Mutations in Splicing Factor Genes Are a Major Cause of Autosomal Dominant Retinitis Pigmentosa in Belgian Families

Cauwenbergh, Caroline Van; Coppieters, Frauke; Roels, Dimitri; Jaegere, Sarah De; Flipts, Helena; Zaeytijd, Julie De; Walraedt, Sophie; Claes, Charlotte; Fransen, Erik; Camp, Guy Van; Depasse, Fanny; Casteels, Ingele; Ravel, Thomy de; Leroy, Bart P.; Baere, Elfride De

doi:10.1371/journal.pone.0170038

Cited by 47 publications

(50 citation statements)

References 72 publications

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“…Previous functional studies have demonstrated that p.Ala615Thr variant is a benign polymorphism, and by itself only slightly affects the enzymatic activity of HGSNAT (Feldhammer, Durand, & Pshezhetsky, ). This change, however, has been linked to the phenotype of retinitis pigmentosa when present in homozygosity or heterozygosity (either in cis or trans ) with other HGSNAT mutations (Comander et al, ; Haer‐Wigman et al, ; Van Cauwenbergh et al, ). p.Ala615Thr shows the highest allele frequency (0.01462 in gnomAD) in the Ashkenazi Jewish population (Table S6B).…”

Section: Resultsmentioning

confidence: 89%

Molecular characterization of a large group of Mucopolysaccharidosis type IIIC patients reveals the evolutionary history of the disease

et al. 2019

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Mucopolysaccharidosis type IIIC (MPSIIIC) is a severe, rare autosomal recessive disorder caused by variants in the heparan‐α‐glucosaminide N‐acetyltransferase (HGSNAT) gene which result in lysosomal accumulation of heparan sulfate. We analyzed clinical presentation, molecular defects and their haplotype context in 78 (27 novel) MPSIIIC cases from 22 countries, the largest group studied so far. We describe for the first time disease‐causing variants in the patients from Brazil, Algeria, Azerbaijan, and Iran, and extend their spectrum within Canada, Colombia, Turkey, and the USA. Six variants are novel: two missense, c.773A>T/p.N258I and c.1267G>T/p.G423W, a nonsense c.164T>A/p.L55*, a splice‐site mutation c.494−1G>A/p.[P165_L187delinsQSCYVTQAGVRWHHLGSLQALPPGFTPFSYLSLLSSWNC,P165fs], a deletion c.1348delG/p.(D450fs) and an insertion c.1479dupA/p.(Leu494fs). The missense HGSNAT variants lacked lysosomal targeting, enzymatic activity, and likely the correct folding. The haplotype analysis identified founder mutations, p.N258I, c.525dupT, and p.L55* in the Brazilian state of Paraiba, c.493+1G>A in Eastern Canada/Quebec, p.A489E in the USA, p.R384* in Poland, p.R344C and p.S518F in the Netherlands and suggested that variants c.525dupT, c.372−2G>A, and c.234+1G>A present in cis with c.564‐98T>C and c.710C>A rare single‐nucleotide polymorphisms, have been introduced by Portuguese settlers in Brazil. Altogether, our results provide insights into the origin, migration roots and founder effects of HGSNAT disease‐causing variants, and reveal the evolutionary history of MPSIIIC.

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Section: Resultsmentioning

confidence: 89%

Molecular characterization of a large group of Mucopolysaccharidosis type IIIC patients reveals the evolutionary history of the disease

et al. 2019

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“…Despite this correlation between splicing factor levels and splicing outcomes during aging, it is not clear whether the decreased expression of splicing factors causes the observed age‐associated changes in splicing. As several splicing factors are mutated in age‐related eye disease, understanding the link between individual splicing regulators and age‐associated changes in splicing could have important implications for human health (Daiger, Sullivan, & Bowne, 2013; Sullivan et al, 2006; Van Cauwenbergh et al, 2017). …”

Section: Introductionmentioning

confidence: 99%

Proper splicing contributes to visual function in the aging Drosophila eye

et al. 2018

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Changes in splicing patterns are a characteristic of the aging transcriptome; however, it is unclear whether these age‐related changes in splicing facilitate the progressive functional decline that defines aging. In Drosophila, visual behavior declines with age and correlates with altered gene expression in photoreceptors, including downregulation of genes encoding splicing factors. Here, we characterized the significance of these age‐regulated splicing‐associated genes in both splicing and visual function. To do this, we identified differential splicing events in either the entire eye or photoreceptors of young and old flies. Intriguingly, aging photoreceptors show differential splicing of a large number of visual function genes. In addition, as shown previously for aging photoreceptors, aging eyes showed increased accumulation of circular RNAs, which result from noncanonical splicing events. To test whether proper splicing was necessary for visual behavior, we knocked down age‐regulated splicing factors in photoreceptors in young flies and examined phototaxis. Notably, many of the age‐regulated splicing factors tested were necessary for proper visual behavior. In addition, knockdown of individual splicing factors resulted in changes in both alternative splicing at age‐spliced genes and increased accumulation of circular RNAs. Together, these data suggest that cumulative decreases in splicing factor expression could contribute to the differential splicing, circular RNA accumulation, and defective visual behavior observed in aging photoreceptors.

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“…Pan et al 19 suggested that patients harboring the mutation c.3260C>T may be associated with a more severe phenotype than patients with the mutation c.2042G>A. We therefore compared the reported symptoms and age at onset, as well the phenotype, of all mutations published to date [4][5][6][7][8][9][10][11][12]19,[27][28][29][30][31][32][33][34][35][36] in Table 5. Reduced vision and night blindness, less often visual field changes, are the most commonly reported symptoms.…”

Section: Discussionmentioning

confidence: 99%

Genotype–Phenotype Analysis of a Novel Recessive and a Recurrent Dominant SNRNP200 Variant Causing Retinitis Pigmentosa

Gerth‐Kahlert

Koller

Hanson

et al. 2019

Invest. Ophthalmol. Vis. Sci.

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PURPOSE. To compare phenotype variability in retinitis pigmentosa patients with recessive and dominant mutations in the SNRNP200 gene. METHODS. In a retrospective study, patients of two unrelated families were identified: family A, five patients aged 36 to 77 years; family B, one patient aged 9 years and his asymptomatic parents and sister. All patients received a comprehensive eye examination with a detailed retinal functional and morphologic assessment. Genetic testing was performed by whole exome sequencing (WES) in the index patient from each family. Genes described to be involved in eye diseases (n > 450) were screened for rare variants and segregation analysis was performed. RESULTS. A known heterozygous missense variant (c.3260C>T, p.(Ser1087Leu)) in the SNRNP200 gene was identified in the index patient of family A while a novel homozygous missense mutation (c.1634G>A, p.(Arg545His)) was found in the index patient of family B. Nyctalopia and photophobia were reported by 6/6 and 2/6 patients, respectively. The phenotype associated with the dominant mutation was characterized by variable disease onset (early childhood to the sixth decade of life), disease severity (visual acuity of 20/20-20/ 200 in the seventh to eighth decade), and advanced rod-cone dysfunction. Characteristics of recessive disease included distinct fundus changes of dot-like hypopigmentation together with retinal atrophy and severe rod-cone dysfunction. CONCLUSIONS. The phenotype characteristics in autosomal dominant and recessive SNRNP200 mutations show distinct features, with earlier severe disease in the recessive case and a variable disease expression in the dominant inheritance pattern.

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Mutations in Splicing Factor Genes Are a Major Cause of Autosomal Dominant Retinitis Pigmentosa in Belgian Families

Cited by 47 publications

References 72 publications

Molecular characterization of a large group of Mucopolysaccharidosis type IIIC patients reveals the evolutionary history of the disease

Molecular characterization of a large group of Mucopolysaccharidosis type IIIC patients reveals the evolutionary history of the disease

Proper splicing contributes to visual function in the aging Drosophila eye

Genotype–Phenotype Analysis of a Novel Recessive and a Recurrent Dominant SNRNP200 Variant Causing Retinitis Pigmentosa

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