Claes L, Del-Favero J, Ceulemans B, Lagae L, Van Broeckhoven C, De Jonghe P
Department of Molecular Genetics, University of Antwerp, B-2610 Antwerpen, Belgium.
Am J Hum Genet. 2001 Jun;68(6):1327-32. doi: 10.1086/320609. Epub 2001 May 15.
Severe myoclonic epilepsy of infancy (SMEI) is a rare disorder that occurs in isolated patients. The disease is characterized by generalized tonic, clonic, and tonic-clonic seizures that are initially induced by fever and begin during the first year of life. Later, patients also manifest other seizure types, including absence, myoclonic, and simple and complex partial seizures. Psychomotor development stagnates around the second year of life. Missense mutations in the gene that codes for a neuronal voltage-gated sodium-channel alpha-subunit (SCN1A) were identified in families with generalized epilepsy with febrile seizures plus (GEFS+). GEFS+ is a mild type of epilepsy associated with febrile and afebrile seizures. Because both GEFS+ and SMEI involve fever-associated seizures, we screened seven unrelated patients with SMEI for mutations in SCN1A. We identified a mutation in each patient: four had frameshift mutations, one had a nonsense mutation, one had a splice-donor mutation, and one had a missense mutation. All mutations are de novo mutations and were not observed in 184 control chromosomes.
婴儿严重肌阵挛癫痫(SMEI)是一种罕见的疾病,仅发生于个别患者。该疾病的特征为全身性强直、阵挛和强直阵挛发作,最初由发热诱发,始于生命的第一年。之后,患者还会出现其他发作类型,包括失神发作、肌阵挛发作以及简单和复杂部分性发作。精神运动发育在生命的第二年左右停滞。在伴有热性惊厥附加症(GEFS+)的全身性癫痫家族中,发现了编码神经元电压门控钠通道α亚基(SCN1A)的基因突变。GEFS+是一种与热性和无热惊厥相关的轻度癫痫类型。由于GEFS+和SMEI都涉及与发热相关的惊厥,我们对7名无关的SMEI患者进行了SCN1A基因突变筛查。我们在每位患者中都发现了一个突变:4人有移码突变,1人有 nonsense 突变,1人有剪接供体突变,1人有错义突变。所有突变均为新发突变,在184条对照染色体中未观察到。
