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. 2016 Aug;135(8):953-61.
doi: 10.1007/s00439-016-1697-z. Epub 2016 Jun 25.

Spectrum of DNA variants for non-syndromic deafness in a large cohort from multiple continents

Denise Yan  1 Demet Tekin  1 Guney Bademci  2 Joseph Foster 2nd  1   2 F Basak Cengiz  2 Abhiraami Kannan-Sundhari  1 Shengru Guo  2 Rahul Mittal  1 Bing Zou  1 Mhamed Grati  1 Rosemary I Kabahuma  3 Mohan Kameswaran  4 Taye J Lasisi  5 Waheed A Adedeji  5 Akeem O Lasisi  5 Ibis Menendez  2 Marianna Herrera  6 Claudia Carranza  6 Reza Maroofian  7 Andrew H Crosby  7 Mariem Bensaid  8 Saber Masmoudi  8 Mahdiyeh Behnam  9 Majid Mojarrad  10 Yong Feng  11 Duygu Duman  12 Alex M Mawla  13   14 Alex S Nord  13   14 Susan H Blanton  1   2   15 Xue Z Liu  16   17   18 Mustafa Tekin  19   20   21
Affiliations

Spectrum of DNA variants for non-syndromic deafness in a large cohort from multiple continents

Denise Yan et al. Hum Genet. 2016 Aug.

Abstract

Hearing loss is the most common sensory deficit in humans with causative variants in over 140 genes. With few exceptions, however, the population-specific distribution for many of the identified variants/genes is unclear. Until recently, the extensive genetic and clinical heterogeneity of deafness precluded comprehensive genetic analysis. Here, using a custom capture panel (MiamiOtoGenes), we undertook a targeted sequencing of 180 genes in a multi-ethnic cohort of 342 GJB2 mutation-negative deaf probands from South Africa, Nigeria, Tunisia, Turkey, Iran, India, Guatemala, and the United States (South Florida). We detected causative DNA variants in 25 % of multiplex and 7 % of simplex families. The detection rate varied between 0 and 57 % based on ethnicity, with Guatemala and Iran at the lower and higher end of the spectrum, respectively. We detected causative variants within 27 genes without predominant recurring pathogenic variants. The most commonly implicated genes include MYO15A, SLC26A4, USH2A, MYO7A, MYO6, and TRIOBP. Overall, our study highlights the importance of family history and generation of databases for multiple ethnically discrete populations to improve our ability to detect and accurately interpret genetic variants for pathogenicity.

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Conflict of interest statement

Conflict of interest The authors declare no conflict of interest.

Figures

Fig. 1
Fig. 1
Representation of solved, unsolved and uncertain families, based on ethnicity and simplex/multiplex status (A). Number of solved families for each gene and ethnicity (B).
See this image and copyright information in PMC

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Supplementary concepts