非同义代换
外显子组测序
遗传学
桑格测序
DNA测序
肌萎缩侧索硬化
生物
基因
外显子组
离子半导体测序
多重聚合酶链反应
聚合酶链反应
突变
医学
基因组
疾病
病理
作者
Ryoichi Nakamura,Jun Sone,Naoki Atsuta,Genki Tohnai,Hazuki Watanabe,Daichi Yokoi,Masahiro Nakatochi,Hirohisa Watanabe,Mizuki Ito,Jo Senda,Masahisa Katsuno,Fumiaki Tanaka,Yuanzhe Li,Yuishin Izumi,Mitsuya Morita,Akira Taniguchi,Osamu Kano,Masaya Oda,Satoshi Kuwabara,Koji Abe
标识
DOI:10.1016/j.neurobiolaging.2015.11.030
摘要
We investigated the frequency and contribution of variants of the 28 known amyotrophic lateral sclerosis (ALS)-related genes in Japanese ALS patients. We designed a multiplex, polymerase chain reaction-based primer panel to amplify the coding regions of the 28 ALS-related genes and sequenced DNA samples from 257 Japanese ALS patients using an Ion Torrent PGM sequencer. We also performed exome sequencing and identified variants of the 28 genes in an additional 251 ALS patients using an Illumina HiSeq 2000 platform. We identified the known ALS pathogenic variants and predicted the functional properties of novel nonsynonymous variants in silico. These variants were confirmed by Sanger sequencing. Known pathogenic variants were identified in 19 (48.7%) of the 39 familial ALS patients and 14 (3.0%) of the 469 sporadic ALS patients. Thirty-two sporadic ALS patients (6.8%) harbored 1 or 2 novel nonsynonymous variants of ALS-related genes that might be deleterious. This study reports the first extensive genetic screening of Japanese ALS patients. These findings are useful for developing genetic screening and counseling strategies for such patients.
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