Molecular Epidemiology and Functional Assessment of Novel Allelic Variants of SLC26A4 in Non-Syndromic Hearing Loss Patients with Enlarged Vestibular Aqueduct in China
Yongyi Yuan,Weiwei Guo,Jie Tang,Guozheng Zhang,Guojian Wang,Mingyu Han,Xun Zhang,Shiming Yang,David Z.Z. He,Pu Dai +9 more
TL;DR: The functional assessment procedure can be applied to identification of pathogenicity of variants and are valuable for genetic diagnosis, genetic counseling, prenatal testing and pre-implantation diagnosis in EVA families.
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Abstract: Background
Mutations in SLC26A4, which encodes pendrin, are a common cause of deafness. SLC26A4 mutations are responsible for Pendred syndrome and non-syndromic enlarged vestibular aqueduct (EVA). The mutation spectrum of SLC26A4 varies widely among ethnic groups. To investigate the incidence of EVA in Chinese population and to provide appropriate genetic testing and counseling to patients with SLC26A4 variants, we conducted a large-scale molecular epidemiological survey of SLC26A4.
Methods
A total of 2352 unrelated non-syndromic hearing loss patients from 27 different regions of China were included. Hot spot regions of SLC26A4, exons 8, 10 and 19 were sequenced. For patients with one allelic variant in the hot spot regions, the other exons were sequenced one by one until two mutant alleles had been identified. Patients with SLC26A4 variants were then examined by temporal bone computed tomography scan for radiological diagnosis of EVA. Ten SLC26A4 variants were cloned for functional study. Confocal microscopy and radioisotope techniques were used to examine the membrane expression of pendrin and transporter function.
Results
Of the 86 types of variants found, 47 have never been reported. The ratio of EVA in the Chinese deaf population was at least 11%, and that in patients of Han ethnicity reached at least 13%. The mutational spectrum and mutation detection rate of SLC26A4 are distinct among both ethnicities and regions of Mainland China. Most of the variants caused retention of pendrin in the intracellular region. All the mutant pendrins showed significantly reduced transport capability.
Conclusion
An overall description of the molecular epidemiological findings of SLC26A4 in China is provided. The functional assessment procedure can be applied to identification of pathogenicity of variants. These findings are valuable for genetic diagnosis, genetic counseling, prenatal testing and pre-implantation diagnosis in EVA families.
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Citations
Expert specification of the ACMG/AMP variant interpretation guidelines for genetic hearing loss.
Andrea M. Oza,Andrea M. Oza,Marina T. DiStefano,Marina T. DiStefano,Sarah E. Hemphill,Brandon J. Cushman,Andrew R. Grant,Rebecca K. Siegert,Jun Shen,Jun Shen,Jun Shen,Alex Chapin,Nicole J. Boczek,Lisa A. Schimmenti,Jaclyn B. Murry,Linda Hasadsri,Kiyomitsu Nara,Margaret A. Kenna,Margaret A. Kenna,Kevin T. Booth,Kevin T. Booth,Hela Azaiez,Andrew J. Griffith,Karen B. Avraham,Hannie Kremer,Heidi L. Rehm,Sami S. Amr,Sami S. Amr,Sami S. Amr,Ahmad N. Abou Tayoun,Ahmad N. Abou Tayoun +30 more
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Genetic etiology study of the non-syndromic deafness in Chinese Hans by targeted next-generation sequencing.
TL;DR: Mutations in the less commonly screened deafness genes were heterogeneous and contributed to a significant percentage (17.4%) of causes for non-syndromic deafness.
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TL;DR: In this article , a clinical practice resource offers information about the frequency, causes, and presentations of hearing loss and suggests approaches to the clinical and genetic evaluation of deaf and hard-of-hearing individuals aimed at identifying an etiologic diagnosis and providing informative and effective patient education and genetic counseling.
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Comparative analysis of functional assay evidence use by ClinGen Variant Curation Expert Panels
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TL;DR: Current VCEP recommendations for functional assay evidence are a useful tool to improve the accessibility of functional data by providing a starting point for curators to identify approved functional assays and key metrics, however, the analysis suggests that further guidance is needed to standardize this process.
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