The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia

Standard

The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia. / Pshennikova, Vera G; Teryutin, Fedor M; Borisova, Tuyara V et al.

In: Journal of human genetics, 2025.

Research output: Contribution to journal › Article › peer-review

Harvard

Pshennikova, VG, Teryutin, FM, Borisova, TV, Romanov, GP, Cherdonova, AM, Nikanorova, AA, Morozov, IV, Bondar, AA, Solovyev, AV, Fedorova, SA & Barashkov, NA 2025, 'The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia', Journal of human genetics. https://doi.org/10.1038/s10038-025-01406-1

APA

Pshennikova, V. G., Teryutin, F. M., Borisova, T. V., Romanov, G. P., Cherdonova, A. M., Nikanorova, A. A., Morozov, I. V., Bondar, A. A., Solovyev, A. V., Fedorova, S. A., & Barashkov, N. A. (2025). The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia. Journal of human genetics. https://doi.org/10.1038/s10038-025-01406-1

Vancouver

Pshennikova VG, Teryutin FM, Borisova TV, Romanov GP, Cherdonova AM, Nikanorova AA et al. The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia. Journal of human genetics. 2025. Epub 2025 Sept 16. doi: 10.1038/s10038-025-01406-1

Author

Pshennikova, Vera G ; Teryutin, Fedor M ; Borisova, Tuyara V et al. / The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia. In: Journal of human genetics. 2025.

BibTeX

@article{21225f1bd0d145eea75025b222758ec7,

title = "The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia",

abstract = "Previously only two families were known with progressive autosomal recessive deafness 103 (DFNB103, OMIM616042) caused by pathogenic variants of the CLIC5 gene. In this study we present the novel truncating variant c.644 G > A p.(Trp215*) of this gene which was found in homozygous state among 22 patients with hearing loss (HL) from 16 unrelated families living in the Sakha Republic of Russia (Eastern Siberia). Genotype-phenotype analysis in patients with DFNB103 showed that HL was sensorineural, symmetrical and variable by severity (from moderate to profound). Audiograms mostly have a down curve configuration, with pronounced loss of high and mid frequencies. In most cases this form of HL was detected in the post-lingual period (mean age 7.9 ± 1.2 years) and has a significant severity progression with age. In average the patients with DFNB103 lost 7.4 ± 13.65 dB on the speech frequency range in pure tone averages (PTA0.5,1.0,2.0,4.0 kHz) per year until reaching profound deafness in the second or third decade of the life. The high frequency of c.644 G > A p.(Trp215*) was found among Siberian GJB2-negative patients (9.9%) and this variant was not detected in GJB2-negative patients of Caucasian descent (predominantly Russians). The haplotype analysis based on the 730,000 whole genome SNP-markers indicates common origin of all studied mutant chromosomes. We conclude that the high prevalence of DFNB103 in Eastern Siberia is the result of founder effect, which occurred ~2500 years ago (~78 generations). These findings expand our knowledge of causative role of pathogenic variants in CLIC5 gene to the etiology of the HL.",

author = "Pshennikova, {Vera G} and Teryutin, {Fedor M} and Borisova, {Tuyara V} and Romanov, {Georgii P} and Cherdonova, {Alexandra M} and Nikanorova, {Alena A} and Morozov, {Igor V} and Bondar, {Alexander A} and Solovyev, {Aisen V} and Fedorova, {Sardana A} and Barashkov, {Nikolay A}",

note = "This study was supported by the YSC CMP project “Study of the genetic structure and burden of hereditary pathology of the populations of the Republic of Sakha (Yakutia)” and by the Ministry of Science and Higher Education of the Russian Federation (FSRG-2023-0003). The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia / V. G. Pshennikova, F. M. Teryutin, T. V. Borisova, G. P. Romanov, A. M. Cherdonova, A. A. Nikanorova, I. V. Morozov, A. A. Bondar, A. V. Solovyev, S. A. Fedorova, N. A. Barashkov // Journal of human genetics. - 2025. ",

year = "2025",

doi = "10.1038/s10038-025-01406-1",

language = "English",

journal = "Journal of human genetics",

issn = "1434-5161",

publisher = "Springer Nature",

}

RIS

TY - JOUR

T1 - The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia

AU - Pshennikova, Vera G

AU - Teryutin, Fedor M

AU - Borisova, Tuyara V

AU - Romanov, Georgii P

AU - Cherdonova, Alexandra M

AU - Nikanorova, Alena A

AU - Morozov, Igor V

AU - Bondar, Alexander A

AU - Solovyev, Aisen V

AU - Fedorova, Sardana A

AU - Barashkov, Nikolay A

N1 - This study was supported by the YSC CMP project “Study of the genetic structure and burden of hereditary pathology of the populations of the Republic of Sakha (Yakutia)” and by the Ministry of Science and Higher Education of the Russian Federation (FSRG-2023-0003). The c.644 G > A p.(Trp215*) founder variant in the CLIC5 gene causes progressive autosomal recessive deafness 103 (DFNB103) in Eastern Siberia / V. G. Pshennikova, F. M. Teryutin, T. V. Borisova, G. P. Romanov, A. M. Cherdonova, A. A. Nikanorova, I. V. Morozov, A. A. Bondar, A. V. Solovyev, S. A. Fedorova, N. A. Barashkov // Journal of human genetics. - 2025.

PY - 2025

Y1 - 2025

N2 - Previously only two families were known with progressive autosomal recessive deafness 103 (DFNB103, OMIM616042) caused by pathogenic variants of the CLIC5 gene. In this study we present the novel truncating variant c.644 G > A p.(Trp215*) of this gene which was found in homozygous state among 22 patients with hearing loss (HL) from 16 unrelated families living in the Sakha Republic of Russia (Eastern Siberia). Genotype-phenotype analysis in patients with DFNB103 showed that HL was sensorineural, symmetrical and variable by severity (from moderate to profound). Audiograms mostly have a down curve configuration, with pronounced loss of high and mid frequencies. In most cases this form of HL was detected in the post-lingual period (mean age 7.9 ± 1.2 years) and has a significant severity progression with age. In average the patients with DFNB103 lost 7.4 ± 13.65 dB on the speech frequency range in pure tone averages (PTA0.5,1.0,2.0,4.0 kHz) per year until reaching profound deafness in the second or third decade of the life. The high frequency of c.644 G > A p.(Trp215*) was found among Siberian GJB2-negative patients (9.9%) and this variant was not detected in GJB2-negative patients of Caucasian descent (predominantly Russians). The haplotype analysis based on the 730,000 whole genome SNP-markers indicates common origin of all studied mutant chromosomes. We conclude that the high prevalence of DFNB103 in Eastern Siberia is the result of founder effect, which occurred ~2500 years ago (~78 generations). These findings expand our knowledge of causative role of pathogenic variants in CLIC5 gene to the etiology of the HL.

AB - Previously only two families were known with progressive autosomal recessive deafness 103 (DFNB103, OMIM616042) caused by pathogenic variants of the CLIC5 gene. In this study we present the novel truncating variant c.644 G > A p.(Trp215*) of this gene which was found in homozygous state among 22 patients with hearing loss (HL) from 16 unrelated families living in the Sakha Republic of Russia (Eastern Siberia). Genotype-phenotype analysis in patients with DFNB103 showed that HL was sensorineural, symmetrical and variable by severity (from moderate to profound). Audiograms mostly have a down curve configuration, with pronounced loss of high and mid frequencies. In most cases this form of HL was detected in the post-lingual period (mean age 7.9 ± 1.2 years) and has a significant severity progression with age. In average the patients with DFNB103 lost 7.4 ± 13.65 dB on the speech frequency range in pure tone averages (PTA0.5,1.0,2.0,4.0 kHz) per year until reaching profound deafness in the second or third decade of the life. The high frequency of c.644 G > A p.(Trp215*) was found among Siberian GJB2-negative patients (9.9%) and this variant was not detected in GJB2-negative patients of Caucasian descent (predominantly Russians). The haplotype analysis based on the 730,000 whole genome SNP-markers indicates common origin of all studied mutant chromosomes. We conclude that the high prevalence of DFNB103 in Eastern Siberia is the result of founder effect, which occurred ~2500 years ago (~78 generations). These findings expand our knowledge of causative role of pathogenic variants in CLIC5 gene to the etiology of the HL.

UR - https://pubmed.ncbi.nlm.nih.gov/40957967/

UR - https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=105016818650&origin=inward

UR - https://www.mendeley.com/catalogue/f35f2641-0830-3d8a-92ed-0392c0f96d09/

U2 - 10.1038/s10038-025-01406-1

DO - 10.1038/s10038-025-01406-1

M3 - Article

C2 - 40957967

JO - Journal of human genetics

JF - Journal of human genetics

SN - 1434-5161

ER -

ID: 69974251