McCann Emily P, Henden Lyndal, Fifita Jennifer A, Zhang Katharine Y, Grima Natalie, Bauer Denis C, Chan Moi Fat Sandrine, Twine Natalie A, Pamphlett Roger, Kiernan Matthew C, Rowe Dominic B, Williams Kelly L, Blair Ian P
Macquarie University Centre for Motor Neuron Disease Research, Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Macquarie University, Sydney, New South Wales, Australia.
Transformational Bioinformatics, Commonwealth Scientific and Industrial Research Organisation, Sydney, New South Wales, Australia.
J Med Genet. 2020 May 14. doi: 10.1136/jmedgenet-2020-106866.
Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease with phenotypic and genetic heterogeneity. Approximately 10% of cases are familial, while remaining cases are classified as sporadic. To date, >30 genes and several hundred genetic variants have been implicated in ALS.
Seven hundred and fifty-seven sporadic ALS cases were recruited from Australian neurology clinics. Detailed clinical data and whole genome sequencing (WGS) data were available from 567 and 616 cases, respectively, of which 426 cases had both datasets available. As part of a comprehensive genetic analysis, 853 genetic variants previously reported as ALS-linked mutations or disease-associated alleles were interrogated in sporadic ALS WGS data. Statistical analyses were performed to identify correlation between clinical variables, and between phenotype and the number of ALS-implicated variants carried by an individual. Relatedness between individuals carrying identical variants was assessed using identity-by-descent analysis.
Forty-three ALS-implicated variants from 18 genes, including , , and were identified in Australian sporadic ALS cases. One-third of cases carried at least one variant and 6.82% carried two or more variants, implicating a potential oligogenic or polygenic basis of ALS. Relatedness was detected between two sporadic ALS cases carrying a p.I114T mutation, and among three cases carrying a p.K238E mutation. Oligogenic/polygenic sporadic ALS cases showed earlier age of onset than those with no reported variant.
We confirm phenotypic associations among ALS cases, and highlight the contribution of genetic variation to all forms of ALS.
肌萎缩侧索硬化症(ALS)是一种具有表型和遗传异质性的致命神经退行性疾病。约10%的病例为家族性,其余病例归类为散发性。迄今为止,已有超过30个基因和数百个遗传变异与ALS相关。
从澳大利亚神经科诊所招募了757例散发性ALS病例。分别有567例和616例可获得详细的临床数据和全基因组测序(WGS)数据,其中426例同时具备这两个数据集。作为全面遗传分析的一部分,在散发性ALS的WGS数据中对先前报告为与ALS相关的突变或疾病相关等位基因的853个遗传变异进行了研究。进行统计分析以确定临床变量之间以及表型与个体携带的ALS相关变异数量之间的相关性。使用同源性分析评估携带相同变异个体之间的亲缘关系。
在澳大利亚散发性ALS病例中鉴定出18个基因的43个与ALS相关的变异,包括 、 、 和 。三分之一的病例携带至少一个变异,6.82%的病例携带两个或更多变异,这暗示了ALS可能存在寡基因或多基因基础。在携带 p.I114T突变的两个散发性ALS病例之间以及在携带 p.K238E突变的三个病例之间检测到亲缘关系。寡基因/多基因散发性ALS病例的发病年龄比未报告变异的病例更早。
我们证实了ALS病例之间的表型关联,并强调了遗传变异对所有形式ALS的贡献。
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