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法裔加拿大人非萎缩性肌强直的临床、电生理及遗传学研究

Clinical, electrophysiologic, and genetic study of non-dystrophic myotonia in French-Canadians.

作者信息

Dupré Nicolas, Chrestian Nicolas, Bouchard Jean-Pierre, Rossignol Elsa, Brunet Denis, Sternberg Damien, Brais Bernard, Mathieu Jean, Puymirat Jack

机构信息

Department of Neurological Sciences, CHAUQ (Enfant-Jésus), Faculty of Medicine, Laval University, Quebec City, QC, Canada.

出版信息

Neuromuscul Disord. 2009 May;19(5):330-4. doi: 10.1016/j.nmd.2008.01.007. Epub 2008 Mar 11.

Abstract

Thirty-three French-Canadian families with non-dystrophic myotonia were identified. Fifty subjects were recruited and submitted to a complete clinical, electrophysiologic and genetic evaluation. Thirteen mutations were identified in CLCN1 and five mutations were identified in SCN4A. Onset in the lower extremities, presence of tongue myotonia and transient weakness suggested recessive CLCN1 mutations. Lid myotonia, absence of hypertrophy and exacerbation with cold temperature suggested SCN4A mutations. Pain was not a feature of dominant CLCN1 mutations while it could be seen in the others, more frequently in SCN4A mutations. Warm up phenomenon, hand grip myotonia, percussion myotonia, lid lag and hormonal effects were not distinguishing features. Repetitive nerve stimulation and short exercise test showed either a large (>50%) or mild-moderate (10-50%) decrement with recessive CLCN1 mutations while they showed only mild or no decrement with dominant CLCN1 and SCN4A mutations. The French-Canadian population shows wide phenotypic and genotypic heterogeneity in non-dystrophic myotonias.

摘要

我们识别出了33个患有非营养不良性肌强直的法裔加拿大家庭。招募了50名受试者,并对他们进行了全面的临床、电生理和基因评估。在CLCN1基因中识别出13个突变,在SCN4A基因中识别出5个突变。下肢发病、存在舌肌强直和短暂性肌无力提示为隐性CLCN1突变。眼睑肌强直、无肥大且遇冷加重提示为SCN4A突变。疼痛不是显性CLCN1突变的特征,但在其他突变中可见,在SCN4A突变中更常见。热身现象、握力性肌强直、叩击性肌强直、眼睑滞后和激素效应不是鉴别特征。重复神经刺激和短时间运动试验显示,隐性CLCN1突变可导致大幅度(>50%)或轻度至中度(10-50%)递减,而显性CLCN1和SCN4A突变仅导致轻度递减或无递减。法裔加拿大人在非营养不良性肌强直方面表现出广泛的表型和基因型异质性。

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