Next-generation sequencing (NGS) as a diagnostic tool for retinal degeneration reveals a much higher detection rate in early-onset disease

Next-generation sequencing (NGS) as a diagnostic tool for retinal degeneration reveals a much higher detection rate in early-onset disease

Inherited retinal degeneration (IRD) is a common cause of visual impairment (prevalence ∼1/3500). There is considerable phenotype and genotype heterogeneity, making a specific diagnosis very difficult without molecular testing. We investigated targeted capture combined with next-generation sequencin...

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Veröffentlicht in:European journal of human genetics : EJHG 2013-03, Vol.21 (3), p.274-280
Hauptverfasser: Shanks, Morag E, Downes, Susan M, Copley, Richard R, Lise, Stefano, Broxholme, John, Hudspith, Karl Az, Kwasniewska, Alexandra, Davies, Wayne Il, Hankins, Mark W, Packham, Emily R, Clouston, Penny, Seller, Anneke, Wilkie, Andrew Om, Taylor, Jenny C, Ragoussis, Jiannis, Németh, Andrea H
Format: Artikel
Sprache:eng
Schlagworte:
Age
Age of Onset
Diagnosis
Dystrophy
Family medical history
Genes
Genetics
Genotypes
Humans
Laboratories
Mutation
Neurosciences
Pathogenicity
Patients
Phenotypes
Retina
Retinal degeneration
Retinal Degeneration - diagnosis
Retinal Degeneration - epidemiology
Retinal Degeneration - genetics
Retinitis
Retinitis pigmentosa
Retinitis Pigmentosa - diagnosis
Retinitis Pigmentosa - genetics
Rhodopsin
Rhodopsin - genetics
Sequence Analysis, DNA - methods
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Zusammenfassung:Inherited retinal degeneration (IRD) is a common cause of visual impairment (prevalence ∼1/3500). There is considerable phenotype and genotype heterogeneity, making a specific diagnosis very difficult without molecular testing. We investigated targeted capture combined with next-generation sequencing using Nimblegen 12plex arrays and the Roche 454 sequencing platform to explore its potential for clinical diagnostics in two common types of IRD, retinitis pigmentosa and cone-rod dystrophy. 50 patients (36 unknowns and 14 positive controls) were screened, and pathogenic mutations were identified in 25% of patients in the unknown, with 53% in the early-onset cases. All patients with new mutations detected had an age of onset
ISSN:1018-4813
1476-5438
DOI:10.1038/ejhg.2012.172