxidases - metabolism
Neutrophils - enzymology
Neutrophils - metabolism
Phosphatidylinositol Phosphates - metabolism
Phospholipids - metabolism
Phosphoproteins - chemistry
Phosphoproteins - genetics
Phosphoproteins - metabolism
Proline - genetics
Proline - metabolism
Protein Structure, Tertiary
rac GTP-Binding Proteins - genetics
rac GTP-Binding Proteins - metabolism
Recombinant Proteins - genetics
Recombinant Proteins - metabolism
Sodium Dodecyl Sulfate - chemistry
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Zusammenfassung:The PX domain of p47phox is thought to be involved in autoinhibition. However, when the domain was deleted, the ability to activate the phagocyte NADPH oxidase was markedly diminished. We have mutated the proline-rich region of the PX domain and examined the mutants for the ability to activate. Substitution of Gln for Pro-73 of p47phox(1-286) (P73Q) resulted in a considerably lower activity than the wild type and P73Q had a much lower affinity for the oxidase complex. Whereas, Gln substitution for Pro-76 (P76Q) showed a slightly enhanced activation and the mutant had a slightly higher affinity for the complex than the wild type. Affinity for p67phox(1-210) was slightly decreased either by P73Q or P76Q. Optimal SDS concentration for the activation was lowered by these mutations. Binding of PX domain with phosphatidylinositol-3,4-bisphosphate was diminished by P73Q mutation. The results in this study suggest that Pro-73 has a role in interaction with the catalytic component cytochrome b558.
ISSN:0003-9861