瑞典北部常染色体显性遗传和常染色体隐性遗传视网膜色素变性的突变谱。
Mutation spectra in autosomal dominant and recessive retinitis pigmentosa in northern Sweden.
机构信息
Department of Medical and Clinical Genetics, Umeå University, Umeå, Sweden.
出版信息
Adv Exp Med Biol. 2010;664:255-62. doi: 10.1007/978-1-4419-1399-9_29.
Abstract
Retinal degenerations represent a heterogeneous group of disorders affecting the function of the retina. The frequency of retinitis pigmentosa (RP) is 1/3500 worldwide, however, in northern Sweden it is 1/2000 due to limited migration and a 'founder' effect. In this study we identified genetic mechanisms underlying autosomal dominant and recessive RP present in northern Sweden. Several novel mutations unique for this region were found. In an autosomal recessive form of RP, Bothnia dystrophy caused by mutations in the RLBP1 gene, bi-allelic mutations R234W, M226K and compound heterozygosity, M226K+R234W was detected.In dominant form of RP mapped to 19q13.42 a 59 kb genomic deletion including the PRPF31 and three other genes was found.These data provide additional information on the molecular mechanisms of RP evolvement and in the future might be useful in development of therapeutic strategies. Identification of the disease-causing mutations allowed introducing molecular genetic testing of the patients and their families into the clinical practice.
摘要
视网膜变性是一组影响视网膜功能的异质性疾病。全世界范围内色素性视网膜炎(RP)的发病率为 1/3500,但由于瑞典北部移民受限和“奠基者”效应,其发病率为 1/2000。在本研究中,我们鉴定了在瑞典北部存在的常染色体显性和隐性 RP 的遗传机制。发现了一些该地区特有的新突变。在由 RLBP1 基因突变引起的常染色体隐性形式的 RP 中,发现了 Bothnia 营养不良,该疾病由 R234W、M226K 双等位基因突变和复合杂合性 M226K+R234W 引起。在定位于 19q13.42 的显性 RP 中,发现了包含 PRPF31 和另外三个基因的 59 kb 基因组缺失。这些数据为 RP 演变的分子机制提供了更多信息,并且将来可能对治疗策略的发展有用。致病突变的鉴定使得对患者及其家族进行分子遗传测试能够引入临床实践。
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