Your search keyword '"Vestibular Diseases genetics"' showing total 56 results

1. Genotype-Phenotype Correlations of Pathogenic COCH Variants in DFNA9: A HuGE Systematic Review and Audiometric Meta-Analysis.

Author

Robijn SMM, Smits JJ, Sezer K, Huygen PLM, Beynon AJ, van Wijk E, Kremer H, de Vrieze E, Lanting CP, and Pennings RJE

Subjects

Genetic Association Studies, Humans, Mutation, Prospective Studies, Extracellular Matrix Proteins genetics, Hearing Loss, Sensorineural genetics, Vestibular Diseases genetics, Vestibular Diseases pathology

Abstract

Pathogenic missense variants in COCH are associated with DFNA9, an autosomal dominantly inherited type of progressive sensorineural hearing loss with or without vestibular dysfunction. This study is a comprehensive overview of genotype-phenotype correlations using the PRISMA and HuGENet guidelines. Study characteristics, risk of bias, genotyping and data on the self-reported age of onset, symptoms of vestibular dysfunction, normative test results for vestibular function, and results of audiovestibular examinations were extracted for each underlying pathogenic COCH variant. The literature search yielded 48 studies describing the audiovestibular phenotypes of 27 DFNA9-associated variants in COCH . Subsequently, meta-analysis of audiometric data was performed by constructing age-related typical audiograms and by performing non-linear regression analyses on the age of onset and progression of hearing loss. Significant differences were found between the calculated ages of onset and progression of the audiovestibular phenotypes of subjects with pathogenic variants affecting either the LCCL domain of cochlin or the vWFA2 and Ivd1 domains. We conclude that the audiovestibular phenotypes associated with DFNA9 are highly variable. Variants affecting the LCCL domain of cochlin generally lead to more progression of hearing loss when compared to variants affecting the other domains. This review serves as a reference for prospective natural history studies in anticipation of mutation-specific therapeutic interventions.

Published

2022

2. Generation and characterization of a P2rx2 V60L mouse model for DFNA41.

Author

Chen X, Abad C, Chen ZY, Young JI, Gurumurthy CB, Walz K, and Liu XZ

Subjects

Adenosine Triphosphate metabolism, Animals, Disease Models, Animal, Gene Knock-In Techniques, Hair Cells, Auditory, Inner pathology, Hearing Loss, Sensorineural pathology, Heterozygote, Humans, Mice, Mutation genetics, Pedigree, Phenotype, Synapses genetics, Synapses pathology, Vestibular Diseases genetics, Vestibular Diseases pathology, Hearing Loss, Sensorineural genetics, Receptors, Purinergic P2X2 genetics

Abstract

P2RX2 encodes the P2X2 receptor, which is an adenosine triphosphate (ATP) gated (purinoreceptor) ion channel. P2RX2 c. 178G > T (p.V60L) mutation was previously identified in two unrelated Chinese families, as the cause of human DFNA41, a form of dominant, early-onset and progressive sensorineural hearing loss. We generated and characterized a knock-in mouse model based on human p.V60L mutation that recapitulates the human phenotype. Heterozygous KI mice started to exhibit hearing loss at 21-day-old and progressed to deafness by 6-month-old. Vestibular dysfunction was also observed in mutant mice. Abnormal morphology of the inner hair cells and ribbon synapses was progressively observed in KI animals suggesting that P2rx2 plays a role in the membrane spatial location of the ribbon synapses. These results suggest that P2rx2 is essential for acoustic information transfer, which can be the molecular mechanism related to hearing loss., (© The Author(s) 2021. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2021

3. Gene therapy restores auditory and vestibular function in a mouse model of Usher syndrome type 1c.

Author

Pan B, Askew C, Galvin A, Heman-Ackah S, Asai Y, Indzhykulian AA, Jodelka FM, Hastings ML, Lentz JJ, Vandenberghe LH, Holt JR, and Géléoc GS

Subjects

Animals, Cell Cycle Proteins, Cytoskeletal Proteins, Female, Gene Knock-In Techniques, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural genetics, Male, Mice, Mice, Inbred C57BL, Plasmids administration & dosage, Plasmids genetics, Recovery of Function genetics, Treatment Outcome, Vestibular Diseases diagnosis, Vestibular Diseases genetics, Carrier Proteins genetics, Genetic Therapy methods, Hearing Loss, Sensorineural therapy, Usher Syndromes genetics, Usher Syndromes therapy, Vestibular Diseases therapy

Abstract

Because there are currently no biological treatments for hearing loss, we sought to advance gene therapy approaches to treat genetic deafness. We focused on Usher syndrome, a devastating genetic disorder that causes blindness, balance disorders and profound deafness, and studied a knock-in mouse model, Ush1c c.216G>A, for Usher syndrome type IC (USH1C). As restoration of complex auditory and balance function is likely to require gene delivery systems that target auditory and vestibular sensory cells with high efficiency, we delivered wild-type Ush1c into the inner ear of Ush1c c.216G>A mice using a synthetic adeno-associated viral vector, Anc80L65, shown to transduce 80-90% of sensory hair cells. We demonstrate recovery of gene and protein expression, restoration of sensory cell function, rescue of complex auditory function and recovery of hearing and balance behavior to near wild-type levels. The data represent unprecedented recovery of inner ear function and suggest that biological therapies to treat deafness may be suitable for translation to humans with genetic inner ear disorders.

Published

2017

4. Novel COCH p.V123E Mutation, Causative of DFNA9 Sensorineural Hearing Loss and Vestibular Disorder, Shows Impaired Cochlin Post-Translational Cleavage and Secretion.

Author

Jung J, Kim HS, Lee MG, Yang EJ, and Choi JY

Subjects

Adult, Amino Acid Sequence, Cell Line, Extracellular Matrix Proteins chemistry, Extracellular Matrix Proteins metabolism, Genes, Dominant, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural metabolism, Hearing Tests, High-Throughput Nucleotide Sequencing, Humans, Magnetic Resonance Imaging, Middle Aged, Pedigree, Protein Multimerization, Protein Processing, Post-Translational, Protein Transport, Proteolysis, Tomography, X-Ray Computed, Vestibular Diseases diagnosis, Vestibular Diseases metabolism, Amino Acid Substitution, Codon, Extracellular Matrix Proteins genetics, Hearing Loss, Sensorineural genetics, Mutation, Vestibular Diseases genetics

Abstract

DFNA9 is an autosomal dominant disorder characterized by late-onset, non-syndromic hearing loss, and vestibular dysfunction. Mutations in the COCH (coagulation factor C homology) gene encoding cochlin are etiologically linked to DFNA9. Previous studies have shown that cochlin is cleaved by aggrecanase-1 during inflammation in the spleen and that the cleaved LCCL domain functions as an innate immune mediator. However, the physiological role of cochlin in the inner ear is not completely understood. Here, we report that cochlins containing DFNA9-linked mutations (p.P51S, p.V66G, p.G88E, p.I109T, p.W117R, p.V123E, and p.C162Y) demonstrate reduced cleavage by aggrecanase. Notably, in families affected with DFNA9, we found a novel COCH mutation causing p.V123E substitution in cochlin, which significantly reduced protein susceptibility to cleavage by aggrecanase (to about 20.5% of the wild-type). These results suggest that the impaired post-translational cleavage of cochlin mutants may be associated with pathological mechanisms underlying DFNA9-related sensorineural hearing loss., (© 2015 WILEY PERIODICALS, INC.)

Published

2015

5. Novel mutation in GRXCR1 at DFNB25 lead to progressive hearing loss and dizziness.

Author

Mori K, Miyanohara I, Moteki H, Nishio SY, Kurono Y, and Usami S

Subjects

Adult, Asian People genetics, DNA Mutational Analysis, Deafness genetics, Disease Progression, Female, Humans, Male, Pedigree, Dizziness genetics, Glutaredoxins genetics, Hearing Loss, Sensorineural genetics, Vestibular Diseases genetics

Abstract

Objective: We identified 2 patients in 1 family who had novel mutations in GRXCR1, which caused progressive hearing loss., Methods: One thousand one hundred twenty Japanese hearing loss patients with sensorineural hearing loss from unrelated families were enrolled in this study. Targeted genomic enrichment with massively parallel sequencing of all known nonsyndromic hearing loss genes was used to identify the genetic causes of hearing loss., Results: In this study, 2 affected individuals with compound heterozygous mutations-c.439C>T (p.R147C) and c.784C>T (p.R262X)-in GRXCR1 were identified. The proband had moderate to severe hearing loss and suffered from dizziness with bilateral canal paralysis., Conclusion: Our cases are the first identified in the Japanese population and are consistent with previously reported cases. The frequency of mutations in GRXCR1 seems to be extremely rare. This study underscores the importance of using comprehensive genetic testing for hearing loss. Furthermore, longitudinal audiologic assessment and precise vestibular testing are necessary for a better understanding of the mechanisms of hearing loss and vestibular dysfunction caused by GRXCR1 mutations., (© The Author(s) 2015.)

Published

2015

6. [Genotype--phenotype correlation limits in sensorineural hearing loss: case report of a three-year-old child with a bilateral cochleovestibular impairment and a molecular variant of the COCH gene].

Author

Montava M, Roman S, Sigaudy S, Marlin S, Nicollas R, and Triglia JM

Subjects

Child, Preschool, Humans, Male, Amino Acid Sequence, Extracellular Matrix Proteins genetics, Hearing Loss, Sensorineural genetics, Sequence Deletion genetics, Vestibular Diseases genetics

Abstract

Mutations of the COCH gene inherited in an autosomal dominant mode are responsible for late-onset cochleovestibular impairment on both sides. Our objective is to report the youngest patient (3 years) associating a molecular variant of the COCH gene and a cochleovestibular impairment on both sides. The clinical sequence has started with a vestibular dysfunction in a two-year-old child: recurrent rotatory dizziness during 12 months. At the age of 3, a sensorineural hearing loss on both sides has occured associated with spontaneous variation during 6 months. The lack of mutation of the connexin 26, connexin 30 and pendrin genes has reorientated the genetic investigation. A molecular variant of the COCH gene was found in the vWFA2 domain. It was an in-frame deletion predicting the synthesis of an abnormal protein in which 21 aminoacid were missing. Others family members with mutation were asymptomatics. In this isolated case report, the study was in favor of a non pathogenic molecular variant of the COCH gene. For all that, mutations of the COCH gene could be searched in progressive cochleovestibular dysfunctions on both sides in children, even without family affect.

Published

2012

7. An ENU-induced mutation of Cdh23 causes congenital hearing loss, but no vestibular dysfunction, in mice.

Author

Manji SS, Miller KA, Williams LH, Andreasen L, Siboe M, Rose E, Bahlo M, Kuiper M, and Dahl HH

Subjects

Alleles, Amino Acid Sequence, Animals, Cadherins chemistry, Cadherins genetics, DNA Mutational Analysis, Ethylnitrosourea pharmacology, Hearing, Hearing Loss, Sensorineural congenital, Humans, Mice, Mice, Transgenic, Models, Molecular, Molecular Sequence Data, Protein Conformation, Sequence Homology, Amino Acid, Vestibular Diseases genetics, Vestibule, Labyrinth pathology, Cadherins physiology, Hearing Loss, Sensorineural genetics, Mutation, Vestibular Diseases pathology

Abstract

Mutations in the human cadherin 23 (CDH23) gene cause deafness, neurosensory, autosomal recessive 12 (DFNB12) nonsyndromic hearing loss or Usher syndrome, type 1D (characterized by hearing impairment, vestibular dysfunction, and visual impairment). Reported waltzer mouse strains each harbor a Cdh23-null mutation and present with hearing loss and vestibular dysfunction. Two additional Cdh23 mouse mutants, salsa and erlong, each carry a homozygous Cdh23 missense mutation and have progressive hearing loss. We report the identification of a novel mouse strain, jera, with inherited hearing loss caused by an N-ethyl-N-nitrosourea-induced c.7079T>A mutation in the Cdh23 gene. The mutation generates a missense change, p.V2360E, in Cdh23. Affected mice have profound sensorineural deafness, with no vestibular dysfunction. The p.V2360E mutation is semidominant because heterozygous mice have milder and more progressive hearing loss in advanced age. The mutation affects a highly conserved Ca(2+)-binding motif in extracellular domain 22, thought to be important for Cdh23 structure and dimerization. Molecular modeling suggests that the Cdh23(V2360E/V2360E) mutation alters the structural conformation of the protein and affects Ca(2+)-binding properties. Similar to salsa mice, but in contrast to waltzer mice, hair bundle development is normal in jera and hearing loss appears to be due to the loss of tip links. Thus, jera is a novel mouse model for DFNB12., (Copyright © 2011 American Society for Investigative Pathology. Published by Elsevier Inc. All rights reserved.)

Published

2011

8. Hearing and vestibular deficits in the Coch(-/-) null mouse model: comparison to the Coch(G88E/G88E) mouse and to DFNA9 hearing and balance disorder.

Author

Jones SM, Robertson NG, Given S, Giersch AB, Liberman MC, and Morton CC

Subjects

Acoustic Stimulation, Age Factors, Aging, Analysis of Variance, Animals, Auditory Threshold, Cochlea metabolism, Cochlea pathology, Disease Models, Animal, Evoked Potentials, Auditory, Brain Stem, Extracellular Matrix Proteins, Gene Knock-In Techniques, Genotype, Hearing Loss, Sensorineural genetics, Hearing Loss, Sensorineural metabolism, Hearing Loss, Sensorineural pathology, Mice, Mice, Inbred CBA, Mice, Knockout, Phenotype, Proteins genetics, Vestibular Diseases genetics, Vestibular Diseases metabolism, Vestibular Diseases pathology, Vestibular Evoked Myogenic Potentials, Vestibule, Labyrinth metabolism, Cochlea physiopathology, Hearing, Hearing Loss, Sensorineural physiopathology, Postural Balance, Proteins metabolism, Vestibular Diseases physiopathology, Vestibule, Labyrinth physiopathology

Abstract

Two mouse models, the Coch(G88E/G88E) or "knock-in" and the Coch(-/-) or "knock-out" (Coch null), have been developed to study the human late-onset, progressive, sensorineural hearing loss and vestibular dysfunction known as DFNA9. This disorder results from missense and in-frame deletion mutations in COCH (coagulation factor C homology), encoding cochlin, the most abundantly detected protein in the inner ear. We have performed hearing and vestibular analyses by auditory brainstem response (ABR) and vestibular evoked potential (VsEP) testing of the Coch(-/-) and Coch(G88E/G88E) mouse models. Both Coch(-/-) and Coch(G88E/G88E) mice show substantially elevated ABRs at 21 months of age, but only at the highest frequency tested for the former and all frequencies for the latter. At 21 months, 9 of 11 Coch(-/-) mice and 4 of 8 Coch(G88E/G88E) mice have absent ABRs. Interestingly Coch(-/+) mice do not show hearing deficits, in contrast to Coch(G88E/+), which demonstrate elevated ABR thresholds similar to homozyotes. These results corroborate the DFNA9 autosomal dominant mode of inheritance, in addition to the observation that haploinsufficiency of Coch does not result in impaired hearing. Vestibular evoked potential (VsEP) thresholds were analyzed using a two factor ANOVA (Age X Genotype). Elevated VsEP thresholds are detected in Coch(-/-) mice at 13 and 21 months, the two ages tested, and as early as seven months in the Coch(G88E/G88E) mice. These results indicate that in both mouse models, vestibular function is compromised before cochlear function. Analysis and comparison of hearing and vestibular function in these two DFNA9 mouse models, where deficits occur at such an advanced age, provide insight into the pathology of DFNA9 and age-related hearing loss and vestibular dysfunction as well as an opportunity to investigate potential interventional therapies., (Copyright © 2010 Elsevier B.V. All rights reserved.)

Published

2011

9. Progressive sensorineural hearing loss and normal vestibular function in a Dutch DFNB7/11 family with a novel mutation in TMC1.

Author

de Heer AM, Collin RW, Huygen PL, Schraders M, Oostrik J, Rouwette M, Kunst HP, Kremer H, and Cremers CW

Subjects

Auditory Threshold, Base Sequence, Disease Progression, Female, Genotype, Hearing Loss, Sensorineural diagnosis, Humans, Male, Membrane Proteins chemistry, Molecular Sequence Data, Pedigree, Phenotype, Point Mutation, Polymorphism, Single Nucleotide, Protein Structure, Tertiary, RNA Splice Sites genetics, Severity of Illness Index, Vestibular Diseases diagnosis, Hearing Loss, Sensorineural genetics, Hearing Loss, Sensorineural physiopathology, Membrane Proteins genetics, Vestibular Diseases genetics, Vestibular Diseases physiopathology

Abstract

In a Dutch family with autosomal recessive hearing loss, genome-wide single-nucleotide polymorphism analysis mapped the genetic defect to the DFNB7/11 locus. A novel homozygous A-to-G change in the TMC1 gene was detected near the splice donor site of intron 19 (c.1763+3A→G) segregating with the hearing loss in this family. One of the 6 transmembrane domains and the actual TMC channel domain are predicted to be absent in the mutant protein. The sensorineural hearing impairment in this DFNB7/11 family has a postlingual onset. Audiometric analysis initially showed a steeply downward-sloping threshold configuration. The progressive phenotype in this family resembles the phenotype previously described for families with dominant TMC1 mutations (DFNA36) rather than that of families with recessive TMC1 mutations (DFNB7/11) which invariably cause severe-to-profound prelingual hearing impairment., (Copyright © 2010 S. Karger AG, Basel.)

Published

2011

10. [Phenotypic evaluation of patients with Pendred syndrome].

Author

Maciaszczyk K, Pniewska-Siark B, Gajewicz W, Stefańczyk L, Durko T, Lewiński A, and Pajor A

Subjects

Adolescent, Adult, Evoked Potentials, Auditory, Brain Stem, Female, Goiter genetics, Hearing Loss, Sensorineural genetics, Humans, Male, Middle Aged, Poland, Syndrome, Thyroid Gland physiopathology, Vestibular Diseases genetics, Vestibular Function Tests, Young Adult, Goiter diagnosis, Hearing Loss, Sensorineural diagnosis, Phenotype, Vestibular Diseases diagnosis

Abstract

Introduction: The Pendred syndrome (PS) is an autosomally recessively inherited disease. Its diagnosis requires identification of the classical triad of symptoms, including hypoacusis, thyroid goitre and iodine organification defect in the thyroid, which may lead to thyroid functional disorders of hypothyroidism. SP is accompanied by anatomical anomalies. The objective is the hearing and balance system evaluation and the analysis of the inner ear structure and also the assessment of the function and structure of thyroid gland., Material and Methods: For the research four families were qualified, 7 persons with PS, 12 persons altogether. In all the patients the anamnesis in the form of a questionnaire and laryngological examination were performed. It was followed by pure tone, speech and impedance audiometry and brainstem response testing as well. ENG was also conducted. Patients with hearing loss were subjected to magnetic resonance of temporal bone. For the whole group thyroid hormones levels and iodine organification in the thyroid identified in a test with potassium perchlorate were measured and also USG and scyntography were conducted., Results: In audiological examination in 3 cases deafness, in 2 cases profound hypoacusis and in 2 mild hypoacusis were recognised. In the group in 2 patients the hypoacusis was of a mixed type. In radiological assessment the labirynth showed anatomical anomalies in the form of enlargement of the vestibular aqueduct and the endolyphatic sac, yet in 3 patients the anomalies also concerned the structure of cochlear and semicircular canals. Endocrine examination showed hypothyroidism in 5, its subclinical form in 1, diffuse thyroid goitre in 4 and nodular thyroid goiter in 2 cases., Conclusions: A complex clinical evaluation: endocrine and audiological, together with radiological diagnostic imaging, supported by molecular studies of SLC26A4 gene, are the procedures, necessary for complete and accurate diagnosis of PS and EVAS.

Published

2008

11. Truncating mutation of the DFNB59 gene causes cochlear hearing impairment and central vestibular dysfunction.

Author

Ebermann I, Walger M, Scholl HP, Charbel Issa P, Lüke C, Nürnberg G, Lang-Roth R, Becker C, Nürnberg P, and Bolz HJ

Subjects

Audiometry, Child, Child, Preschool, Chromosome Mapping, Consanguinity, DNA Mutational Analysis, Female, Genes, Recessive, Hair Cells, Auditory physiopathology, Haplotypes, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural diagnosis, Homozygote, Humans, Male, Morocco, Pedigree, RNA Splice Sites genetics, Retina pathology, Retinal Degeneration complications, Retinal Degeneration diagnosis, Sequence Deletion, Siblings, Vestibular Diseases complications, Vestibular Diseases diagnosis, c-Mer Tyrosine Kinase, Chromosomes, Human, Pair 2 genetics, Hearing Loss, Sensorineural genetics, Mutation, Nerve Tissue Proteins genetics, Proto-Oncogene Proteins genetics, Receptor Protein-Tyrosine Kinases genetics, Retinal Degeneration genetics, Vestibular Diseases genetics

Abstract

We have identified a consanguineous family from Morocco segregating autosomal recessive congenital progressive hearing loss (ARNSHL) and retinal degeneration. Detailed clinical investigation of the six siblings revealed combined severe cone-rod dystrophy (CORD) and severe/profound hearing impairment in two of them, while there is isolated CORD in three and nonsyndromic profound hearing loss in one. We therefore assumed a partial overlap of two nonsyndromic autosomal recessive conditions instead of a monogenic syndrome and performed genomewide linkage analysis. The disease loci were mapped to chromosome 2q31.1-2q32.1 for ARNSHL and to 2q13-2q14.1 for CORD, respectively. The retinal phenotype was shown to be due to homozygosity for a novel splice site mutation, c.2189+1G>T, in the retinitis pigmentosa gene MERTK. The ARNSHL interval comprised the DFNB59 locus. The DFNB59 gene has been identified recently, and two missense mutations (p.R183W and p.T54I) have been shown to cause auditory neuropathy in both humans and transgenic mice. Mutation screening in the DFNB59 gene in our family revealed homozygosity for a 1-bp insertion in exon 2 (c.113_114insT), predicting a truncated protein of 47 amino acids, in all three hearing impaired subjects. This is the first description of biallelic putative loss-of-function of the DFNB59 gene. Detailed audiological investigation clearly indicated hair cell dysfunction and, in contrast to cases reported previously, excluded auditory neuropathy. We show that besides otoferlin (OTOF), DFNB59 is the second known gene in which mutations can result in these two distinct forms of hearing impairment. Moreover, all patients in our family with homozygosity for the DFNB59 mutation display central vestibular dysfunction., ((c) 2007 Wiley-Liss, Inc.)

Published

2007

12. Vertical corneal striae in families with autosomal dominant hearing loss: DFNA9/COCH.

Author

Bischoff AM, Pauw RJ, Huygen PL, Aandekerk AL, Kremer H, Cremers CW, and Cruysberg JR

Subjects

Adult, Cochlear Diseases genetics, Cornea pathology, Corneal Diseases diagnosis, Extracellular Matrix Proteins, Family, Female, Genes, Dominant, Haplotypes, Heterozygote, Humans, Intraocular Pressure, Male, Middle Aged, Pedigree, Prospective Studies, Vestibular Diseases genetics, Visual Acuity, Corneal Diseases genetics, Deafness genetics, Hearing Loss, Sensorineural genetics, Point Mutation, Proteins genetics

Abstract

Purpose: Investigation of a possible association between vertical corneal striae and mutations in the COCH gene, observed in four DFNA9 families with autosomal dominant hearing loss and vestibular dysfunction., Design: Prospective case series., Methods: Ophthalmologic examinations with photography of the cornea after instillation of fluorescein were performed in 98 family members with 61 mutation carriers of four DFNA9 families at the Radboud University Nijmegen Medical Centre. Families 1 and 2 harbor the Pro51Ser mutation, and families 3 and 4 harbor the Gly88Glu and the Gly87Trp mutation, respectively. Statistical analysis was performed to find an association between the vertical corneal striae and the COCH mutation for each family and to test whether the four families were different in this respect., Results: The vertical corneal striae were exclusively visible after instillation of fluorescein. They caused minor problems, as dry eye symptoms, and were not present in the general Dutch ophthalmologic population. The striae were present from an age of 47 years in 32 individuals, of whom 27 individuals had a COCH mutation. Statistical analysis on the striae and the COCH mutations showed a significant association in families 1, 2, and 3 (P = .0006), but not in family 4 (P = .63)., Conclusions: Data analysis demonstrated a significant association between vertical corneal striae and the Pro51Ser and Gly88Glu mutations in the COCH gene in DFNA9 families 1, 2, and 3 with cochleovestibular dysfunction. Our findings suggest that the vertical corneal striae and cochleovestibular dysfunction may be caused by the same COCH mutations.

Published

2007

13. Phenotype description of a novel DFNA9/COCH mutation, I109T.

Author

Pauw RJ, Huygen PL, Collin RW, Cruysberg JR, Hoefsloot LH, Kremer H, and Cremers CW

Subjects

Adult, Aged, Audiometry, Pure-Tone, Auditory Threshold, DNA Mutational Analysis, Extracellular Matrix Proteins, Female, Heterozygote, Humans, Linear Models, Male, Middle Aged, Netherlands, Pedigree, Phenotype, Hearing Loss, Sensorineural genetics, Mutation, Proteins genetics, Vestibular Diseases genetics

Abstract

Objectives: This is a report of the audiological and vestibular characteristics of a Dutch DFNA9 family with a novel mutation, I109T, in the LCCL domain of COCH., Methods: From the family with the novel I109T COCH mutation, audiometric data were collected and analyzed longitudinally. Results were compared to those obtained in previously identified P51 S, G88E, and G87W COCH mutation carriers. Special attention was also given to a comparison of age-related features such as progressive hearing loss and vestibular impairment., Results: A novel mutation (I109T) in COCH segregates with hearing impairment and vestibular dysfunction in the present family. Pure tone thresholds, phoneme recognition scores, and vestibular responses of the I109T mutation carriers were essentially similar to those previously established in P51S, G87W, and G88E mutation carriers. Deterioration of hearing in the I109T mutation carriers started at 43 years of age, and vestibular function deteriorated at least 7 years later., Conclusions: The phenotype associated with the novel COCH (I109T) mutation is largely similar to that associated with P51S and G88E mutation carriers. However, subtle differences in terms of onset age and rate of progression seem to exist.

Published

2007

14. Good speech recognition and quality-of-life scores after cochlear implantation in patients with DFNA9.

Author

Vermeire K, Brokx JP, Wuyts FL, Cochet E, Hofkens A, De Bodt M, and Van de Heyning PH

Subjects

Adult, Aged, Aged, 80 and over, Auditory Threshold, Case-Control Studies, Cross-Sectional Studies, Extracellular Matrix Proteins, Female, Hearing Loss, Sensorineural complications, Humans, Male, Middle Aged, Prospective Studies, Speech Reception Threshold Test, Treatment Outcome, Vestibular Diseases complications, Vestibular Diseases genetics, Cochlear Implants, Hearing Loss, Sensorineural genetics, Hearing Loss, Sensorineural rehabilitation, Proteins genetics, Quality of Life, Speech Perception

Abstract

Objective: To compare audiometric and quality-of-life results in DFNA 9 patients who received a cochlear implant with cochlear implant patients with adult-onset progressive sensorineural hearing loss., Study Design: Prospective comparative design; results were collected cross-sectionally., Setting: Tertiary referral center., Patients: Eleven DFNA 9 patients were included in the study as well as a comparative group of 39 post-lingually deafened cochlear implant subjects with adult-onset progressive sensorineural hearing loss., Interventions: All patients received a cochlear implant. Subjects were implanted with either the Nucleus 24 M/RCS or Med-el Combi 40+ cochlear implant systems implementing the SPEAK, ACE, or CIS+ coding strategies., Mean Outcome Measures: Speech recognition was determined by means of phonetically balanced monosyllabic word lists. The Hearing Handicap Inventory for Adults, the Glasgow Benefit Inventory, and the Scale for the Prediction of Hearing Disability in Sensorineural Hearing Loss were used to quantify the quality of life., Results: The results show that the speech perception and the quality of life of the DFNA 9 patients do not differ significantly from the control group (p=0.179; p=0.56)., Conclusion: In spite of the fact that DFNA 9 is a disease that is known to involve cochlear dendrites, cochlear implantation is a good option for treatment of deafness in DFNA 9.

Published

2006

15. Identification of a novel mutation in the myosin VIIA motor domain in a family with autosomal dominant hearing loss (DFNA11).

Author

Di Leva F, D'Adamo P, Cubellis MV, D'Eustacchio A, Errichiello M, Saulino C, Auletta G, Giannini P, Donaudy F, Ciccodicola A, Gasparini P, Franzè A, and Marciano E

Subjects

Amino Acid Sequence, Auditory Threshold, Base Sequence, Chromosome Mapping, Dyneins chemistry, Female, Genotype, Humans, Male, Models, Molecular, Molecular Sequence Data, Myosin VIIa, Myosins chemistry, Pedigree, Vestibular Diseases complications, Vestibular Diseases genetics, Chromosome Disorders genetics, Dyneins genetics, Hearing Loss, Sensorineural genetics, Mutation, Missense genetics, Myosins genetics

Abstract

We ascertained a large Italian family with an autosomal dominant form of non-syndromic sensorineural hearing loss with vestibular involvement. A genome-wide scan found linkage to locus DFNA11. Sequencing of the MYO7A gene in the linked region identified a new missense mutation resulting in an Ala230Val change in the motor domain of the myosin VIIA. Myosin VIIA has already been implicated in several forms of deafness, but this is the third mutation causing a dominant form of deafness, located in the myosin VIIA motor domain in a region never involved in hearing loss until now. A modelled protein structure of myosin VII motor domain provides evidence for a significant functional effect of this missense mutation., (Copyright (c) 2006 S. Karger AG, Basel.)

Published

2006

16. [From gene to disease; a progressive cochlear-vestibular dysfunction with onset in middle-age (DFNA9)].

Author

Cremers CW, Kemperman MH, Bom SJ, Huygen PL, Verhagen WI, and Kremer JM

Subjects

Adult, Age of Onset, DNA Mutational Analysis, Extracellular Matrix Proteins, Humans, Pedigree, Hearing Loss, Sensorineural genetics, Mutation, Proteins genetics, Vestibular Diseases genetics

Abstract

DFNA9 is an autosomal dominant genetic inner-ear hearing impairment that starts to show itself in the 3rd and 4th decades of life. This hearing impairment may be of a different degree of severity in each ear. Progression of hearing loss is about 3 dB/year. In about one in three patients severe vestibular symptoms similar to those in Ménière's disease are present as a result of a progressive impairment of the vestibular system. Several mutations were found in the COCH-gene on chromosome 14. There are indications that some of the mutations disrupt the folding of the cochlin protein, an important component of the extracellular matrix in the inner ear. DNA-diagnostics confirming the diagnosis ofDFNA9 are possible.

Published

2005

17. Large vestibular aqueduct syndrome: audiological, radiological, clinical, and genetic features.

Author

Berrettini S, Forli F, Bogazzi F, Neri E, Salvatori L, Casani AP, and Franceschini SS

Subjects

Acoustic Impedance Tests, Adolescent, Adult, Audiometry, Child, Child, Preschool, DNA Mutational Analysis, Evoked Potentials, Auditory, Brain Stem physiology, Female, Hearing Loss, Sensorineural genetics, Humans, Male, Middle Aged, Syndrome, Vestibular Diseases genetics, Vestibular Function Tests, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural physiopathology, Vestibular Aqueduct pathology, Vestibular Diseases diagnosis, Vestibular Diseases physiopathology

Abstract

Purpose: The aim of this study was to analyze the clinical, audiological, radiological, and genetic features of a group of patients affected with large vestibular aqueduct syndrome., Materials and Methods: Seventeen patients affected with large vestibular aqueduct syndrome (LVAS), diagnosed by means of high-resolution magnetic resonance imaging of the inner ear, with 3-dimensional reconstructions of the labyrinth and by high-resolution spiral computed tomography of the temporal bone, performed only on the oldest patients, have been submitted to a complete audiological evaluation, a thyroid functional and ultrasonographic study, and a molecular study of the PDS gene., Results: The clinical presentation of LVAS was very variable in our group of patients. The enlarged vestibular aqueduct was bilateral in 15 cases and unilateral in 2; it was the only malformation of the labyrinth in 12 patients, whereas it was associated with other inner ear anomalies in the other 5. The hearing loss was very variable in degree (from mild to profound), age at onset, and progression. Moreover, among the 17 patients, 10 were clinically affected by Pendred's syndrome (PS), 3 by distal renal tubular acidosis associated with large vestibular aqueduct, whereas in 3 patients the large vestibular aqueduct was not syndromal. Finally, we identified mutations in the PDS gene in 5 of 10 patients with PS., Conclusions: Our data underscore the frequent role of the large vestibular aqueduct syndrome in the pathogenesis of sensorineural hearing loss and the overall wide variability in its audiological features. It is also highlighted that LVAS is often part of some syndromal diseases, most of which are PS, which is often misdiagnosed because of the varying degree of thyroid symptoms. This study also underscores the possible role of hydro-electrolyte and acid-base endolymphatic fluid disorders in the pathogenesis of enlarged vestibular aqueduct syndrome.

Published

2005

18. [Enlarged vestibular aqueduct syndrome: report of 3 cases and literature review].

Author

Pinto JA, Mello CF Jr, Marqui AC, Perfeito DJ, Ferreira RD, and Silva RH

Subjects

Adolescent, Adult, Age Factors, Child, Cochlear Implantation, Diagnosis, Differential, Female, Hearing Loss, Sensorineural genetics, Hearing Loss, Sensorineural therapy, Humans, Male, Syndrome, Tomography, X-Ray Computed, Vestibular Diseases genetics, Vestibular Diseases therapy, Hearing Loss, Sensorineural diagnosis, Vestibular Aqueduct diagnostic imaging, Vestibular Diseases diagnosis

Abstract

The Enlarged Vestibular Aqueduct Syndrome is characterized by a widening of the vestibular aqueduct, associated with sensorineural hearing loss, or sometimes with mixed hearing loss, which may be congenital or acquired during childhood. The sensorineural hearing loss may be classified into mild, moderate and severe, associated with sudden periods of improvement or aggravation. The enlargement of the vestibular aqueduct is the most common inner ear anomaly. This syndrome is admitted as a result of a genetic abnormality of the vestibular aqueduct development, previous to the fifth week of gestation. The incidence of this syndrome ranges from 1% to 1.3%, with the possibility of getting up to 7%, depending on the examined population. The aim of this study was to analyze three cases of LVAS seen at the Otorhinolaryngology and Radiology Department of Sao Camilo Hospital - Sao Paulo. Two of these three cases were of brothers, from the same mother but from different fathers. Two were male and one was female and the ages ranged from 9 to 30 years old. The diagnosed method of election was CT, Computerized Tomography of the temporal bones. The procedure for the cases was that of observation, with exception for those of cranial traumatisms, barotraumas and, when necessary, the use of auditive prosthesis.

Published

2005

19. Mutation screening of USH3 gene (clarin-1) in Spanish patients with Usher syndrome: low prevalence and phenotypic variability.

Author

Aller E, Jaijo T, Oltra S, Alió J, Galán F, Nájera C, Beneyto M, and Millán JM

Subjects

Adolescent, Adult, Child, Genetic Testing, Humans, Male, Mutation, Phenotype, Spain, Syndrome, Hearing Loss, Sensorineural genetics, Membrane Proteins genetics, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

Usher syndrome type III is an autosomal recessive disorder clinically characterized by the association of retinitis pigmentosa (RP), variable presence of vestibular dysfunction and progressive hearing loss, being the progression of the hearing impairment the critical parameter classically used to distinguish this form from Usher syndrome type I and Usher syndrome type II. Usher syndrome type III clinical subtype is the rarest form of Usher syndrome in Spain, accounting only for 6% of all Usher syndrome Spanish cases. The gene responsible for Usher syndrome type III is named clarin-1 and it is thought to be involved in hair cell and photoreceptor cell synapses. Here, we report a screening for mutations in clarin-1 gene among our series of Usher syndrome Spanish patients. Clarin-1 has been found to be responsible for the disease in only two families: the first one is a previously reported family homozygous for Y63X mutation and the second one, described here, is homozygous for C40G. This accounts for 1.7% of Usher syndrome Spanish families. It is noticeable that, whereas C40G family is clinically compatible with Usher syndrome type III due to the progression of the hearing loss, Y63X family could be diagnosed as Usher syndrome type I because the hearing impairment is profound and stable. Thus, we consider that the progression of hearing loss is not the definitive key parameter to distinguish Usher syndrome type III from Usher syndrome type I and Usher syndrome type II.

Published

2004

20. Genetic analysis of a four generation Indian family with Usher syndrome: a novel insertion mutation in MYO7A.

Author

Kumar A, Babu M, Kimberling WJ, and Venkatesh CP

Subjects

Adolescent, Adult, Amino Acid Sequence, Base Sequence, Child, DNA Mutational Analysis, Female, Genotype, Hearing Loss, Sensorineural ethnology, Humans, India ethnology, Male, Molecular Sequence Data, Myosin VIIa, Pedigree, Polymerase Chain Reaction, Polymorphism, Single-Stranded Conformational, Retinitis Pigmentosa ethnology, Syndrome, Vestibular Diseases ethnology, Dyneins genetics, Hearing Loss, Sensorineural genetics, Mutation, Missense, Myosins genetics, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

Purpose: Usher syndrome (USH) is a rare autosomal recessive disorder characterized by deafness and retinitis pigmentosa. The purpose of this study was to determine the genetic cause of USH in a four generation Indian family., Methods: Peripheral blood samples were collected from individuals for genomic DNA isolation. To determine the linkage of this family to known USH loci, microsatellite markers were selected from the candidate regions of known loci and used to genotype the family. Exon specific intronic primers for the MYO7A gene were used to amplify DNA samples from one affected individual from the family. PCR products were subsequently sequenced to detect mutation. PCR-SSCP analysis was used to determine if the mutation segregated with the disease in the family and was not present in 50 control individuals., Results: All affected individuals had a classic USH type I (USH1) phenotype which included deafness, vestibular dysfunction and retinitis pigmentosa. Pedigree analysis suggested an autosomal recessive mode of inheritance of USH in the family. Haplotype analysis suggested linkage of this family to the USH1B locus on chromosome 11q. DNA sequence analysis of the entire coding region of the MYO7A gene showed a novel insertion mutation c.2663_2664insA in a homozygous state in all affected individuals, resulting in truncation of MYO7A protein., Conclusions: This is the first study from India which reports a novel MYO7A insertion mutation in a four generation USH family. The mutation is predicted to produce a truncated MYO7A protein. With the novel mutation reported here, the total number of USH causing mutations in the MYO7A gene described to date reaches to 75.

Published

2004

21. Genetic heterogeneity in Usher syndrome.

Author

Keats BJ and Savas S

Subjects

Adaptor Proteins, Signal Transducing, Ankyrin Repeat, Cadherin Related Proteins, Cell Cycle Proteins, Cytoskeletal Proteins, Diagnosis, Differential, Genetic Testing, Humans, Syndrome, Vestibular Diseases genetics, Cadherins genetics, Carrier Proteins genetics, Hearing Loss, Sensorineural genetics, Nerve Tissue Proteins genetics, Protein Precursors genetics, Retinitis Pigmentosa genetics

Abstract

Mutations in seven different genes have been associated with Usher syndrome, and an additional four loci have been mapped. The identified genes encode myosin VIIa, harmonin (a PDZ-domain protein), cadherin 23, protocadherin 15, sans (a scaffold-like protein), usherin and clarin. Three clinical types of Usher syndrome have been described: USH1 patients have severe to profound congenital hearing loss, vestibular dysfunction, and retinal degeneration beginning in childhood, those with USH2 have moderate to severe congenital hearing loss, normal vestibular function, and later onset of retinitis pigmentosa, and USH3 patients have progressive hearing loss, which distinguishes them from the other two types. The shaker-1, waltzer, Ames waltzer, and Jackson shaker mice provide murine models for four of the genetic forms of Usher syndrome. Ongoing studies are enabling early diagnosis of Usher syndrome in children who present with hearing loss, thus providing time to prepare for the onset of visual loss., (Copyright 2004 Wiley-Liss, Inc.)

Published

2004

22. Variable clinical features in patients with CDH23 mutations (USH1D-DFNB12).

Author

Pennings RJ, Topsakal V, Astuto L, de Brouwer AP, Wagenaar M, Huygen PL, Kimberling WJ, Deutman AF, Kremer H, and Cremers CW

Subjects

Adult, Audiometry, Pure-Tone, Cadherin Related Proteins, Consanguinity, Diagnostic Techniques, Ophthalmological, Electronystagmography, Female, Genotype, Hearing Loss, Sensorineural diagnosis, Humans, Linear Models, Male, Middle Aged, Pedigree, Reflex, Vestibulo-Ocular, Syndrome, Cadherins genetics, Hearing Loss, Sensorineural genetics, Mutation, Missense, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

Objective: To describe the findings of audiovestibular and ophthalmologic examinations in four families with mutations in the CDH23 gene., Study Design: Family study., Setting: Tertiary referral center., Patients: Four DFNB12 patients from a large consanguineous Dutch family and six patients from three different Usher syndrome Type ID families were examined. All were identified by at least one pathogenic mutation in the CDH23 gene., Methods: Audiovestibular examinations consisted of standard pure-tone audiometry, vestibulo-ocular reflex, optokinetic nystagmus, and in some cases the cervico-ocular reflex. Linear regression analysis was used to evaluate progression of hearing impairment, and the degree of hearing impairment of DFNB12 was compared with that found for USH1D. Ophthalmologic examinations consisted of best-corrected visual acuity, Goldmann perimetry, slit-lamp examinations, color vision testing, dark adaptation, electroretinography, electro-oculography, funduscopy and photography of the retina, and sometimes fluorescein angiography., Results: The USH1D patients had significantly worse hearing impairment than the DFNB12 patients. The DFNB12 patients, identified by missense mutations in CDH23, had normal retinal and vestibular function. All USH1D patients had splice-site mutations in CDH23 and a typical Usher syndrome Type I phenotype. One DFNB12 patient had slightly abnormal yellowish flecks in the posterior poles of both eyes., Conclusion: Recessive missense mutations in CDH23 lead to a milder phenotype (DFNB12) than splice-site mutations (USH1D); however, abnormal bilateral flecks, suggestive for lipofuscin accumulation, can be observed in DFNB12 patients.

Published

2004

23. Clinical and genetic linkage analysis of a large Venezuelan kindred with Usher syndrome.

Author

Keogh IJ, Godinho RN, Wu TP, Diaz de Palacios AM, Palacios N, Bello de Alford M, De Almada MI, MarPalacios N, Vazquez A, Mattei R, Seidman C, Seidman J, and Eavey RD

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Chromosome Mapping, Congenital Abnormalities epidemiology, Consanguinity, Dyneins genetics, Female, Hearing Loss, Sensorineural epidemiology, Humans, Infant, Lod Score, Male, Middle Aged, Myosin VIIa, Myosins genetics, Pedigree, Polymerase Chain Reaction, Retinitis Pigmentosa epidemiology, Socioeconomic Factors, Syndrome, Venezuela epidemiology, Vestibular Diseases epidemiology, Vision Disorders epidemiology, Congenital Abnormalities genetics, Hearing Loss, Sensorineural genetics, Retinitis Pigmentosa genetics, Vestibular Diseases genetics, Vision Disorders genetics

Abstract

Objective: To undertake a comprehensive investigation into the very high incidence of congenital deafness on the Macano peninsula of Margarita Island, Venezuela., Methods: Numerous visits were made to the isolated island community over a 4-year-period. During these visits, it became apparent that a significant number of individuals complained of problems with hearing and vision. Socioeconomic assessments, family pedigrees and clinical histories were recorded on standard questionnaires. All individuals underwent thorough otolaryngologic and ophthalmologic examinations. Twenty milliliters of peripheral venous blood was obtained from each participant. A genome-wide linkage analysis study was performed. Polymorphic microsatellite markers were amplified by polymerase chain reaction and separated on polyacrylamide gels. An ABI 377XL sequencer was used to separate fragments and LOD scores were calculated by using published software., Results: Twenty-four families were identified, comprising 329 individuals, age range 1-80 years, including 184 children. All families were categorized in the lower two (least affluent) socioeconomic categories. A high incidence of consanguinity was detected. Fifteen individuals (11 adults, 4 children) had profound congenital sensorineural hearing loss, vestibular areflexia and retinitis pigmentosa. A maximum LOD score of 6.76 (Linkage >3.0), between markers D11s4186 and D11s911, confirmed linkage to chromosome 11q13.5. The gene myosin VIIA (MYO7A) was confirmed in the interval. Clinical and genetic findings are consistent with a diagnosis of Usher syndrome 1B for those with hearing and vision problems., Conclusions: We report 15 Usher syndrome 1B individuals from a newly detected Latin American socio-demographic origin, with a very high prevalence of 76 per 100,000 population.

Published

2004

24. Genetic homogeneity and phenotypic variability among Ashkenazi Jews with Usher syndrome type III.

Author

Ness SL, Ben-Yosef T, Bar-Lev A, Madeo AC, Brewer CC, Avraham KB, Kornreich R, Desnick RJ, Willner JP, Friedman TB, and Griffith AJ

Subjects

Adult, Aged, Europe, Eastern ethnology, Female, Genotype, Homozygote, Humans, Male, Membrane Proteins genetics, Middle Aged, Mutation, Pedigree, Phenotype, Syndrome, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural ethnology, Hearing Loss, Sensorineural genetics, Jews genetics, Retinitis Pigmentosa diagnosis, Retinitis Pigmentosa ethnology, Retinitis Pigmentosa genetics, Vestibular Diseases diagnosis, Vestibular Diseases ethnology, Vestibular Diseases genetics

Published

2003

25. Mutations in the COCH gene are a frequent cause of autosomal dominant progressive cochleo-vestibular dysfunction, but not of Meniere's disease.

Author

Usami S, Takahashi K, Yuge I, Ohtsuka A, Namba A, Abe S, Fransen E, Patthy L, Otting G, and Van Camp G

Subjects

Adult, DNA Mutational Analysis, Deafness genetics, Exons, Extracellular Matrix Proteins, Genes, Dominant, Humans, Japan, Middle Aged, Models, Molecular, Pedigree, Point Mutation, Protein Binding, Protein Structure, Tertiary, Vertigo genetics, Hearing Loss, Sensorineural genetics, Meniere Disease genetics, Mutation, Proteins genetics, Vestibular Diseases genetics

Abstract

The COCH gene is the only gene identified in man that causes autosomal dominantly inherited hearing loss associated with vestibular dysfunction. The condition is rare and only five mutations have been reported worldwide. All affected families showed a similar progressive hearing loss and vestibular dysfunction. Since Meniere's disease-like symptoms have also been described in some families, it was suggested that COCH mutations might be present in some patients diagnosed with Meniere's disease. In this study, using a Japanese population, we performed a COCH mutation analysis in 23 patients from independent families with autosomal dominant hearing impairment, four of whom reported vestibular symptoms, and also in 20 Meniere's patients. While a new point mutation, A119 T, was found in a patient with autosomal dominant hearing loss and vestibular symptoms, no mutations were found in the Meniere's patients. Like all other previously identified COCH mutations, the mutation identified here is a missense mutation located in the FCH domain of the protein. The current mutation is located in close spatial proximity to W117, in which a mutation (W117R) had previously been associated with autosomal dominant hearing loss. Model building suggests that, like the W117R mutation, the A119 T mutation does not affect the structural integrity of the FCH domain, but may interfere with the interaction with a yet unknown binding partner. We conclude that mutations in the COCH gene are responsible for a significant fraction of patients with autosomal dominantly inherited hearing loss accompanied by vestibular symptoms, but not for dominant hearing loss without vestibular dysfunction, or sporadic Meniere's disease.

Published

2003

26. Progressive late-onset sensorineural hearing loss and vestibular impairment with vertigo (DFNA9/COCH): longitudinal analyses in a belgian family.

Author

Lemaire FX, Feenstra L, Huygen PL, Fransen E, Devriendt K, Van Camp G, Vantrappen G, Cremers CW, Wackym PA, and Koss JC

Subjects

Adult, Aged, Aged, 80 and over, Audiometry, Pure-Tone, Belgium, Chromosome Aberrations, Chromosome Mapping, DNA Mutational Analysis, Deafness diagnosis, Disease Progression, Extracellular Matrix Proteins, Female, Genes, Dominant, Genetic Carrier Screening, Hearing Loss, Sensorineural diagnosis, Humans, Karyotyping, Longitudinal Studies, Male, Meniere Disease diagnosis, Middle Aged, Presbycusis diagnosis, Speech Reception Threshold Test, Vestibular Diseases diagnosis, Vestibular Function Tests, Deafness genetics, Hearing Loss, Sensorineural genetics, Meniere Disease genetics, Presbycusis genetics, Proteins genetics, Vestibular Diseases genetics

Abstract

Objective: To evaluate audiometric and vestibular signs and symptoms in a new DFNA9 family., Setting: Tertiary referral centers., Methods: A multigeneration Belgian family with late-onset progressive sensorineural hearing loss and concomitant ves-tibular impairment with an autosomal dominant pattern of inheritance underwent clinical and genetic evaluation. Medical history was recorded. Blood samples were taken for genetic linkage and mutation analyses. Pure-tone audiometry, speech audiometry and vestibular examinations were performed. Onset and progression in hearing impairment were evaluated with linear regression analysis of longitudinal threshold-on-age data., Results: Linkage to DFNA9 was confirmed and mutation analysis revealed a P51S mutation in the COCH gene. Several patients had a Ménière's-like presentation. All patients developed late-onset progressive sensorineural hearing loss eventually leading to severe deafness and vestibular failure.

Published

2003

27. Subcellular localisation, secretion, and post-translational processing of normal cochlin, and of mutants causing the sensorineural deafness and vestibular disorder, DFNA9.

Author

Robertson NG, Hamaker SA, Patriub V, Aster JC, and Morton CC

Subjects

3T3 Cells, Animals, Blotting, Western, COS Cells, Cell Line, Extracellular Matrix Proteins, Glycosylation, Humans, Immunohistochemistry, Mice, Mutation, Mutation, Missense, Plasmids genetics, Proteins genetics, Transfection, Hearing Loss, Sensorineural genetics, Protein Processing, Post-Translational, Proteins metabolism, Vestibular Diseases genetics

Abstract

Five missense mutations in the FCH/LCCL domain of the COCH gene, encoding the protein cochlin, are pathogenic for the autosomal dominant hearing loss and vestibular dysfunction disorder, DFNA9. To date, the function of cochlin and the mechanism of pathogenesis of the mutations are unknown. We have used the biological system of transient transfections of the entire protein coding region of COCH into several mammalian cell lines, to investigate various functional properties of cochlin. By western blot analysis of lysates prepared from transfected cells, we show that cochlin is a secreted protein. Immunocytochemistry shows concentrated localisation of cochlin in perinuclear structures consistent with the Golgi apparatus and endoplasmic reticulum, showing intracellular passage through these secretory compartments. We detected that cochlin is proteolytically cleaved between the FCH/LCCL domain and the downstream vWFA domains, resulting in a smaller cochlin isoform of approximately 50 kDa. Interestingly, this isoform lacks the entire mutation bearing FCH/LCCL domain. We have also shown that cochlin is N-glycosylated in its mature secreted form. Previous studies of the FCH/LCCL domain alone, expressed in bacteria, have demonstrated that three of four DFNA9 mutations cause misfolding of this domain. Characteristic eosinophilic deposits in DFNA9 affected inner ear structures could be the result of aberrant folding, secretion, or solubility of mutated cochlins, as in certain other pathological states in which misfolded proteins accumulate and aggregate causing toxicity. To examine the biological consequences of cochlin misfolding, we made separate constructs with three of the DFNA9 mutations and performed parallel studies of the mutated and wild type cochlins. We detected that mutated cochlins are not retained intracellularly, and are able to be secreted adequately by the cells, through the Golgi/ER secretory pathway, and also undergo proteolytic cleavage and glycosylation. These results suggest that DFNA9 mutations may manifest deleterious effects beyond the point of secretion, in the unique environment of the extracellular matrix of the inner ear by disrupting cochlin function or interfering with protein-protein interactions involving the FCH/LCCL domain. It is also possible that the mutations may result in aggregation of cochlin in vivo over a longer time course, as supported by the late onset and progressive nature of this disorder.

Published

2003

28. [From gene to disease; genetic causes of hearing loss and visual impairment sometimes accompanied by vestibular problems (Usher syndrome)].

Author

Pennings RJ, Kremer H, Deutman AF, Kimberling WJ, and Cremers CW

Subjects

Genes, Recessive, Humans, Mutation, Pedigree, Syndrome, Hearing Loss, Sensorineural genetics, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

Usher syndrome is an autosomal recessively inherited disease, characterised by sensorineural hearing loss, tapetoretinal degeneration and in some cases vestibular problems. Based on the clinical heterogeneity, the disease can be classified into three clinical types (I, II and III), which have their own genetic subtypes (Usher 1A-Usher IG, Usher 2A-Usher 2C and Usher 3). The majority of the Usher type I cases are caused by mutations in the MYO7A gene (Usher 1B) while mutations in the USH2A gene (Usher 2A) are the cause of most cases of type II. Usher syndrome type III, caused by mutations in the USH3 gene, is frequently seen only in Finland.

Published

2002

29. Hearing impairment in Usher's syndrome.

Author

Pennings RJ, Wagenaar M, van Aarem A, Huygen PL, Kimberling WJ, and Cremers CW

Subjects

Audiometry, Extracellular Matrix Proteins genetics, Genotype, Hearing Loss, Sensorineural classification, Hearing Loss, Sensorineural diagnosis, Humans, Mutation, Phenotype, Retinitis Pigmentosa genetics, Syndrome, Vestibular Diseases genetics, Hearing Loss, Sensorineural genetics

Published

2002

30. Clinical presentation of DFNA11 (MYO7A).

Author

Tamagawa Y, Ishikawa K, Ishikawa K, Ishida T, Kitamura K, Makino S, Tsuru T, and Ichimura K

Subjects

Adolescent, Adult, Age of Onset, Aged, Auditory Threshold, Child, Disease Progression, Dyneins, Female, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural diagnosis, Humans, Male, Middle Aged, Mutation, Myosin VIIa, Pedigree, Vestibular Diseases complications, Vestibular Diseases genetics, Hearing Loss, Sensorineural genetics, Myosins genetics, Phenotype

Published

2002

31. DFNA9/COCH and its phenotype.

Author

Kemperman MH, Bom SJ, Lemaire FX, Verhagen WI, Huygen PL, and Cremers CW

Subjects

Auditory Threshold, Cochlea metabolism, Cochlea pathology, Disease Progression, Ear, Inner pathology, Extracellular Matrix Proteins, Gene Expression, Hearing Loss, High-Frequency genetics, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural pathology, Humans, Mutation, Missense, Vestibular Diseases complications, Vestibular Diseases genetics, Deafness genetics, Hearing Loss, Sensorineural genetics, Phenotype, Proteins genetics

Published

2002

32. Clinical presentation of DFNB12 and Usher syndrome type 1D.

Author

Bork JM, Morell RJ, Khan S, Riazuddin S, Wilcox ER, Friedman TB, and Griffith AJ

Subjects

Adolescent, Adult, Aged, Cadherin Related Proteins, Child, Child, Preschool, Female, Genetic Linkage, Hearing Loss, Sensorineural diagnosis, Humans, Male, Middle Aged, Mutation, Missense, Retinitis Pigmentosa genetics, Syndrome, Vestibular Diseases genetics, Cadherins genetics, Hearing Loss, Sensorineural genetics, Phenotype

Published

2002

33. Hereditary cochleovestibular dysfunction due to a COCH gene mutation (DFNA9): a follow-up study of a family.

Author

Verhagen WI, Bom SJ, Fransen E, Van Camp G, Huygen PL, Theunissen EJ, and Cremers CW

Subjects

Adult, Age of Onset, Aged, Amino Acid Substitution, Audiometry, Pure-Tone, Chromosomes, Human, Pair 14 genetics, Cochlear Diseases complications, Cochlear Diseases diagnosis, Disease Progression, Female, Follow-Up Studies, Genotype, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural diagnosis, Heterozygote, Humans, Longitudinal Studies, Male, Meniere Disease genetics, Middle Aged, Pedigree, Vertigo complications, Vertigo genetics, Vestibular Diseases complications, Vestibular Diseases diagnosis, Vestibular Function Tests, Cochlear Diseases genetics, Hearing Loss, Sensorineural genetics, Mutation, Point Mutation, Vestibular Diseases genetics

Abstract

Cochleovestibular impairment was evaluated, in relation to age, in a longitudinal follow-up study on a Dutch family with a DFNA9 trait caused by a Pro51Ser mutation in the COCH gene on chromosome 14q12-q13. Fourteen cases were genotyped. The onset age of progressive impairment reported by the mutation carriers was between age 35 and 45 years. Pure-tone thresholds deteriorated by about 2-7 dB per year (mean 3.8 dB per year) in a variable, often asymmetrical, fashion. One mutation carrier developed recurrent episodes of vertigo accompanied by nausea and vomiting, resembling Ménière's disease. Two others developed special susceptibility for motion sickness and appeared to have a hyperactive vestibulo-ocular reflex. More advanced stages of vestibular impairment, i.e. vestibular hyporeflexia and complete vestibular areflexia, were eventually found in a number of cases. DFNA9/COCH should be considered as a possible cause in patients developing combined progressive cochlear and vestibular impairment, or suspected hereditary Ménière-like disease, from around middle age.

Published

2001

34. Inner ear localization of mRNA and protein products of COCH, mutated in the sensorineural deafness and vestibular disorder, DFNA9.

Author

Robertson NG, Resendes BL, Lin JS, Lee C, Aster JC, Adams JC, and Morton CC

Subjects

Adult, Animals, Antibodies, Monoclonal immunology, Blotting, Western, Ear, Inner chemistry, Ear, Inner embryology, Extracellular Matrix Proteins, Gene Expression, Gene Expression Regulation, Developmental, Hearing Loss, Sensorineural metabolism, Hearing Loss, Sensorineural pathology, Humans, Immunohistochemistry, In Situ Hybridization, Mice, Mutation, Proteins genetics, Proteins immunology, RNA, Messenger metabolism, Tissue Distribution, Vestibular Diseases metabolism, Vestibular Diseases pathology, Ear, Inner metabolism, Hearing Loss, Sensorineural genetics, Proteins metabolism, RNA, Messenger genetics, Vestibular Diseases genetics

Abstract

Missense mutations in the COCH gene, which is expressed preferentially at high levels in the inner ear, cause the autosomal dominant sensorineural deafness and vestibular disorder, DFNA9 (OMIM 601369). By in situ hybridization of mouse and human inner ear sections, we find high-level expression of COCH mRNA in the fibrocytes of the spiral limbus and of the spiral ligament in the cochlea, and in the fibrocytes of the connective tissue stroma underlying the sensory epithelium of the crista ampullaris of the semicircular canals. A polyclonal antibody against the human COCH protein product, cochlin, was raised against the N-terminal 135 amino acid residues of cochlin, corresponding to the Limulus factor C-homology (cochFCH) domain; this domain harbors all five known point mutations in DFNA9. On western blots of human fetal cochlear extracts, anti-cochlin reacts with a cochlin band of the predicted full-length size as well as a smaller isoform. Immunohistochemistry performed with anti-cochlin shows staining predominantly in the regions of the fibrocytes of the spiral limbus and of the spiral ligament in mouse and in human fetal and adult tissue sections. These sites correspond to those areas that express COCH mRNA as determined by in situ hybridization, and to the regions of the inner ear which show histological abnormalities in DFNA9. The fibrocytes expressing mRNA and protein products of COCH are the very cell types which are either absent or markedly reduced and replaced by eosinophilic acellular material in temporal bone sections of individuals affected with DFNA9.

Published

2001

35. Targeted disruption of mouse Pds provides insight about the inner-ear defects encountered in Pendred syndrome.

Author

Everett LA, Belyantseva IA, Noben-Trauth K, Cantos R, Chen A, Thakkar SI, Hoogstraten-Miller SL, Kachar B, Wu DK, and Green ED

Subjects

Animals, Goiter pathology, Goiter physiopathology, Hair Cells, Auditory abnormalities, Hair Cells, Auditory ultrastructure, Hearing Loss, Sensorineural pathology, Hearing Loss, Sensorineural physiopathology, Mice, Mice, Knockout, Mice, Neurologic Mutants, Microscopy, Electron, Scanning, Sulfate Transporters, Syndrome, Thyroid Gland pathology, Thyroid Gland physiopathology, Vestibular Diseases genetics, Vestibular Diseases pathology, Vestibular Diseases physiopathology, Vestibule, Labyrinth abnormalities, Vestibule, Labyrinth ultrastructure, Carrier Proteins genetics, Ear, Inner abnormalities, Goiter genetics, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins

Abstract

Following the positional cloning of PDS, the gene mutated in the deafness/goitre disorder Pendred syndrome (PS), numerous studies have focused on defining the role of PDS in deafness and PS as well as elucidating the function of the PDS-encoded protein (pendrin). To facilitate these efforts and to provide a system for more detailed study of the inner-ear defects that occur in the absence of pendrin, we have generated a Pds-knockout mouse. Pds(-/-) mice are completely deaf and also display signs of vestibular dysfunction. The inner ears of these mice appear to develop normally until embryonic day 15, after which time severe endolymphatic dilatation occurs, reminiscent of that seen radiologically in deaf individuals with PDS mutations. Additionally, in the second postnatal week, severe degeneration of sensory cells and malformation of otoconia and otoconial membranes occur, as revealed by scanning electron and fluorescence confocal microscopy. The ultrastructural defects seen in the Pds(-/-) mice provide important clues about the mechanisms responsible for the inner-ear pathology associated with PDS mutations.

Published

2001

36. A common ancestor for COCH related cochleovestibular (DFNA9) patients in Belgium and The Netherlands bearing the P51S mutation.

Author

Fransen E, Verstreken M, Bom SJ, Lemaire F, Kemperman MH, De Kok YJ, Wuyts FL, Verhagen WI, Huygen PL, McGuirt WT, Smith RJ, Van Maldergem LV, Declau F, Cremers CW, Van De Heyning PH, Cremers FP, and Van Camp G

Subjects

Alleles, Amino Acid Substitution, Belgium, Chromosomes, Artificial, Yeast, Chromosomes, Human, Pair 14 genetics, Cochlear Diseases genetics, Contig Mapping, Extracellular Matrix Proteins, Family Health, Female, Gene Frequency, Haplotypes, Humans, Male, Microsatellite Repeats, Netherlands, Point Mutation, Vestibular Diseases genetics, Hearing Loss, Sensorineural genetics, Proteins genetics

Published

2001

37. DFNA9 is a progressive audiovestibular dysfunction with a microfibrillar deposit in the inner ear.

Author

Khetarpal U

Subjects

Adult, Disease Progression, Glycosaminoglycans, Hearing Loss, Sensorineural pathology, Humans, Immunohistochemistry, Microscopy, Electron, Mutation, Prospective Studies, Temporal Bone diagnostic imaging, Temporal Bone pathology, Ultrasonography, Vestibular Diseases pathology, Hearing Loss, Sensorineural genetics, Vestibular Diseases genetics

Abstract

Objectives: Several mutations in the COCH gene were recently identified in American and European families with DFNA9, an autosomal dominant progressive sensorineural hearing loss with onset in high frequencies. Our preliminary vestibular studies in one American family indicated progressive vestibular dysfunction. More complete vestibular studies in European families have shown vestibular abnormalities in the affected individuals. Our temporal bone studies on two families with DFNA9 revealed, in addition to neurosensory degeneration, a unique acidophilic deposit in the membranous labyrinths of the affected individuals. The purposes of this study were 1) to further investigate the vestibular abnormalities in members of one American family for the purposes of genotype-phenotype correlation and 2) to investigate the electron microscopic structure of the acidophilic deposit to obtain further insights into the pathogenesis of DFNA9., Study Design: Prospective analysis., Methods: Extensive vestibular testing was performed in some unaffected and affected members of a family with DFNA9. One temporal bone was analyzed by electron microscopy of celloidin-embedded tissue., Results and Conclusions: The findings indicate progressive vestibular dysfunction in many of the patients affected with hearing loss. Thus, despite different mutations in the COCH gene, the American and European families manifest auditory and vestibular dysfunction. Electron microscopic analysis shows the spiral ligament to be enriched for a highly branched non-banded microfibrillar substance that is decorated with glycosaminoglycan granules. Additionally, the spiral ligament lacks the 67-nm-thick straight periodically banded bundles of type II collagen that are normally abundant in this structure. A speculative pathogenetic model is proposed for this unique disease and its relationship with other late-onset or adult-onset audiovestibular diseases and Meniere's disease is investigated.

Published

2000

38. Audiovestibular phenotype associated with a COL11A1 mutation in Marshall syndrome.

Author

Griffith AJ, Gebarski SS, Shepard NT, and Kileny PR

Subjects

Audiometry, Pure-Tone, Electronystagmography, Female, Humans, Male, Phenotype, RNA Splicing, Syndrome, Temporal Bone diagnostic imaging, Tomography, X-Ray Computed, Craniofacial Abnormalities genetics, Hearing Loss, Sensorineural genetics, Mutation, Vestibular Diseases genetics

Abstract

Background: Marshall syndrome is a dominant disorder characterized by craniofacial and skeletal abnormalities, sensorineural hearing loss, myopia, and cataracts, and is associated with splicing mutations in COL11A1., Objective: To determine the auditory and vestibular phenotypes associated with a COL11A1 splicing., Design: Clinical otolaryngologic, audiologic, vestibular, and radiologic evaluations of the auditory and vestibular systems., Subjects: Three affected individuals from a family cosegregating Marshall syndrome and a COL11A1 splice site mutation., Results: The study subjects have progressive sensorineural hearing loss that is predominantly cochlear in origin and asymptomatic dysfunction of the central and peripheral vestibular systems. Computed tomography detected no malformations of temporal bone structures., Conclusions: The observed auditory and vestibular abnormalities are not caused by defective morphogenesis of the osseous labyrinth, but by more direct effects of the COL11A1 mutation on the membranous labyrinth and the central nervous system. The onset and degree of hearing loss associated with COL11A1 mutations are useful clinical features to differentiate Marshall syndrome from the phenotypically similar Stickler syndrome.

Published

2000

39. A sequence-ready map of the Usher syndrome type III critical region on chromosome 3q.

Author

Joensuu T, Hämäläinen R, Lehesjoki AE, de la Chapelle A, and Sankila EM

Subjects

Chromosomes, Bacterial, Expressed Sequence Tags, Finland, Genes, Recessive, Genetic Vectors, Humans, Linkage Disequilibrium, Molecular Sequence Data, Syndrome, Chromosomes, Human, Pair 3 genetics, Hearing Loss, Sensorineural genetics, Retinal Degeneration genetics, Vestibular Diseases genetics

Abstract

Usher syndrome type 3 (USH3; MIM 276902) is an autosomal recessive disorder associated with progressive hearing loss and retinal degeneration. We recently refined the localization of USH3 to a 1-cM genetic interval between markers D3S1299 and D3S3625. We have now constructed a bacterial artificial chromosome contig over the region. Novel polymorphic markers were generated and physically fine-mapped, allowing further narrowing of the critical interval to a 250-kb genomic fragment. Of seven ESTs mapping to the initial critical region, WI-11588 and SHGC-133 represent the human SIAH2 gene, which was excluded as a candidate for USH3 by sequencing and subsequently, by its position. KIAA0001 and D3S3882 derive from the transcript of a putative G-protein-coupled receptor gene that was excluded as a candidate by sequencing of patient DNA. These data provide a basis for the sequencing and final characterization of the USH3 region and isolation of the disease gene., (Copyright 2000 Academic Press.)

Published

2000

40. Erratum: analysis of DNA elements that modulate myosin VIIa expression in humans.

Author

Orten DJ, Weston MD, Kelley PM, Cremers CW, Wagenaar M, Jacobson SG, and Kimberling WJ

Subjects

Amino Acid Substitution, Cell Line, Dyneins, HeLa Cells, Hearing Loss, Sensorineural metabolism, Humans, Linkage Disequilibrium, Mutation, Missense, Myosin VIIa, Myosins biosynthesis, Pedigree, Pigment Epithelium of Eye metabolism, Polymerase Chain Reaction, Polymorphism, Restriction Fragment Length, Retinitis Pigmentosa metabolism, Syndrome, Vestibular Diseases metabolism, Gene Expression Regulation, Hearing Loss, Sensorineural genetics, Myosins genetics, Promoter Regions, Genetic, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

Usher syndromeIb (USH1B), an autosomal recessive disorder caused by mutations in myosin VIIa (MYO7A), is characterized by congenital profound hearing loss, vestibular abnormalities and retinitis pigmentosa. Promoter elements in the 5 kb upstream of the translation start were identified using adult retinal pigment epithelium cells (ARPE-19) as a model system. A 160 bp minimal promoter within the first intron was active in ARPE-19 cells, but not in HeLa cells that do not express MYO7A. A 100 bp sequence, 5' of the first exon, and repeated with 90% homology within the first intron, appeared to modulate expression in both cell lines. Segments containing these elements were screened by heteroduplex analysis. No heteroduplexes were detected in the minimal promoter, suggesting that this sequence is conserved. A -2568 A>T transversion in the 5' 100 bp repeat, eliminating a CCAAT element, was found only in USH1B patients. However, in all 5 families, -2568 A>T was in cis with the same missense mutation in the myosin VIIa tail (Arg1240Gln), and 4 of the 5 families were Dutch. These observations suggest either 1) linkage disequilibrium or 2)that a combination of a promoter mutation with a less active myosin VIIa protein results in USH1B., (Copyright 2000 Wiley-Liss, Inc.)

Published

2000

41. Isolated large vestibular aqueduct syndrome in a family.

Author

Nowak KC and Messner AH

Subjects

Audiometry, Pure-Tone methods, Child, Preschool, Female, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural genetics, Humans, Male, Severity of Illness Index, Syndrome, Tomography, X-Ray Computed, Vestibular Diseases complications, Vestibular Diseases diagnosis, Hearing Loss, Sensorineural etiology, Vestibular Aqueduct abnormalities, Vestibular Aqueduct diagnostic imaging, Vestibular Diseases genetics

Abstract

This paper presents the second case in the literature of large vestibular aqueduct syndrome without associated cochlear anomalies in 2 members of the same family. The syndrome is frequently associated with sensorineural hearing loss presenting in childhood. The onset is commonly sudden, following an event causing increased intracranial pressure. On the basis of an emerging pattern of inheritance, we recommend screening siblings of an affected child. We also discuss the importance of characterizing the extent of disease of the inner ear.

Published

2000

42. Analysis of DNA elements that modulate myosin VIIA expression in humans.

Author

Orten DJ, Weston MD, Kelley PM, Cremers CW, Wagenaar M, Jacobson SG, and Kimberling WJ

Subjects

Cells, Cultured, Chromosomes, Human, Pair 11, DNA Mutational Analysis, Dyneins, HeLa Cells, Hearing Loss, Sensorineural metabolism, Humans, Mutation, Missense, Myosin VIIa, Pigment Epithelium of Eye metabolism, Promoter Regions, Genetic, Retinitis Pigmentosa metabolism, Syndrome, Vestibular Diseases metabolism, Gene Expression Regulation, Hearing Loss, Sensorineural genetics, Myosins biosynthesis, Myosins genetics, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

Usher syndromeIb (USH1B), an autosomal recessive disorder caused by mutations in myosin VIIa (MYO7A), is characterized by congenital profound hearing loss, vestibular abnormalities and retinitis pigmentosa. Promoter elements in the 5 kb upstream of the translation start were identified using adult retinal pigment epithelium cells (ARPE-19) as a model system. A 160 bp minimal promoter within the first intron was active in ARPE-19 cells, but not in HeLa cells that do not express MYO7A. A 100 bp sequence, 5' of the first exon, and repeated with 90% homology within the first intron, appeared to modulate expression in both cell lines. Segments containing these elements were screened by heteroduplex analysis. No heteroduplexes were detected in the minimal promoter, suggesting that this sequence is conserved. A -2568 A>T transversion in the 5' 100 bp repeat, eliminating a CCAAT element, was found only in USH1B patients. However, in all 5 families, -2568 A>T was in cis with the same missense mutation in the myosin VIIa tail (Arg1240Gln), and 4 of the 5 families were Dutch. These observations suggest either 1) linkage disequilibrium or 2)that a combination of a promoter mutation with a less active myosin VIIa protein results in USH1B., (Copyright 1999 Wiley-Liss, Inc.)

Published

1999

43. Tailchaser (Tlc): a new mouse mutation affecting hair bundle differentiation and hair cell survival.

Author

Kiernan AE, Zalzman M, Fuchs H, Hrabe de Angelis M, Balling R, Steel KP, and Avraham KB

Subjects

Animals, Auditory Threshold, Behavior, Animal, Cell Survival genetics, Chromosome Mapping, Cilia genetics, Cilia pathology, Cilia ultrastructure, Cochlea pathology, Cochlea ultrastructure, Genes, Dominant, Hair Cells, Auditory ultrastructure, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural pathology, Mice, Microscopy, Electron, Scanning, Mutation, Otolithic Membrane cytology, Vestibular Diseases complications, Vestibular Diseases pathology, Cell Differentiation genetics, Hair Cells, Auditory pathology, Hearing Loss, Sensorineural genetics, Mice, Neurologic Mutants genetics, Vestibular Diseases genetics

Abstract

We have undertaken a phenotypic approach in the mouse to identifying molecules involved in inner ear function by N-ethyl-N-nitrosourea mutagenesis followed by screening for new dominant mutations affecting hearing or balance. The pathology and genetic mapping of the first of these new mutants, tailchaser (Tlc), is described here. Tlc/+ mutants display classic behavioural symptoms of a vestibular dysfunction, including head-shaking and circling. Behavioural testing of ageing mice revealed a gradual deterioration of both hearing and balance function, indicating that the pathology caused by the Tlc mutation is progressive, similar to many dominant nonsyndromic deafnesses in humans. Based on scanning electron microscopy (SEM) studies, Tlc clearly plays a developmental role in the hair cells of the cochlea since the stereocilia bundles fail to form the characteristic V-shape pattern around the time of birth. By young adult stages, Tlc/+ outer hair bundles are grossly disorganised although inner hair bundles appear relatively normal by SEM. Increased compound action potential thresholds revealed that the Tlc/+ cochlear hair cells were not functioning normally in young adults. Similar to inner hair cells, the hair bundles of the vestibular hair cells also do not appear grossly disordered. However, all types of hair cells in the Tlc/+ inner ear eventually degenerate, apparently regardless of the degree of organisation of their hair bundles. We have mapped the Tlc mutation to a 12 cM region of chromosome 2, between D2Mit164 and D2Mit423. Based on the mode of inheritance and map location, Tlc appears to be a novel mouse mutation affecting both hair cell survival and stereocilia bundle development.

Published

1999

44. Progressive cochleovestibular impairment caused by a point mutation in the COCH gene at DFNA9.

Author

Bom SJ, Kemperman MH, De Kok YJ, Huygen PL, Verhagen WI, Cremers FP, and Cremers CW

Subjects

Adult, Aged, Deafness genetics, Female, Humans, Linear Models, Male, Middle Aged, Pedigree, Reflex, Abnormal, Reflex, Vestibulo-Ocular, Chromosomes, Human, Pair 14, Cochlear Diseases genetics, Hearing Loss, Sensorineural genetics, Point Mutation, Vestibular Diseases genetics

Abstract

Objectives: Analysis of phenotype-genotype correlation., Study Design: Family study., Methods: Auditory and vestibulo-ocular functions were examined in a Dutch family with autosomal dominantly inherited sensorineural hearing impairment caused by a 208C > T mutation in the COCH gene, located in chromosome 14q12-q13 (DFNA9). Linear regression analysis of individual longitudinal hearing threshold data (n = 11) on age was performed., Results: Fifteen of the 16 genetically affected persons could be evaluated. They all developed hearing and vestibular impairment symptoms--and in many cases also cardiovascular disease--in the fourth to fifth decade. At the low frequencies (0.25-2 kHz), hearing loss started at the age of about 40 years and showed an average annual progression of approximately 3 dB, finally resulting in profound hearing losses. In two exceptional cases, annual progression attained levels of up to 24 dB. At the high frequencies (4-8 kHz), the average threshold increased from about 50 dB at the age of 35 years to about 120 dB at the age of 75 years (which amounts to 1.8 dB annual threshold increase). All affected individuals tested showed normal ocular motor functions. The patients older than 46 years generally showed absence of the vestibulo-ocular reflex, but their cervico-ocular reflex was enhanced compared with normal subjects, whereas those aged 40 to 46 years showed either severe vestibular hyporeflexia or unilateral caloric areflexia., Conclusion: These findings suggest a gradual development of cochleovestibular impairment caused by the new mutation found.

Published

1999

45. A new mouse insertional mutation that causes sensorineural deafness and vestibular defects.

Author

Alagramam KN, Kwon HY, Cacheiro NL, Stubbs L, Wright CG, Erway LC, and Woychik RP

Subjects

Animals, Chromosome Mapping, Cochlea embryology, Cochlea pathology, Crosses, Genetic, Epithelial Cells pathology, Hearing Loss, Sensorineural pathology, Mice, Mice, Transgenic, Mutagenesis, Insertional, Organ of Corti abnormalities, Organ of Corti embryology, Organ of Corti pathology, Phenotype, Vestibular Diseases pathology, Vestibule, Labyrinth embryology, Vestibule, Labyrinth pathology, Hearing Loss, Sensorineural genetics, Mice, Neurologic Mutants genetics, Vestibular Diseases genetics

Abstract

This article describes a new recessive insertional mutation in the transgenic line TgN2742Rpw that causes deafness and circling behavior in mice. Histologic analysis revealed virtually complete loss of the cochlear neuroepithelium (the organ of Corti) in adult mutant mice. In association with the neuroepithelial changes, there is a dramatic reduction of the cochlear nerve supply. Adult mutants also show morphological defects of the vestibular apparatus, including degeneration of the saccular neuroepithelium and occasional malformation of utricular otoconia. Audiometric evaluations demonstrated that the mice displaying the circling phenotype are completely deaf. Molecular analysis of this mutant line revealed that the transgenic insertion occurred without creating a large deletion of the host DNA sequences. The mutant locus was mapped to a region on mouse chromosome 10, where other spontaneous, recessive mutations causing deafness in mice have been mapped.

Published

1999

46. A Pro51Ser mutation in the COCH gene is associated with late onset autosomal dominant progressive sensorineural hearing loss with vestibular defects.

Author

de Kok YJ, Bom SJ, Brunt TM, Kemperman MH, van Beusekom E, van der Velde-Visser SD, Robertson NG, Morton CC, Huygen PL, Verhagen WI, Brunner HG, Cremers CW, and Cremers FP

Subjects

Age of Onset, Amino Acid Substitution, Base Sequence, Chromosome Mapping, Chromosomes, Human, Pair 14 genetics, DNA chemistry, DNA genetics, DNA Mutational Analysis, Deafness genetics, Extracellular Matrix Proteins, Female, Genetic Linkage, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural pathology, Humans, Male, Microsatellite Repeats, Pedigree, Point Mutation, Proline genetics, Serine genetics, Vestibular Diseases complications, Vestibular Diseases pathology, Genes, Dominant genetics, Hearing Loss, Sensorineural genetics, Proteins genetics, Vestibular Diseases genetics

Abstract

We analysed a Dutch family with autosomal dominant non-syndromic progressive sensorineural hearing loss and mapped the underlying gene defect by genetic linkage analysis to a 11.0 cM region overlapping the DFNA9 interval on chromosome 14q12-q13. Clinically, the Dutch family differs from the original DFNA9 family by a later age at onset and a more clearly established vestibular impairment. A gene that is highly and specifically expressed in the human fetal cochlea and vestibule, COCH (previously described as Coch5B2 ), was mapped to the DFNA9 critical region. Sequence analysis revealed a 208C-->T mutation in the COCH gene, resulting in a Pro51Ser substitution in the predicted protein in all affected individuals of the family but not in unaffected family members and 200 control individuals. The same mutation was also identified in three apparently unrelated families with a similar phenotype, suggesting the presence of a Dutch founder mutation. The function of COCH is unknown but several characteristics of the protein point to a structural role in the extracellular matrix. The mutant serine at position 51 is situated between cysteines and possibly interferes with proper COCH protein folding or its interaction with extracellular matrix proteins.

Published

1999

47. Early-onset sensorineural hearing loss and late-onset neurologic complaints caused by a mitochondrial mutation at position 7472.

Author

Ensink RJ, Verhoeven K, Marres HA, Huygen PL, Padberg GW, ter Laak H, van Camp G, Willems PJ, and Cremers CW

Subjects

Adolescent, Aged, Audiometry, Child, Female, Humans, Male, Mitochondria, Muscle pathology, DNA, Mitochondrial, Hearing Loss, Sensorineural genetics, Mutation, Nervous System Diseases genetics, Vestibular Diseases genetics

Abstract

Objectives: To detect a mitochondrial mutation responsible for maternally transmitted hearing loss with late-onset neurologic features in a 3-generation Dutch family, and to describe the hearing loss, associated symptoms, and vestibular dysfunction., Patients and Methods: All maternally related family members (n = 69) were investigated using standard audiometry. In a selected group, vestibulo-ocular examinations and additional neurologic and ophthalmologic examinations were performed. Twenty milliliters of venous blood was taken from all participants for genetic studies., Setting: University medical center., Results: All maternally related individuals carried an extra C at position 7472 of the mitochondrial genome. Hearing loss was the only symptom or presenting symptom in most family members and most pronounced at higher frequencies. Hearing loss at lower frequencies was demonstrated in individuals 10 years and older. Most patients had vestibular hyperreactivity and were susceptible to motion sickness, suggesting vestibulocerebellar dysfunction. Neurologic complaints were infrequent and presented by older individuals; however, numerous enlarged mitochondria were found in a muscle biopsy specimen of an individual with hearing impairment but without neurologic symptoms., Conclusions: Respiratory chain dysfunction should be considered as a possible cause of progressive sensorineural hearing loss. More research into the causes of high-frequency impairment should be considered, especially when sensorineural hearing loss, syndromal or nonsyndromal, is exclusively maternally transmitted. Maternal transmission of hearing impairment can also be valuable in the diagnosis of unclear neurologic syndromes.

Published

1998

48. Usher syndrome in the Samaritans: strengths and limitations of using inbred isolated populations to identify genes causing recessive disorders.

Author

Bonné-Tamir B, Nystuen A, Seroussi E, Kalinsky H, Kwitek-Black AE, Korostishevsky M, Adato A, and Sheffield VC

Subjects

Arginine chemistry, Base Sequence, DNA analysis, DNA chemistry, DNA genetics, Female, Genetic Linkage, Haplotypes, Hearing Loss, Sensorineural congenital, Hearing Loss, Sensorineural epidemiology, Humans, Male, Middle East epidemiology, Pedigree, Point Mutation, Polymerase Chain Reaction, Polymorphism, Genetic, Polymorphism, Single-Stranded Conformational, Syndrome, Tryptophan chemistry, Vestibular Diseases congenital, Vestibular Diseases epidemiology, Vision Disorders congenital, Vision Disorders epidemiology, Chromosomes, Human, Pair 11, Consanguinity, Genes, Recessive, Genetics, Population, Hearing Loss, Sensorineural genetics, Vestibular Diseases genetics, Vision Disorders genetics

Abstract

We have previously reported significant linkage between markers on 11q13.5 and Usher syndrome type 1 (USH1B) in a large Samaritan kindred. USH1B is an autosomal recessive disease characterized by profound congenital sensorineural deafness, vestibular dysfunction and progressive visual loss. A unique haplotype found only in all USH1B carriers and affected individuals implied that the disease-causing mutation probably entered the community from a single founder. Screening for mutations in a gene called GARP, which was mapped to the same genetic interval as USH1B, revealed a base substitution in the coding region of the gene, in a homozygous state in all affected individuals. This base substitution, which results in an arginine to tryptophane change, is not found in control individuals and occurs at an amino acid residue that is conserved across species, including mouse, gorilla, chimpanzee and macaque. This study emphasizes the strength of using an isolated inbred population for efficient identification of the primary linkage and for narrowing the disease interval, but also demonstrates its limitations in distinguishing between mutations causing the disease and those representing unique and private polymorphisms.

Published

1997

49. Myosin VIIA gene: heterogeneity of the mutations responsible for Usher syndrome type IB.

Author

Lévy G, Levi-Acobas F, Blanchard S, Gerber S, Larget-Piet D, Chenal V, Liu XZ, Newton V, Steel KP, Brown SD, Munnich A, Kaplan J, Petit C, and Weil D

Subjects

Base Sequence, DNA, Dyneins, Genes, Humans, Molecular Sequence Data, Mutagenesis, Myosin VIIa, Syndrome, Genetic Heterogeneity, Hearing Loss, Sensorineural genetics, Myosins genetics, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

Usher syndrome is recognized as the most frequent cause of hereditary deaf-blindness. Usher syndrome type I (USH1), the most severe form of the disease, is characterized by profound congenital sensorineural deafness, constant vestibular dysfunction, and retinitis pigmentosa of prepubertal onset. This form is genetically heterogeneous and five loci (USH1A-E) have been mapped thusfar. However, only the gene responsible for USH1 B (which accounts for approximately 75% of USH1 cases) has been characterized. It encodes a long-tailed unconventional myosin, myosin VIIA, with a predicted 2215 amino acid sequence. Primers covering the complete myosin VIIA coding sequence as well as the 3' non coding sequence were designed, allowing direct sequence analysis of each of the 48 coding exons and flanking splice sites in seven patients affected by USH1. Four novel mutations were thereby identified. The possibility should now be considered of a sequence-based prenatal diagnosis in some of the families affected by this very severe form of Usher syndrome.

Published

1997

50. Refined mapping of the Usher syndrome type III locus on chromosome 3, exclusion of candidate genes, and identification of the putative mouse homologous region.

Author

Joensuu T, Blanco G, Pakarinen L, Sistonen P, Kääriäinen H, Brown S, Chapelle A, and Sankila EM

Subjects

Alleles, Animals, Chromosome Mapping, Chromosomes, Artificial, Yeast genetics, Finland epidemiology, Founder Effect, Haplotypes genetics, Hearing Loss, Sensorineural classification, Hearing Loss, Sensorineural epidemiology, Humans, Linkage Disequilibrium, Lod Score, Microfilament Proteins genetics, Profilins, Retinitis Pigmentosa classification, Retinitis Pigmentosa epidemiology, Sequence Homology, Species Specificity, Syndrome, Vestibular Diseases classification, Vestibular Diseases epidemiology, Chromosomes, Human, Pair 3 genetics, Contractile Proteins, Hearing Loss, Sensorineural genetics, Mice genetics, Retinitis Pigmentosa genetics, Vestibular Diseases genetics

Abstract

A locus for Usher syndrome type III (USH3; MIM No. 276902) was recently assigned to a 5-cM region on chromosome 3q. We constructed a yeast artificial chromosome contig that allowed us to position novel polymorphisms in the region. These were typed in a total of 32 pedigrees from a geographically isolated Finnish founder population in which a putative single ancestral USH3 mutation segregates. A multipoint linkage analysis assigned USH3 to a 4-cM region between D3S1555 and a novel marker D3S3625. By analysis of linkage disequilibrium and historical recombinations in 77 USH3 chromosomes, the location of the Finnish USH3 mutation could be narrowed to an approximately 1-cM interval between the markers D3S1299 and D3S3625. A gene for profilin-2 (PFN2) was mapped in the vicinity and excluded as a candidate for USH3 by sequencing. The putative mouse homolog of PFN2 was mapped to mouse chromosome 3, thus suggesting a localization for the mouse homolog of USH3.

Published

1996