Clinical and molecular characteristics of myotonia congenita in China: Case series and a literature review.

Yifan Li, Mao Li, Zhenfu Wang, Fei Yang, Hongfen Wang, Xiujuan Bai, Bo Sun, Siyu Chen, Xusheng Huang
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引用次数: 2

Abstract

Myotonia congenita (MC) is a rare genetic disease caused by mutations in the skeletal muscle chloride channel gene (CLCN1), encoding the voltage-gated chloride channel ClC-1 in skeletal muscle. Our study reported the clinical and molecular characteristics of six patients with MC and systematically review the literature on Chinese people. We retrospectively analyzed demographics, clinical features, family history, creatine kinase (CK), electromyography (EMG), treatment, and genotype data of our patients and reviewed the clinical data and CLCN1 mutations in literature. The median ages at examination and onset were 26.5 years (range 11-50 years) and 6.5 years (range 1.5-11 years), respectively, in our patients, and 21 years (range 3.5-65 years, n = 45) and 9 years (range 0.5-26 years, n = 50), respectively, in literature. Similar to previous reports, myotonia involved limb, lids, masticatory, and trunk muscles to varying degrees. Warm-up phenomenon (5/6), percussion myotonia (3/5), and grip myotonia (6/6) were common. Menstruation triggered myotonia in females, not observed in Chinese patients before. The proportion of abnormal CK levels (4/5) was higher than data from literature. Electromyography performed in six patients revealed myotonic changes (100%). Five novel CLCN1 mutations, including a splicing mutation (c.853 + 4A>G), a deletion mutation (c.2010_2014del), and three missense mutations (c.2527C>T, c.1727C>T, c.2017 G > C), were identified. The c.892 G > A (p.A298T) mutation was the most frequent mutation in the Chinese population. Our study expanded the clinical and genetic spectrum of patients with MC in the China. The MC phenotype in Chinese people is not different from that found in the West, while the genotype is different.

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中国先天性肌强直的临床和分子特征:病例系列和文献回顾。
先天性肌强直(MC)是一种由骨骼肌氯离子通道基因(CLCN1)突变引起的罕见遗传病,该基因编码骨骼肌电压门控氯离子通道ClC-1。本研究报告了6例MC患者的临床和分子特征,并系统地回顾了有关中国人的文献。我们回顾性分析了患者的人口统计学、临床特征、家族史、肌酸激酶(CK)、肌电图(EMG)、治疗和基因型数据,并回顾了临床数据和文献中的CLCN1突变。在我们的患者中,检查和发病时的中位年龄分别为26.5岁(范围11-50岁)和6.5岁(范围1.5-11岁),文献中分别为21岁(范围3.5-65岁,n = 45)和9岁(范围0.5-26岁,n = 50)。与以往报道相似,肌强直不同程度地累及肢体、眼睑、咀嚼肌和躯干肌。常见的有热身现象(5/6)、打击肌强直(3/5)、握力肌强直(6/6)。月经引发女性肌强直,在中国患者中未见。CK水平异常比例(4/5)高于文献数据。6例患者肌电图显示肌强直性改变(100%)。5个新的CLCN1突变,包括一个剪接突变(c.853 + 4A>G)、一个缺失突变(c.2010_2014del)和三个错义突变(c.2527C>T, c.1727C>T, c.2017)G > C)。的c.892G > A (p.A298T)突变是中国人群中最常见的突变。我们的研究扩大了中国MC患者的临床和遗传谱。中国人的MC表型与西方人没有差异,但基因型不同。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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