Your search keyword '"Arbones ML"' showing total 3 results

1. Mutations in the TMPRSS3 gene are a rare cause of childhood nonsyndromic deafness in Caucasian patients

Author

Andreas Pampanos, Annamaria Pasquadibisceglie, Colette Rossier, Maria L. Arbonés, Barbara Montserrat-Sentis, Michael B. Petersen, Sura Alwan, Raquel Rabionet, Hans-Henrik M. Dahl, Theofilos Iliades, Xavier Estivill, Torsten Schwede, Hamish S. Scott, Paolo Gasparini, Loretta Dougherty, Mario Vincenzo Di Iorio, Stylianos E. Antonarakis, Marie Wattenhofer, Marcello D'Amelio, Wattenhofer, M, DI IORIO, Mv, Rabionet, R, Dougherty, L, Pampanos, A, Schwede, T, MONTSERRAT SENTIS, B, Arbones, Ml, Iliades, T, Pasquadibisceglie, A, D'Amelio, M, Alwan, S, Rossier, C, Dahl, Hh, Petersen, Mb, Estivill, X, Gasparini, Paolo, Scott, H, and Antonarakis, Se

Subjects

Male, Models, Molecular, Chromosomes, Human, Pair 21, Deafness, medicine.disease_cause, Connexins, Catalytic Domain, Exons/genetics, Drug Discovery, Prevalence, Serine Endopeptidases/chemistry/ genetics, Nonsyndromic deafness, Child, Genetics (clinical), ddc:616, Genetics, Mutation, education.field_of_study, Amino Acid Sequence/genetics, European Continental Ancestry Group/ genetics, Serine Endopeptidases, Chromosomes, Human, Pair 21/genetics, Mutation/ genetics, Exons, Syndrome, Membrane Proteins/ genetics, Pedigree, Connexin 26, Peptide Mapping/methods, Molecular Medicine, Female, medicine.symptom, Hearing loss, Molecular Sequence Data, Population, Biology, Peptide Mapping, White People, Frameshift mutation, otorhinolaryngologic diseases, medicine, Humans, Amino Acid Sequence, Allele, education, Gene, Base Sequence, Membrane Proteins, Base Sequence/genetics, medicine.disease, Introns, Chromosome 21, Deafness/enzymology/epidemiology/ etiology/ genetics

Abstract

Two loci for nonsyndromic recessive deafness located on chromosome 21q22.3 have previously been reported, DFNB8 and DFNB10. Recently a gene which encodes a transmembrane serine protease, TMPRSS3 or ECHOS1, was found to be responsible for both the DFNB8 and DFNB10 phenotypes. To determine the contribution of TMPRSS3 mutations in the general congenital/childhood nonsyndromic deaf population we performed mutation analysis of the TMPRSS3 gene in 448 unrelated deaf patients from Spain, Italy, Greece, and Australia who did not have the common 35delG GJB2 mutation. From the 896 chromosomes studied we identified two novel pathogenic mutations accounting for four mutant alleles and at least 16 nonpathogenic sequence variants. The pathogenic mutations were a 1-bp deletion resulting in a frameshift and an amino acid substitution in the LDLRA domain of TMPRSS3. From this and another study we estimate the frequency of TMPRSS3 mutations in our sample as 0.45%, and approximately 0.38% in the general Caucasian childhood deaf population. However, TMPRSS3 is still an important contributor to genetic deafness in populations with large consanguineous families.

Published

2002

2. A common frameshift mutation and other variants in GJB4 (connexin 30.3): Analysis of hearing impairment families

Author

Nuria Lopez-Bigas, Melchionda, S., Gasparini, P., Borragán, A., Arbonés, M. L., Estivill, X., LOPEZ BIGAS, N, Melchionda, S, Gasparini, Paolo, Borragan, A, Arbones, Ml, and Estivill, X.

Subjects

Male, Base Sequence, DNA Mutational Analysis, Homozygote, Molecular Sequence Data, Genetic Variation, Deafness, Skin Diseases, Connexins, Pedigree, Protein Structure, Tertiary, Connexin 26, Humans, Female, Amino Acid Sequence, Frameshift Mutation, Polymorphism, Single-Stranded Conformational

Abstract

Mutations in GJB1, GJB2, GJB3 and GJB6 are involved in hearing impairment. GJB2, GJB3 and GJB6 are also mutated in patients with hyperproliferative skin disorders. The human GJB4 gene has been deduced in silico and a mutation in a family with erythrokeratodermia variabilis has been reported. We describe here the analysis of the GJB4 gene in hearing impairment patients and control subjects. We have identified a common (4%) frameshift mutation (154del4) in GJB4 in both affected and hearing subjects, one patient being homozygous for the mutation. We have also detected five amino acid variants (R103C, R124Q, R160C, C169W and E204A) in individuals that have not skin disorders. While mutation 154del4 is not associated with hearing impairment the involvement of some of the amino acid variants detected here is uncertain. These GJB4 variants should help to define the putative role of connexin 30.3 in both skin disorders and hearing impairment.

Published

2002

3. Molecular Basis of childhood deafness resulting from mutations in the GJB2 (connexin26) gene

Author

Paolo Gasparini, Leopoldo Zelante, Salvatore Melchionda, Nuria Lopez-Bigas, Maria L. Arbonés, Raquel Rabionet, Gabriella Restagno, Leonardo D'Agruma, Xavier Estivill, Rabionet, R, Zelante, L, LOPEZ BIGAS, N, D?agruma, L, Melchionda, S, Restagno, G, Arbones, Ml, Gasparini, Paolo, and Estivill, X.

Subjects

Hearing Loss, Sensorineural, media_common.quotation_subject, Nonsense, Mutation, Missense, Genes, Recessive, medicine.disease_cause, Connexins, Frameshift mutation, otorhinolaryngologic diseases, Genetics, medicine, Humans, Missense mutation, Allele, Child, Frameshift Mutation, Gene, Alleles, Genetics (clinical), media_common, Mutation, biology, Phenotype, Connexin 26, biology.protein, Gene Deletion, GJB6

Abstract

Mutations in the GJB2 gene have been identified in many patients with childhood deafness, 35delG being the most common mutation in Caucasoid populations. We have analyzed a total of 576 families/unrelated patients with recessive or sporadic deafness from Italy and Spain, 193 of them being referred as autosomal recessive, and the other 383 as apparently sporadic cases (singletons). Of the 1,152 unrelated GJB2 chromosomes analyzed from these patients, 37% had GJB2 mutations. Twenty-three different mutations were detected (1 in-frame deletion, 4 nonsense, 5 frameshift, and 13 missense mutations). Mutation 35delG was the most common, accounting for 82% of all GJB2 deafness alleles. The relative frequency of 35delG in Italy and Spain was different, representing 88% of the alleles in Italian patients and only 55% in the Spanish cases. Eight non-35delG mutations were detected more than once (V37I, E47X, 167delT, L90P, 312de114, 334delAA, R143W, and R184P), with relative frequencies ranging between 0.5 and 1.6% of the GJB2 deafness alleles. The information based on conservation of amino acid residues, coexistence with a second GJB2 mutation or absence of the mutation in non-deaf control subjects, suggests that most of these missense changes should be responsible for the deafness phenotype.

Published

2000