Department of Molecular Biology and Genetics, Boğaziçi University, 34342, Istanbul, Turkey.
Department of Neurology, School of Medicine, Ankara University, 06230, Ankara, Turkey.
Neurogenetics. 2017 Dec;18(4):237-243. doi: 10.1007/s10048-017-0527-3. Epub 2017 Oct 31.
Amyotrophic lateral sclerosis (ALS) is a motor neuron disease eventually leading to death from respiratory failure. Recessive inheritance is very rare. Here, we describe the clinical findings in a consanguineous family with five men afflicted with recessive ALS and the identification of the homozygous mutation responsible for the disorder. The onset of the disease ranged from 12 to 35 years of age, with variable disease progressions. We performed clinical investigations including metabolic and paraneoplastic screening, cranial and cervical imaging, and electrophysiology. We mapped the disease gene to 9p21.1-p12 with a LOD score of 5.2 via linkage mapping using genotype data for single-nucleotide polymorphism markers and performed exome sequence analysis to identify the disease-causing gene variant. We also Sanger sequenced all coding sequences of SIGMAR1, a gene reported as responsible for juvenile ALS in a family. We did not find any mutation in SIGMAR1. Instead, we identified a novel homozygous missense mutation p.(His705Arg) in GNE which was predicted as damaging by online tools. GNE has been associated with inclusion body myopathy and is expressed in many tissues. We propose that the GNE mutation underlies the pathology in the family.
肌萎缩侧索硬化症(ALS)是一种运动神经元疾病,最终会导致呼吸衰竭而死亡。隐性遗传非常罕见。在这里,我们描述了一个患有隐性 ALS 的近亲家庭的临床发现,并确定了导致该疾病的纯合突变。疾病的发病年龄从 12 岁到 35 岁不等,疾病进展情况各不相同。我们进行了临床调查,包括代谢和副肿瘤筛查、颅颈成像和电生理学检查。我们通过连锁分析,利用单核苷酸多态性标记的基因型数据,将疾病基因映射到 9p21.1-p12,连锁值为 5.2。我们还进行了外显子组序列分析,以确定致病基因变异。我们还对 SIGMAR1 的所有编码序列进行了 Sanger 测序,该基因在一个家族中被报道为青少年 ALS 的致病基因。我们没有发现 SIGMAR1 中的任何突变。相反,我们在 GNE 中发现了一个新的纯合错义突变 p.(His705Arg),在线工具预测该突变具有破坏性。GNE 与包涵体肌病有关,并在许多组织中表达。我们提出 GNE 突变是该家族发病的基础。
