SCN8A Mutation in Infantile Epileptic Encephalopathy: Report of Two Cases.

Journal of epilepsy research Pub Date : 2019-12-31 eCollection Date: 2019-12-01 DOI:10.14581/jer.19017
Kanij Fatema, Md Mizanur Rahman, Omar Faruk
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引用次数: 1

Abstract

Early infantile epileptic encephalopathy type 13 is a severe form of epilepsy caused by mutations in the sodium channel 8 alpha (SCN8A) gene. This gene encodes the neuronal voltage-gated sodium channel which plays vital role in neuronal excitability. Here we present two cases with SCN8A encephalopathy. Both cases had mutation in p.Arg1872Gin the SCN8A gene, which was detected by targeted next generation sequencing. Case 1 was a 14-month old boy, who had a normal birth history with normal development up to 6 months and then developed repeated generalized seizure, which was nonresponsive to multiple antiepileptic drugs. He also had neuroregression and dystonia. His electroencephalogram (EEG) showed progressive background abnormality with burst suppression pattern. His metabolic panel was normal and had partial response to carbamazepine. The second case was for an 11-month old boy with the onset of seizure at the age of 7 months. Seizure was generalized, resistant to multiple antiepileptic drugs. He had developmental delay from beginning, no movement disorder. EEG showed focal discharge from left temporal and occipital region. He showed partial response to oxcarbazepine. Our cases had similarities with the previously reported cases. The detailed discussion of our cases would contribute to early detection and targeted treatment of SCN8A encephalopathy. This also gives special emphasis on a genetic test in infants with intractable epilepsy, movement disorder and developmental delay.

小儿癫痫性脑病SCN8A突变:附2例报告
早期婴儿癫痫性脑病13型是一种由钠通道8 α (SCN8A)基因突变引起的严重癫痫。该基因编码在神经元兴奋性中起重要作用的电压门控钠通道。我们在此报告两例SCN8A脑病。这两个病例都有p.a arg1872gin (SCN8A基因)突变,通过靶向下一代测序检测到。病例1为14个月大的男婴,出生史正常,6个月前发育正常,后反复出现全身性癫痫发作,对多种抗癫痫药物无反应。他还有神经退化和肌张力障碍。他的脑电图显示进行性背景异常,伴有脉冲抑制模式。代谢指标正常,对卡马西平有部分反应。第二个病例是一名11个月大的男孩,在7个月大时癫痫发作。癫痫发作全身性,对多种抗癫痫药物耐药。他从一开始就发育迟缓,没有运动障碍。脑电图显示左侧颞枕区局灶性放电。他对奥卡西平有部分反应。我们的病例与以前报道的病例有相似之处。对我们病例的详细讨论将有助于SCN8A脑病的早期发现和靶向治疗。这也特别强调对患有顽固性癫痫、运动障碍和发育迟缓的婴儿进行基因检测。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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