Your search keyword '"Usher Syndromes classification"' showing total 21 results

1. The Study of a 231 French Patient Cohort Significantly Extends the Mutational Spectrum of the Two Major Usher Genes MYO7A and USH2A .

Author

Mansard L, Baux D, Vaché C, Blanchet C, Meunier I, Willems M, Faugère V, Baudoin C, Moclyn M, Bianchi J, Dollfus H, Gilbert-Dussardier B, Dupin-Deguine D, Bonneau D, Drumare I, Odent S, Zanlonghi X, Claustres M, Koenig M, Kalatzis V, and Roux AF

Subjects

Adult, Female, France, Humans, Male, Extracellular Matrix Proteins genetics, Genotype, Mutation, Missense, Myosin VIIa genetics, RNA Splice Sites, Usher Syndromes classification, Usher Syndromes genetics

Abstract

Usher syndrome is an autosomal recessive disorder characterized by congenital hearing loss combined with retinitis pigmentosa, and in some cases, vestibular areflexia. Three clinical subtypes are distinguished, and MYO7A and USH2A represent the two major causal genes involved in Usher type I, the most severe form, and type II, the most frequent form, respectively. Massively parallel sequencing was performed on a cohort of patients in the context of a molecular diagnosis to confirm clinical suspicion of Usher syndrome. We report here 231 pathogenic MYO7A and USH2A genotypes identified in 73 Usher type I and 158 Usher type II patients. Furthermore, we present the ACMG classification of the variants, which comprise all types. Among them, 68 have not been previously reported in the literature, including 12 missense and 16 splice variants. We also report a new deep intronic variant in USH2A . Despite the important number of molecular studies published on these two genes, we show that during the course of routine genetic diagnosis, undescribed variants continue to be identified at a high rate. This is particularly pertinent in the current era, where therapeutic strategies based on DNA or RNA technologies are being developed.

Published

2021

2. Atypical and ultra-rare Usher syndrome: a review.

Author

Nolen RM, Hufnagel RB, Friedman TB, Turriff AE, Brewer CC, Zalewski CK, King KA, Wafa TT, Griffith AJ, Brooks BP, and Zein WM

Subjects

Animals, Genotype, Humans, Rare Diseases classification, Usher Syndromes classification, Chromosome Aberrations, Phenotype, Rare Diseases genetics, Rare Diseases pathology, Usher Syndromes genetics, Usher Syndromes pathology

Abstract

Usher syndrome has classically been described as a combination of hearing loss and rod-cone dystrophy; vestibular dysfunction is present in many patients. Three distinct clinical subtypes were documented in the late 1970s. Genotyping efforts have led to the identification of several genes associated with the disease. Recent literature has seen multiple publications referring to "atypical" Usher syndrome presentations. This manuscript reviews the molecular etiology of Usher syndrome, highlighting rare presentations and molecular causes. Reports of "atypical" disease are summarized noting the wide discrepancy in the spectrum of phenotypic deviations from the classical presentation. Guidelines for establishing a clear nomenclature system are suggested.

Published

2020

3. [The Usher Syndrome, a Human Ciliopathy].

Author

Wolfrum U and Nagel-Wolfrum K

Subjects

Animals, Ciliopathies classification, Ciliopathies genetics, Ciliopathies therapy, DNA Mutational Analysis, Deaf-Blind Disorders classification, Deaf-Blind Disorders diagnosis, Deaf-Blind Disorders genetics, Deaf-Blind Disorders therapy, Disease Models, Animal, Female, Humans, Infant, Newborn, Mice, Neonatal Screening, Photoreceptor Cells, Vertebrate physiology, Pregnancy, Usher Syndromes classification, Usher Syndromes genetics, Usher Syndromes therapy, Ciliopathies diagnosis, Rare Diseases, Usher Syndromes diagnosis

Abstract

The human Usher syndrome (USH) is a complex, rare disease manifesting in its most common form of inherited deaf-blindness. Due to the heterogeneous manifestation of the clinical symptoms, three clinical types (USH1-3) are distinguished according to the severity of the disease pattern. For a correct diagnosis, in addition to the auditory tests in early newborn screening, ophthalmological examinations and molecular genetic analysis are important. Ten known USH genes encode proteins, which are from heterogeneous protein families, interact in functional protein networks. In the eye and in the ear, USH proteins are expressed primarily in the mechano-sensitive hair cells and the rod and cone photoreceptor cells, respectively. In the hair cells, the USH protein networks are essential for the correct differentiation of the hair bundles as well as for the function of the mechano-electrical transduction complex in the matured cell. In the photoreceptor cells, USH proteins are located in the ciliary region and participate in intracellular transport processes. In addition, a USH protein network is present in the so-called calyceal processes. The lack of calyceal processes and the absence of a prominent visual phenotype in the mouse disqualifies mice as models for studies on the ophthalmic component of USH. While hearing impairments can be compensated with hearing aids and cochlear implants, there is no practical therapy for USH in the eye. Currently, gene-based therapy concepts, such as gene addition, applications of antisense oligonucleotides and TRIDs ("translational readthrough inducing drugs") for the readthrough of nonsense mutations are preclinically evaluated. For USH1B/MYO7A the UshStat gene therapy clinical trial is ongoing., Competing Interests: Die Autoren geben an, dass kein Interessenkonflikt besteht., (Georg Thieme Verlag KG Stuttgart · New York.)

Published

2018

4. Targeted next generation sequencing in Italian patients with Usher syndrome: phenotype-genotype correlations.

Author

Eandi CM, Dallorto L, Spinetta R, Micieli MP, Vanzetti M, Mariottini A, Passerini I, Torricelli F, Alovisi C, and Marchese C

Subjects

Adolescent, Adult, Child, DNA Mutational Analysis, Female, Genetic Association Studies, Genetic Predisposition to Disease, Genotype, High-Throughput Nucleotide Sequencing, Humans, Italy, Male, Middle Aged, Mutation, Missense genetics, Myosin VIIa, Pedigree, Sequence Deletion genetics, Usher Syndromes classification, Usher Syndromes pathology, Young Adult, Extracellular Matrix Proteins genetics, Myosins genetics, Receptors, G-Protein-Coupled genetics, Usher Syndromes genetics

Abstract

We report results of DNA analysis with next generation sequencing (NGS) of 21 consecutive Italian patients from 17 unrelated families with clinical diagnosis of Usher syndrome (4 USH1 and 17 USH2) searching for mutations in 11 genes: MYO7A, CDH23, PCDH15, USH1C, USH1G, USH2A, ADGVR1, DFNB31, CLRN1, PDZD7, HARS. Likely causative mutations were found in all patients: 25 pathogenic variants, 18 previously reported and 7 novel, were identified in three genes (USH2A, MYO7A, ADGRV1). All USH1 presented biallelic MYO7A mutations, one USH2 exhibited ADGRV1 mutations, whereas 16 USH2 displayed USH2A mutations. USH1 patients experienced hearing problems very early in life, followed by visual impairment at 1, 4 and 6 years. Visual symptoms were noticed at age 20 in a patient with homozygous novel MYO7A missense mutation c.849G > A. USH2 patients' auditory symptoms, instead, arose between 11 months and 14 years, while visual impairment occurred later on. A homozygous c.5933_5940del;5950_5960dup in USH2A was detected in one patient with early deafness. One patient with homozygous deletion from exon 23 to 32 in USH2A suffered early visual symptoms. Therefore, the type of mutation in USH2A and MYO7A genes seems to affect the age at which both auditory and visual impairment occur in patients with USH.

Published

2017

5. The contribution of GPR98 and DFNB31 genes to a Spanish Usher syndrome type 2 cohort.

Author

García-García G, Besnard T, Baux D, Vaché C, Aller E, Malcolm S, Claustres M, Millan JM, and Roux AF

Subjects

Codon, Nonsense, Cohort Studies, Extracellular Matrix Proteins genetics, Frameshift Mutation, Haplotypes, Homozygote, Humans, Sequence Deletion, Spain, Usher Syndromes classification, Usher Syndromes physiopathology, Membrane Proteins genetics, Mutation, Receptors, G-Protein-Coupled genetics, Usher Syndromes genetics

Abstract

Background: Usher syndrome type 2 (USH2) is an autosomal recessive disease characterized by moderate to severe hearing loss and retinitis pigmentosa. To date, three disease-causing genes have been identified, USH2A, GPR98, and DFNB31, of which USH2A is clearly the major contributor. The aim of this work was to determine the contribution of GPR98 and DFNB31 genes in a Spanish cohort of USH2A negative patients using exhaustive molecular analysis, including sequencing, dosage, and splicing analysis., Methods: Linkage analysis was performed to prioritize the gene to study, followed by sequencing of exons and intron-exon boundaries of the selected gene, GPR98 (90 exons) or DFNB31 (12 exons). Functional splicing analyses and comparative genomic hybridization array to detect large rearrangements were performed when appropriate., Results: We confirmed that mutations in GPR98 contribute a significant but minor role to Usher syndrome type 2. In a group of patients referred for molecular diagnosis, 43 had been found to be positive for USH2A mutations, the remaining 19 without USH2A alterations were screened, and seven different mutations were identified in the GPR98 gene in seven patients (five in the homozygous state), of which six were novel. All detected mutations result in a truncated protein; deleterious missense mutations were not found. No pathological mutations were identified in the DFNB31 gene., Conclusions: In Spain, USH2A and GPR98 are responsible for 95.8% and 5.2% of USH2 mutated cases, respectively. DFNB31 plays a minor role in the Spanish population. There was a group of patients in whom no mutation was found. These findings confirm the importance of including at least GPR98 analysis for comprehensive USH2 molecular diagnosis.

Published

2013

6. Mutational screening of the USH2A gene in Spanish USH patients reveals 23 novel pathogenic mutations.

Author

Garcia-Garcia G, Aparisi MJ, Jaijo T, Rodrigo R, Leon AM, Avila-Fernandez A, Blanco-Kelly F, Bernal S, Navarro R, Diaz-Llopis M, Baiget M, Ayuso C, Millan JM, and Aller E

Subjects

Adolescent, Adult, DNA Mutational Analysis, Exons, Female, Genotype, Humans, Male, Middle Aged, Mutation, Missense, Phenotype, Spain, Usher Syndromes classification, Young Adult, Extracellular Matrix Proteins genetics, Mutation, Usher Syndromes genetics

Abstract

Background: Usher Syndrome type II (USH2) is an autosomal recessive disorder, characterized by moderate to severe hearing impairment and retinitis pigmentosa (RP). Among the three genes implicated, mutations in the USH2A gene account for 74-90% of the USH2 cases., Methods: To identify the genetic cause of the disease and determine the frequency of USH2A mutations in a cohort of 88 unrelated USH Spanish patients, we carried out a mutation screening of the 72 coding exons of this gene by direct sequencing. Moreover, we performed functional minigene studies for those changes that were predicted to affect splicing., Results: As a result, a total of 144 DNA sequence variants were identified. Based upon previous studies, allele frequencies, segregation analysis, bioinformatics' predictions and in vitro experiments, 37 variants (23 of them novel) were classified as pathogenic mutations., Conclusions: This report provide a wide spectrum of USH2A mutations and clinical features, including atypical Usher syndrome phenotypes resembling Usher syndrome type I. Considering only the patients clearly diagnosed with Usher syndrome type II, and results obtained in this and previous studies, we can state that mutations in USH2A are responsible for 76.1% of USH2 disease in patients of Spanish origin.

Published

2011

7. Auditory and vestibular hair cell stereocilia: relationship between functionality and inner ear disease.

Author

Ciuman RR

Subjects

Adaptation, Physiological, Animals, Auditory Threshold physiology, Calcium physiology, Child, Hair Cells, Auditory cytology, Hair Cells, Auditory pathology, Hair Cells, Vestibular cytology, Hair Cells, Vestibular pathology, Humans, Labyrinth Diseases metabolism, Mechanotransduction, Cellular physiology, Myosins metabolism, Sensory Gating physiology, Stereocilia metabolism, Stereocilia pathology, Usher Syndromes classification, Usher Syndromes physiopathology, Hair Cells, Auditory physiology, Hair Cells, Vestibular physiology, Labyrinth Diseases physiopathology, Stereocilia physiology, Usher Syndromes genetics

Abstract

The stereocilia of the inner ear are unique cellular structures which correlate anatomically with distinct cochlear functions, including mechanoelectrical transduction, cochlear amplification, adaptation, frequency selectivity and tuning. Their function is impaired by inner ear stressors, by various types of hereditary deafness, syndromic hearing loss and inner ear disease (e.g. Ménière's disease). The anatomical and physiological characteristics of stereocilia are discussed in relation to inner ear malfunctions.

Published

2011

8. Four-year follow-up of diagnostic service in USH1 patients.

Author

Roux AF, Faugère V, Vaché C, Baux D, Besnard T, Léonard S, Blanchet C, Hamel C, Mondain M, Gilbert-Dussardier B, Edery P, Lacombe D, Bonneau D, Holder-Espinasse M, Ambrosetti U, Journel H, David A, Lina-Granade G, Malcolm S, and Claustres M

Subjects

Chromosome Mapping, Cohort Studies, DNA Mutational Analysis, Follow-Up Studies, France, Genetic Heterogeneity, Genetic Testing, Genotype, Haplotypes, Homozygote, Humans, Mutation, Missense, Myosin VIIa, Myosins genetics, Usher Syndromes classification, Mutation, Usher Syndromes diagnosis, Usher Syndromes genetics

Abstract

Purpose: The purpose of this study was to establish the mutation spectrum of an Usher type I cohort of 61 patients from France and to describe a diagnostic strategy, including a strategy for estimating the pathogenicity of sequence changes., Methods: To optimize the identification of Usher (USH)-causative mutations, taking into account the genetic heterogeneity, preliminary haplotyping at the five USH1 loci was performed to prioritize the gene to be sequenced, as previously described. Coding exons and flanking intronic sequences were sequenced and, where necessary, semiquantitative PCR and multiplex ligation-dependent probe amplification (MLPA) were performed to detect large genomic rearrangements., Results: Four years ' experience confirms that the chosen approach provides an efficient diagnostic service. Sixty-one patients showed an abnormal genotype in one of the five USH1 genes. Genetic heterogeneity was confirmed, and, although MYO7A remains the major gene, involvement of other genes is considerable. Distribution of missense, splicing, premature termination codons (PTCs; due to point substitution and small deletions/ or insertions), and large genomic alterations was determined among the USH genes and clearly highlights the need to pay special attention to the diagnostic approach and interpretation, depending on the mutated gene., Conclusions: Over the 4 years of a diagnostic service offering USH1 patient testing, pathogenic genotypes were identified in most cases (>90%). The complexity and heterogeneity of mutations reinforces the need for a comprehensive approach. Because 32% of the mutations are newly described, the results show that a screening strategy based on known mutations would have solved less than 55% of the cases.

Published

2011

9. Usher syndrome in Puerto Rico: a clinical and genetic study.

Author

Colón-Casasnovas JE, Izquierdo NJ, and Millán JM

Subjects

Adult, Aged, Audiometry, Pure-Tone, DNA Mutational Analysis, Electroretinography, Fovea Centralis pathology, Genetic Heterogeneity, Humans, Macula Lutea pathology, Macular Edema genetics, Macular Edema pathology, Male, Middle Aged, Mutation, Phenotype, Puerto Rico epidemiology, Tomography, Optical Coherence, Usher Syndromes classification, Usher Syndromes diagnosis, Usher Syndromes genetics, Visual Fields, Usher Syndromes epidemiology

Abstract

Purpose: To evaluate patients with the Usher syn drome in Puerto Rico., Methods: Three patients with the Usher syndrome underwent an ophthalmic and audiologic evaluation; and genetic linkage analysis., Results: All patients were legally blind based on visual acuity and visual field results. Two patients had macular edema as shown on Stratus OCT. All patients had moderate hearing loss as part of the syndrome. A patient, and two family members had three mutations leading to protein changes including: p.S4588Y; p.Y4505C; and p.14474M., Conclusions: Phenotypic findings in patients with the Usher syndrome in Puerto Rico are similar to those previously reported. However, to our knowledge, neither these mutations nor OCT findings have been previously described in patients with the syndrome.

Published

2010

10. Usher syndrome.

Subjects

Early Diagnosis, Genetic Testing, Humans, School Nursing, United States epidemiology, Usher Syndromes classification, Usher Syndromes diagnosis, Usher Syndromes epidemiology, Usher Syndromes genetics

Published

2010

11. GPR98 mutations cause Usher syndrome type 2 in males.

Author

Ebermann I, Wiesen MH, Zrenner E, Lopez I, Pigeon R, Kohl S, Löwenheim H, Koenekoop RK, and Bolz HJ

Subjects

DNA Mutational Analysis, Family Health, Female, Humans, Male, Pedigree, Usher Syndromes classification, Usher Syndromes pathology, Young Adult, Mutation, Receptors, G-Protein-Coupled genetics, Usher Syndromes genetics

Abstract

Mutations in the large GPR98 gene underlie Usher syndrome type 2C (USH2C), and all patients described to date have been female. It was speculated that GPR98 mutations cause a more severe, and eventually lethal, phenotype in males. We describe for the first time two male patients with USH2 with novel GPR98 mutations. Clinical characterization of a male patient and his affected sister revealed a typical USH2 phenotype in both. GPR98 may have been excluded from systematic investigation in previous studies, and the proportion of patients with USH2C probably underestimated. GPR98 should be considered in patients with USH2 of both sexes.

Published

2009

12. A large deletion in GPR98 causes type IIC Usher syndrome in male and female members of an Iranian family.

Author

Hilgert N, Kahrizi K, Dieltjens N, Bazazzadegan N, Najmabadi H, Smith RJ, and Van Camp G

Subjects

Consanguinity, DNA Mutational Analysis, Family Health, Female, Humans, Iran, Male, Pedigree, Usher Syndromes classification, Usher Syndromes pathology, Gene Deletion, Receptors, G-Protein-Coupled genetics, Usher Syndromes genetics

Abstract

Background: Usher syndrome (USH) is a clinically and genetically heterogeneous disease. The three recognised clinical phenotypes (types I, II and III; USH1, USH2 and USH3) are caused by mutations in nine different genes. USH2C is characterised by moderate to severe hearing loss, retinitis pigmentosa and normal vestibular function. One earlier report describes mutations in GPR98 (VLGR1) in four families segregating this phenotype., Objective: To detect the disease-causing mutation in an Iranian family segregating USH2C. In this family, five members had a phenotype compatible with Usher syndrome, and two others had nonsyndromic hearing loss., Methods: Mutation analysis of all 90 coding exons of GPR98., Results: Consistent with these clinical findings, the five subjects with USH carried a haplotype linked to the USH2C locus, whereas the two subjects with nonsyndromic hearing loss did not. We identified a new mutation in GPR98 segregating with USH2C in this family. The mutation is a large deletion g.371657_507673del of exons 84 and 85, presumably leading to a frameshift., Conclusions: A large GPR98 deletion of 136 017 bp segregates with USH2C in an Iranian family. To our knowledge, this is only the second report of a GPR98 mutation, and the first report on male subjects with USH2C and a GPR98 mutation.

Published

2009

13. Novel human pathological mutations. Gene symbol: GPR98. Disease: Usher syndrome 2C.

Author

Hilgert N

Subjects

Exons, Humans, Introns, Molecular Sequence Data, Usher Syndromes classification, Receptors, G-Protein-Coupled genetics, Sequence Deletion, Usher Syndromes genetics

Published

2009

14. Long-term ophthalmic health care in Usher syndrome type I from an ICF perspective.

Author

Möller K, Eriksson K, Sadeghi AM, Möller C, and Danermark B

Subjects

Adult, Disabled Persons classification, Female, Health Status, Humans, Ophthalmology, Patient Care Team, Quality of Health Care, Retrospective Studies, Usher Syndromes classification, Vision, Low etiology, Vision, Low therapy, Visual Acuity, Usher Syndromes therapy

Abstract

Purpose: The aim was to explore ophthalmic health care in female patients with Usher Syndrome type I (USH I) over 20 years and to evaluate the relationship between the ophthalmic health care and the health state of the patients from a health perspective., Methods: A retrospective study of records from ophthalmology departments (OD) and low vision clinics (LVC) from 1985 to 2004. Assessment of the reports was performed based on the International Classification of Functioning, Disability and Health (ICF). Findings were analysed by manifest content analysis with ICF as a framework and using four themes: health care system, procedure examinations, patient's functioning and disability and procedure actions., Results: The records of nine female patients (aged 25-39 years, 1985) with USH I were selected from the national database of USH. A great number of notes were collected (OD 344 and LVC 566). Procedure examinations were exclusively oriented towards body structure and function. All patients showed aggravated visual impairment over and above the hearing and vestibular impairment. Procedure actions were oriented towards environmental factors. No correlation was found between procedures performed and patient's experience of disability., Conclusions: The high degree of resource allocation was not correlated to the patients' impairment. The study indicates that the ophthalmic health care was characterised by inefficiency. This conclusion is very serious because patients very likely face severe disability and emotional difficulties. ICF is ought to be incorporated in ophthalmic health care strategy to improve the health care.

Published

2009

15. Spectrum of USH2A mutations in Scandinavian patients with Usher syndrome type II.

Author

Dreyer B, Brox V, Tranebjaerg L, Rosenberg T, Sadeghi AM, Möller C, and Nilssen O

Subjects

Codon, Nonsense, DNA genetics, DNA Mutational Analysis, Exons, Female, Genotype, Humans, Introns, Male, Membrane Proteins genetics, Mutation, Missense, Scandinavian and Nordic Countries, Sequence Deletion, Usher Syndromes classification, Extracellular Matrix Proteins genetics, Mutation, Usher Syndromes genetics

Abstract

Usher syndrome type II (USH2) is an autosomal recessive disorder, characterised by moderate to severe high-frequency hearing impairment, normal balance function and progressive visual impairment due to retinitis pigmentosa. Usher syndrome type IIa, the most common subtype, is defined by mutations in the USH2A gene encoding a short and a recently discovered long usherin isoform comprising 21 and 73 exons, respectively. More than 120 different disease-causing mutations have been reported, however, most of the previous reports concern mutations restricted to exons 1-21 of the USH2A gene. To explore the spectrum of USH2A disease-causing mutations among Scandinavian USH2 cases, patients from 118 unrelated families of which 27 previously had been found to carry mutations in exons 1-21 were subjected to extensive DNA sequence analysis of the full size USH2A gene. Altogether, 122 USH2A DNA sequence alterations were identified of which 57 were predicted to be disease-causing, 7 were considered to be of uncertain pathogenicity and 58 were predicted to be benign variants. Of 36 novel pathogenic USH2A mutations 31 were located in exons 22-73, specific to the long isoform. USH2A mutations were identified in 89/118 (75.4%) families. In 79/89 (88.8%) of these families two pathogenic mutations were identified whereas in 10/89 (11.2%) families the second mutation remained unidentified. In 5/118 (4.2%) families the USH phenotype could be explained by mutations in the USH3A gene. The results presented here provide a comprehensive picture of the genetic aetiology of Usher syndrome type IIA in Scandinavia as it is known to date.

Published

2008

16. Usher syndrome type 1 due to missense mutations on both CDH23 alleles: investigation of mRNA splicing.

Author

Becirovic E, Ebermann I, Nagy D, Zrenner E, Seeliger MW, and Bolz HJ

Subjects

Alleles, Amino Acid Sequence, Amino Acid Substitution, Base Sequence, Cadherin Related Proteins, Cadherins chemistry, Cadherins metabolism, DNA Primers genetics, DNA, Complementary genetics, Exons, Humans, Introns, Molecular Sequence Data, RNA Splicing, RNA, Messenger genetics, RNA, Messenger metabolism, Usher Syndromes classification, Usher Syndromes metabolism, Cadherins genetics, Mutation, Missense, Usher Syndromes genetics

Abstract

Usher syndrome (USH) is an autosomal recessive condition characterized by sensorineural hearing loss, vestibular dysfunction, and visual impairment due to retinitis pigmentosa. Truncating mutations in the cadherin-23 gene (CDH23) result in Usher syndrome type 1D (USH1D), whereas missense mutations affecting strongly conserved motifs of the CDH23 protein cause non-syndromic deafness (DFNB12). Four missense mutations constitute an exception from this genotype-phenotype correlation: they have been described in USH1 patients in homozygous state. Using a minigene assay, we have investigated these changes (c.1450G>C, p.A484P; c.3625A>G, p.T1209A; c.4520G>A, p.R1507Q; and c.5237G>A, p.R1746Q) for a possible impact on mRNA splicing which could explain the syndromic phenotype. While in silico analysis suggested impairment of splicing in all four cases, we found aberrant splicing for only one mutation, p.R1746Q. However, splicing was normal in case of p.A484P, p.T1209A and p.R1507Q. These three latter CDH23 missense mutations could interfere with functions of both, the auditory and the visual system. Alternatively, they could represent rare non-pathogenic polymorphisms.

Published

2008

17. A novel Usher protein network at the periciliary reloading point between molecular transport machineries in vertebrate photoreceptor cells.

Author

Maerker T, van Wijk E, Overlack N, Kersten FF, McGee J, Goldmann T, Sehn E, Roepman R, Walsh EJ, Kremer H, and Wolfrum U

Subjects

Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Animals, COS Cells, Cell Cycle Proteins, Chlorocebus aethiops, Cytoskeletal Proteins, Extracellular Matrix Proteins genetics, Extracellular Matrix Proteins metabolism, Humans, In Vitro Techniques, Membrane Proteins genetics, Membrane Proteins metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Microscopy, Immunoelectron, Models, Biological, NIH 3T3 Cells, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Photoreceptor Cells, Vertebrate ultrastructure, Protein Interaction Mapping, Receptors, G-Protein-Coupled deficiency, Receptors, G-Protein-Coupled genetics, Subcellular Fractions metabolism, Transfection, Usher Syndromes classification, Xenopus genetics, Xenopus metabolism, Photoreceptor Cells, Vertebrate metabolism, Usher Syndromes genetics, Usher Syndromes metabolism

Abstract

The human Usher syndrome (USH) is the most frequent cause of combined deaf-blindness. USH is genetically heterogeneous with at least 12 chromosomal loci assigned to three clinical types, USH1-3. Although these USH types exhibit similar phenotypes in human, the corresponding gene products belong to very different protein classes and families. The scaffold protein harmonin (USH1C) was shown to integrate all identified USH1 and USH2 molecules into protein networks. Here, we analyzed a protein network organized in the absence of harmonin by the scaffold proteins SANS (USH1G) and whirlin (USH2D). Immunoelectron microscopic analyses disclosed the colocalization of all network components in the apical inner segment collar and the ciliary apparatus of mammalian photoreceptor cells. In this complex, whirlin and SANS directly interact. Furthermore, SANS provides a linkage to the microtubule transport machinery, whereas whirlin may anchor USH2A isoform b and VLGR1b (very large G-protein coupled receptor 1b) via binding to their cytodomains at specific membrane domains. The long ectodomains of both transmembrane proteins extend into the gap between the adjacent membranes of the connecting cilium and the apical inner segment. Analyses of Vlgr1/del7TM mice revealed the ectodomain of VLGR1b as a component of fibrous links present in this gap. Comparative analyses of mouse and Xenopus photoreceptors demonstrated that this USH protein network is also part of the periciliary ridge complex in Xenopus. Since this structural specialization in amphibian photoreceptor cells defines a specialized membrane domain for docking and fusion of transport vesicles, we suggest a prominent role of the USH proteins in cargo shipment.

Published

2008

18. In vitro and ex vivo suppression by aminoglycosides of PCDH15 nonsense mutations underlying type 1 Usher syndrome.

Author

Rebibo-Sabbah A, Nudelman I, Ahmed ZM, Baasov T, and Ben-Yosef T

Subjects

Animals, Base Sequence, COS Cells, Cadherin Related Proteins, Cadherins metabolism, Cell Line, Chlorocebus aethiops, DNA, Complementary genetics, Humans, In Vitro Techniques, Protein Biosynthesis drug effects, Recombinant Proteins genetics, Recombinant Proteins metabolism, Transfection, Usher Syndromes classification, Usher Syndromes metabolism, Aminoglycosides pharmacology, Cadherins genetics, Codon, Nonsense drug effects, Usher Syndromes drug therapy, Usher Syndromes genetics

Abstract

Type 1 Usher syndrome (USH1) is a recessively inherited condition, characterized by profound prelingual deafness, vestibular areflexia, and prepubertal onset of retinitis pigmentosa (RP). While the auditory component of USH1 can be treated by cochlear implants, to date there is no effective treatment for RP. USH1 can be caused by mutations in each of at least six genes. While truncating mutations of these genes cause USH1, some missense mutations of the same genes cause nonsyndromic deafness. These observations suggest that partial or low level activity of the encoded proteins may be sufficient for normal retinal function, although not for normal hearing. In individuals with USH1 due to nonsense mutations, interventions enabling partial translation of a full-length functional protein may delay the onset and/or progression of RP. One such possible therapeutic approach is suppression of nonsense mutations by small molecules such as aminoglycosides. We decided to test this approach as a potential therapy for RP in USH1 patients due to nonsense mutations. We initially focused on nonsense mutations of the PCDH15 gene, underlying USH1F. Here, we show suppression of several PCDH15 nonsense mutations, both in vitro and ex vivo. Suppression was achieved both by commercial aminoglycosides and by NB30, a new aminoglycoside-derivative developed by us. NB30 has reduced cytotoxicity in comparison to commercial aminoglycosides, and thus may be more efficiently used for therapeutic purposes. The research described here has important implications for the development of targeted interventions that are effective for patients with USH1 caused by various nonsense mutations.

Published

2007

19. Screening of the USH1G gene among Spanish patients with Usher syndrome. Lack of mutations and evidence of a minor role in the pathogenesis of the syndrome.

Author

Aller E, Jaijo T, Beneyto M, Nájera C, Morera C, Pérez-Garrigues H, Ayuso C, and Millán J

Subjects

Amino Acid Sequence, DNA Mutational Analysis, Humans, Molecular Sequence Data, Mutation, Spain, Usher Syndromes classification, Genetic Testing, Nerve Tissue Proteins genetics, Usher Syndromes genetics

Abstract

The Usher syndrome (USH) is an autosomal recessive hereditary disorder characterized by the association of sensorineural hearing loss, retinitis pigmentosa (RP) and, in some cases, vestibular dysfunction. The USH1G gene, encoding SANS, has been found to cause both Usher syndrome type I and atypical Usher syndrome. 109 Spanish unrelated patients suffering from Usher syndrome type I, type II, type III and unclassified Usher syndrome were screened for mutations in this gene, but only eight different changes without a clear pathogenic effect have been detected. Based on these results as well as previous studies in other populations where mutational analysis of this gene has been carried out, one can conclude that USH1G has a minor involvement in Usher syndrome pathogenesis.

Published

2007

20. The Usher lifestyle survey: maintaining independence: a multi-centre study.

Author

Damen GW, Krabbe PF, Kilsby M, and Mylanus EA

Subjects

Adult, Aging, Communication, Cross-Sectional Studies, Europe, Humans, Life Style, Middle Aged, Surveys and Questionnaires, Usher Syndromes classification, Activities of Daily Living, Disability Evaluation, Usher Syndromes rehabilitation

Abstract

Patients with Usher syndrome face a special set of challenges in order to maintain their independence when their sight and hearing worsen. Three different types of Usher (I, II and III) are distinguished by differences in onset, progression and severity of hearing loss, and by the presence or absence of balance problems. In this study 93 Usher patients from seven European countries filled out a questionnaire on maintaining independence (60 patients type I, 25 patients type II, four patients type III and four patients type unknown). Results of Usher type I and II patients are presented. Following the Nordic definition of maintaining independence in deaf-blindness, three domains are investigated: access to information, communication and mobility. Research variables in this study are: age and type of Usher, considered hearing loss- and the number of retinitis pigmentosa-related sight problems. Usher type I patients tend to need more help than Usher type II patients and the amount of help that they need grows when patients get older or when considered hearing loss worsens. No patterns in results were seen for the number of retinitis pigmentosa related sight problems.

Published

2005

21. Identification of a rat model for usher syndrome type 1B by N-ethyl-N-nitrosourea mutagenesis-driven forward genetics.

Author

Smits BM, Peters TA, Mul JD, Croes HJ, Fransen JA, Beynon AJ, Guryev V, Plasterk RH, and Cuppen E

Subjects

Animals, Chromosome Disorders, Codon, Terminator, Dyneins genetics, Genes, Recessive, Genetic Linkage, Humans, Male, Myosin VIIa, Myosins genetics, Point Mutation, Polymorphism, Single Nucleotide, Rats, Rats, Wistar, Usher Syndromes classification, Disease Models, Animal, Ethylnitrosourea pharmacology, Mutagenesis, Mutagens pharmacology, Usher Syndromes genetics

Abstract

The rat is the most extensively studied model organism and is broadly used in biomedical research. Current rat disease models are selected from existing strains and their number is thereby limited by the degree of naturally occurring variation or spontaneous mutations. We have used ENU mutagenesis to increase genetic variation in laboratory rats and identified a recessive mutant, named tornado, showing aberrant circling behavior, hyperactivity, and stereotypic head shaking. More detailed analysis revealed profound deafness due to disorganization and degeneration of the organ of Corti that already manifests at the onset of hearing. We set up a single nucleotide polymorphism (SNP)-based mapping strategy to identify the affected gene, revealing strong linkage to the central region of chromosome 1. Candidate gene resequencing identified a point mutation that introduces a premature stopcodon in Myo7a. Mutations in human MYO7A result in Usher syndrome type 1B, a severe autosomal inherited recessive disease that involves deafness and vestibular dysfunction. Here, we present the first characterized rat model for this disease. In addition, we demonstrate proof of principle for the generation and cloning of human disease models in rat using ENU mutagenesis, providing good perspectives for systematic phenotypic screens in the rat.

Published

2005