Your search keyword '"Avila‐Fernandez, Almudena"' showing total 4 results

1. Mutation analysis of 272 Spanish families affected by autosomal recessive retinitis pigmentosa using a genotyping microarray

Author

Avila-Fernandez, Almudena, Cantalapiedra, Diego, Aller, Elena, Vallespin, Elena, Aguirre-Lamban, Jana, Blanco-Kelly, Fiona, Marta Corton, Riveiro-Alvarez, Rosa, Allikmets, Rando, Jose Trujillo-Tiebas, Maria, Millan, Jose M., Cremers, Frans P. M., and Ayuso, Carmen

Subjects

genetic structures, Genetics and epigenetic pathways of disease [NCMLS 6], eye diseases

Abstract

Contains fulltext : 89342.pdf (Publisher’s version ) (Open Access) PURPOSE: Retinitis pigmentosa (RP) is a genetically heterogeneous disorder characterized by progressive loss of vision. The aim of this study was to identify the causative mutations in 272 Spanish families using a genotyping microarray. METHODS: 272 unrelated Spanish families, 107 with autosomal recessive RP (arRP) and 165 with sporadic RP (sRP), were studied using the APEX genotyping microarray. The families were also classified by clinical criteria: 86 juveniles and 186 typical RP families. Haplotype and sequence analysis were performed to identify the second mutated allele. RESULTS: At least one-gene variant was found in 14% and 16% of the juvenile and typical RP groups respectively. Further study identified four new mutations, providing both causative changes in 11% of the families. Retinol Dehydrogenase 12 (RDH12) was the most frequently mutated gene in the juvenile RP group, and Usher Syndrome 2A (USH2A) and Ceramide Kinase-Like (CERKL) were the most frequently mutated genes in the typical RP group. The only variant found in CERKL was p.Arg257Stop, the most frequent mutation. CONCLUSIONS: The genotyping microarray combined with segregation and sequence analysis allowed us to identify the causative mutations in 11% of the families. Due to the low number of characterized families, this approach should be used in tandem with other techniques.

Published

2010

2. Genotyping microarray: Mutation screening in Spanish families with autosomal dominant retinitis pigmentosa

Author

Blanco-Kelly, Fiona, Garcia-Hoyos, Maria, Marta Corton, Avila-Fernandez, Almudena, Riveiro-Alvarez, Rosa, Gimenez, Ascension, Hernan, Inma, Carballo, Miguel, and Ayuso, Carmen

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Rhodopsin, Genotype, Sensitivity and Specificity, eye diseases, White People, Pedigree, Spain, Mutation, Humans, Genetic Testing, Artifacts, Eye Proteins, Retinitis Pigmentosa, Research Article, Genes, Dominant, Oligonucleotide Array Sequence Analysis

Abstract

Purpose Presently, 22 genes have been described in association with autosomal dominant retinitis pigmentosa (adRP); however, they explain only 50% of all cases, making genetic diagnosis of this disease difficult and costly. The aim of this study was to evaluate a specific genotyping microarray for its application to the molecular diagnosis of adRP in Spanish patients. Methods We analyzed 139 unrelated Spanish families with adRP. Samples were studied by using a genotyping microarray (adRP). All mutations found were further confirmed with automatic sequencing. Rhodopsin (RHO) sequencing was performed in all negative samples for the genotyping microarray. Results The adRP genotyping microarray detected the mutation associated with the disease in 20 of the 139 families with adRP. As in other populations, RHO was found to be the most frequently mutated gene in these families (7.9% of the microarray genotyped families). The rate of false positives (microarray results not confirmed with sequencing) and false negatives (mutations in RHO detected with sequencing but not with the genotyping microarray) were established, and high levels of analytical sensitivity (95%) and specificity (100%) were found. Diagnostic accuracy was 15.1%. Conclusions The adRP genotyping microarray is a quick, cost-efficient first step in the molecular diagnosis of Spanish patients with adRP.

3. Mutational screening of splicing factor genes in cases with autosomal dominant retinitis pigmentosa

Author

Benaglio, Paola, San Jose, Patricia Fernandez, Avila-Fernandez, Almudena, Ascari, Giulia, Harper, Shyana, Manes, Gaël, Ayuso, Carmen, Hamel, Christian, Berson, Eliot L., and Rivolta, Carlo

Subjects

3. Good health

4. Exome sequencing identifies PEX6 mutations in three cases diagnosed with Retinitis Pigmentosa and hearing impairment

Author

Garcia-Garcia, Gema, Sanchez-Navarro, Iker, Aller, Elena, Jaijo, Teresa, Fuster-Garcia, Carla, Rodriguez-Munoz, Ana, Vallejo, Elena, Jose Telleria, Juan, Vazquez, Selma, Beltran, Sergi, Derdak, Sophia, Zurita, Olga, Villaverde-Montero, Cristina, Avila-Fernandez, Almudena, Marta Corton, Blanco-Kelly, Fiona, Hakonarson, Hakon, Millan, Jose M., and Ayuso, Carmen

Subjects

Retinitis pigmentària, Discapacitats auditius, PEROXISOME BIOGENESIS DISORDERS, HEIMLER SYNDROME, Proteïnes, PATIENT, Genètica

Abstract

PURPOSE: The aim of the present work is the molecular diagnosis of three patients with deafness and retinal degeneration. METHODS: Three patients from two unrelated families were initially analyzed with custom gene panels for Usher genes, non-syndromic hearing loss, or inherited syndromic retinopathies and further investigated by means of clinical or whole exome sequencing. RESULTS: The study allowed us to detect likely pathogenic variants in PEX6, a gene typically involved in peroxisomal biogenesis disorders (PBDs). Beside deaf-blindness, both families showed additional features: Siblings from Family 1 showed enamel alteration and abnormal peroxisome. In addition, the brother had mild neurodevelopmental delay and nephrolithiasis. The case II:1 from Family 2 showed intellectual disability, enamel alteration, and dysmorphism. CONCLUSIONS: We have reported three new cases with pathogenic variants in PEX6 presenting with milder forms of the Zellweger spectrum disorders (ZSD). The three cases showed distinct clinical features. Thus, expanding the phenotypic spectrum of PBDs and ascertaining exome sequencing is an effective strategy for an accurate diagnosis of clinically overlapping and genetically heterogeneous disorders such as deafness-blindness association. This work was financially supported by grants of the Institute of Health Carlos III (ISCIII /FEDER), (Ref.: PI13/00638 PI16/00415, PI16/00539 and CIBER-ER 06/07/0036; Biobank FJD (RD09/0076/00101),); Fundación ONCE (Ref.: 2015/0398) ONCE & Fundaluce, Sponsored Chair IIS-FJD, UAM of Genomics Medicine. CNAG's 2013 call “300 exomes to elucidate rare diseases.” Institutional Development Fund at CAG from The Children’s Hospital of Philadelphia. CFG, ISN and MCP are recipients of fellowships from the ISCIII (Ref.: IFI14/00021; Sara Borrell CD13–00085 and Miguel Servet CPII17_00006 respectively)