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首页> 外文期刊>Brain & Development >Paroxysmal movement disorders in severe myoclonic epilepsy in infancy.
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Paroxysmal movement disorders in severe myoclonic epilepsy in infancy.

机译:婴儿时期严重的肌阵挛性癫痫发作性运动障碍。

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We report on the electroclinical findings and the results of a molecular genetic study of a patient with typical severe myoclonic epilepsy in infancy (TSME) and three with borderline SME (BSME) who showed paroxysmal movement disorders, such as choreoathetosis, dystonia and ballismus, during their clinical course. BSME was defined as a clinical entity that shares common characteristics with TSME but lacks myoclonic seizures associated with ictal EEG changes. When the paroxysmal movement disorders were first observed, all the patients in this study were being treated with polytherapy including phenytoin (PHT), and these abnormal movements disappeared when PHT was discontinued or reduced. However, on other occasions, two of our cases also showed the same abnormal movements even when not being treated with PHT. One patient with TSME and two of the three patients with BSME had SCN1A gene mutations that lead to truncation of the associated protein. We conclude that paroxysmal movement disorders seen in SME patients were closely related to their AED therapy, especially the use of PHT. It is thought that patients with both TSME and BSME have some predisposition toward paroxysmal movement disorders, and that this predisposition is partly related to sodium channel dysfunction, although some other factors might influence the occurrence of this phenomenon.
机译:我们报告了婴儿期典型重症肌阵挛性癫痫(TSME)和三例边缘性SME(BSME)表现为阵发性运动障碍(如胆囊性运动,肌张力障碍和弹道性疾病)的患者的电临床研究结果和分子遗传学研究结果。他们的临床过程。 BSME被定义为与TSME具有共同特征但缺乏与发作性EEG变化相关的肌阵挛性发作的临床实体。首次观察到阵发性运动障碍时,本研究中的所有患者均接受包括苯妥英钠(PHT)在内的多种疗法治疗,并且当PHT停用或降低时,这些异常运动消失了。但是,在其他情况下,即使不进行PHT治疗,我们的两个病例也显示出相同的异常运动。 TSME的一名患者和BSME的三名患者中的两名患有SCN1A基因突变,导致相关蛋白的截短。我们得出的结论是,在SME患者中发现的阵发性运动障碍与他们的AED治疗(尤其是PHT的使用)密切相关。认为TSME和BSME的患者都有阵发性运动障碍的易感性,尽管某些其他因素可能影响这种现象的发生,但这种易感性与钠通道功能障碍有关。

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