Ozmen Meral, Dilber Cengiz, Tatlı Burak, Aydınlı Nur, Calışkan Mine, Ekici Barış
Department of Pediatric Neurology, Istanbul Medical Faculty, Istanbul.
Ann Indian Acad Neurol. 2011 Jul;14(3):178-81. doi: 10.4103/0972-2327.85879.
Mutations of the α-1 subunit sodium channel gene (SCN1A) cause severe myoclonic epilepsy of infancy (SMEI). To date, over 300 mutations related to SMEI have been described. In the present study, we report new SCN1A mutations and the clinical features of SMEI cases.
We studied the clinical and genetic features of nine patients diagnosed with SMEI at the Pediatric Neurology Department of Istanbul Medical Faculty.
Five patients had nonsense mutations, two had missense mutations, one had a splice site mutation and one had a deletion mutation of the SCN1A gene. Mutations at c.3705+5G splice site, p.trip153X nonsense mutation and deletion at c.2416_2946 have not been previously described. The seizures started following whole cell pertussis vaccination in all patients. The seizures ceased in one patient and continued in the other eight patients. Developmental regression was severe in three patients, with frequent status epilepticus. The type of mutation was not predictive for the severity of the disease. Two of the three patients with severe regression had nonsense and missense mutations.
Dravet syndrome can be result of several different types of mutation in SCN1A gene. Onset of the seizures after pertussis vaccination is an important clue for the diagnosis and neuro- developmental delay should be expected in all patients.
α-1亚基钠通道基因(SCN1A)突变可导致婴儿严重肌阵挛性癫痫(SMEI)。迄今为止,已描述了300多种与SMEI相关的突变。在本研究中,我们报告了新的SCN1A突变以及SMEI病例的临床特征。
我们研究了伊斯坦布尔医学院儿科神经科确诊为SMEI的9例患者的临床和遗传特征。
5例患者存在无义突变,2例存在错义突变,1例存在剪接位点突变,1例存在SCN1A基因缺失突变。c.3705+5G剪接位点突变、p.trip153X无义突变和c.2416_2946缺失此前尚未见报道。所有患者的癫痫发作均在全细胞百日咳疫苗接种后开始。1例患者癫痫发作停止,其他8例患者仍继续发作。3例患者出现严重发育倒退,频繁发生癫痫持续状态。突变类型不能预测疾病的严重程度。3例严重发育倒退的患者中有2例存在无义突变和错义突变。
Dravet综合征可能是由SCN1A基因的几种不同类型突变引起的。百日咳疫苗接种后癫痫发作是诊断的重要线索,所有患者均应预期有神经发育迟缓。
