Abstract
Chronic granulomatous disease is an inherited disorder in which phagocytes lack a functional NADPH oxidase and so cannot generate superoxide anions (O −2 ). The most common form is caused by mutations in CYBB encoding gp91 phox, the heavy chain of flavocytochrome b558 (XCGD). We investigated 11 male patients and their families suspected of suffering from X-linked CGD. These XCGD patients were classified as having different variants (X910, X91− or X91+) according to their cytochrome b558 expression and NADPH oxidase activity. Nine patients had X910 CGD, one had X91− CGD and one had X91+ CGD. Six mutations in CYBB were novel. Of the four new X910 CGD cases, three were point mutations: G65A in exon 2, G387T in exon 5 and G970T in exon 9, leading to premature stop codons at positions Try18, Try125 and Glu320, respectively, in gp91 phox. One case of X910 CGD originated from a new 1005G deletion detected in exon 9. Surprisingly, four nonsense mutations in exon 5 led to the generation of two mRNAs, one with a normal size containing the mutation and the other in which exon 5 had been spliced. A novel X91− CGD case with low gp91 phox expression was diagnosed. It was caused by an 11-bp deletion in the linking region between exon 12 and intron 12, activating a new cryptic site. Finally, a new X91+ CGD case was detected, characterized by a missense mutation Leu505Arg in the potential NADPH-binding site of gp91 phox. No clear correlation between the severity of the clinical symptoms and the sub-type of XCGD could be established.
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Acknowledgements
The authors are grateful to Dr. D. Roos and Dr. A. J. Verhoeven for the generous gift of mAb 449 and mAb 48 raised against the two subunits of cytochrome b558. We also thank Ms. Linda Northrup for editing the manuscript. This work was supported by grants from the Université Joseph Fourier, Faculté de Médecine; the Région Rhône-Alpes, programme Emergence; the Ministère de l’Education et de la Recherche; MENRT; the Direction de la Recherche Régionale Clinique; Laboratoire Merck-Sharp and Dohme-Chibret; and the Programme conjoint de recherche Tempra/Mira 2001-Région Rhône-Alpes.
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Stasia, M.J., Bordigoni, P., Floret, D. et al. Characterization of six novel mutations in the CYBB gene leading to different sub-types of X-linked chronic granulomatous disease. Hum Genet 116, 72–82 (2005). https://doi.org/10.1007/s00439-004-1208-5
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DOI: https://doi.org/10.1007/s00439-004-1208-5