Géraldine Batot scite author profile

Géraldine Batot

2Publications

80Citation Statements Received

34Citation Statements Given

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Affiliations

Centre Hospitalier Universitaire de Grenoble, Joseph Fourier University

Publications

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Characterization of Neutrophil NADPH Oxidase Activity Reconstituted in a Cell‐Free Assay Using Specific Monoclonal Antibodies Raised Against Cytochrome b₅₅₈

Batot

Martel

Capdeville

et al. 1995

European Journal of Biochemistry

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The immunochemical characterization of NADPH oxidase activity of cytochrome b,,, purified from human neutrophils was determined after reconstitution in a cell-free assay using the native hemoprotein and recombinant purified cytosolic activating factors. The oxidase activity showed a strict dependence on the heme content at each step of the hemoprotein purification process. The immunochemical properties of the reconstituted oxidase made use of monoclonal antibodies raised against membrane-bound and octyl-glucoside-extracted cytochrome h. From nine specific monoclonal antibodies reacting with gp91-phox cytochrome b,,,, two were selected, both of which were found to bind to the subunit of cytochrome b,,, and to inhibit superoxide formation in the oxidase reconstituted cell-free assay. The extent of inhibition was dependent on the phospholipid environment. Neutrophil membrane extracts from X-linked chronic granulomatous disease patients did not produce 0; in the reconstituted system and did not bind to the antibodies.

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Biochemical and immunochemical properties of B lymphocyte cytochrome b558

Batot

Paclet

Doussière

et al. 1998

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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Like neutrophils, Epstein-Barr virus (EBV)-immortalized B lymphocytes express all constituents of the NADPH oxidase complex necessary to generate superoxide anion O2-. The NADPH oxidase activity in EBV-B lymphocytes is only 5% of that measured in neutrophils upon PMA stimulation. Cytochrome b558 is the sole redox membrane component of NADPH oxidase; it is the protein core around which cytosolic factors assemble in order to mediate oxidase activity. In the present study, we have compared the structural and functional properties of cytochrome b558 from EBV-B lymphocytes and neutrophils. Cytochrome b558 from EBV-B lymphocyte plasma membrane, like that from neutrophils, is characterized by a heterodimeric structure with a highly glycosylated beta subunit, known as gp91-phox. While the amount of cytochrome b558 recovered after purification from EBV-B lymphocytes (approximately 0.24 nmol from 1010 cells) was low compared to that recovered from neutrophils (approximately 10 nmol), the biochemical properties of purified cytochrome b558 from both EBV-B lymphocytes and neutrophils were quite similar with respect to their differential spectra, redox potential, and FAD binding site. Once cytochrome b558 was extracted from the EBV-B lymphocyte membrane, it was able to mediate, in a reconstituted system of O2- production the same oxidase turnover as that found for cytochrome b558 extracted from neutrophils. A comparison between membrane bound and soluble cytochrome b558 suggested that the weak oxidase activity measured in intact EBV-B cells might be the result not only of the small amount of expressed cytochrome b558, but also of a defect of the activation process in lymphocyte membrane.

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