Feng Huiru, Zhou Hongyu
Department of Neurology, West China Hospital, Sichuan University, Chengdu, China.
Medicine (Baltimore). 2017 Dec;96(51):e8981. doi: 10.1097/MD.0000000000008981.
Congenital myasthenic syndromes (CMS) are a group of genetic disorders that stem mostly from molecular defects in nicotinic acetylcholine receptors (AChRs). Defects in the cholinergic receptor nicotinic delta subunit (CHRND) gene can cause a series of myasthenic syndromes. Here, we report 2 new compound heterozygous variants of the CHRND gene in a Chinese male with CMS.
A 43-year-old Chinese male presented with progressive muscle weakness, difficulty chewing, and an inability to lift his head from the time he was 8 years old. He was treated with pyridostigmine, which was partially effective. Two weeks prior, he was hospitalized for dyspnea. Upon examination, he was unable to drum his cheeks and exhibited fatigable muscle weakness and facial muscle atrophy. Sequencing of his exome revealed 2 previously unreported mutations in CHRND, c.59G>A (exon2) and c.423G>C (exon5).
We identified a new mutational site that contributes to the onset of CMS.
先天性肌无力综合征(CMS)是一组遗传性疾病,主要源于烟碱型乙酰胆碱受体(AChR)的分子缺陷。胆碱能受体烟碱型δ亚基(CHRND)基因缺陷可导致一系列肌无力综合征。在此,我们报告一名患有CMS的中国男性中CHRND基因的2种新的复合杂合变异。
一名43岁的中国男性自8岁起出现进行性肌肉无力、咀嚼困难及无法抬头。他接受了吡啶斯的明治疗,部分有效。两周前,他因呼吸困难住院。检查时,他无法鼓起脸颊,表现出易疲劳的肌肉无力和面部肌肉萎缩。对其外显子组进行测序发现CHRND基因中有2个先前未报道的突变,即c.59G>A(外显子2)和c.423G>C(外显子5)。
我们鉴定出一个导致CMS发病的新突变位点。