[A pedigree of myotonia congenita with a novel mutation p.F343C of the CLCN1 gene].

Q4 Medicine Clinical Neurology Pub Date : 2024-05-24 Epub Date: 2024-04-20 DOI:10.5692/clinicalneurol.cn-001929
Yoshitsugu Nakamura, Hidenori Sato, Kensuke Kakiuchi, Yuki Miyano, Takafumi Hosokawa, Shigeki Arawaka
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Abstract

A Japanese woman experienced slowness of movement in her early teens and difficulty in opening her hands during pregnancy. On admission to our hospital at 42 years of age, she showed grip myotonia with warm-up phenomenon. However, she had neither muscle weakness, muscle atrophy, cold-induced symptomatic worsening nor episodes of transient weakness of the extremities. Needle electromyography of the first dorsal interosseous and anterior tibial muscles demonstrated myotonic discharges. Whole exome sequencing of the patient revealed a heterozygous single-base substitution in the CLCN1 gene (c.1028T>G, p.F343C). The same substitution was identified in affected members of her family (mother and brother) by Sanger sequencing, but not in healthy family members (father and a different brother). We diagnosed myotonia congenita (Thomsen disease) with a novel CLCN1 mutation in this pedigree. This mutation causes a single amino acid substitution in the I-J extracellular loop region of CLCN1. Amino acid changes in the I-J loop region are rare in an autosomal-dominantly inherited form of myotonia congenita. We think that this pedigree is precious to understand the pathogenesis of myotonia congenita.

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[CLCN1基因p.F343C新型突变的先天性肌张力障碍血统]。
一名日本妇女在十几岁时就出现行动迟缓,在怀孕期间双手难以张开。她在 42 岁入院时出现了握肌强直,并伴有热身现象。然而,她既没有肌无力、肌肉萎缩,也没有寒冷引起的症状加重或短暂的四肢无力发作。第一背侧骨间肌和胫骨前肌的针式肌电图显示有肌张力放电。该患者的全外显子组测序结果显示,CLCN1 基因存在杂合性单碱基置换(c.1028T>G,p.F343C)。通过桑格(Sanger)测序,我们在其家族中受影响的成员(母亲和兄弟)身上也发现了相同的置换,但在健康的家族成员(父亲和另一个兄弟)身上却没有发现。我们诊断该血统中的先天性肌张力障碍(汤姆森病)与新型 CLCN1 基因突变有关。该突变导致 CLCN1 的 I-J 细胞外环区发生单个氨基酸置换。在常染色体显性遗传的先天性肌张力障碍中,I-J环区的氨基酸变化非常罕见。我们认为,这一血统对于了解先天性肌张力障碍的发病机制非常重要。
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来源期刊
Clinical Neurology
Clinical Neurology Medicine-Neurology (clinical)
CiteScore
0.30
自引率
0.00%
发文量
147
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