Schulz Heidi L, Grassmann Felix, Kellner Ulrich, Spital Georg, Rüther Klaus, Jägle Herbert, Hufendiek Karsten, Rating Philipp, Huchzermeyer Cord, Baier Maria J, Weber Bernhard H F, Stöhr Heidi
Institute of Human Genetics, University of Regensburg, Regensburg, Germany.
Rare Retinal Disease Center, AugenZentrum Siegburg, MVZ ADTC Siegburg GmbH, Siegburg, Germany 3RetinaScience, Bonn, Germany.
Invest Ophthalmol Vis Sci. 2017 Jan 1;58(1):394-403. doi: 10.1167/iovs.16-19936.
Stargardt disease (STGD1) is an autosomal recessive retinopathy, caused by mutations in the retina-specific ATP-binding cassette transporter (ABCA4) gene. To establish the mutational spectrum and to assess effects of selected deep intronic and common genetic variants on disease, we performed a comprehensive sequence analysis in a large cohort of German STGD1 patients.
DNA samples of 335 STGD1 patients were analyzed for ABCA4 mutations in its 50 coding exons and adjacent intronic sequences by resequencing array technology or next generation sequencing (NGS). Parts of intron 30 and 36 were screened by Sanger chain-terminating dideoxynucleotide sequencing. An in vitro splicing assay was used to test selected variants for their splicing behavior. By logistic regression analysis we assessed the association of common ABCA4 alleles while a multivariate logistic regression model calculated a genetic risk score (GRS).
Our analysis identified 148 pathogenic or likely pathogenic mutations, of which 48 constitute so far unpublished ABCA4-associated disease alleles. Four rare deep intronic variants were found once in 472 alleles analyzed. In addition, we identified six risk-modulating common variants. Genetic risk score estimates suggest that defined common ABCA4 variants influence disease risk in carriers of a single pathogenic ABCA4 allele.
Our study adds to the mutational spectrum of the ABCA4 gene. Moreover, in our cohort, deep intronic variants in intron 30 and 36 likely play no or only a minor role in disease pathology. Of note, our findings demonstrate a possible modifying effect of common sequence variants on ABCA4-associated disease.
斯塔加特病(STGD1)是一种常染色体隐性视网膜病变,由视网膜特异性ATP结合盒转运蛋白(ABCA4)基因突变引起。为了确定突变谱并评估特定的内含子深处和常见基因变异对疾病的影响,我们对一大群德国STGD1患者进行了全面的序列分析。
通过重测序阵列技术或下一代测序(NGS)分析335例STGD1患者的DNA样本,检测ABCA4基因50个编码外显子及其相邻内含子序列中的突变。利用桑格双脱氧链终止测序法对第30和36内含子的部分区域进行筛查。采用体外剪接试验检测选定变异的剪接行为。通过逻辑回归分析评估常见ABCA4等位基因的关联性,同时使用多变量逻辑回归模型计算遗传风险评分(GRS)。
我们的分析鉴定出148个致病或可能致病的突变,其中48个是迄今未发表的与ABCA4相关的疾病等位基因。在分析的472个等位基因中,发现了4个罕见的内含子深处变异。此外,我们还鉴定出6个调节风险的常见变异。遗传风险评分估计表明,特定的常见ABCA4变异会影响单个致病ABCA4等位基因携带者的疾病风险。
我们的研究增加了ABCA4基因的突变谱。此外,在我们的队列中,第30和36内含子中的内含子深处变异在疾病病理中可能不起作用或仅起次要作用。值得注意的是,我们的研究结果证明了常见序列变异对ABCA4相关疾病可能具有修饰作用。
