Chinese Journal of Contemporary Neurology and Neurosurgery ›› 2019, Vol. 19 ›› Issue (5): 349-353. doi: 10.3969/j.issn.1672-6731.2019.05.009

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Treatment of Becker myotonia congenita with lamotrigine: one case report and review of literatures

ZHONG Jie, LIN Jin-fu, ZHANG Cheng, ZHONG Xin-jing, CHEN Xue-ling, LI Jing, ZHU Yu-ling   

  1. Department of Neurology, the First Affiliated Hospital, Sun Yat-sen University, Guangzhou 510080, Guangdong, China
  • Online:2019-05-25 Published:2019-05-24
  • Contact: ZHANG Cheng (Email: zhangch6@mail.sysu.edu.cn)
  • Supported by:

    This study was supported by the National Natural Science Foundation of China (No. 81471280, 81771359), the National Natural Science Foundation for Young Scientists of China (No. 81601087), and 2015 Production, Study and Research Special Project of Guangzhou, Guangdong Province, China (No. 1561000153).

拉莫三嗪治疗 Becker型先天性肌强直一例并文献复习

钟洁, 林金福, 张成, 钟欣静, 陈雪玲, 利婧, 朱瑜龄   

  1. 510080 广州,中山大学附属第一医院神经科[钟洁(现在广西中医药大学第一附属医院脑病科,邮政编码:530023)、钟欣静(现在广西医科大学第六附属医院老年病科,邮政编码:537000)、陈雪玲(现在海南省琼海市人民医院神经内科,邮政编码:571400)]
  • 通讯作者: 张成,Email:zhangch6@mail.sysu.edu.cn
  • 基金资助:

    国家自然科学基金资助项目(项目编号:81471280);国家自然科学基金资助项目(项目编号:81771359);国家自然科学基金青年科学基金资助项目(项目编号:81601087);广东省广州市 2015 年产学研专项项目(项目编号:1561000153)

Abstract:

Objective To report the efficacy and safety of lamotrigine in the treatment of one case of Becker myotonia congenita. Methods and Results A 17-year-old male had muscle stiffness in the limbs as the first symptom, which could be alleviated after repeated exercise. The creatine kinase (CK) level was normal. Genetic testing showed there were two missense mutations c.1205C > T (p.Ala402Val) and c.896T > C (p.Val299Ala) located in exon 11 and 8 of CLCN1 gene respectively in the proband. The missense mutation c.1205C > T (p.Ala402Val) in exon 11 was found out in his mother and c.896T > C (p.Val299Ala) located in exon 8 was found out in his father. The latter, exon 8 c.896T > C of CLCN1 gene has not been reported. The proband was clearly diagnosed as Becker myotonia congenita, and his family was diagnosed as Becker myotonia congenita pedigree. After 5 years' treatment with lamotrigine, the symptom of myotonia was significantly improved and no adverse reactions was observed. Conclusions The missense mutation in exon 8 c.896T > C in this patient further expanded the CLCN1 gene mutation spectrum. Lamotrigine is effective in treating Becker myotonia congenita, providing a new idea for the treatment of myotonia congenita.

Key words: Myotonia congenita, Triazines, Genes, Mutation, missense, Pedigree

摘要:

目的 报道拉莫三嗪治疗 1 例 Becker 型先天性肌强直患者的疗效及安全性。方法与结果 17 岁男性患者,以四肢肌肉僵硬为首发症状,反复运动后症状减轻,血清肌酸激酶水平正常,基因检测提示存在 CLCN1 基因外显子 11 c.1205C > T(p.Ala402Val)及 CLCN1 基因外显子 8 c.896T > C(p.Val299Ala)错义突变,确诊为 Becker 型先天性肌强直;其母为 CLCN1 基因外显子 11 c.1205C > T(p.Ala402Val)、其父为 CLCN1 基因外显子 8 c.896T > C(p.Val299Ala)错义突变,确诊为 Becker 型先天性肌强直家系,其中 CLCN1 基因外显子 8 c.896T > C 突变尚无报道。经拉莫三嗪连续治疗 5 年后肌强直症状长期缓解,且无任何药物不良反应。结论 该例 CLCN1基因外显子8 c.896T > C 错义突变进一步扩展了CLCN1基因突变谱。拉莫三嗪治疗效果良好,为 Becker型先天性肌强直的治疗提供了新的思路。

关键词: 先天性肌强直, 三嗪类, 基因, 突变, 误义, 系谱