中国肌萎缩侧索硬化症患者存在罕见变异与生存率低有关。

IF 3.7 Q2 GENETICS & HEREDITY Phenomics (Cham, Switzerland) Pub Date : 2023-02-12 eCollection Date: 2023-04-01 DOI:10.1007/s43657-022-00093-8
Siqi Dong, Xianhong Yin, Kun Wang, Wenbo Yang, Jiatong Li, Yi Wang, Yanni Zhou, Xiaoni Liu, Jiucun Wang, Xiangjun Chen
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摘要

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。最近的研究表明,ALS是一种寡基因基础,其中两种或多种基因变体的共同出现具有相加或协同的有害影响。为了评估可能的寡基因遗传的贡献,我们对来自中国东部五个家系的57名散发性ALS(sALS)患者和8名家族性ALS患者的43个相关基因进行了分析。我们使用外显子集合联盟、1000个基因组和华标项目的组合过滤罕见变体。我们分析了43个已知ALS致病基因中存在多种罕见变异的患者及其基因型-表型相关性。总的来说,我们在16个不同的基因中检测到了30种罕见的变体,并发现16名sALS患者和所有接受检查的fALS患者在所研究的基因中至少携带一种变体,其中两名sALS和四名fALS病人携带两种或多种变体。值得注意的是,ALS基因有一个或多个变异的sALS患者的生存率比没有变异的患者差。通常,在一个有三种变体的fALS谱系中,有三种变异的家族成员(超氧化物歧化酶1(SOD1)p.V48A、视神经磷酸酶(OPTN)p.A433V和TANK结合激酶1(TBK1)p.R573H)表现出比携带一种变异的成员(TBK1 p.R573H)更严重的疾病表型。我们的研究结果表明,罕见的变异可能会产生负面的预后影响,从而支持ALS的寡基因遗传。
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Presence of Rare Variants is Associated with Poorer Survival in Chinese Patients with Amyotrophic Lateral Sclerosis.

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disorder with phenotypic and genetic heterogeneity. Recent studies have suggested an oligogenic basis of ALS, in which the co-occurrence of two or more genetic variants has additive or synergistic deleterious effects. To assess the contribution of possible oligogenic inheritance, we profiled a panel of 43 relevant genes in 57 sporadic ALS (sALS) patients and eight familial ALS (fALS) patients from five pedigrees in east China. We filtered rare variants using the combination of the Exome Aggregation Consortium, the 1000 Genomes and the HuaBiao Project. We analyzed patients with multiple rare variants in 43 known ALS causative genes and the genotype-phenotype correlation. Overall, we detected 30 rare variants in 16 different genes and found that 16 of the sALS patients and all the fALS patients examined harbored at least one variant in the investigated genes, among which two sALS and four fALS patients harbored two or more variants. Of note, the sALS patients with one or more variants in ALS genes had worse survival than the patients with no variants. Typically, in one fALS pedigree with three variants, the family member with three variants (Superoxide dismutase 1 (SOD1) p.V48A,  Optineurin (OPTN) p.A433V and TANK binding kinase 1 (TBK1) p.R573H) exhibited much more severe disease phenotype than the member carrying one variant (TBK1 p.R573H). Our findings suggest that rare variants could exert a negative prognostic effect, thereby supporting the oligogenic inheritance of ALS.

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