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Mutations in the human alpha-tectorin gene cause autosomal dominant non-syndromic hearing impairment

机译:人类α-tectorin基因突变导致常染色体显性遗传性非综合征性听力障碍

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The tectorial membrane is an extracellular matrix of the inner ear that contacts the stereocilia bundles of specialized sensory hair cells. Sound induces movement of these hair cells relative to the tectorial membrane, deflects the stereocilia, and leads to fluctuations in hair-cell membrane potential, transducing sound into electrical signals. alpha-tectorin is one of the major non-collagenous components of the tectorial membrane(1,2). Recently, the gene encoding mouse alpha-tectorin (Tecta) was mapped to a region of mouse chromosome 9, which shows evolutionary conservation with human chromosome 11q (ref. 3), where linkage was found in two families, one Belgian (DFNA12; ref. 4) and the other, Austrian (DFNA8; unpublished data), with autosomal dominant non-syndromic hearing impairment. We determined the complete sequence and the intron-exon structure of the human TECTA gene. In both families, mutation analysis revealed missense mutations which replace conserved amino-acid residues within the zona pellucida domain of TECTA. These findings indicate that mutations in TECTA are responsible for hearing impairment in these families, and implicate a new type of protein in the pathogenesis of hearing impairment. [References: 20]
机译:保护膜是内耳的细胞外基质,与特殊的感觉毛细胞的纤毛束接触。声音引起这些毛细胞相对于盖膜的运动,使纤毛偏斜,并导致毛细胞膜电位的波动,从而将声音转换为电信号。 α-tectorin是覆盖膜的主要非胶原成分之一(1,2)。最近,编码小鼠α-tectorin(Tecta)的基因被定位到小鼠9号染色体区域,该区域显示了与人类11q号染色体的进化保守性(参考文献3),在两个家族中发现了连锁,其中一个是比利时人(DFNA12;参考文献4)和另一个奥地利人(DFNA8;未发表的数据),具有常染色体显性遗传性非综合征性听力障碍。我们确定了人类TECTA基因的完整序列和内含子-外显子结构。在这两个家族中,突变分析均显示错义突变,这些突变取代了TECTA透明带结构域内的保守氨基酸残基。这些发现表明,TECTA中的突变是导致这些家族中听力障碍的原因,并在听力障碍的发病机理中暗示了一种新型蛋白质。 [参考:20]

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