Your search keyword '"Duygu Duman"' showing total 3 results

1. A truncating mutation in GPSM2 is associated with recessive non-syndromic hearing loss

Author

Adil Cinar Akkaynak, Hatice Akay, Mary Claire King, Kemal O. Yariz, Tom Walsh, Mustafa Tekin, and Duygu Duman

Subjects

Male, Genotype, Turkey, Hearing loss, Genes, Recessive, Consanguinity, Biology, Polymorphism, Single Nucleotide, Article, otorhinolaryngologic diseases, Genetics, medicine, Humans, Hearing Loss, Genetics (clinical), Truncating mutation, Genetic heterogeneity, Homozygote, Intracellular Signaling Peptides and Proteins, Phenotype, Mutation, Mutation (genetic algorithm), Female, Allelic heterogeneity, medicine.symptom

Abstract

Yariz KO, Walsh T, Akay H, Duman D, Akkaynak AC, King M-C, Tekin M. A truncating mutation in GPSM2 is associated with recessive non-syndromic hearing loss. Hereditary deafness is a genetically heterogeneous phenotype for which more than 100 genomic loci have been identified thus far. By analysis of a consanguineous Palestinian family, GPSM2 was recently discovered to be the cause of autosomal recessive non-syndromic hearing loss DFNB82. Here, we report a second truncating mutation, GPSM2 p.Q562X, identified via autozygosity mapping in a consanguineous Turkish family. This report provides evidence for allelic heterogeneity of GPSM2 and confirms its causative role for non-syndromic deafness.

Published

2011

2. A founderTMIEmutation is a frequent cause of hearing loss in southeastern Anatolia

Author

Mustafa Tekin, Duygu Duman, Armagan Incesulu, S Taşır-Yılmaz, Seyra Erbek, Hatice Ozturkmen-Akay, Asli Sirmaci, and Hilal Özdağ

Subjects

Turkey, Hearing loss, Hearing Loss, Sensorineural, DNA Mutational Analysis, Molecular Sequence Data, Consanguinity, Biology, Compound heterozygosity, Polymorphism, Single Nucleotide, Connexins, Gene Frequency, Genetics, medicine, Humans, Point Mutation, Genetic Testing, Allele frequency, Genetics (clinical), Base Sequence, Genome, Human, Point mutation, Haplotype, Membrane Proteins, DNA, medicine.disease, Connexin 26, Amino Acid Substitution, Haplotypes, Sensorineural hearing loss, medicine.symptom, Founder effect

Abstract

Using Affymetrix 10K arrays, we searched for regions of homozygosity in 51 Turkish families including at least three members with either congenital or prelingual autosomal recessive non-syndromic sensorineural hearing loss (ARNSSNHL), and identified four families whose deafness mapped to the DFNB6 locus on 3p21 containing the TMIE gene. Mutation analysis revealed the p.R84W mutation in all four families. Screening of this mutation in 254 families with ARNSSNHL, without GJB2 mutations, revealed four additional affected families. A novel mutation was found in a non-complementary marriage between a deaf couple who were homozygous for p.R84W and p.W57X, respectively with two affected children who were compound heterozygotes. Six of the TMIE families originated from southeastern Anatolia, making p.R84W a common cause of hearing loss in that region with a relative frequency of 10.3% (95% CI is 2.5-18.1%). The overall prevalence of the p.R84W mutation in ARNSSNHL in Turkey is 2.4% (95% CI is 0.7-4.0%). Genotyping of single-nucleotide polymorphisms flanking the TMIE gene revealed a conserved haplotype, suggesting a single origin for p.R84W from a common ancestor 1250 years ago (95% CI is 650-2500 years). We conclude that p.R84W could be a common mutation in other Middle Eastern populations and should be included in mutation screening offered to individuals with ARNSSNHL.

Published

2009

3. Homozygous FGF3 mutations result in congenital deafness with inner ear agenesis, microtia, and microdontia

Author

Suat Fitoz, Levent Sennaroglu, S Birnbaum, EB Yüksel Konuk, Mustafa Tekin, Walter E. Nance, Senem Senturk, Ergul Tuncbilek, Filiz Basak Cengiz, Duygu Duman, Armagan Incesulu, H. Ozturkmen Akay, I Cebeci, A Hasanefendioğlu Bayrak, and Gülen Eda Utine

Subjects

Adult, Male, Proband, animal structures, Adolescent, DNA Mutational Analysis, Fibroblast Growth Factor 3, Emissary veins, Deafness, Biology, medicine.disease_cause, Nuclear Family, Genetics, medicine, Microdontia, Humans, Child, Genetics (clinical), Auricle, Mutation, Tooth Abnormalities, Homozygote, Microtia, Infant, Aplasia, Anatomy, medicine.disease, stomatognathic diseases, medicine.anatomical_structure, Ear, Inner, Agenesis, Blood Vessels, Female

Abstract

Homozygous mutations in the fibroblast growth factor 3 (FGF3) gene have recently been discovered in an autosomal recessive form of syndromic deafness characterized by complete labyrinthine aplasia (Michel aplasia), microtia, and microdontia (OMIM 610706 - LAMM). In order to better characterize the phenotypic spectrum associated with FGF3 mutations, we sequenced the FGF3 gene in 10 unrelated families in which probands had congenital deafness associated with various inner ear anomalies, including Michel aplasia, with or without tooth or external ear anomalies. FGF3 sequence changes were not found in eight unrelated probands with isolated inner ear anomalies or with a cochlear malformation along with auricle and tooth anomalies. We identified two new homozygous FGF3 mutations, p.Leu6Pro (c.17T > C) and p. Ile85MetfsX15 (c.254delT), in four subjects from two unrelated families with LAMM. The p.Leu6Pro mutation occurred within the signal site of FGF3 and is predicted to impair its secretion. The c.254delT mutation results in truncation of FGF3. Both mutations completely co-segregated with the phenotype, and heterozygotes did not have any of the phenotypic findings of LAMM. Some affected children had large skin tags on the upper side of the auricles, which is a distinctive clinical component of the syndrome. Enlarged collateral emissary veins associated with stenosis of the jugular foramen were noted on computerized tomographies of most affected subjects with FGF3 mutations. However, similar venous anomalies were also detected in persons with non-syndromic Michel aplasia, suggesting that a direct causative role of impaired FGF3 signaling is unlikely.

Published

2008