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dc.contributor.authorRae, J.
dc.contributor.authorNewburger, Peter E.
dc.contributor.authorDinauer, Mary C.
dc.contributor.authorNoack, D.
dc.contributor.authorHopkins, Penelope J.
dc.contributor.authorKuruto, R.
dc.contributor.authorCurnutte, John T.
dc.date2022-08-11T08:10:11.000
dc.date.accessioned2022-08-23T16:58:35Z
dc.date.available2022-08-23T16:58:35Z
dc.date.issued1998-06-01
dc.date.submitted2012-04-25
dc.identifier.citationAm J Hum Genet. 1998 Jun;62(6):1320-31. doi 10.1086/301874
dc.identifier.issn0002-9297 (Linking)
dc.identifier.doi10.1086/301874
dc.identifier.pmid9585602
dc.identifier.urihttp://hdl.handle.net/20.500.14038/43401
dc.description.abstractChronic granulomatous disease (CGD) is a hereditary disorder of host defense due to absent or decreased activity of phagocyte NADPH oxidase. The X-linked form of the disease derives from defects in the CYBB gene, which encodes the 91-kD glycoprotein component (termed "gp91-phox") of the oxidase. We have identified the mutations in the CYBB gene responsible for X-linked CGD in 131 consecutive independent kindreds. Screening by SSCP analysis identified mutations in 124 of the kindreds, and sequencing of all exons and intron boundary regions revealed the other seven mutations. We detected 103 different specific mutations; no single mutation appeared in more than seven independent kindreds. The types of mutations included large and small deletions (11%), frameshifts (24%), nonsense mutations (23%), missense mutations (23%), splice-region mutations (17%), and regulatory-region mutations (2%). The distribution of mutations within the CYBB gene exhibited great heterogeneity, with no apparent mutational hot spots. Evaluation of 87 available mothers revealed X-linked carrier status in all but 10. The heterogeneity of mutations and the lack of any predominant genotype indicate that the disease represents many different mutational events, without a founder effect, as is expected for a disorder with a previously lethal phenotype.
dc.language.isoen_US
dc.relation<a href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=9585602&dopt=Abstract">Link to article in PubMed</a>
dc.relation.urlhttp://www.ncbi.nlm.nih.gov/pmc/articles/PMC1377153/pdf/9585602.pdf
dc.subjectDNA Mutational Analysis
dc.subjectGenetic Linkage
dc.subjectGranulomatous Disease, Chronic
dc.subjectHumans
dc.subjectMembrane Glycoproteins
dc.subjectMolecular Sequence Data
dc.subject*Mutation
dc.subjectNADPH Oxidase
dc.subjectPolymorphism, Single-Stranded Conformational
dc.subjectRespiratory Burst
dc.subject*X Chromosome
dc.subjectHematology
dc.subjectOncology
dc.subjectPediatrics
dc.titleX-Linked chronic granulomatous disease: mutations in the CYBB gene encoding the gp91-phox component of respiratory-burst oxidase
dc.typeJournal Article
dc.source.journaltitleAmerican journal of human genetics
dc.source.volume62
dc.source.issue6
dc.identifier.legacycoverpagehttps://escholarship.umassmed.edu/peds_hematology/8
dc.identifier.contextkey2796495
html.description.abstract<p>Chronic granulomatous disease (CGD) is a hereditary disorder of host defense due to absent or decreased activity of phagocyte NADPH oxidase. The X-linked form of the disease derives from defects in the CYBB gene, which encodes the 91-kD glycoprotein component (termed "gp91-phox") of the oxidase. We have identified the mutations in the CYBB gene responsible for X-linked CGD in 131 consecutive independent kindreds. Screening by SSCP analysis identified mutations in 124 of the kindreds, and sequencing of all exons and intron boundary regions revealed the other seven mutations. We detected 103 different specific mutations; no single mutation appeared in more than seven independent kindreds. The types of mutations included large and small deletions (11%), frameshifts (24%), nonsense mutations (23%), missense mutations (23%), splice-region mutations (17%), and regulatory-region mutations (2%). The distribution of mutations within the CYBB gene exhibited great heterogeneity, with no apparent mutational hot spots. Evaluation of 87 available mothers revealed X-linked carrier status in all but 10. The heterogeneity of mutations and the lack of any predominant genotype indicate that the disease represents many different mutational events, without a founder effect, as is expected for a disorder with a previously lethal phenotype.</p>
dc.identifier.submissionpathpeds_hematology/8
dc.contributor.departmentDepartment of Pediatrics
dc.source.pages1320-31


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