| Literature DB >> 19646679 |
Saima Riazuddin1, Saima Anwar, Martin Fischer, Zubair M Ahmed, Shahid Y Khan, Audrey G H Janssen, Ahmad U Zafar, Ute Scholl, Tayyab Husnain, Inna A Belyantseva, Penelope L Friedman, Sheikh Riazuddin, Thomas B Friedman, Christoph Fahlke.
Abstract
BSND encodes barttin, an accessory subunit of renal and inner ear chloride channels. To date, all mutations of BSND have been shown to cause Bartter syndrome type IV, characterized by significant renal abnormalities and deafness. We identified a BSND mutation (p.I12T) in four kindreds segregating nonsyndromic deafness linked to a 4.04-cM interval on chromosome 1p32.3. The functional consequences of p.I12T differ from BSND mutations that cause renal failure and deafness in Bartter syndrome type IV. p.I12T leaves chloride channel function unaffected and only interferes with chaperone function of barttin in intracellular trafficking. This study provides functional data implicating a hypomorphic allele of BSND as a cause of apparent nonsyndromic deafness. We demonstrate that BSND mutations with different functional consequences are the basis for either syndromic or nonsyndromic deafness.Entities:
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Year: 2009 PMID: 19646679 PMCID: PMC2725234 DOI: 10.1016/j.ajhg.2009.07.003
Source DB: PubMed Journal: Am J Hum Genet ISSN: 0002-9297 Impact factor: 11.025