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01.10.2012

Clinical, Functional and Genetic Analysis of Twenty-Four Patients with Chronic Granulomatous Disease – Identification of Eight Novel Mutations in CYBB and NCF2 Genes

verfasst von: Cécile Martel, Michelle Mollin, Sylvain Beaumel, Jean Paul Brion, Charles Coutton, Véronique Satre, Gaëlle Vieville, Mary Callanan, Christine Lefebvre, Alexandra Salmon, Anne Pagnier, Dominique Plantaz, Cécile Bost-Bru, Laurence Eitenschenck, Isabelle Durieu, Daniel Floret, Claire Galambrun, Hervé Chambost, Gérard Michel, Jean-Louis Stephan, Olivier Hermine, Stéphane Blanche, Nathalie Blot, Hervé Rubié, Guillaume Pouessel, Stephanie Drillon-Haus, Bernard Conrad, Klara M. Posfay-Barbe, Zuzana Havlicekova, Tamara Voskresenky-Baricic, Kelecic Jadranka, Maria Cristina Arriazu, Luis Alberto Garcia, Lamia Sfaihi Ben Mansour, Pierre Bordigoni, Marie José Stasia

Erschienen in: Journal of Clinical Immunology | Ausgabe 5/2012

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Abstract

Chronic granulomatous disease is an inherited disorder in which phagocytes lack a functional NADPH oxidase and cannot produce superoxide anions. The most common form is caused by mutations in CYBB encoding gp91phox. We investigated 24 CGD patients and their families. Twenty-one mutations in CYBB were classified as X91⁰, X91⁺ or X91⁻ variants according to cytochrome b ₅₅₈ expression. Point mutations in encoding regions represented 50 % of the mutations found in CYBB, splice site mutations 27 %, deletions and insertions 23 %. Eight mutations in CYBB were novel leading to X91⁰CGD cases. Two of these were point mutations: c493G>T and a double mutation c625C>G in exon 6 and c1510C>T in exon 12 leading to a premature stop codon at Gly165 in gp91phox and missense mutations His209Arg/Thr503Ile respectively. Two novel splice mutations in 5′intronic regions of introns 1 and 6 were found. A novel deletion/insertion c1024_1026delCTG/insT results in a frameshift introducing a stop codon at position 346 in gp91phox. The last novel mutation was the insertion of a T at c1373 leading to a frameshift and a premature stop codon at position 484 in gp91phox. For the first time the precise size of two large mutations in CYBB was determined by array-comparative genomic hybridization and carriers’ status were evaluated by multiplex ligation-dependent probe amplification assay. No clear correlation between clinical severity and CYBB mutations could be established. Of three mutations in CYBA, NCF1 and NCF2 leading to rare autosomal recessive CGD, one nonsense mutation c29G>A in exon 1 of NCF2 was new.

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Titel: Clinical, Functional and Genetic Analysis of Twenty-Four Patients with Chronic Granulomatous Disease – Identification of Eight Novel Mutations in CYBB and NCF2 Genes
verfasst von: Cécile Martel
Michelle Mollin
Sylvain Beaumel
Jean Paul Brion
Charles Coutton
Véronique Satre
Gaëlle Vieville
Mary Callanan
Christine Lefebvre
Alexandra Salmon
Anne Pagnier
Dominique Plantaz
Cécile Bost-Bru
Laurence Eitenschenck
Isabelle Durieu
Daniel Floret
Claire Galambrun
Hervé Chambost
Gérard Michel
Jean-Louis Stephan
Olivier Hermine
Stéphane Blanche
Nathalie Blot
Hervé Rubié
Guillaume Pouessel
Stephanie Drillon-Haus
Bernard Conrad
Klara M. Posfay-Barbe
Zuzana Havlicekova
Tamara Voskresenky-Baricic
Kelecic Jadranka
Maria Cristina Arriazu
Luis Alberto Garcia
Lamia Sfaihi Ben Mansour
Pierre Bordigoni
Marie José Stasia
Publikationsdatum: 01.10.2012
Verlag: Springer US
Erschienen in: Journal of Clinical Immunology / Ausgabe 5/2012
Print ISSN: 0271-9142
Elektronische ISSN: 1573-2592
DOI: https://doi.org/10.1007/s10875-012-9698-8

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