Clinical and genetic analysis of children with hearing loss and bilateral enlarged vestibular aqueducts.

Atsuko Nakano Yukiko Arimoto Hideki Mutai Kiyomitsu Nara Satomi Inoue Tatsuo Matsunaga

Int J Pediatr Otorhinolaryngol

Division of Hearing and Balance Research, National Institute of Sensory Organs, National Hospital Organization Tokyo Medical Center, 2-5-1 Higashigaoka, Meguro-ku, Tokyo, 152-8902, Japan; Medical Genetics Center, National Hospital Organization Tokyo Medical Center, 2-5-1 Higashigaoka, Meguro-ku, Tokyo, 152-8902, Japan.

Published: January 2022

The study aimed to assess the clinical and genetic characteristics of children with hearing loss related to bilateral enlargement of vestibular aqueducts (EVA), a common inner ear malformation, by examining 28 children diagnosed between 2008 and 2019.
Results showed that a majority experienced hearing fluctuations and progressive hearing loss, with 39.2% reporting vertigo. Genetic testing revealed that 88.9% had pathogenic variants of the SLC26A4 gene, linked to Pendred syndrome/DFNB4.
The findings indicate that existing newborn hearing screenings may miss some cases of bilateral EVA, and that nearly half of the subjects might not have received genetic diagnoses if relying solely

Objectives: To evaluate the clinical and genetic features of children with hearing loss associated with one of the most common malformations of the inner ear: bilateral enlargement of vestibular aqueducts (EVA).

Methods: Clinical and genetic features were investigated in 28 children with hearing loss diagnosed with bilateral EVA by computed tomography from January 2008 to September 2019.

Results: Fourteen subjects had undergone newborn hearing screening (NHS). Nine subjects (64.3%) were referred in both ears, 4 subjects (28.6%) were referred in one ear, and one subject (7.1%) passed in both ears. Nineteen of 26 subjects (73.1%) who were followed for more than 3 years had hearing fluctuations, while 17 (65.4%) had hearing loss progression. Eleven of 28 subjects (39.2%) had vertigo attacks. Pathogenic variants were identified in two alleles of the SLC26A4 gene in 24 of 27 subjects (88.9%) by sequencing of all exons and flanking introns, leading to genetic diagnosis of Pendred syndrome/DFNB4. Our results indicate that genetic screening for specific SLC26A4 variants using a commercial clinical laboratory test in Japan would have achieved genetic diagnoses in 13 of the 27 subjects (54.2%). Although there was no statistically significance in the frequency of hearing fluctuation or progression depending on the presence or absence of the gene variant, mean hearing level was severe in subjects with two pathogenic variants in SLC26A4 gene. The most common variant detected in our subjects was p.His723Arg (13 alleles, 27.1%), followed by c. 919-2A > G (four alleles, 8.3%). Two novel variants were detected in this study: c.1544+1G > T and c.1614+5G > A.

Conclusions: Our data suggest that some subjects may present with bilateral EVA that cannot be detected by NHS. We estimated that genetic diagnosis for SLC264 gene would not have been made in almost half subjects with the commercial genetic screening approach used in the present study in Japan. Although there were some limitations in this study, the subjects with pathogenic variants in two alleles of the SLC26A4 gene could have more severe hearing loss.

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http://dx.doi.org/10.1016/j.ijporl.2021.110975	DOI Listing

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