Spectrum of Mutations in the RPGR Gene That Are Identified in 20% of Families with X-Linked Retinitis Pigmentosa |
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| Authors: | Monika Buraczynska,Weiping Wu,Ricardo Fujita,Kinga Buraczynska,Ellen Phelps,Sten André asson,Jean Bennett,David G. Birch,Gerald A. Fishman,Dennis R. Hoffman,George Inana,Samuel G. Jacobson,Maria A. Musarella,Paul A. Sieving,Anand Swaroop |
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| Affiliation: | M Buraczynska, W Wu, R Fujita, K Buraczynska, E Phelps, S Andréasson, J Bennett, D G Birch, G A Fishman, D R Hoffman, G Inana, S G Jacobson, M A Musarella, P A Sieving, and A Swaroop |
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| Abstract: | The RPGR (retinitis pigmentosa GTPase regulator) gene for RP3, the most frequent genetic subtype of X-linked retinitis pigmentosa (XLRP), has been shown to be mutated in 10%-15% of European XLRP patients. We have examined the RPGR gene for mutations in a cohort of 80 affected males from apparently unrelated XLRP families, by direct sequencing of the PCR-amplified products from the genomic DNA. Fifteen different putative disease-causing mutations were identified in 17 of the 80 families; these include four nonsense mutations, one missense mutation, six microdeletions, and four intronic-sequence substitutions resulting in splice defects. Most of the mutations were detected in the conserved N-terminal region of the RPGR protein, containing tandem repeats homologous to those present in the RCC-1 protein (a guanine nucleotide-exchange factor for Ran-GTPase). Our results indicate that mutations either in as yet uncharacterized sequences of the RPGR gene or in another gene located in its vicinity may be a more frequent cause of XLRP. The reported studies will be beneficial in establishing genotype-phenotype correlations and should lead to further investigations seeking to understand the mechanism of disease pathogenesis. |
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| Keywords: | Author Keywords: Retinal degeneration Dystrophy Blindness Ocular disease Genetic defect Guanine nucleotide-exchange factor |
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