Inés Pereiro scite author profile

Retinitis pigmentosa is a genetically heterogeneous group of inherited ocular disorders characterized by progressive photoreceptor cell loss, night blindness, constriction of the visual field, and progressive visual disability. Homozygosity mapping and gene expression studies identified a 2 exon gene, C2ORF71. The encoded protein has no homologs and is highly expressed in the eye, where it is specifically expressed in photoreceptor cells. Two mutations were found in C2ORF71 in human RP patients: A nonsense mutation (p.W253X) in the first exon is likely to be a null allele; the second, a missense mutation (p.I201F) within a highly conserved region of the protein, leads to proteosomal degradation. Bioinformatic and functional studies identified and validated sites of lipid modification within the first three amino acids of the C2ORF71 protein. Using morpholino oligonucleotides to knockdown c2orf71 expression in zebrafish results in visual defects, confirming that C2ORF71 plays an important role in the development of normal vision. Finally, localization of C2ORF71 to primary cilia in cultured cells suggests that the protein is likely to localize to the connecting cilium or outer segment of photoreceptor cells.

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Arrayed primer extension technology simplifies mutation detection in Bardet–Biedl and Alström syndrome

Pereiro

Hoskins²,

Marshall

et al. 2010

Eur J Hum Genet

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Bardet-Biedl syndrome (BBS; OMIM no. 209 900) and Alströ m syndrome (ALMS; OMIM no. 203 800) are rare, multisystem genetic disorders showing both a highly variable phenotype and considerable phenotypic overlap; they are included in the emerging group of diseases called ciliopathies. The genetic heterogeneity of BBS with 14 causal genes described to date, serves to further complicate mutational analysis. The development of the BBS-ALMS array which detects known mutations in these genes has allowed us to detect at least one mutation in 40.5% of BBS families and in 26.7% of ALMS families validating this as an efficient and cost-effective first pass screening modality. Furthermore, using this method, we found two BBS families segregating three BBS alleles further supporting oligogenicity or modifier roles for additional mutations. We did not observe more than two mutations in any ALMS family.

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Overview of Bardet–Biedl syndrome in Spain: identification of novel mutations in BBS1,BBS10 and BBS12 genes

et al. 2014

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Complexity of Phenotype–Genotype Correlations in Spanish Patients withRDH12Mutations

Valverde

Pereiro

Vallespín

et al. 2009

Invest. Ophthalmol. Vis. Sci.

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Algorithm for the molecular analysis of Bardet–Biedl syndrome in Spain

Castro-Sánchez

Álvarez-Satta

Pereiro

et al. 2015

Medicina Clínica (English Edition)

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Inés Pereiro

Discovery and Functional Analysis of a Retinitis Pigmentosa Gene, C2ORF71

Arrayed primer extension technology simplifies mutation detection in Bardet–Biedl and Alström syndrome

Overview of Bardet–Biedl syndrome in Spain: identification of novel mutations in BBS1,BBS10 and BBS12 genes

Complexity of Phenotype–Genotype Correlations in Spanish Patients withRDH12Mutations

Algorithm for the molecular analysis of Bardet–Biedl syndrome in Spain

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