Arslan Ateş Esra, Türkyılmaz Ayberk, Eltan Sevgi Bilgiç, Barış Safa, Güney Ahmet Ilter
Department of Medical Genetics, Marmara University Pendik Training and Research Hospital, Istanbul, Turkey.
Department of Medical Genetics, Karadeniz Technical University Faculty of Medicine, Trabzon, Turkey.
Mol Syndromol. 2022 Feb;13(1):80-84. doi: 10.1159/000518629. Epub 2021 Oct 15.
Ataxia-telangiectasia (AT) is an autosomal recessive disorder characterized by progressive ataxia, choreoathetosis and immunodeficiency beginning in early childhood. An 8-year-old girl was referred with a diagnosis of AT. She had gait disturbance and dysarthria for 3years. Multiple cutaneous telangiectases were observed on her face, trunk and limbs. Sequence analysis of the gene revealed a homozygous c.7308-15A>G mutation in IVS49. Human Splicing Finder predicted that the mutation could activate an intronic cryptic acceptor site. We designed primers for amplification of related exons (48-50) from cDNA for evaluating splicing pattern. Sequencing of exons 48-50 revealed a 14-nucleotide insertion from intron 49, between exons 49 and 50, resulting in premature termination of translation at codon 2439. To conclude, we report a novel mutation in a classical AT case, which resulted in an alternatively spliced transcript and was predicted to form a truncated protein or null protein due to nonsense-mediated decay.
共济失调毛细血管扩张症(AT)是一种常染色体隐性疾病,其特征为始于儿童早期的进行性共济失调、舞蹈指划样动作和免疫缺陷。一名8岁女孩因被诊断为AT前来就诊。她有3年的步态障碍和构音障碍。在她的面部、躯干和四肢观察到多处皮肤毛细血管扩张。该基因的序列分析显示在第49内含子中有一个纯合的c.7308-15A>G突变。人类剪接预测器预测该突变可能激活一个内含子隐蔽性受体位点。我们设计了引物用于从cDNA扩增相关外显子(48-50)以评估剪接模式。外显子48-50的测序显示在第49内含子中有一个14个核苷酸的插入,位于外显子49和50之间,导致在密码子2439处翻译提前终止。总之,我们报告了一例经典AT病例中的一种新突变,该突变导致了一个选择性剪接的转录本,并预计由于无义介导的衰变形成截短蛋白或无蛋白。
