Musa Nurul Huda, Thilakavathy Karuppiah, Mohamad Nur Afiqah, Kennerson Marina L, Inche Mat Liyana Najwa, Loh Wei Chao, Abdul Rashid Anna Misyail, Baharin Janudin, Ibrahim Azliza, Wan Sulaiman Wan Aliaa, Hoo Fan Kee, Basri Hamidon, Yusof Khan Abdul Hanif Khan
Department of Biomedical Science, Faculty of Medicine and Health Sciences, Universiti Putra Malaysia, Serdang, Malaysia.
Centre of Foundation Studies, Universiti Teknologi MARA, Cawangan Selangor, Kampus Dengkil, Dengkil, Selangor, Malaysia.
Front Genet. 2023 Jan 3;13:972007. doi: 10.3389/fgene.2022.972007. eCollection 2022.
Myotonia congenita (MC) is a rare neuromuscular disease caused by mutations within the gene encoding skeletal muscle chloride channels. MC is characterized by delayed muscle relaxation during contraction, resulting in muscle stiffness. There is a lack of MC case reports and data on the prevalence among Malaysians. We report a clinical case of a 50-year-old woman presents with muscle stiffness and cramp episodes that started in early childhood. She had difficulty initiating muscle movement and presented with transient muscle weakness after rest, which usually improved after repeated contraction (warm-up phenomenon). She was diagnosed with MC after myotonic discharge on electromyography (EMG). Her brother had similar symptoms; however, no additional family members showed MC symptoms. Serum creatine kinase levels were elevated in both the proband and her brother with 447 U/L and 228 U/L recorded, respectively. Genetic analysis by whole-exome sequencing (WES) revealed a previously reported pathogenic gene variant c.1667T>A (p.I556N). Genetic screening of all family members revealed that the same variant was observed in the children of both the proband and her brother; however, the children did not present with either clinical or electrophysiological MC symptoms. The multiplex ligation-dependent probe amplification (MLPA) analysis conducted identified neither exon deletion nor duplication in . In conclusion, this report describes the first case of MC in Malaysia in which incomplete penetrance observed in this family is caused by a known pathogenic variant.
先天性肌强直(MC)是一种罕见的神经肌肉疾病,由编码骨骼肌氯离子通道的基因突变引起。MC的特征是收缩时肌肉松弛延迟,导致肌肉僵硬。马来西亚缺乏MC病例报告及患病率数据。我们报告一例临床病例,一名50岁女性自幼起出现肌肉僵硬和痉挛发作。她开始肌肉运动困难,休息后出现短暂性肌无力,反复收缩后通常会改善(热身现象)。经肌电图(EMG)检查发现肌强直放电后,她被诊断为MC。她的哥哥有类似症状;然而,没有其他家庭成员表现出MC症状。先证者及其哥哥的血清肌酸激酶水平均升高,分别记录为447 U/L和228 U/L。通过全外显子组测序(WES)进行的基因分析揭示了一个先前报道的致病基因变异c.1667T>A(p.I556N)。对所有家庭成员的基因筛查显示,先证者和她哥哥的孩子中都观察到了相同的变异;然而,这些孩子既没有出现临床症状,也没有出现电生理MC症状。进行的多重连接依赖探针扩增(MLPA)分析未发现该基因的外显子缺失或重复。总之,本报告描述了马来西亚首例MC病例,该家族中观察到的不完全外显率是由一个已知的致病基因变异引起的。
