| Literature DB >> 19309289 |
Hanen Belguith1, Mounira Aifa-Hmani, Houria Dhouib, Mariem Ben Said, Mohamed Ali Mosrati, Imed Lahmar, Jihen Moalla, Ilhem Charfeddine, Nabil Driss, Saida Ben Arab, Abdelmonem Ghorbel, Hammadi Ayadi, Saber Masmoudi.
Abstract
Recessive mutations of MYO15A are associated with nonsyndromic hearing loss (HL) in humans (DFNB3) and in the shaker-2 mouse. Human MYO15A has 66 exons and encodes unconventional myosin XVA. Analysis of 77 Tunisian consanguineous families segregating recessive deafness revealed evidence of linkage to microsatellite markers for DFNB3 in four families. In two families, sequencing of MYO15A led to the identification of two novel homozygous mutations: a nonsense (c.4998C>A (p.C1666X) in exon 17 and a splice site mutation in intron 54 (c.9229 + 1G>A). A novel mutation of unknown significance, c.7395 + 3G>C, was identified in the third family, and no mutation was found in the fourth family. In conclusion, we discovered three novel mutations of MYO15A, and our data suggest the possibility that there are two distinct genes at the DFNB3 locus.Entities:
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Year: 2009 PMID: 19309289 DOI: 10.1089/gtmb.2008.0077
Source DB: PubMed Journal: Genet Test Mol Biomarkers ISSN: 1945-0257