Joensuu T, Hämäläinen R, Yuan B, Johnson C, Tegelberg S, Gasparini P, Zelante L, Pirvola U, Pakarinen L, Lehesjoki A E, de la Chapelle A, Sankila E M
The Folkhälsan Institute of Genetics, Biomedicum Helsinki, University of Helsinki, Helsinki, Finland.
Am J Hum Genet. 2001 Oct;69(4):673-84. doi: 10.1086/323610. Epub 2001 Aug 27.
Usher syndrome type 3 (USH3) is an autosomal recessive disorder characterized by progressive hearing loss, severe retinal degeneration, and variably present vestibular dysfunction, assigned to 3q21-q25. Here, we report on the positional cloning of the USH3 gene. By haplotype and linkage-disequilibrium analyses in Finnish carriers of a putative founder mutation, the critical region was narrowed to 250 kb, of which we sequenced, assembled, and annotated 207 kb. Two novel genes-NOPAR and UCRP-and one previously identified gene-H963-were excluded as USH3, on the basis of mutational analysis. USH3, the candidate gene that we identified, encodes a 120-amino-acid protein. Fifty-two Finnish patients were homozygous for a termination mutation, Y100X; patients in two Finnish families were compound heterozygous for Y100X and for a missense mutation, M44K, whereas patients in an Italian family were homozygous for a 3-bp deletion leading to an amino acid deletion and substitution. USH3 has two predicted transmembrane domains, and it shows no homology to known genes. As revealed by northern blotting and reverse-transcriptase PCR, it is expressed in many tissues, including the retina.
3型Usher综合征(USH3)是一种常染色体隐性疾病,其特征为进行性听力丧失、严重视网膜变性以及程度不一的前庭功能障碍,定位于3q21 - q25。在此,我们报告USH3基因的定位克隆。通过对芬兰可能存在奠基者突变携带者进行单倍型和连锁不平衡分析,关键区域被缩小至250 kb,我们对其中207 kb进行了测序、组装和注释。基于突变分析,两个新基因——NOPAR和UCRP,以及一个先前已鉴定的基因——H963,被排除在USH3之外。我们鉴定出的候选基因USH3编码一种含120个氨基酸的蛋白质。52名芬兰患者为终止突变Y100X的纯合子;两个芬兰家族的患者为Y100X与错义突变M44K的复合杂合子,而一个意大利家族的患者为导致氨基酸缺失和替换的3 bp缺失的纯合子。USH3有两个预测的跨膜结构域,且与已知基因无同源性。通过Northern印迹法和逆转录酶PCR显示,它在包括视网膜在内的许多组织中表达。
