Your search keyword '"DFNB4"' showing total 48 results

1. Functional Studies of Deafness-Associated Pendrin and Prestin Variants.

Author

Takahashi, Satoe, Kojima, Takashi, Wasano, Koichiro, and Homma, Kazuaki

Subjects

*ION transport (Biology), *MEMBRANE proteins, *MISSENSE mutation, *BINDING sites, *HEARING disorders

Abstract

Pendrin and prestin are evolutionary-conserved membrane proteins that are essential for normal hearing. Dysfunction of these proteins results in hearing loss in humans, and numerous deafness-associated pendrin and prestin variants have been identified in patients. However, the pathogenic impacts of many of these variants are ambiguous. Here, we report results from our ongoing efforts to experimentally characterize pendrin and prestin variants using in vitro functional assays. With previously established fluorometric anion transport assays, we determined that many of the pendrin variants identified on transmembrane (TM) 10, which contains the essential anion binding site, and on the neighboring TM9 within the core domain resulted in impaired anion transport activity. We also determined the range of functional impairment in three deafness-associated prestin variants by measuring nonlinear capacitance (NLC), a proxy for motor function. Using the results from our functional analyses, we also evaluated the performance of AlphaMissense (AM), a computational tool for predicting the pathogenicity of missense variants. AM prediction scores correlated well with our experimental results; however, some variants were misclassified, underscoring the necessity of experimentally assessing the effects of variants. Together, our experimental efforts provide invaluable information regarding the pathogenicity of deafness-associated pendrin and prestin variants. [ABSTRACT FROM AUTHOR]

Published

2024

2. Single-cell RNA-sequencing of stria vascularis cells in the adult Slc26a4-/- mouse.

Author

Koh, Jin-Young, Affortit, Corentin, Ranum, Paul T., West, Cody, Walls, William D., Yoshimura, Hidekane, Shao, Jian Q., Mostaert, Brian, and Smith, Richard J.H.

Subjects

*COATED vesicles, *RNA sequencing, *GENE expression profiling, *ADAPTOR proteins, *CELL separation, *INNER ear, *OCHRATOXINS

Abstract

Background: The primary pathological alterations of Pendred syndrome are endolymphatic pH acidification and luminal enlargement of the inner ear. However, the molecular contributions of specific cell types remain poorly characterized. Therefore, we aimed to identify pH regulators in pendrin-expressing cells that may contribute to the homeostasis of endolymph pH and define the cellular pathogenic mechanisms that contribute to the dysregulation of cochlear endolymph pH in Slc26a4−/− mice. Methods: We used single-cell RNA sequencing to identify both Slc26a4-expressing cells and Kcnj10-expressing cells in wild-type (WT, Slc26a4+/+) and Slc26a4−/− mice. Bioinformatic analysis of expression data confirmed marker genes defining the different cell types of the stria vascularis. In addition, specific findings were confirmed at the protein level by immunofluorescence. Results: We found that spindle cells, which express pendrin, contain extrinsic cellular components, a factor that enables cell-to-cell communication. In addition, the gene expression profile informed the pH of the spindle cells. Compared to WT, the transcriptional profiles in Slc26a4−/− mice showed downregulation of extracellular exosome-related genes in spindle cells. Immunofluorescence studies in spindle cells of Slc26a4−/− mice validated the increased expression of the exosome-related protein, annexin A1, and the clathrin-mediated endocytosis-related protein, adaptor protein 2. Conclusion: Overall, cell isolation of stria vascularis from WT and Slc26a4−/− samples combined with cell type-specific transcriptomic analyses revealed pH-dependent alternations in spindle cells and intermediate cells, inspiring further studies into the dysfunctional role of stria vascularis cells in SLC26A4-related hearing loss. [ABSTRACT FROM AUTHOR]

Published

2023

3. Analysis of SLC26A4, FOXI1, and KCNJ10 Gene Variants in Patients with Incomplete Partition of the Cochlea and Enlarged Vestibular Aqueduct (EVA) Anomalies.

Author

Klarov, Leonid A., Pshennikova, Vera G., Romanov, Georgii P., Cherdonova, Aleksandra M., Solovyev, Aisen V., Teryutin, Fedor M., Luginov, Nikolay V., Kotlyarov, Petr M., and Barashkov, Nikolay A.

Subjects

*INNER ear, *GENETIC variation, *COCHLEA, *HEREDITY, *AQUEDUCTS, *ARNOLD-Chiari deformity, *COCHLEAR implants

Abstract

Pathogenic variants in the SLC26A4, FOXI1, and KCNJ10 genes are associated with hearing loss (HL) and specific inner ear abnormalities (DFNB4). In the present study, phenotype analyses, including clinical data collection, computed tomography (CT), and audiometric examination, were performed on deaf individuals from the Sakha Republic of Russia (Eastern Siberia). In cases with cochleovestibular malformations, molecular genetic analysis of the coding regions of the SLC26A4, FOXI1, and KCNJ10 genes associated with DFNB4 was completed. In six of the 165 patients (3.6%), CT scans revealed an incomplete partition of the cochlea (IP-1 and IP-2), in isolation or combined with an enlarged vestibular aqueduct (EVA) anomaly. Sequencing of the SLC26A4, FOXI1, and KCNJ10 genes was performed in these six patients. In the SLC26A4 gene, we identified four variants, namely c.85G>C p.(Glu29Gln), c.757A>G p.(Ile253Val), c.2027T>A p.(Leu676Gln), and c.2089+1G>A (IVS18+1G>A), which are known as pathogenic, as well as c.441G>A p.(Met147Ile), reported previously as a variant with uncertain significance. Using the AlphaFold algorithm, we found in silico evidence of the pathogenicity of this variant. We did not find any causative variants in the FOXI1 and KCNJ10 genes, nor did we find any evidence of digenic inheritance associated with double heterozygosity for these genes with monoallelic SLC26A4 variants. The contribution of biallelic SLC26A4 variants in patients with IP-1, IP-2, IP-2+EVA, and isolated EVA was 66.7% (DFNB4 in three patients, Pendred syndrome in one patient). Seventy-five percent of SLC26A4-biallelic patients had severe or profound HL. The morphology of the inner ear anomalies demonstrated that, among SLC26A4-biallelic patients, all types of incomplete partition of the cochlea are possible, from IP-1 and IP-2, to a normal cochlea. However, the dominant type of anomaly was IP-2+EVA (50.0%). This finding is very important for cochlear implantation, since the IP-2 anomaly does not have an increased risk of "gushers" and recurrent meningitis. [ABSTRACT FROM AUTHOR]

Published

2022

4. SLC26A4 Phenotypic Variability Influences Intra- and Inter-Familial Diagnosis and Management.

Author

Tawalbeh, Mohamed, Aburizeg, Dunia, Abu Alragheb, Bayan O., Alaqrabawi, Wala Sami, Dardas, Zain, Srour, Luma, Altarayra, Baraah Hatem, Zayed, Ayman A., El Omari, Zaid, and Azab, Bilal

Subjects

*PHENOTYPIC plasticity, *SENSORINEURAL hearing loss, *TEMPORAL bone, *GENETIC variation, *COMPUTED tomography

Abstract

SLC26A4 is one of the most common genes causing autosomal recessive non-syndromic sensorineural hearing loss (SNHL). It has been reported to cause Pendred Syndrome (PDS) and DFNB4 which is deafness with enlarged vestibular aqueduct (EVA). However, mutated SLC26A4 is not conclusive for having either DFNB4 or PDS. Three unrelated Jordanian families consisting of eight affected individuals with congenital bilateral hearing loss (HL) participated in this study. Whole-exome and Sanger sequencing were performed to investigate the underlying molecular etiology of HL. Further clinical investigations, including laboratory blood workup for the thyroid gland, CT scan for the temporal bone, and thyroid ultrasound were performed. Three disease-causing variants were identified in SLC26A4 in the three families, two of which were novel. Two families had a novel pathogenic homozygous splice-site accepter variant (c.165-1G>C), while the third family had compound heterozygous pathogenic variants (c.1446G>A; p.Trp482* and c.304G>A; p.Gly102Arg). Our approach helped in redirecting the diagnosis of several affected members of three different families from non-syndromic HL to syndromic HL. Two of the affected individuals had typical PDS, one had DFNB4, while the rest had atypical PDS. Our work emphasized the intra- and inter-familial variability of SLC26A4-related phenotypes. In addition, we highlighted the variable phenotypic impact of SLC26A4 on tailoring a personalized healthcare management. [ABSTRACT FROM AUTHOR]

Published

2022

5. Molecular Features of SLC26A4 Common Variant p.L117F.

Author

Matulevičius, Arnoldas, Bernardinelli, Emanuele, Brownstein, Zippora, Roesch, Sebastian, Avraham, Karen B., and Dossena, Silvia

Subjects

*ION transport (Biology), *JEWISH communities, *ENDOPLASMIC reticulum, *GENE frequency, *CONFOCAL microscopy

Abstract

The SLC26A4 gene, which encodes the anion exchanger pendrin, is involved in determining syndromic (Pendred syndrome) and non-syndromic (DFNB4) autosomal recessive hearing loss. SLC26A4 c.349C>T, p.L117F is a relatively common allele in the Ashkenazi Jewish community, where its minor allele frequency is increased compared to other populations. Although segregation and allelic data support the pathogenicity of this variant, former functional tests showed characteristics that were indistinguishable from those of the wild-type protein. Here, we applied a triad of cell-based assays, i.e., measurement of the ion transport activity by a fluorometric method, determination of the subcellular localization by confocal microscopy, and assessment of protein expression levels, to conclusively assign or exclude the pathogenicity of SLC26A4 p.L117F. This protein variant showed a moderate, but significant, reduction in ion transport function, a partial retention in the endoplasmic reticulum, and a strong reduction in expression levels as a consequence of an accelerated degradation by the Ubiquitin Proteasome System, all supporting pathogenicity. The functional and molecular features of human pendrin p.L117F were recapitulated by the mouse ortholog, thus indicating that a mouse carrying this variant might represent a good model of Pendred syndrome/DFNB4. [ABSTRACT FROM AUTHOR]

Published

2022

6. Genetic Determinants of Non-Syndromic Enlarged Vestibular Aqueduct: A Review

Author

Sebastian Roesch, Gerd Rasp, Antonio Sarikas, and Silvia Dossena

Subjects

enlarged vestibular aqueduct, pendrin (SLC26A4), hearing loss, genetic testing, DFNB4, Otorhinolaryngology, RF1-547

Abstract

Hearing loss is the most common sensorial deficit in humans and one of the most common birth defects. In developed countries, at least 60% of cases of hearing loss are of genetic origin and may arise from pathogenic sequence alterations in one of more than 300 genes known to be involved in the hearing function. Hearing loss of genetic origin is frequently associated with inner ear malformations; of these, the most commonly detected is the enlarged vestibular aqueduct (EVA). EVA may be associated to other cochleovestibular malformations, such as cochlear incomplete partitions, and can be found in syndromic as well as non-syndromic forms of hearing loss. Genes that have been linked to non-syndromic EVA are SLC26A4, GJB2, FOXI1, KCNJ10, and POU3F4. SLC26A4 and FOXI1 are also involved in determining syndromic forms of hearing loss with EVA, which are Pendred syndrome and distal renal tubular acidosis with deafness, respectively. In Caucasian cohorts, approximately 50% of cases of non-syndromic EVA are linked to SLC26A4 and a large fraction of patients remain undiagnosed, thus providing a strong imperative to further explore the etiology of this condition.

Published

2021

7. Interpreting pendred syndrome as a foetal hydrops: Clinical and animal model evidence.

Author

Simon, François, Denoyelle, Françoise, and Beraneck, Mathieu

Subjects

*EDEMA, *ANIMAL models in research, *LABORATORY mice, *MENIERE'S disease, *HEARING disorders, *HYDROPS fetalis

Abstract

BACKGROUND: Menière disease (MD) and SLC26A4 related deafness (Pendred syndrome (PS) or DFNB4) are two different inner ear disorders which present with fluctuating and progressive hearing loss, which could be a direct consequence of endolymphatic hydrops. OBJECTIVE: To present similarities between both pathologies and explore how the concept of hydrops may be applied to PS/DFNB4. METHODS: Review of the literature on MD, PS/DFNB4 and mouse model of PS/DFNB4. RESULTS: MD and PS/DFNB4 share a number of similarities such as fluctuating and progressive hearing loss, acute episodes with vertigo and tinnitus, MRI and histological evidence of endolymphatic hydrops (although with different underlying mechanisms). MD is usually diagnosed during the fourth decade of life whereas PS/DFNB4 is congenital. The PS/DFNB4 mouse models have shown that biallelic slc26a4 mutations lead to Na+ and water retention in the endolymph during the perinatal period, which in turn induces degeneration of the stria vascularis and hearing loss. Crossing clinical/imagery characteristics and animal models, evidence seems to support the hypothesis of PS being a foetal hydrops. CONCLUSIONS: When understanding PS/DFNB4 as a developmental hydrops, treatments used in MD could be repositioned to PS. [ABSTRACT FROM AUTHOR]

Published

2021

8. Genetic Determinants of Non-Syndromic Enlarged Vestibular Aqueduct: A Review.

Author

Roesch, Sebastian, Rasp, Gerd, Sarikas, Antonio, and Dossena, Silvia

Subjects

CONGENITAL disorders, AQUEDUCTS, HEARING disorders, INNER ear, HUMAN abnormalities, DEVELOPED countries, VESTIBULO-ocular reflex, RECESSIVE genes

Abstract

Hearing loss is the most common sensorial deficit in humans and one of the most common birth defects. In developed countries, at least 60% of cases of hearing loss are of genetic origin and may arise from pathogenic sequence alterations in one of more than 300 genes known to be involved in the hearing function. Hearing loss of genetic origin is frequently associated with inner ear malformations; of these, the most commonly detected is the enlarged vestibular aqueduct (EVA). EVA may be associated to other cochleovestibular malformations, such as cochlear incomplete partitions, and can be found in syndromic as well as non-syndromic forms of hearing loss. Genes that have been linked to non-syndromic EVA are SLC26A4, GJB2, FOXI1, KCNJ10, and POU3F4. SLC26A4 and FOXI1 are also involved in determining syndromic forms of hearing loss with EVA, which are Pendred syndrome and distal renal tubular acidosis with deafness, respectively. In Caucasian cohorts, approximately 50% of cases of non-syndromic EVA are linked to SLC26A4 and a large fraction of patients remain undiagnosed, thus providing a strong imperative to further explore the etiology of this condition. [ABSTRACT FROM AUTHOR]

Published

2021

9. SLC26A4-linked CEVA haplotype correlates with phenotype in patients with enlargement of the vestibular aqueduct

Author

Janet R. Chao, Parna Chattaraj, Tina Munjal, Keiji Honda, Kelly A. King, Christopher K. Zalewski, Wade W. Chien, Carmen C. Brewer, and Andrew J. Griffith

Subjects

Deafness, DFNB4, Haplotype, Hearing, Noncoding, Pendred syndrome, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Recessive mutations of coding regions and splice sites of the SLC26A4 gene cause hearing loss with enlargement of the vestibular aqueduct (EVA). Some patients also have a thyroid iodination defect that can lead to multinodular goiter as part of Pendred syndrome. A haplotype of variants upstream of SLC26A4, called CEVA, acts as a pathogenic recessive allele in trans to mutations affecting the coding regions or splice sites of SLC26A4. Our first hypothesis is that CEVA, acting as a pathogenic recessive allele, is correlated with a less severe phenotype than mutations affecting the coding regions and splice sites of SLC26A4. Our second hypothesis is that CEVA acts as a modifier of the phenotype in patients with EVA caused by mutations affecting the coding regions or splice sites of both alleles of SLC26A4 or EVA caused by other factors. Methods This was a prospective cohort study of 114 individuals and 202 ears with EVA. To test our first hypothesis, we compared the thyroid and auditory phenotypes of subjects with mutations affecting coding regions of both alleles of SLC26A4 with those of subjects carrying CEVA in trans to mutations affecting the coding regions. To test our second hypothesis, we compared the phenotypes associated with the presence versus absence of CEVA among subjects with no coding region mutations, as well as among subjects with mutations affecting coding regions of both alleles. Results Subjects carrying CEVA in trans to a mutation of SLC26A4 have a normal thyroid phenotype and less severe hearing loss in comparison to individuals with mutations affecting coding regions of both alleles of SLC26A4. In subjects with no mutant alleles of SLC26A4, hearing loss was more severe in subjects who carry the CEVA haplotype in comparison to non-carriers. There was no correlation of CEVA with the phenotype of subjects with mutations affecting coding regions of both alleles. Conclusions CEVA, acting as a likely pathogenic recessive allele, is associated with a less severe phenotype than alleles with a mutation affecting the coding regions or splice sites of SLC26A4. CEVA may act as a genetic modifier in patients with EVA caused by other factors.

Published

2019

10. Effect of Cochlear Implantation on Hearing Fluctuation in Patients with Biallelic SLC26A4 Variants.

Author

Na, Gina, Lee, Jeon Mi, Lee, Hyun Jin, Jeong, Yeonsu, Jung, Jinsei, and Choi, Jae Young

Abstract

Introduction: Fluctuating hearing loss is a distinctive feature caused by SLC26A4 variants. We investigated whether cochlear implantation had protective or deleterious effect on hearing fluctuation in patients with biallelic SLC26A4 variants.Methods: Patients with biallelic SLC26A4 variants (N = 16; age = 10.24 ± 9.20 years) who had unilateral cochlear implantation and consecutive postsurgical, bilateral pure-tone audiograms more than 3 times were selected. We retrospectively reviewed the patients' medical records from 2008 to 2019 obtained from a tertiary medical center and used the auditory threshold change (Shift) over time as a marker of hearing fluctuation. Fluctuation events were counted, and the Shift of the implanted and contralateral ears was compared using logistic regression with a generalized estimating equation and linear mixed model. A total of 178 values were included.Results: The odds of fluctuating hearing frequency were 11.185-fold higher in the unimplanted ears than in the implanted ears postoperatively (p = 0.001). The extent of fluctuation at 250 and 500 Hz was also significantly lower in the implanted ears than in the unimplanted ears after adjusting for every other effect (p = 0.003 and p < 0.001, respectively). Notably, higher residual hearing was rather associated with lesser fluctuation in frequency and the extent of fluctuation at 500 Hz, indicating residual hearing function is not the positive predictor for hearing fluctuation.Conclusion: In patients with biallelic SLC26A4 variants, cochlear implantation may reduce the frequency and extent of hearing fluctuations. [ABSTRACT FROM AUTHOR]

Published

2021

11. Contribution of SLC26A4 to the molecular diagnosis of nonsyndromic prelingual sensorineural hearing loss in a Brazilian cohort

Author

Simone da Costa e Silva Carvalho, Carlos Henrique Paiva Grangeiro, Clarissa Gondim Picanço-Albuquerque, Thaís Oliveira dos Anjos, Greice Andreotti De Molfetta, Wilson Araujo Silva, and Victor Evangelista de Faria Ferraz

Subjects

Nonsyndromic hearing loss, SLC26A4, Mutation screening, DFNB4, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objective Hereditary hearing loss (HL) is the most common sensorineural disorder in humans. Besides mutations in GJB2 and GJB6 genes, pathogenic variants in the SLC26A4 gene have been reported as a cause of hereditary HL due to its role in the physiology of the inner ear. In this research we wanted to investigate the prevalence of mutations in SLC26A4 in Brazilian patients with nonsyndromic prelingual sensorineural HL. We applied the high-resolution melting technique to screen 88 DNA samples from unrelated deaf individuals that were previously screened for GJB2, GJB6 and MT-RNR1 mutations. Results The frequency of mutations in the SLC26A4 gene was 28.4%. Two novel mutations were found: p.Ile254Val and p.Asn382Lys. The mutation c.-66C>G (rs17154282) in the promoter region of SLC26A4, was the most frequent mutation found and was significantly associated with nonsyndromic prelingual sensorineural HL. After mutations in the GJB2, GJB6 and mitochondrial genes, SLC26A4 mutations are considered the next most common cause of hereditary HL in Brazilian as well as in other populations, which corroborates with our data. Furthermore, we suggest the inclusion of the SCL26A4 gene in the investigation of hereditary HL since there was an increase in the frequency of the mutations found, up to 22.7%.

Published

2018

12. Pendrin-Linked Deafness in Humans

Author

Roesch, Sebastian, Tóth, Miklós, Rasp, Gerd, Dossena, Silvia, editor, and Paulmichl, Markus, editor

Published

2017

13. Genetic analysis of SLC26A4 gene (pendrin) related deafness among a cohort of assortative mating families from southern India.

Author

Chandru, Jayasankaran, Jeffrey, Justin Margret, Pavithra, Amritkumar, Vanniya, S. Paridhy, Devi, G. Nandhini, Mahalingam, Subathra, Karthikeyen, Natarajan Padmavathy, and Srisailapathy, C. R. Srikumari

Subjects

*ASSORTATIVE mating, *DEAFNESS, *GENE frequency, *GENES, *RECESSIVE genes, *HEARING impaired

Abstract

Purpose: Assortative mating (AM) or preferential mating is known to influence the genetic architecture of the hearing-impaired (HI) population. AM is now seen as a universal phenomenon with individuals seeking partners based on quantitative, qualitative, and behavioral phenotypes. However, the molecular genetic dynamics of AM among the HI tested in real time are limited to the DFNB1 locus. Methods: A total of 113 HI partners from 82 South Indian families (52 deaf marrying deaf and 30 deaf marrying normal), previously excluded for DFNB1 (GJB2/6) etiology, were screened for SLC26A4 gene (DFNB4) variants. Results: A spectrum of seven pathogenic variants viz., p.S90L, p.V239D, p.V359E, p.Gly389Trpfs*79 (novel), p.T410M, p.N457K and p.K715N were identified. The pathogenic allele frequency of SLC26A4 variants identified in this study was 3.98% (9/226). Conclusion: We recommend a preliminary screening of mutational hotspots for future investigations to rapidly test for its recurrence among South Indian HI population. This will be the first study to comprehensively account for the incidence of SLC26A4 gene variants and the real-time dynamics of DFNB4 variants among this type of a HI cohort. [ABSTRACT FROM AUTHOR]

Published

2020

14. Different Rates of the SLC26A4-Related Hearing Loss in Two Indigenous Peoples of Southern Siberia (Russia)

Author

Valeriia Yu. Danilchenko, Marina V. Zytsar, Ekaterina A. Maslova, Marita S. Bady-Khoo, Nikolay A. Barashkov, Igor V. Morozov, Alexander A. Bondar, and Olga L. Posukh

Subjects

hearing loss, genetic diagnosis, SLC26A4, DFNB4, Tuvinians, Altaians, Medicine (General), R5-920

Abstract

Hereditary hearing loss (HL) is known to be highly locus/allelic heterogeneous, and the prevalence of different HL forms significantly varies among populations worldwide. Investigation of region-specific landscapes of hereditary HL is important for local healthcare and medical genetic services. Mutations in the SLC26A4 gene leading to nonsyndromic recessive deafness (DFNB4) and Pendred syndrome are common genetic causes of hereditary HL, at least in some Asian populations. We present for the first time the results of a thorough analysis of the SLC26A4 gene by Sanger sequencing in the large cohorts of patients with HL of unknown etiology belonging to two neighboring indigenous Turkic-speaking Siberian peoples (Tuvinians and Altaians). A definite genetic diagnosis based on the presence of biallelic SLC26A4 mutations was established for 28.2% (62/220) of all enrolled Tuvinian patients vs. 4.3% (4/93) of Altaian patients. The rate of the SLC26A4-related HL in Tuvinian patients appeared to be one of the highest among populations worldwide. The SLC26A4 mutational spectrum was characterized by the presence of Asian-specific mutations c.919-2A>G and c.2027T>A (p.Leu676Gln), predominantly found in Tuvinian patients, and c.2168A>G (p.His723Arg), which was only detected in Altaian patients. In addition, a novel pathogenic variant c.1545T>G (p.Phe515Leu) was found with high frequency in Tuvinian patients. Overall, based on the findings of this study and our previous research, we were able to uncover the genetic causes of HL in 50.5% of Tuvinian patients and 34.5% of Altaian patients.

Published

2021

15. A Novel Frameshift Mutation of in a Korean Family With Nonsyndromic Hearing Loss and Enlarged Vestibular Aqueduct

Author

Borum Sagong, Jeong-In Baek, Kyu-Yup Lee, and Un-Kyung Kim

Subjects

DFNB4, Hearing Loss, Enlarged Vestibular Aqueduct, Novel Mutation, Medicine, Otorhinolaryngology, RF1-547

Abstract

Objectives We aimed to identify the causative mutation for siblings in a Korean family with nonsyndromic hearing loss (HL) and enlarged vestibular aqueduct (EVA). The siblings were a 19-year-old female with bilateral profound HL and an 11-year-old male with bilateral moderately severe HL. Methods We extracted genomic DNA from blood samples of the siblings with HL, their parents, and 100 controls. We performed mutation analysis for SLC26A4 using direct sequencing. Results The two siblings were compound heterozygotes with the novel mutation p.I713LfsX8 and the previously described mutation p.H723R. Their parents had heterozygous mono-allelic mutations. Father had p.I713LfsX8 mutation as heterozygous, and mother had p.H723R mutation as heterozygous. However, novel mutation p.I713LfsX8 was not detected in 100 unrelated controls. Conclusion Both mutations identified in this study were located in the sulfate transporter and anti-sigma factor antagonist domain, the core region for membrane targeting of SulP/SLC26 anion transporters, which strongly suggests that failure in membrane trafficking by SLC26A4 is a direct cause of HL in this family. Our study could therefore provide a foundation for further investigations elucidating the SLC26A4-related mechanisms of HL.

Published

2017

16. Systematic quantification of the anion transport function of pendrin (SLC26A4) and its disease‐associated variants.

Author

Wasano, Koichiro, Takahashi, Satoe, Rosenberg, Samuel K., Kojima, Takashi, Mutai, Hideki, Matsunaga, Tatsuo, Ogawa, Kaoru, and Homma, Kazuaki

Abstract

Thanks to the advent of rapid DNA sequencing technology and its prevalence, many disease‐associated genetic variants are rapidly identified in many genes from patient samples. However, the subsequent effort to experimentally validate and define their pathological roles is extremely slow. Consequently, the pathogenicity of most disease‐associated genetic variants is solely speculated in silico, which is no longer deemed compelling. We developed an experimental approach to efficiently quantify the pathogenic effects of disease‐associated genetic variants with a focus on SLC26A4, which is essential for normal inner ear function. Alterations of this gene are associated with both syndromic and nonsyndromic hereditary hearing loss with various degrees of severity. We established HEK293T‐based stable cell lines that express pendrin missense variants in a doxycycline‐dependent manner, and systematically determined their anion transport activities with high accuracy in a 96‐well plate format using a high throughput plate reader. Our doxycycline dosage‐dependent transport assay objectively distinguishes missense variants that indeed impair the function of pendrin from those that do not (functional variants). We also found that some of these putative missense variants disrupt normal messenger RNA splicing. Our comprehensive experimental approach helps determine the pathogenicity of each pendrin variant, which should guide future efforts to benefit patients. [ABSTRACT FROM AUTHOR]

Published

2020

17. Association of SLC26A4 mutations, morphology, and hearing in pendred syndrome and NSEVA.

Author

Mey, Kristianna, Muhamad, Ali A., Tranebjærg, Lisbeth, Rendtorff, Nanna D., Rasmussen, Stig H., Bille, Michael, Cayé‐Thomasen, Per, Tranebjaerg, Lisbeth, and Cayé-Thomasen, Per

Abstract

Objective: To investigate the relations of monoallelic (M1), biallelic (M2), or the absence of mutations (M0) in SLC26A4 to inner ear morphology and hearing levels in individuals with Pendred syndrome (PS) or nonsyndromic enlarged vestibular aqueduct (NSEVA) associated with hearing loss.Methods: In a cohort of 139 PS/NSEVA individuals, 115 persons from 95 unrelated families had full genetic sequencing of SLC26A4, and 113 had retrievable images for re-assessment of inner ear morphology. The association between the number of mutant alleles in SLC26A4, inner ear morphology (including endolymphatic sac size and protein content on magnetic resonance imaging), and hearing level (pure tone average) was explored.Results: Biallelic SLC26A4 mutations (M2) occurred in three-quarters of the cohort and was invariably associated with poor hearing; in 87%, it was associated with incomplete partition type II of the cochlea as well as enlarged endolymphatic sac and vestibular aqueduct. M1 or M0 individuals exhibited a greater variability in inner ear morphology. Endolymphatic sac size and presence of "high-protein" sac contents were significantly higher in M2 individuals compared to M1 and M0 individuals.Conclusion: The number of SLC26A4 mutations is associated with severity and variability of inner ear morphology and hearing level in individuals with PS or NSEVA. M2 individuals have poorer hearing and present largely incomplete partition type II of the cochleas with enlarged endolymphatic sacs, whereas individuals with M1 and no detectable SLC26A4 mutations have less severe hearing loss and more diverse inner ear morphology.Level Of Evidence: 4. Laryngoscope, 129:2574-2579, 2019. [ABSTRACT FROM AUTHOR]

Published

2019

18. SLC26A4 Pathogenic Variants as a Third Cause of Hearing Loss: Role of Three Exons in DFNB4 Deafness in Iran.

Author

Davoudi-Dehaghani, Elham, Mahdieh, Nejat, Shirkavand, Atefeh, Bagherian, Hamideh, DabbaghBagheri, Samira, and Zeinali, Sirous

Subjects

*HEARING disorders, *MICROSATELLITE repeats, *GENETIC testing, *HOMOZYGOSITY

Abstract

Context: Pathogenic variants in SLC26A4 gene are the third-most frequent cause of autosomal recessive hearing loss in different populations. Aims: This article reports results of homozygosity mapping and SLC26A4 variant analysis in Iran. Settings and Design: A case series study was performed on forty GJB2-negative Iranian deaf families. Subjects and Methods: Homozygosity mapping, using microsatellite markers flanking the SLC26A4 gene, was performed on GJB2-negative Iranian deaf families. The SLC26A4 variant analysis was done by Sanger sequencing. A literature review was performed to identify all reported SLC26A4 pathogenic variants in Iran. Results: In one of the families, the hearing loss showed co-segregation with the DFNB4 STR markers. A previously reported SLC26A4 pathogenic variant was identified in homozygous state in all the affected members of this family. The literature review showed that variant screening of only three SLC26A4 exons and their boundary regions can detect variants responsible for deafness in about half of all DFNB4 Iranian deaf cases. Conclusions: The results of this study emphasize the important role of SLC26A4 pathogenic variants in the development of deafness in Iran. More information on the frequency of pathogenic variants can help in choosing faster and cost-effective methods for genetic testing. [ABSTRACT FROM AUTHOR]

Published

2019

19. Novel small molecule-mediated restoration of the surface expression and anion exchange activity of mutated pendrin causing Pendred syndrome and DFNB4.

Author

Jung, Jinsei, Noh, Shin Hye, Jo, Sungwoo, Song, Doona, Kang, Min Jin, Shin, Mi Hwa, Lee, Hyun Jae, Pyun, Jae-Chul, Namkung, Wan, Han, Gyoonhee, Lee, Min Goo, and Choi, Jae Young

Subjects

*GENE expression, *SMALL molecules, *GENETIC variation, *HIGH throughput screening (Drug development), *SYNDROMES, *VESTIBULAR apparatus diseases

Abstract

Variants in SLC26A4 (pendrin) are the most common reasons for genetic hearing loss and vestibular dysfunction in East Asians. In patients with Pendred syndrome and DFNB4 (autosomal recessive type of genetic hearing loss 4), caused by variants in SLC26A4 , the hearing function is residual at birth and deteriorates over several years, with no curative treatment for these disorders. In the present study, we revealed that a novel small molecule restores the expression and function of mutant pendrin. High-throughput screening of 54,000 small molecules was performed. We observed that pendrin corrector (PC2–1) increased the surface expression and anion exchange activity of p.H723R pendrin (H723R-PDS), the most prevalent genetic variant that causes Pendred syndrome and DFNB4. Furthermore, in endogenous H723R-PDS-expressing human nasal epithelial cells, PC2–1 significantly increased the surface expression of pendrin. PC2–1 exhibited high membrane permeability in vitro and high micromolar concentrations in the cochlear perilymph in vivo. In addition, neither inhibition of Kv11.1 activity in the human ether-a-go-go-related gene assay nor cell toxicity in the cell proliferation assay was observed at a high PC2–1 concentration (30 μM). These preclinical data support the hypothesis of the druggability of mutant pendrin using the novel corrector molecule PC2–1. In conclusion, PC2–1 may be a new therapeutic molecule for ameliorating hearing loss and treating vestibular disorders in patients with Pendred syndrome or DFNB4. [ABSTRACT FROM AUTHOR]

Published

2023

20. Internal interaction changes within the mutation of SLC26A4 STAS domain.

Author

Kim, Jae In, Chang, Hyunjoon, Lee, Myeongsang, and Na, Sungsoo

Subjects

*PENDRED syndrome, *GENETIC mutation, *PROTEIN structure, *PROTEIN conformation, *MOLECULAR dynamics

Abstract

Graphical abstract Highlights • Wildtype and six mutated SLC26A4 STAS domains were designed using homology modeling. • STAS domain models were stabilized using 100–150 ns molecular dynamics simulation. • Cross-correlation weighted contact map revealed interaction-based contacts. • Network analysis revealed secondary structure communications within the STAS domain. • α2, α3, and β2-β3 were mostly involved in secondary structure communication change. Abstract Pendrin (SLC26A4) is a protein associated with the auditory system. Pendred syndrome (PDS) and DFNB4 are typical auditory disorders caused by mutations in the SLC26A4 STAS domain. We generated an SLC26A4 STAS domain model and six mutated STAS domain models related to PDS, DFNB4, and PDS/DFNB4 by homology modeling. Molecular dynamics simulation was performed to find the equilibration conformation and fluctuation information. Using fluctuation information, we calculated betweenness centrality and edge betweenness to reveal communication between secondary structures of STAS domain. The edge betweenness results showed that mutated models generate communication signals that are less clear than WT models. [ABSTRACT FROM AUTHOR]

Published

2018

21. Molecular Features of SLC26A4 Common Variant p.L117F

Author

Arnoldas Matulevičius, Emanuele Bernardinelli, Zippora Brownstein, Sebastian Roesch, Karen B. Avraham, and Silvia Dossena

Subjects

hearing loss, SLC26A4, pendrin, DFNB4, Pendred syndrome, functional testing, General Medicine

Abstract

The SLC26A4 gene, which encodes the anion exchanger pendrin, is involved in determining syndromic (Pendred syndrome) and non-syndromic (DFNB4) autosomal recessive hearing loss. SLC26A4 c.349C>T, p.L117F is a relatively common allele in the Ashkenazi Jewish community, where its minor allele frequency is increased compared to other populations. Although segregation and allelic data support the pathogenicity of this variant, former functional tests showed characteristics that were indistinguishable from those of the wild-type protein. Here, we applied a triad of cell-based assays, i.e., measurement of the ion transport activity by a fluorometric method, determination of the subcellular localization by confocal microscopy, and assessment of protein expression levels, to conclusively assign or exclude the pathogenicity of SLC26A4 p.L117F. This protein variant showed a moderate, but significant, reduction in ion transport function, a partial retention in the endoplasmic reticulum, and a strong reduction in expression levels as a consequence of an accelerated degradation by the Ubiquitin Proteasome System, all supporting pathogenicity. The functional and molecular features of human pendrin p.L117F were recapitulated by the mouse ortholog, thus indicating that a mouse carrying this variant might represent a good model of Pendred syndrome/DFNB4.

Published

2022

22. Interpreting pendred syndrome as a foetal hydrops: Clinical and animal model evidence

Author

François Simon, Mathieu Beraneck, Françoise Denoyelle, Centre Neurosciences intégratives et Cognition (INCC - UMR 8002), and Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP)

Subjects

hydrops, Pathology, medicine.medical_specialty, Hearing loss, Endolymph, [SDV.NEU.NB]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Neurobiology, Hearing Loss, Sensorineural, Hydrops Fetalis, Mice, 03 medical and health sciences, 0302 clinical medicine, Animal model, Vertigo, otorhinolaryngologic diseases, medicine, DFNB4, Animals, Humans, Endolymphatic Hydrops, Inner ear, [SDV.MHEP.OS]Life Sciences [q-bio]/Human health and pathology/Sensory Organs, Endolymphatic hydrops, 030223 otorhinolaryngology, mouse, Pendred syndrome, biology, business.industry, General Neuroscience, medicine.disease, biology.organism_classification, Sensory Systems, 3. Good health, medicine.anatomical_structure, Menière, Otorhinolaryngology, Models, Animal, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, Tinnitus, pendred, Goiter, Nodular

Abstract

International audience; BACKGROUND: Menière disease (MD) and SLC26A4 related deafness (Pendred syndrome (PS) or DFNB4) are two different inner ear disorders which present with fluctuating and progressive hearing loss, which could be a direct consequence of endolymphatic hydrops. OBJECTIVE: To present similarities between both pathologies and explore how the concept of hydrops may be applied to PS/DFNB4. METHODS: Review of the literature on MD, PS/DFNB4 and mouse model of PS/DFNB4. RESULTS: MD and PS/DFNB4 share a number of similarities such as fluctuating and progressive hearing loss, acute episodes with vertigo and tinnitus, MRI and histological evidence of endolymphatic hydrops (although with different underlying mechanisms). MD is usually diagnosed during the fourth decade of life whereas PS/DFNB4 is congenital. The PS/DFNB4 mouse models have shown that biallelic slc26a4 mutations lead to Na+ and water retention in the endolymph during the perinatal period, which in turn induces degeneration of the stria vascularis and hearing loss. Crossing clinical/imagery characteristics and animal models, evidence seems to support the hypothesis of PS being a foetal hydrops. CONCLUSIONS: When understanding PS/DFNB4 as a developmental hydrops, treatments used in MD could be repositioned to PS.

Published

2021

23. Molecular characterization of autosomal recessive non syndromic hearing loss in selected families from District Mardan, Pakistan.

Author

Hussain, Shahid, Khan Khattak, Jabar Zaman, Ismail, Mohammad, Mansoor, Qaisar, and Haroon Khan, Mohammad

Abstract

Deafness is the most common sensory disorder, which affects 1/1000 neonates globally. Genetic factors are major contributors for hearing impairment. This study was conducted to explore the linkage of DFNB loci and their mutations with NSHL in selected Pakistani families. We included 10 families with history of deafness from district Mardan, Pakistan. Blood sample (5ml) along with personal and clinical information was collected from the available family members including both diseased and un-affected individuals. Genomic DNA was amplified using loci specific STR markers to investigate the linkage of DFNB loci. Family found linked with DFNB4 locus was screened for SLC26A4 mutations. One out of the ten explored families was found linked with DFNB4 locus which was further investigated for SLC26A4 gene mutation through direct DNA sequencing. Two novel mutations were observed in the studied family, one at splice donor site (164+2T>G) and the other at position 164+5C>G only in the affected members of the linked family. DFNB4 locus was found linked in the present study which harbors SLC26A4 gene. The novel mutation of SLC26A4 gene at the splice donor site results in skipping of the first coding exon and thus can lead to loss of expression of SLC26A4 product in the inner ear. [ABSTRACT FROM AUTHOR]

Published

2018

24. DNAJC14 Ameliorates Inner Ear Degeneration in the DFNB4 Mouse Model

Author

Jae Young Choi, Byunghwa Noh, Seong Kug Eo, Hye Ji Choi, Sushil Devkota, Hyunjae Lee, Min Goo Lee, Jin Young Choi, Han Woong Lee, Ik Hyun Jeon, and Jinsei Jung

Subjects

0301 basic medicine, Genetically modified mouse, pendrin, lcsh:QH426-470, Hearing loss, Pendred syndrome, H723R, KCNJ10, Article, 03 medical and health sciences, 0302 clinical medicine, flavivirus, unconventional secretion, Genetics, medicine, otorhinolaryngologic diseases, DFNB4, chaperone, Inner ear, Endolymphatic hydrops, lcsh:QH573-671, Molecular Biology, DNAJC14, biology, lcsh:Cytology, genetic hearing loss, Pendrin, slc26a4, medicine.disease, Cell biology, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Spiral ligament, biology.protein, Molecular Medicine, sense organs, medicine.symptom

Abstract

The His723Arg (H723R) mutation in SLC26A4, encoding pendrin, is the most prevalent mutation in East Asia, resulting in DFNB4, an autosomal recessive type of genetic hearing loss. Although the main pathological mechanism of H723R was identified as a protein-folding defect in pendrin, there is still no curative treatment for associated hearing loss. Here, we show that H723R-pendrin expression and activity are rescued by activation of the chaperonin DNAJC14. In vitro, DNAJC14 was activated via Japanese encephalitis virus (JEV) inoculation, and toxin-attenuated JEV rescued the surface expression and anion exchange activity of H723R-pendrin. Human H723R-pendrin transgenic mice (hH723R Tg) were established in a mouse slc26a4 knockout background, in which only hH723R-pendrin was expressed in the inner ear (Pax2-Cre dependent) to mimic human DFNB4 pathology. Crossing hH723R Tg with DNAJC14-overexpressing mice resulted in reduced cochlear hydrops and more preserved outer hair cells in the cochlea compared to those in hH723R Tg mice. Furthermore, the stria vascularis and spiral ligament were thicker and KCNJ10 expression was increased with DNAJC14 overexpression; however, hearing function and enlarged endolymphatic hydrops were not recovered. These results indicate that DNAJC14 overexpression ameliorates the cochlear degeneration caused by misfolded pendrin and might be a potential therapeutic target for DFNB4.

Published

2020

25. SLC26A4 genotypes associated with enlarged vestibular aqueduct malformation in south Italian children with sensorineural hearing loss.

Author

Franzè, Annamaria, Esposito, Gabriella, Di Domenico, Carmela, Iossa, Sandra, Sauchelli, Giuliana, Fioretti, Tiziana, Cavaliere, Michele, Auletta, Gennaro, Corvino, Virginia, Laria, Carla, Malesci, Rita, Marciano, Elio, and Salvatore, Francesco

Subjects

*GENETIC research, *DEAFNESS in children, *GENETIC mutation, *PATHOGENIC microorganisms, RISK of deafness

Abstract

The article discusses the analysis of the SLC26A4 gene of 30 Italian children with severe-to-profound congenital sensorineural hearing loss (SNHL). It states the identification of 10 independent mutated alleles and another variant p.I655V that is indicated as pathogenic only in gene-specific mutation/SNP databases. It mentions that mutation of SLC26A4 is relevant cause of deafness.

Published

2016

26. Slc26a4 expression prevents fluctuation of hearing in a mouse model of large vestibular aqueduct syndrome.

Author

Nishio, Ayako, Ito, Taku, Cheng, Hui, Fitzgerald, Tracy S., Wangemann, Philine, and Griffith, Andrew J.

Subjects

*DEAFNESS prevention, *DOXYCYCLINE, *TREATMENT of deafness, *GENE expression, *VESTIBULAR aqueduct, *EAR abnormalities, *GENETIC mutation, *LABORATORY mice, *THERAPEUTICS

Abstract

SLC26A4 mutations cause fluctuating and progressive hearing loss associated with enlargement of the vestibular aqueduct (EVA). SLC26A4 encodes a transmembrane anion exchanger called pendrin expressed in nonsensory epithelial cells of the lateral wall of cochlea, vestibular organs and endolymphatic sac. We previously described a transgenic mouse model of EVA with doxycycline (dox)-inducible expression of Slc26a4 in which administration of dox from conception to embryonic day 17.5 (DE17.5) resulted in hearing fluctuation between 1 and 3 months of age. In the present study, we hypothesized that Slc26a4 is required to stabilize hearing in DE17.5 ears between 1 and 3 months of age. We tested our hypothesis by evaluating the effect of postnatal re-induction of Slc26a4 expression on hearing. Readministration of dox to DE17.5 mice at postnatal day 6 (P6), but not at 1 month of age, resulted in reduced click-evoked auditory brainstem response (ABR) thresholds, less fluctuation of hearing and a higher surface density of pendrin expression in spindle-shaped cells of the stria vascularis. Pendrin expression in spindle-shaped cells was inversely correlated with ABR thresholds. These findings suggest that stabilization of hearing by readministration of dox at P6 is mediated by pendrin expression in spindle-shaped cells. We conclude that early re-induction of Slc26a4 expression can prevent fluctuation of hearing in our Slc26a4 -insufficient mouse model. Restoration of SLC26A4 expression and function could reduce or prevent fluctuation of hearing in EVA patients. [ABSTRACT FROM AUTHOR]

Published

2016

27. Vestibular function is associated with residual low-frequency hearing loss in patients with bi-allelic mutations in the SLC26A4 gene.

Author

Jung, Jinsei, Seo, Young Wook, Choi, Jae Young, and Kim, Sung Huhn

Subjects

*VESTIBULAR function tests, *HEARING disorders, *GENETIC mutation, *DISEASE susceptibility, *AUDIOLOGY

Abstract

DFNB4 is non-syndromic, autosomal recessive type of hearing loss with an enlarged vestibular aqueduct (EVA) caused by mutations in SLC26A4/pendrin . Although the characteristics of hearing loss are well known in DFNB4, vestibular function remains inconclusive. We evaluated the vestibular function of 31 patients with bi-allelic mutations in SLC26A4/pendrin and analyzed genetic, radiological, and audiological correlations with vestibular function. In a caloric test, unilateral and bilateral vestibulopathies were detected in 45.2% and 6.4% of patients, respectively; however, only 22.6% had subjective vertigo symptoms. While vestibular phenotype was not significantly associated with specific mutations in genetic alleles or the sizes of the endolymphatic sac and vestibular aqueduct, a residual hearing threshold at a low frequency (500 Hz) was definitely correlated with vestibular function in DFNB4 (p = 0.005). These findings may indicate that vestibular function in DFNB4 deteriorates unilaterally in ears when hearing loss occurs. In conclusion, DFNB4 shows vestibular dysfunction, which is strongly linked to hearing loss at low frequencies without any allelic or anatomical predisposing factor. [ABSTRACT FROM AUTHOR]

Published

2016

28. Mutation analysis of the SLC26A4, FOXI1 and KCNJ10 genes in individuals with congenital hearing loss

Author

Lynn M. Pique, Marie-Luise Brennan, Colin J. Davidson, Frederick Schaefer, John Greinwald Jr, and Iris Schrijver

Subjects

Pendred, MLPA, DFNB4, SLC26A4, FOXI1 and KCNJ10, Genotyping, Medicine, Biology (General), QH301-705.5

Abstract

Pendred syndrome (PDS) and DFNB4 comprise a phenotypic spectrum of sensorineural hearing loss disorders that typically result from biallelic mutations of the SLC26A4 gene. Although PDS and DFNB4 are recessively inherited, sequencing of the coding regions and splice sites of SLC26A4 in individuals suspected to be affected with these conditions often fails to identify two mutations. We investigated the potential contribution of large SLC26A4 deletions and duplications to sensorineural hearing loss (SNHL) by screening 107 probands with one known SLC26A4 mutation by Multiplex Ligation-dependent Probe Amplification (MLPA). A heterozygous deletion, spanning exons 4–6, was detected in only one individual, accounting for approximately 1% of the missing mutations in our cohort. This low frequency is consistent with previously published MLPA results. We also examined the potential involvement of digenic inheritance in PDS/DFNB4 by sequencing the coding regions of FOXI1 and KCNJ10. Of the 29 probands who were sequenced, three carried nonsynonymous variants including one novel sequence change in FOXI1 and two polymorphisms in KCNJ10. We performed a review of prior studies and, in conjunction with our current data, conclude that the frequency of FOXI1 (1.4%) and KCNJ10 (3.6%) variants in PDS/DFNB4 individuals is low. Our results, in combination with previously published reports, indicate that large SLC26A4 deletions and duplications as well as mutations of FOXI1 and KCNJ10 play limited roles in the pathogenesis of SNHL and suggest that other genetic factors likely contribute to the phenotype.

Published

2014

29. Subgroups of enlarged vestibular aqueduct in relation to SLC26A4 mutations and hearing loss.

Author

Okamoto, Yasuhide, Mutai, Hideki, Nakano, Atsuko, Arimoto, Yukiko, Sugiuchi, Tomoko, Masuda, Sawako, Morimoto, Noriko, Sakamoto, Hirokazu, Ogahara, Noboru, Takagi, Akira, Taiji, Hidenobu, Kaga, Kimitaka, Ogawa, Kaoru, and Matsunaga, Tatsuo

Abstract

Objectives/Hypothesis To investigate possible association of hearing loss and SLC26A4 mutations with the subgroups of enlarged vestibular aqueduct (EVA) morphology in Japanese subjects with hearing loss. Study Design Retrospective multicenter study. Methods Forty-seven subjects who had vestibular aqueduct with midpoint diameter >1 mm by computed tomography of the temporal bone were enrolled at multiple sites across Japan, and DNA samples and clinical data were collected. EVA morphology was classified into four subgroups by the pattern of enlargement: aperture, aperture and midpoint, midpoint, and borderline enlargement. Venous blood DNA samples were subjected to polymerase chain reaction-based direct sequencing of all exons and exon-intron boundaries of the SLC26A4. Results Four novel SLC26A4 mutations were identified in the present study. SLC26A4 mutations were detected in almost all subjects with aperture, aperture and midpoint, and midpoint enlargement. In contrast, 71% of subjects with borderline enlargement had no SLC26A4 mutation. No significant difference was found in the distribution of truncating and nontruncating SLC26A4 mutations between the EVA subgroups. In addition, no significant correlation was observed between the EVA subgroups and hearing levels, incidence of hearing fluctuation, or progression of hearing loss. Conclusions Subgroups of EVA morphology were significantly correlated with the presence or absence of SLC26A4 mutation. In a subgroup analysis of subjects with SLC26A4 mutations, however, differences in the EVA subgroups were not correlated with SLC26A4 genotypes or characteristics of hearing loss. Level of Evidence NA. Laryngoscope, 124:E134-E140, 2014 [ABSTRACT FROM AUTHOR]

Published

2014

30. SLC26A4 Mutations in Patients with Moderate to Severe Hearing Loss.

Author

Khan, Muhammad, Bashir, Rasheeda, and Naz, Sadaf

Subjects

*GENETIC mutation, *GENETICS of deafness, *SEQUENCE analysis, *ETIOLOGY of diseases, *EPISTASIS (Genetics), *PHENOTYPES

Abstract

Mutations in SLC26A4 cause either syndromic or nonsyndromic hearing loss. We identified a link between hearing loss and DFNB4 in 3 of the 50 families participating in this study. Sequencing analysis revealed two SLC26A4 mutations, p.V239D and p.S57X, in affected members of the 3 families. These mutations have been previously reported in deaf individuals from the subcontinent, all of whom manifested profound deafness. The patients investigated in our study exhibited moderate to severe hearing loss. Our results show that inactivating SLC26A4 mutations that cause profound deafness can also be involved in the etiology of moderate to severe hearing loss. The type of mutation cannot predict the severity of the hearing loss in all cases, and there may be additional epistatic interactions that could modify the phenotype. [ABSTRACT FROM AUTHOR]

Published

2013

31. A novel insertion-induced frameshift mutation of the SLC26A4 gene in a Korean family with Pendred syndrome

Author

Sagong, Borum, Seok, Jun Ho, Kwon, Tae-Jun, Kim, Un-Kyung, Lee, Sang-Heun, and Lee, Kyu-Yup

Subjects

*TREATMENT of deafness, *FRAMESHIFT mutation, *GENETICS of deafness, *IODINE deficiency diseases, *ALLELES, *BRAIN stem, *AUDIOMETRY, *STEROIDS

Abstract

Abstract: Pendred syndrome (PS) is an autosomal recessive disorder characterized by congenital bilateral sensorineural hearing loss, goiter, and incomplete iodide organification. Patients with PS also have structural anomalies of the inner ear such as enlarged vestibular aqueducts (EVA) and Mondini''s malformation. The goiter, which is a major clinical manifestation of PS, usually develops around adolescence. PS is caused by biallelic mutations of the SLC26A4 gene, while nonsyndromic bilateral EVA is associated with zero or one SLC26A4 mutant allele. We report here a Korean family including a young female with PS who had goiter and progressive, fluctuating sensorineural hearing loss that could be partially recovered by oral steroid treatment. Genetic investigation revealed compound heterozygous mutations for p.R677AfsX11, a novel frameshift mutation, and p.H723R in the SLC26A4 gene. Our findings provide detailed information regarding the distribution of mutant alleles for PS and may serve as a foundation for studies to comprehend the genetic portion of syndromic hearing loss. [Copyright &y& Elsevier]

Published

2012

32. Novel mutations in the SLC26A4 gene

Author

Busi, Micol, Castiglione, Alessandro, Taddei Masieri, Marina, Ravani, Anna, Guaran, Valeria, Astolfi, Laura, Trevisi, Patrizia, Ferlini, Alessandra, and Martini, Alessandro

Subjects

*GENETICS of deafness, *GENETIC mutation, *EAR abnormalities, *SYMPTOMS, *NUCLEOTIDE sequence, *MITOCHONDRIAL DNA, *GENETIC carriers

Abstract

Abstract: Objectives: Mutations in the SLC26A4 gene (7q22.3–7q31.1) are considered one of the most common causes of genetic hearing loss. There are two clinical forms related to these mutations: syndromic and non-syndromic deafness. The first one is named Pendred Syndrome (PS) when deafness is associated with thyroid goiter; the second is called DFNB4, when no other symptoms are present. Both are transmitted as an autosomal recessive trait, but simple heterozygotes can develop both forms of deafness. Actually it is thought that Pendred Syndrome occurs when both alleles of SLC26A4 gene are mutated; DFNB4 seems due to monoallelic mutations. PS and DFNB4 can be associated with inner ear malformations. In most of the cases (around 80%), these consist in Enlarged Vestibular Aqueduct (EVA). EVA can also be present without SLC26A4 mutations. Understanding the role of new SLC26A4 variants should facilitate clinical assessment, as well as diagnostic and therapeutic approaches. This investigation aims to detect and report genetic causes of two unrelated Italian boys with hearing loss. Methods: Patients and family members underwent clinical, audiological and genetic evaluations. To identify genetic mutations, DNA sequencing of SLC26A4 gene (including all 21 exons, exon-intron boundaries and promoter region) was carried out. Results: Both probands were affected by congenital, progressive and fluctuating mixed hearing loss. Temporal bone imaging revealed a bilateral EVA with no other abnormalities in both cases. Probands were heterozygotes for previously undescribed mutations in the SLC26A4 gene: R409H/IVS2+1delG (proband 1) and L236P/K590X (proband 2). No other mutations were detected in GJB2, GJB6 genes or mitochondrial DNA (mit-DNA). Conclusions: The IVS2+1delG and K590X mutations have not yet been described in literature but there is some evidence to suggest that they have a pathological role. The results underlined the importance of considering the complete DNA sequencing of the SLC26A4 gene for differential molecular diagnosis of deafness, especially in those patients affected by congenital, progressive and fluctuating mixed hearing loss with bilateral EVA. [Copyright &y& Elsevier]

Published

2012

33. Developmental delays consistent with cochlear hypothyroidism contribute to failure to develop hearing in mice lacking Slc26a4/pendrin expression.

Author

Wangemann, Philine, Hyoung-Mi Kim, Billings, Sara, Nakaya, Kazuhiro, Xiangming Li, Singh, Ruchira, Sharlin, David S., Forrest, Douglas, Marcus, Daniel C., and Peying Fong

Subjects

*DEAFNESS, *DEVELOPMENTAL delay, *GENETIC mutation, *COCHLEA, *HYPOTHYROIDISM, *THYROID diseases, *GENE expression

Abstract

Mutations of SLC26A4 cause an enlarged vestibular aqueduct, nonsyndromic deafness, and deafness as part of Pendred syndrome. SLC26A4 encodes pendrin, an anion exchanger located in the cochlea, thyroid, and kidney. The goal of the present study was to determine whether developmental delays, possibly mediated by systemic or local hypothyroidism, contribute to the failure to develop hearing in mice lacking Slc26a4 (Slc26a4-/-). We evaluated thyroid function by voltage and pH measurements, by array-assisted gene expression analysis, and by determination of plasma thyroxine levels. Cochlear development was evaluated for signs of hypothyroidism by microscopy, in situ hybridization, and quantitative RT-PCR. No differences in plasma thyroxine levels were found in Slc26a4+/- and sex-matched Slc26a4+/- littermates between postnatal day 5 (P5) and P90. In adult Slc26a4+/- mice, the transepithelial potential and the pH of thyroid follicles were reduced. No differences in the expression of genes that participate in thyroid hormone synthesis or ion transport were observed at P15, when plasma thyroxine levels peaked. Scala media of the cochlea was 10-fold enlarged, bulging into and thereby displacing fibrocytes, which express Dio2 to generate a cochlear thyroid hormone peak at P7. Cochlear development, including tunnel opening, arrival of efferent innervation at outer hair cells, endochondral and intramembraneous ossification, and developmental changes in the expression of Dio2, Dio3, and Tectb were delayed by 1-4 days. These data suggest that pendrin functions as a HCO3- transporter in the thyroid, that Slc26a4-/- mice are systemically euthyroid, and that delays in cochlear development, possibly due to local hypothyroidism, lead to the failure to develop hearing. [ABSTRACT FROM AUTHOR]

Published

2009

34. SLC26A4 mutation spectrum associated with DFNB4 deafness and Pendred's syndrome in Pakistanis.

Author

Anwar, Saima, Riazuddin, Saima, Ahmed, Zubair M., Tasneem, Saba, Ateeq-ul-Jaleel, Khan, Shahid Y., Griffith, Andrew J., Friedman, Thomas B., and Riazuddin, Sheikh

Subjects

*GENETICS of deafness, *GOITER, *GENETIC disorders, *INNER ear diseases, *PAKISTANIS, *EXONS (Genetics), *GENETICS, *PATIENTS, *DISEASES

Abstract

Pendred's syndrome (PDS) is an autosomal-recessive disorder characterized by sensorineural hearing loss and goiter. PDS is caused by mutations of the SLC26A4 gene encoding pendrin, a transmembrane exchanger of Cl−, I− and HCO3−, which is expressed in the thyroid and inner ear. SLC26A4 mutations can also be associated with non-syndromic deafness, DFNB4. The goal of our study was to define the identities and frequencies of SLC26A4 mutations in 563 large, consanguineous Pakistani families segregating severe-to-profound recessive deafness. Sequence analyses of SLC26A4 in 46 unreported families segregating deafness linked to DFNB4/PDS revealed 16 probable pathogenic variants, 8 of which are novel. The novel variants include three missense substitutions (p.R24L, p.G139V and p.V231M), two splice site mutations (c.304+2T>C and c.1341+3A>C), one frameshift (p.C565MfsX8) and two different genomic deletions affecting exons 1–2 and 11–18. Each of six pathogenic variants (p.V239D, p.Q446R, p.S90L, p.Y556C, p.R24L and p.K715N) was found in more than one family and haplotype analyses suggest that they are founder mutations. Combined with earlier reported data, SLC26A4 mutations were identified in 56 (7.2%; 95% CI: 5.6–9.2%) of 775 families. Therefore, SLC26A4 mutations are the most common known cause of genetic deafness in this population. As p.V239D (30%), p.S90L (18%) and p.Q446R (18%) account for approximately two-third of the mutant alleles of SLC26A4, hierarchical strategies for mutation detection would be feasible and cost-efficient genetic tests for DFNB4 deafness and PDS in Pakistanis.Journal of Human Genetics (2009) 54, 266–270; doi:10.1038/jhg.2009.21; published online 13 March 2009 [ABSTRACT FROM AUTHOR]

Published

2009

35. SLC26A4 gene is frequently involved in nonsyndromic hearing impairment with enlarged vestibular aqueduct in Caucasian populations.

Author

Albert, Sébastien, Blons, Hélène, Jonard, Laurence, Feldmann, Delphine, Chauvin, Pierre, Loundon, Nathalie, Sergent-Allaoui, Annie, Houang, Muriel, Joannard, Alain, Schmerber, Sébastien, Delobel, Bruno, Leman, Jacques, Journel, Hubert, Catros, Hélène, Dollfus, Hélène, Eliot, Marie-Madeleine, David, Albert, Calais, Catherine, Drouin-Garraud, Valérie, and Obstoy, Marie-Françoise

Subjects

*HEARING disorders, *EAR diseases, *CAUCASIAN race, *HEARING, *DISEASES, *HUMAN genetics

Abstract

Sensorineural hearing loss is the most frequent sensory deficit of childhood and is of genetic origin in up to 75% of cases. It has been shown that mutations of the SLC26A4 (PDS) gene were involved in syndromic deafness characterized by congenital sensorineural hearing impairment and goitre (Pendred's syndrome), as well as in congenital isolated deafness (DFNB4). While the prevalence of SLC26A4 mutations in Pendred's syndrome is clearly established, it remains to be studied in large cohorts of patients with nonsyndromic deafness and detailed clinical informations. In this report, 109 patients from 100 unrelated families, aged from 1 to 32 years (median age: 10 years), with nonsyndromic deafness and enlarged vestibular aqueduct, were genotyped for SLC26A4 using DHPLC molecular screening and sequencing. In all, 91 allelic variants were observed in 100 unrelated families, of which 19 have never been reported. The prevalence of SLC26A4 mutations was 40% (40/100), with biallelic mutation in 24% (24/100), while six families were homozygous. All patients included in this series had documented deafness, associated with EVA and without any evidence of syndromic disease. Among patients with SLC26A4 biallelic mutations, deafness was more severe, fluctuated more than in patients with no mutation. In conclusion, the incidence of SLC26A4 mutations is high in patients with isolated deafness and enlarged vestibular aqueduct and could represent up to 4% of nonsyndromic hearing impairment. SLC26A4 could be the second most frequent gene implicated in nonsyndromic deafness after GJB2, in this Caucasian population.European Journal of Human Genetics (2006) 14, 773–779. doi:10.1038/sj.ejhg.5201611; published online 29 March 2006 [ABSTRACT FROM AUTHOR]

Published

2006

36. Genetic basis of hearing loss associated with enlarged vestibular aqueducts in Koreans.

Author

Park, H. -J., Lee, S. -J., Jin, H. -S., Lee, J. O., Go, S. -H., Jang, H. S., Moon, S. -K., Lee, S. -C., Chun, Y. -M., Lee, H. -K., Choi, J. -Y., Jung, S. -C., Griffith, A.J., and Koo, S. K.

Subjects

*GENETIC disorders, *HEARING disorders, *AQUEDUCTS, *GENETIC mutation, *NUCLEOTIDE sequence, *KOREANS

Abstract

Park H-J, Lee S-J, Jin H-S, Lee JO, Go S-H, Jang HS, Moon S-K, Lee S-C, Chun Y-M, Lee H-K, Choi J-Y, Jung S-C, Griffith AJ, Koo SK. Genetic basis of hearing loss associated with enlarged vestibular aqueducts in Koreans.Sensorineural hearing loss associated with enlargement of the vestibular aqueduct (EVA) can be associated with mutations of theSLC26A4gene. In western populations, less than one-half of the affected individuals with EVA have two mutantSLC26A4alleles, and EVA is frequently caused by unknown genetic or environmental factors alone or in combination with a singleSLC26A4mutation as part of a complex trait. In this study, we ascertained 26 Korean probands with EVA and performed nucleotide sequence analysis to detectSLC26A4mutations. All subjects had bilateral EVA, and 20 of 26 were sporadic (simplex) cases. Fourteen different mutations were identified, including nine novel mutations. Five mutations were recurrent and accounted for 80% of all mutant alleles, providing a basis for the design and interpretation of cost-efficient mutation detection algorithms. Two mutant alleles were identified in 21 (81%), one mutant allele was detected in three (11%), and zero mutant allele was detected in two (8%) of 26 probands. The high proportion of Korean probands with twoSLC26A4mutations may reflect a reduced frequency of other genetic or environmental factors causing EVA in comparison to western populations. [ABSTRACT FROM AUTHOR]

Published

2005

37. Bimodal strategy for excellent audiological rehabilitation in a subject with a novel nonsense mutation of the SLC26A4 gene: A case report

Author

Rita Malesci, Carmela Monzillo, Gennaro Auletta, Roberta Russo, Virginia Corvino, Achille Iolascon, Carla Laria, Annamaria Franzè, Malesci, R., Russo, R., Monzillo, C., Laria, C., Corvino, V., Auletta, G., Iolascon, A., and Franze, A.

Subjects

medicine.medical_specialty, Hearing loss, Pendred syndrome, medicine.medical_treatment, Hearing Loss, Sensorineural, Nonsense mutation, Disease, Audiology, medicine.disease_cause, Vestibular Aqueduct, otorhinolaryngologic diseases, medicine, SLC26A4, DFNB4, Humans, Cochlear implant, Child, Mutation, Rehabilitation, business.industry, Sulfate Transporter, Homozygote, General Medicine, medicine.disease, Otorhinolaryngology, Codon, Nonsense, Sulfate Transporters, Sensorineural hearing lo, Pediatrics, Perinatology and Child Health, Sensorineural hearing loss, Female, sense organs, medicine.symptom, business, Enlarged vestibular aqueduct, Human

Abstract

Sensorineural hearing loss is a heterogeneous disease caused by mutations in many genes. However, in the presence of enlarged vestibular aqueduct, it is frequently associated with mutations in the solute carrier family 26 member 4 (SLC26A4), a gene causative of a syndromic form (Pendred) as well as a non-syndromic form of hearing loss (DFNB4). We describe a clinical case presenting bilateral sensorineural hearing loss and enlarged vestibular aqueduct in which a novel homozygous SLC26A4 mutation was identified. Despite a late diagnosis of hearing loss, a peculiar rehabilitation therapy strategy was identified that provided excellent results.

Published

2019

38. Different Rates of the SLC26A4 -Related Hearing Loss in Two Indigenous Peoples of Southern Siberia (Russia).

Author

Danilchenko, Valeriia Yu., Zytsar, Marina V., Maslova, Ekaterina A., Bady-Khoo, Marita S., Barashkov, Nikolay A., Morozov, Igor V., Bondar, Alexander A., and Posukh, Olga L.

Subjects

HEARING disorders, INDIGENOUS peoples, ASIANS, GENETIC disorder diagnosis, GENETIC mutation, CONDUCTIVE hearing loss

Abstract

Hereditary hearing loss (HL) is known to be highly locus/allelic heterogeneous, and the prevalence of different HL forms significantly varies among populations worldwide. Investigation of region-specific landscapes of hereditary HL is important for local healthcare and medical genetic services. Mutations in the SLC26A4 gene leading to nonsyndromic recessive deafness (DFNB4) and Pendred syndrome are common genetic causes of hereditary HL, at least in some Asian populations. We present for the first time the results of a thorough analysis of the SLC26A4 gene by Sanger sequencing in the large cohorts of patients with HL of unknown etiology belonging to two neighboring indigenous Turkic-speaking Siberian peoples (Tuvinians and Altaians). A definite genetic diagnosis based on the presence of biallelic SLC26A4 mutations was established for 28.2% (62/220) of all enrolled Tuvinian patients vs. 4.3% (4/93) of Altaian patients. The rate of the SLC26A4-related HL in Tuvinian patients appeared to be one of the highest among populations worldwide. The SLC26A4 mutational spectrum was characterized by the presence of Asian-specific mutations c.919-2A>G and c.2027T>A (p.Leu676Gln), predominantly found in Tuvinian patients, and c.2168A>G (p.His723Arg), which was only detected in Altaian patients. In addition, a novel pathogenic variant c.1545T>G (p.Phe515Leu) was found with high frequency in Tuvinian patients. Overall, based on the findings of this study and our previous research, we were able to uncover the genetic causes of HL in 50.5% of Tuvinian patients and 34.5% of Altaian patients. [ABSTRACT FROM AUTHOR]

Published

2021

39. Mutation spectrum and genotype–phenotype correlation of hearing loss patients caused by SLC26A4 mutations in the Japanese: a large cohort study

Author

Masaru Aoyagi, Hiroshi Takenaka, Tomoo Watanabe, Masafumi Sakagami, Shin-ya Nishio, Noboru Yamanaka, Masahiko Higashikawa, Satoshi Iwasaki, Kiyofumi Gyo, Hajime Sano, Kozo Kumakawa, Akihiro Sakai, Naoto Hato, Hiromi Kojima, Shunichi Tomiyama, Shuntaro Shigihara, Kunihiro Fukushima, Yumiko Kobayashi, Kyoko Nagai, Yasuyuki Nomura, Mayumi Sugamura, Yuichi Kurono, Tetsuaki Kawase, Yasushi Naito, Maiko Miyagawa, Toshiaki Yagi, Ikuyo Miyanohara, Tsukasa Ito, Minoru Ikeda, Kotaro Ishikawa, Hiroshi Ogawa, Tetsuya Tono, Akira Ganaha, Koichi Omori, Mikio Suzuki, Satoshi Fukuda, Masako Nakai, Shin-ichi Usami, Keiji Fujihara, Toshimitsu Kobayashi, Hideichi Shinkawa, Hiroshi Moriyama, Kazuhiko Takeuchi, Hiroshi Yamashita, Yuika Sakurai, Atsushi Namba, Yasuhiro Kakazu, Takashi Nakagawa, Nobuhiko Furuya, Yuko Saito, Haruo Takahashi, Hirokazu Kawano, Norihito Takeichi, Kazunori Nishizaki, Shizuo Komune, Hiroaki Sato, Tetsuo Ikezono, Keiichi Ichimura, Kazuma Sugahara, Yukihiko Kanda, and Makito Okamoto

Subjects

Male, Proband, Pediatrics, Pendred syndrome, Congenital hearing loss, Connexins, Cohort Studies, Gene Frequency, Japan, Genotype, Child, Genetics (clinical), Genetics, goiter, medicine.diagnostic_test, Hearing Tests, Exons, Middle Aged, Connexin 26, Phenotype, Sulfate Transporters, Child, Preschool, Original Article, enlarged vestibular aqueduct, Female, medicine.symptom, Adult, medicine.medical_specialty, Adolescent, Hearing loss, Genetic counseling, Young Adult, Asian People, SLC26A4, otorhinolaryngologic diseases, medicine, DFNB4, Humans, Hearing Loss, Alleles, Genetic Association Studies, Genetic testing, business.industry, Infant, Newborn, Infant, Membrane Transport Proteins, medicine.disease, Case-Control Studies, Mutation, sense organs, Tomography, X-Ray Computed, business, congenital hearing loss, Enlarged vestibular aqueduct

Abstract

Mutations in SLC26A4 cause a broad phenotypic spectrum, from typical Pendred syndrome to nonsyndromic hearing loss associated with enlarged vestibular aqueduct. Identification of these mutations is important for accurate diagnosis, proper medical management and appropriate genetic counseling and requires updated information regarding spectrum, clinical characteristics and genotype-phenotype correlations, based on a large cohort. In 100 patients with bilateral enlarged vestibular aqueduct among 1511 Japanese hearing loss probands registered in our gene bank, goiter data were available for 79, of whom 15 had Pendred syndrome and 64 had nonsyndromic hearing loss. We clarified the mutation spectrum for the SLC26A4 mutations and also summarized hearing levels, progression, fluctuation and existence of genotype-phenotype correlation. SLC26A4 mutations were identified in 82 of the 100 patients (82.0%). Of the Pendred syndrome patients, 93% (14/15) were carriers, as were 77% (49/64) of the nonsyndromic hearing loss patients. Clinical characteristics of patients with SLC26A4 mutations were congenital, fluctuating and progressive hearing loss usually associated with vertigo and/or goiter. We found no genotype-phenotype correlations, indicating that, unlike in the case of GJB2 mutations, the phenotype cannot be predicted from the genotype. Our mutation analysis confirmed the importance of mutations in the SLC26A4 gene among hearing loss patients with enlarged vestibular aqueduct and revealed the mutation spectrum, essential information when performing genetic testing.

Published

2014

40. Identification of SLC26A4 gene mutations in Iranian families with hereditary hearing impairment.

Author

Kahrizi, Kimia, Mohseni, Marzieh, Nishimura, Carla, Bazazzadegan, Niloofar, Fischer, Stephanie M., Dehghani, Atefeh, Sayfati, Morteza, Taghdiri, Maryam, Jamali, Payman, Smith, Richard J. H., Azizi, Fereydoun, Najmanabi, Hossein, and Najmabadi, Hossein

Subjects

*GENETIC mutation, *HEARING disorders, *GENOMICS, *GENES, *AMINO acids, *MOLECULAR weights, *BIOLOGICAL transport, *COMPARATIVE studies, *DNA, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *RESEARCH funding, *SYNDROMES, *EVALUATION research, *SEQUENCE analysis, *VESTIBULAR aqueduct, *MEMBRANE transport proteins, *GENOTYPES

Abstract

Mutations in the SLC26A4 gene at the DFNB4 locus are responsible for Pendred syndrome and non-syndromic hereditary hearing loss (DFNB4). This study included 80 nuclear families with two or more siblings segregating presumed autosomal recessive hearing loss. All deaf persons tested negative for mutations in GJB2 at the DFNB1 locus and were, therefore, screened for autozygosity by descent (ABD) using short tandem repeat polymorphisms (STRPs) that flanked SLC26A4. In 12 families, homozygosity for STRPs suggested possible ABD in this genomic region. Affected individuals in five families had a positive perchlorate discharge test. Sequence analysis of SLC26A4 identified ten mutations in eight families (T420I, 1197delT, G334V, R409H, T721M, R79X, S448L, L597S, 965insA and L445W), of which, four are novel (T420I, G334V, 965insA and R79X). These results imply that Pendred syndrome is the most prevalent form of syndromic hereditary hearing loss in Iran. [ABSTRACT FROM AUTHOR]

Published

2009

41. Clinical heterogeneity of the SLC26A4 gene in UAE patients with hearing loss and bioinformatics investigation of DFNB4/Pendred syndrome missense mutations.

Author

Chouchen, Jihen, Mahfood, Mona, Alobathani, Maryam, Eldin Mohamed, Walaa Kamal, and Tlili, Abdelaziz

Subjects

*HEARING disorders, *MISSENSE mutation, *GENETIC disorders, *SYNDROMES, *NUCLEOTIDE sequencing

Abstract

The development of next generation sequencing-based techniques showed an important progress in the identification of pathogenic variants related to monogenetic diseases with genetic and phenotypic heterogeneities. Hereditary hearing loss is considered as one of these heterogeneous diseases, given the large number of deafness causing genes, the different modes of inheritance and the phenotypic variabilities associated to the severity, age of onset and/or presence or absence of other clinical manifestations. In this study, we performed next-generation sequencing (NGS) in 51 UAE patients with hearing loss and no GJB2 mutations. In addition, we reviewed all reported SLC26A4 missense mutations with a confirmed DFNB4/Pendred syndrome phenotype and tried to find a genotype/phenotype correlation using different criteria. By analyzing the NGS data, we identified one new SLC26A4 variant c.1150G > C (p.Glu384Gln) and one known SLC26A4 mutation c.716T > A (p.Val239Asp) in two different patients. Direct Sanger sequencing and segregation analyses confirmed the implication of both DNA variants in the deafness phenotype. Moreover, the clinical examination of both patients showed that one patient has syndromic deafness (Pendred syndrome) and the second one has non-syndromic deafness. The analysis of all confirmed missense mutations didn't reveal a complete genotype/phenotype correlation. To the best of our knowledge, this is the first report of mutations associated with DFNB4/Pendred deafness in the GCC region. [ABSTRACT FROM AUTHOR]

Published

2021

42. Investigation of DFNB4 SLC26A4 mutation in patients with enlarged vestibular aquaduct.

Author

Kınoğlu, Kubilay, Orhan, Kadir Serkan, Kara, Hakan, Öztürk, Oğuz, Polat, Beldan, Aydoğan, Hülya, Çelik, Mehmet, Ceviz, Ayşe Begüm, and Güldiken, Yahya

Subjects

*HEARING disorders, *GENETIC mutation, *INNER ear, *STANDARD deviations, *AQUEDUCTS

Abstract

Mutations of the SLC26A4 gene causing enlarged vestibular aqueduct (EVA) syndrome have not yet been fully elucidated. The study aimed to investigate SLC26A4 mutations in patients with EVA syndrome in the Turkish population. Identifying these mutations may play an essential role in determining the prognosis, follow-up, and management options of these patients. Whole exome sequencing and/or Sanger sequencing of SLC26A4 in 22 patients with sensorineural hearing loss associated with isolated EVA without inner ear anomalies, and 22 controls were performed. Twenty-two patients and 22 control subjects were included in the study. The onset of hearing loss was pre-lingual in 15 patients, and post-lingual in 7. The mean (standard deviation) vestibular aqueduct width of the patients was 3.23 mm (1.28). Twenty SLC26A4 variants, 15 of them unique, were identified in 22 patients. Among them, seven variants were heterozygous, and 13 were homozygous. The variants p.E37X (c.109G > T), p.Y27H (c.79T > C), p.C706Y (c.2117G > A) have not been previously reported. The detection of rare and previously unreported mutations in our study showed that studies with a larger number of patients with EVA might reveal more role of the SLC26A4 gene. Besides, to understand the etiopathogenesis of the disease, other related genes also should be investigated. [ABSTRACT FROM AUTHOR]

Published

2020

43. Bimodal strategy for excellent audiological rehabilitation in a subject with a novel nonsense mutation of the SLC26A4 gene: A case report.

Author

Malesci, Rita, Russo, Roberta, Monzillo, Carmela, Laria, Carla, Corvino, Virginia, Auletta, Gennaro, Iolascon, Achille, and Franzè, Annamaria

Subjects

*NONSENSE mutation, *GENETIC mutation, *HEARING disorders, *REHABILITATION, *COCHLEAR implants

Abstract

Sensorineural hearing loss is a heterogeneous disease caused by mutations in many genes. However, in the presence of enlarged vestibular aqueduct, it is frequently associated with mutations in the solute carrier family 26 member 4 (SLC26A4), a gene causative of a syndromic form (Pendred) as well as a non-syndromic form of hearing loss (DFNB4). We describe a clinical case presenting bilateral sensorineural hearing loss and enlarged vestibular aqueduct in which a novel homozygous SLC26A4 mutation was identified. Despite a late diagnosis of hearing loss, a peculiar rehabilitation therapy strategy was identified that provided excellent results. [ABSTRACT FROM AUTHOR]

Published

2020

44. SLC26A4-linked CEVA haplotype correlates with phenotype in patients with enlargement of the vestibular aqueduct.

Author

Chao, Janet R., Chattaraj, Parna, Munjal, Tina, Honda, Keiji, King, Kelly A., Zalewski, Christopher K., Chien, Wade W., Brewer, Carmen C., and Griffith, Andrew J.

Subjects

RECESSIVE genes, AQUEDUCTS, PHENOTYPES, DEAFNESS, IODINATION, ALLELES

Abstract

Background: Recessive mutations of coding regions and splice sites of the SLC26A4 gene cause hearing loss with enlargement of the vestibular aqueduct (EVA). Some patients also have a thyroid iodination defect that can lead to multinodular goiter as part of Pendred syndrome. A haplotype of variants upstream of SLC26A4, called CEVA, acts as a pathogenic recessive allele in trans to mutations affecting the coding regions or splice sites of SLC26A4. Our first hypothesis is that CEVA, acting as a pathogenic recessive allele, is correlated with a less severe phenotype than mutations affecting the coding regions and splice sites of SLC26A4. Our second hypothesis is that CEVA acts as a modifier of the phenotype in patients with EVA caused by mutations affecting the coding regions or splice sites of both alleles of SLC26A4 or EVA caused by other factors. Methods: This was a prospective cohort study of 114 individuals and 202 ears with EVA. To test our first hypothesis, we compared the thyroid and auditory phenotypes of subjects with mutations affecting coding regions of both alleles of SLC26A4 with those of subjects carrying CEVA in trans to mutations affecting the coding regions. To test our second hypothesis, we compared the phenotypes associated with the presence versus absence of CEVA among subjects with no coding region mutations, as well as among subjects with mutations affecting coding regions of both alleles. Results: Subjects carrying CEVA in trans to a mutation of SLC26A4 have a normal thyroid phenotype and less severe hearing loss in comparison to individuals with mutations affecting coding regions of both alleles of SLC26A4. In subjects with no mutant alleles of SLC26A4, hearing loss was more severe in subjects who carry the CEVA haplotype in comparison to non-carriers. There was no correlation of CEVA with the phenotype of subjects with mutations affecting coding regions of both alleles. Conclusions: CEVA, acting as a likely pathogenic recessive allele, is associated with a less severe phenotype than alleles with a mutation affecting the coding regions or splice sites of SLC26A4. CEVA may act as a genetic modifier in patients with EVA caused by other factors. [ABSTRACT FROM AUTHOR]

Published

2019

45. Mutation analysis of the SLC26A4, FOXI1 and KCNJ10 genes in individuals with congenital hearing loss

Author

Marie-Luise Brennan, Lynn Pique, Colin J. Davidson, John H. Greinwald, Iris Schrijver, and Frederick V. Schaefer

Subjects

Nonsynonymous substitution, Proband, Genotyping, FOXI1 and KCNJ10, lcsh:Medicine, KCNJ10, Congenital hearing loss, medicine.disease_cause, Bioinformatics, Pediatrics, General Biochemistry, Genetics and Molecular Biology, SNHL, Genetics, Pathology, medicine, otorhinolaryngologic diseases, SLC26A4, DFNB4, Multiplex ligation-dependent probe amplification, Pendred syndrome, Mutation, biology, General Neuroscience, Pendred, lcsh:R, General Medicine, medicine.disease, MLPA, Otorhinolaryngology, biology.protein, Sensorineural hearing loss, General Agricultural and Biological Sciences, Medical Genetics

Abstract

Pendred syndrome (PDS) and DFNB4 comprise a phenotypic spectrum of sensorineural hearing loss disorders that typically result from biallelic mutations of the SLC26A4 gene. Although PDS and DFNB4 are recessively inherited, sequencing of the coding regions and splice sites of SLC26A4 in individuals suspected to be affected with these conditions often fails to identify two mutations. We investigated the potential contribution of large SLC26A4 deletions and duplications to sensorineural hearing loss (SNHL) by screening 107 probands with one known SLC26A4 mutation by Multiplex Ligation-dependent Probe Amplification (MLPA). A heterozygous deletion, spanning exons 4-6, was detected in only one individual, accounting for approximately 1% of the missing mutations in our cohort. This low frequency is consistent with previously published MLPA results. We also examined the potential involvement of digenic inheritance in PDS/DFNB4 by sequencing the coding regions of FOXI1 and KCNJ10. Of the 29 probands who were sequenced, three carried nonsynonymous variants including one novel sequence change in FOXI1 and two polymorphisms in KCNJ10. We performed a review of prior studies and, in conjunction with our current data, conclude that the frequency of FOXI1 (1.4%) and KCNJ10 (3.6%) variants in PDS/DFNB4 individuals is low. Our results, in combination with previously published reports, indicate that large SLC26A4 deletions and duplications as well as mutations of FOXI1 and KCNJ10 play limited roles in the pathogenesis of SNHL and suggest that other genetic factors likely contribute to the phenotype.

Published

2014

46. DNAJC14 Ameliorates Inner Ear Degeneration in the DFNB4 Mouse Model.

Author

Choi HJ, Lee HJ, Choi JY, Jeon IH, Noh B, Devkota S, Lee HW, Eo SK, Choi JY, Lee MG, and Jung J

Abstract

The His723Arg (H723R) mutation in SLC26A4 , encoding pendrin, is the most prevalent mutation in East Asia, resulting in DFNB4, an autosomal recessive type of genetic hearing loss. Although the main pathological mechanism of H723R was identified as a protein-folding defect in pendrin, there is still no curative treatment for associated hearing loss. Here, we show that H723R-pendrin expression and activity are rescued by activation of the chaperonin DNAJC14. In vitro , DNAJC14 was activated via Japanese encephalitis virus (JEV) inoculation, and toxin-attenuated JEV rescued the surface expression and anion exchange activity of H723R-pendrin. Human H723R-pendrin transgenic mice (hH723R Tg) were established in a mouse slc26a4 knockout background, in which only hH723R-pendrin was expressed in the inner ear (Pax2-Cre dependent) to mimic human DFNB4 pathology. Crossing hH723R Tg with DNAJC14-overexpressing mice resulted in reduced cochlear hydrops and more preserved outer hair cells in the cochlea compared to those in hH723R Tg mice. Furthermore, the stria vascularis and spiral ligament were thicker and KCNJ10 expression was increased with DNAJC14 overexpression; however, hearing function and enlarged endolymphatic hydrops were not recovered. These results indicate that DNAJC14 overexpression ameliorates the cochlear degeneration caused by misfolded pendrin and might be a potential therapeutic target for DFNB4., (© 2019 The Authors.)

Published

2019

47. Contribution of SLC26A4 to the molecular diagnosis of nonsyndromic prelingual sensorineural hearing loss in a Brazilian cohort.

Author

Carvalho, Simone da Costa e Silva, Grangeiro, Carlos Henrique Paiva, Picanço-Albuquerque, Clarissa Gondim, dos Anjos, Thaís Oliveira, De Molfetta, Greice Andreotti, Silva, Wilson Araujo, and Ferraz, Victor Evangelista de Faria

Subjects

DIAGNOSIS of deafness, GENETIC disorders, GENETIC mutation, HUMAN genetic variation, GENES

Abstract

Objective: Hereditary hearing loss (HL) is the most common sensorineural disorder in humans. Besides mutations in GJB2 and GJB6 genes, pathogenic variants in the SLC26A4 gene have been reported as a cause of hereditary HL due to its role in the physiology of the inner ear. In this research we wanted to investigate the prevalence of mutations in SLC26A4 in Brazilian patients with nonsyndromic prelingual sensorineural HL. We applied the high-resolution melting technique to screen 88 DNA samples from unrelated deaf individuals that were previously screened for GJB2 , GJB6 and MT - RNR1 mutations. Results: The frequency of mutations in the SLC26A4 gene was 28.4%. Two novel mutations were found: p.Ile254Val and p.Asn382Lys. The mutation c.-66C>G (rs17154282) in the promoter region of SLC26A4 , was the most frequent mutation found and was significantly associated with nonsyndromic prelingual sensorineural HL. After mutations in the GJB2 , GJB6 and mitochondrial genes, SLC26A4 mutations are considered the next most common cause of hereditary HL in Brazilian as well as in other populations, which corroborates with our data. Furthermore, we suggest the inclusion of the SCL26A4 gene in the investigation of hereditary HL since there was an increase in the frequency of the mutations found, up to 22.7%. [ABSTRACT FROM AUTHOR]

Published

2018

48. Novel mutations in the SLC26A4 gene

Author

Alessandro Castiglione, Marina Taddei Masieri, Alessandra Ferlini, Patrizia Trevisi, Micol Busi, Laura Astolfi, Valeria Guaran, Alessandro Martini, and Anna Ravani

Subjects

Proband, Male, Hearing loss, Pendred syndrome, Hearing Loss, Sensorineural, Deafness, medicine.disease_cause, Connexins, NO, Autosomal recessive trait, otorhinolaryngologic diseases, medicine, SLC26A4, Humans, DFNB4, Computer Simulation, Allele, Child, Genetics, Enlarged vestibular aqueduct, Mutation, biology, business.industry, Membrane Transport Proteins, Temporal Bone, General Medicine, Sequence Analysis, DNA, medicine.disease, Connexin 26, Radiography, Otorhinolaryngology, Sulfate Transporters, Pediatrics, Perinatology and Child Health, biology.protein, sense organs, medicine.symptom, business, GJB6, Goiter, Nodular

Abstract

Objectives Mutations in the SLC26A4 gene (7q22.3–7q31.1) are considered one of the most common causes of genetic hearing loss. There are two clinical forms related to these mutations: syndromic and non-syndromic deafness. The first one is named Pendred Syndrome (PS) when deafness is associated with thyroid goiter; the second is called DFNB4, when no other symptoms are present. Both are transmitted as an autosomal recessive trait, but simple heterozygotes can develop both forms of deafness. Actually it is thought that Pendred Syndrome occurs when both alleles of SLC26A4 gene are mutated; DFNB4 seems due to monoallelic mutations. PS and DFNB4 can be associated with inner ear malformations. In most of the cases (around 80%), these consist in Enlarged Vestibular Aqueduct (EVA). EVA can also be present without SLC26A4 mutations. Understanding the role of new SLC26A4 variants should facilitate clinical assessment, as well as diagnostic and therapeutic approaches. This investigation aims to detect and report genetic causes of two unrelated Italian boys with hearing loss. Methods Patients and family members underwent clinical, audiological and genetic evaluations. To identify genetic mutations, DNA sequencing of SLC26A4 gene (including all 21 exons, exon-intron boundaries and promoter region) was carried out. Results Both probands were affected by congenital, progressive and fluctuating mixed hearing loss. Temporal bone imaging revealed a bilateral EVA with no other abnormalities in both cases. Probands were heterozygotes for previously undescribed mutations in the SLC26A4 gene: R409H/IVS2+1delG (proband 1) and L236P/K590X (proband 2). No other mutations were detected in GJB2 , GJB6 genes or mitochondrial DNA (mit-DNA). Conclusions The IVS2+1delG and K590X mutations have not yet been described in literature but there is some evidence to suggest that they have a pathological role. The results underlined the importance of considering the complete DNA sequencing of the SLC26A4 gene for differential molecular diagnosis of deafness, especially in those patients affected by congenital, progressive and fluctuating mixed hearing loss with bilateral EVA.

Published

2012