TARDBP公司
C9orf72
SOD1
肌萎缩侧索硬化
疾病
少年
生物
发病年龄
突变
遗传学
基因检测
基因
医学
病理
三核苷酸重复扩增
等位基因
作者
Zhang‐Yu Zou,Mingsheng Liu,Xiaoguang Li,Liying Cui
标识
DOI:10.3109/21678421.2016.1143012
摘要
Juvenile onset ALS is a very rare form of motor neuron disease, with the first symptoms of motor neuron degeneration manifested before 25 years of age. Mutations in the alsin (ALS2), senataxin (SETX), and spatacsin (SPG11) genes have been associated with familial ALS with juvenile onset and slow progression, whereas the genetic architecture of sporadic juvenile ALS remains unclear. We screened mutations in C9orf72, SOD1, FUS, TARDBP, ANG, VCP and PFN1 in 16 juvenile sporadic ALS patients. Four cases (25%) carrying FUS mutations and one individual (6%) harbouring a SOD1 mutation were identified. All cases had an aggressive disease course. Our results suggest that FUS mutations are the most frequent genetic cause in early-onset sporadic ALS patients of Chinese origin. Genetic testing of FUS should be performed in early-onset ALS patients especially those with an aggressive disease course.
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