Mutations in the pre-mRNA splicing factor gene PRPC8 in autosomal dominant retinitis pigmentosa (RP13)

McKie, Arthur B.; McHale, John C.; Keen, T J; Tarttelin, Emma E.; Goliath, René; Lith-Verhoeven, Janneke J.C. van; Greenberg, Jacquie; Ramesar, Raj; Hoyng, Carel B.; Cremers, Frans P.M.; Mackey, David A.; Bhattacharya, Siladitya; Bird, Alan C.; Markham, Alexander F.; Inglehearn, Chris F.

doi:10.1093/hmg/10.15.1555

Cited by 245 publications

(173 citation statements)

References 27 publications

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“…Trans-acting defects arise from mutations or misregulation of splicing regulatory factors. One example is retinitis pigmentosa, characterized by a progressive loss of rod photoreceptor cells, which results from mutations in HPRP3, PRP31, and PRPC8-factors crucial for the assembly and functioning of U small nuclear ribonucleoproteins (snRNPs) in premRNA splicing (McKie et al 2001;Vithana et al 2001;Chakarova et al 2002). Although increasing numbers of splicing-related disorders have been identified, the molecular link between AS regulation and the disease phenotype remains to be elucidated.…”

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confidence: 99%

PQBP1, a factor linked to intellectual disability, affects alternative splicing associated with neurite outgrowth

et al. 2013

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Polyglutamine-binding protein 1 (PQBP1) is a highly conserved protein associated with neurodegenerative disorders. Here, we identify PQBP1 as an alternative messenger RNA (mRNA) splicing (AS) effector capable of influencing splicing of multiple mRNA targets. PQBP1 is associated with many splicing factors, including the key U2 small nuclear ribonucleoprotein (snRNP) component SF3B1 (subunit 1 of the splicing factor 3B [SF3B] protein complex). Loss of functional PQBP1 reduced SF3B1 substrate mRNA association and led to significant changes in AS patterns. Depletion of PQBP1 in primary mouse neurons reduced dendritic outgrowth and altered AS of mRNAs enriched for functions in neuron projection development. Disease-linked PQBP1 mutants were deficient in splicing factor associations and could not complement neurite outgrowth defects. Our results indicate that PQBP1 can affect the AS of multiple mRNAs and indicate specific affected targets whose splice site determination may contribute to the disease phenotype in PQBP1-linked neurological disorders.

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confidence: 99%

PQBP1, a factor linked to intellectual disability, affects alternative splicing associated with neurite outgrowth

et al. 2013

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“…21,32,[42][43][44] Although it is clear that the retina requires a relatively high level of RNA splicing activity for optimal tissue-specific physiological function, 45 how the defects in this essential macromolecular complex transform into a photoreceptorspecific phenotype is unknown. The underlying reason for the RNA intron-splicing factors to be related to adRP is also unclear.…”

Section: Discussionmentioning

confidence: 99%

Contribution of SNRNP200 sequence variations to retinitis pigmentosa

Zhang

Lai

Chiang

et al. 2013

Eye

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Purpose Mutations in the SNRNP200 gene have been reported to cause autosomal dominant retinitis pigmentosa (adRP). In this study, we evaluate the mutation profile of SNRNP200 in a cohort of southern Chinese RP patients. Methods Twenty adRP patients from 11 families and 165 index patients with non-syndromic RP with mixed inheritance patterns were screened for mutations in the mutation hotspots of SNRNP200. These included exons 12-16, 22-32, and 38-45, which covered the two helicase ATP-binding domains in DEAD-box and two sec-63 domains. The targeted regions were amplified by polymerase chain reaction and analyzed by direct DNA sequencing, followed by in silico analyses. Results Totally 26 variants were identified, 18 of which were novel.

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“…Lack of the PRPF31 protein blocks tri-snRNP formation and pre-mRNA splicing [Makarova et al, 2002]. It is interesting to note that two other newly-identified adRP genes also encode proteins involved in pre-mRNA splicing: PRPC8 at 17p13.3 (RP13) coding for PRP8 (a core component of the U5 snRNP) [McKie et al, 2001], and HPRP3 at 1p13-q21 (RP18) for PRP3 (a component of the U4/U6) [Chakarova et al, 2002]. These data together suggest that disruptions in tri-SNP formation and function contribute to the pathogenesis of adRP.…”

Section: Discussionmentioning

confidence: 99%

Novel deletion in the pre‐mRNA splicing gene PRPF31 causes autosomal dominant retinitis pigmentosa in a large Chinese family

Wang

Ribaudo

Zhao

et al. 2003

American J of Med Genetics Pt A

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We report the identification of a novel 12 bp deletion of the pre-mRNA splicing gene PRPF31 in a large Chinese family with autosomal dominant retinitis pigmentosa (adRP). This mutation results in the deletion of four amino acids (ΔH 111 K 112 F 113 I 114 ) including H 111 , an amino acid residue that is highly conserved throughout evolution. The 12 bp deletion co-segregates with the disease phenotype in 19 RP patients in the family, but is not present in unaffected relatives or 100 normal individuals. Our data indicate that the novel 12 bp deletion in PRPF31 causes retinitis pigementosa in this Chinese adRP family. In contrast to the incomplete penetrance observed in most adRP families linked to chromosome band 19q13.4 (RP11), the 12 bp PRPF31 deletion identified in this study appears to show high penetrance. These data expand the spectrum of PRPF31 mutations causing adRP, and confirm the role of PRPF31 in the pathogenesis of RP.

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Mutations in the pre-mRNA splicing factor gene PRPC8 in autosomal dominant retinitis pigmentosa (RP13)

Cited by 245 publications

References 27 publications

PQBP1, a factor linked to intellectual disability, affects alternative splicing associated with neurite outgrowth

PQBP1, a factor linked to intellectual disability, affects alternative splicing associated with neurite outgrowth

Contribution of SNRNP200 sequence variations to retinitis pigmentosa

Novel deletion in the pre‐mRNA splicing gene PRPF31 causes autosomal dominant retinitis pigmentosa in a large Chinese family

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