中国人群先天性肌张力障碍的临床和遗传特征

Channels (Austin, Tex.) Pub Date : 2024-12-01 Epub Date: 2024-05-08 DOI:10.1080/19336950.2024.2349823
Yuting He, Yusen Qiu, Ying Xiong, Yu Shen, Kaiyan Jiang, Hancun Yi, Pengcheng Huang, Yu Zhu, Min Zhu, Meihong Zhou, Daojun Hong, Dandan Tan
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引用次数: 0

摘要

先天性肌营养不良症(MC)是一种罕见的遗传性肌肉疾病,由 CLCN1 基因变异引起。目前,显性型Thomsen(TMC)和隐性型Becker(BMC)之间的表型-基因型相关性仍不确定。我们回顾性地收集了本诊所 MC 患者的临床资料和辅助检查。对11名患者和可用的家庭成员进行了肌电图检查。对所有患者进行了全外显子组测序。回顾性分析了2004年6月至2022年12月期间报告的中国MC患者的临床和实验室数据。研究共纳入11名MC患者,平均发病年龄为(12.64±2.73)岁。主要症状为四肢肌肉僵硬。所有患者均有热身现象和叩击性肌张力障碍。肌电图显示,所有患者和两名无症状携带者都有明显的肌强直症状,而肌肉磁共振成像和活检则显示正常或无特异性变化。在CLCN1中发现了14个基因变异,包括6个新型变异。本研究对98名中国患者进行了重新分析和总结。52名TMC患者和46名BMC患者在人口统计学数据、临床特征和实验室检查结果方面无明显差异。在CLCN1的145个变异中,包括最常见的c.892 G>A变异在内的一些变异在某些家族中可能导致TMC,而在另一些家族中则可能导致BMC。这项研究扩大了中国 MC 患者的临床和遗传谱。仅凭临床、实验室和遗传学特征很难区分TMC和BMC。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical and genetic characteristics of myotonia congenita in Chinese population.

Myotonia congenita (MC) is a rare hereditary muscle disease caused by variants in the CLCN1 gene. Currently, the correlation of phenotype-genotype is still uncertain between dominant-type Thomsen (TMC) and recessive-type Becker (BMC). The clinical data and auxiliary examinations of MC patients in our clinic were retrospectively collected. Electromyography was performed in 11 patients and available family members. Whole exome sequencing was conducted in all patients. The clinical and laboratory data of Chinese MC patients reported from June 2004 to December 2022 were reviewed. A total of 11 MC patients were included in the study, with a mean onset age of 12.64 ± 2.73 years. The main symptom was muscle stiffness of limbs. Warm-up phenomenon and percussion myotonia were found in all patients. Electromyogram revealed significant myotonic charges in all patients and two asymptomatic carriers, while muscle MRI and biopsy showed normal or nonspecific changes. Fourteen genetic variants including 6 novel variants were found in CLCN1. Ninety-eight Chinese patients were re-analyzed and re-summarized in this study. There were no significant differences in the demographic data, clinical characteristics, and laboratory findings between 52 TMC and 46 BMC patients. Among the 145 variants in CLCN1, some variants, including the most common variant c.892 G>A, could cause TMC in some families and BMC in others. This study expanded the clinical and genetic spectrum of Chinese patients with MC. It was difficult to distinguish between TMC and BMC only based on the clinical, laboratory, and genetic characteristics.

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