Abstract

The phagocyte respiratory burst oxidase that generates the superoxide radical plays a central role in host defense and the inflammatory response. Genetic defects in oxidase subunits result in chronic granulomatous disease (CGD), a syndrome characterized by an absent respiratory burst and recurrent infections. A low-potential cytochrome in the plasma membrane is the focal point for oxidase assembly, and contains both flavin and heme redox centers for transfer of electrons from NADPH to O2. This phagocyte-specific cytochrome is comprised of gp91phox, a 91 kD glycoprotein encoded by an X-linked gene that is the site of mutations in X-linked CGD, and p22phox, a non-glycosylated peptide derived from an autosomal CGD locus. Upon oxidase activation, the cytosolic oxidase subunits, p47phox and p67phox, and a small GTPase, Rac, associate with the plasma membrane, and appear to interact directly with the cytochrome to initiate electron transfer. A ras-related small GTPase, Rap1a, co-purifies with the cytochrome b, and may also participate in regulation of oxidase activity. The structural and functional relationships between various oxidase subunits remain incompletely understood. The overall goal of this project is to develop a clearer understanding of how the phagocyte cytochrome b functions in the regulated production of superoxide. The project has four specific objectives, many of which take advantage of a gp91phox-deficient phagocyte cell line recently developed by gene targeting. First, the topologic organization of the cytochrome complex with respect to the plasma membrane will be investigated using site-directed mutagenesis of potential glycosylation sites and by developing monoclonal and antipeptide antibodies using a new mouse model of X-linked CGD. Second, specific cytochrome residues that participate in the transfer of electrons through flavin and heme centers will be identified using site-directed mutagenesis. Third, domains in the gp91phox cytochrome subunit that function in the assembly and regulation of oxidase will be identified, using a strategy that emphasizes site-directed mutagenesis of candidate gp91phox domains followed by expression and analysis of mutant cytochrome function in intact phagocytes. Fourth, a Rap1a-deficient cell line will be generated by gene targeting to further investigate the interaction of the Rap1a GTPase with cytochrome b and its function in the respiratory burst oxidase. Alternative systems using expression of Rap1a transgenes in cultured cells will also be explored. These studies will provide further insight into the superoxide-generating system of the phagocyte, which may lead to new approaches in modulating superoxide formation in the inflammatory response.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL045635-09
Application #
2714026
Study Section
Medical Biochemistry Study Section (MEDB)
Project Start
1991-12-02
Project End
2001-05-31
Budget Start
1998-06-01
Budget End
1999-05-31
Support Year
9
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Indiana University-Purdue University at Indianapolis
Department
Pediatrics
Type
Schools of Medicine
DUNS #
005436803
City
Indianapolis
State
IN
Country
United States
Zip Code
46202

  Publications

Bagaitkar, Juhi; Huang, Jing; Zeng, Melody Yue et al. (2018) NADPH oxidase activation regulates apoptotic neutrophil clearance by murine macrophages. Blood 131:2367-2378
Roos, Dirk; van Buul, Jaap D; Tool, Anton Tj et al. (2014) Two CGD Families with a Hypomorphic Mutation in the Activation Domain of p67(phox). J Clin Cell Immunol 5:
Zeng, Melody Yue; Pham, Duy; Bagaitkar, Juhi et al. (2013) An efferocytosis-induced, IL-4-dependent macrophage-iNKT cell circuit suppresses sterile inflammation and is defective in murine CGD. Blood 121:3473-83
Crotzer, Victoria L; Matute, Juan D; Arias, Andrés A et al. (2012) Cutting edge: NADPH oxidase modulates MHC class II antigen presentation by B cells. J Immunol 189:3800-4
Casbon, Amy-Jo; Long, Matthew E; Dunn, Kenneth W et al. (2012) Effects of IFN-? on intracellular trafficking and activity of macrophage NADPH oxidase flavocytochrome b558. J Leukoc Biol 92:869-82
Jacob, Chaim O; Eisenstein, Miriam; Dinauer, Mary C et al. (2012) Lupus-associated causal mutation in neutrophil cytosolic factor 2 (NCF2) brings unique insights to the structure and function of NADPH oxidase. Proc Natl Acad Sci U S A 109:E59-67
Bagaitkar, Juhi; Matute, Juan D; Austin, Anthony et al. (2012) Activation of neutrophil respiratory burst by fungal particles requires phosphatidylinositol 3-phosphate binding to p40(phox) in humans but not in mice. Blood 120:3385-7
Yamada, Mitsuhiro; Gomez, John C; Chugh, Pauline E et al. (2011) Interferon-? production by neutrophils during bacterial pneumonia in mice. Am J Respir Crit Care Med 183:1391-401
Bustamante, Jacinta; Arias, Andres A; Vogt, Guillaume et al. (2011) Germline CYBB mutations that selectively affect macrophages in kindreds with X-linked predisposition to tuberculous mycobacterial disease. Nat Immunol 12:213-21
Li, Xing Jun; Marchal, Christophe C; Stull, Natalie D et al. (2010) p47phox Phox homology domain regulates plasma membrane but not phagosome neutrophil NADPH oxidase activation. J Biol Chem 285:35169-79

Showing the most recent 10 out of 53 publications