Oberoi Kinsi, Grewal Alam S, Peddareddygari Leema Reddy
Life Sciences Division, Clarivate Analytics, Philadelphia, Pennsylvania, USA.
Dynamic Biologics Inc., Monmouth Junction, New Jersey, USA.
Case Rep Neurol. 2020 Jul 29;12(2):255-259. doi: 10.1159/000509266. eCollection 2020 May-Aug.
Mutations in the () gene can cause a variety of clinical and electrophysiological forms of genetic neuropathies including Charcot-Marie-Tooth (CMT) type 1B disease which is characterized by demyelinating features. We present a father and daughter with neuropathy carrying a novel 31 base pair duplication mutation in the 5' untranslated region of the gene, c.-23_8dup31. Genetic analysis and protein modeling indicated that this is a frameshift mutation resulting in premature truncation of the encoded protein. The daughter underwent repeat neurological examination and electromyography testing over an 11-year time span demonstrating no clinical or electrophysiological change. Our study expands the clinical and genetic spectrum of mutations that can cause CMT type 1B disease and demonstrates the value of sequence analysis of noncoding portions of a gene that are not intronic.
()基因的突变可导致多种临床和电生理形式的遗传性神经病变,包括以脱髓鞘特征为特点的1B型腓骨肌萎缩症(CMT)。我们报告了一对患有神经病变的父女,他们在该基因的5'非翻译区携带一个新的31个碱基对的重复突变,即c.-23_8dup31。遗传分析和蛋白质建模表明,这是一个移码突变,导致编码蛋白过早截断。在11年的时间跨度内,女儿接受了多次神经系统检查和肌电图测试,结果显示没有临床或电生理变化。我们的研究扩展了可导致1B型CMT疾病的突变的临床和遗传谱,并证明了对基因非内含子非编码部分进行序列分析的价值。
