Gonçalves-Rocha Miguel, Oliveira Jorge, Rodrigues Luísa, Santos Rosário
Unidade de Genética Médica, Centro de Genética Médica, Dr. Jacinto de Magalhães, INSA-IP, Praça Pedro Nunes 88, Porto, Portugal.
Genet Test Mol Biomarkers. 2011 May;15(5):319-26. doi: 10.1089/gtmb.2010.0164. Epub 2011 Feb 17.
Autosomal recessive spinal muscular atrophy, the leading genetic cause of infant death, is due to loss of functional SMN1 genes, mainly as a result of homozygous deletions. Carrier frequency in the general population varies widely from 1/50 to 1/125 and has significant counseling implications. In a cohort of 210 patients with spinal muscular atrophy confirmed at the molecular level, 91.9% had a homozygous deletion and 14 were compound heterozygotes. Two novel point mutations were detected (c.524delC and c.734dupC) and the 11 bp duplication c.770_780dup was found at a high frequency. We describe the development of a simple and robust method for homozygous deletion detection, which enabled us to simplify the diagnostic workup. Further, carrier frequency in our population was established by direct quantification with the commercially available MLPA kit, following optimization for the use of dried blood spots as sample specimens.
常染色体隐性脊髓性肌萎缩症是导致婴儿死亡的主要遗传性病因,主要是由于功能性SMN1基因缺失,主要原因是纯合缺失。普通人群中的携带者频率差异很大,从1/50到1/125不等,具有重要的咨询意义。在一组经分子水平确诊的210例脊髓性肌萎缩症患者中,91.9%有纯合缺失,14例为复合杂合子。检测到两个新的点突变(c.524delC和c.734dupC),并且高频发现了11bp重复c.770_780dup。我们描述了一种简单且可靠的纯合缺失检测方法的开发,这使我们能够简化诊断检查。此外,在将干血斑用作样本标本进行优化后,通过使用市售的MLPA试剂盒直接定量确定了我们人群中的携带者频率。
