Oxford Medical Genetics Laboratories, Oxford University Hospitals NHS Foundation Trust, Oxford, UK.
Genomics Quality Assessment (GenQA), Edinburgh, UK.
Eur J Hum Genet. 2020 Sep;28(9):1141-1159. doi: 10.1038/s41431-020-0643-7. Epub 2020 May 18.
Dystrophinopathies are X-linked diseases, including Duchenne muscular dystrophy and Becker muscular dystrophy, due to DMD gene variants. In recent years, the application of new genetic technologies and the availability of new personalised drugs have influenced diagnostic genetic testing for dystrophinopathies. Therefore, these European best practice guidelines for genetic testing in dystrophinopathies have been produced to update previous guidelines published in 2010.These guidelines summarise current recommended technologies and methodologies for analysis of the DMD gene, including testing for deletions and duplications of one or more exons, small variant detection and RNA analysis. Genetic testing strategies for diagnosis, carrier testing and prenatal diagnosis (including non-invasive prenatal diagnosis) are then outlined. Guidelines for sequence variant annotation and interpretation are provided, followed by recommendations for reporting results of all categories of testing. Finally, atypical findings (such as non-contiguous deletions and dual DMD variants), implications for personalised medicine and clinical trials and incidental findings (identification of DMD gene variants in patients where a clinical diagnosis of dystrophinopathy has not been considered or suspected) are discussed.
肌营养不良蛋白病是 X 连锁疾病,包括杜兴氏肌营养不良症和贝克肌营养不良症,这是由于 DMD 基因突变所致。近年来,新的基因技术的应用和新型个体化药物的出现,影响了肌营养不良蛋白病的遗传诊断检测。因此,制定了这些肌营养不良蛋白病基因检测的欧洲最佳实践指南,以更新 2010 年发布的先前指南。这些指南总结了目前推荐用于分析 DMD 基因的技术和方法,包括一个或多个外显子缺失和重复、小变异检测和 RNA 分析。然后概述了诊断、携带者检测和产前诊断(包括非侵入性产前诊断)的遗传检测策略。提供了序列变异注释和解释的指南,然后是对所有类别检测结果报告的建议。最后,讨论了非典型发现(如不连续缺失和双重 DMD 变异)、对个体化医学和临床试验的影响以及偶然发现(在未考虑或怀疑肌营养不良症临床诊断的患者中发现 DMD 基因突变)。
