Haug K, Sander T, Hallmann K, Rau B, Dullinger J S, Elger C E, Propping P, Heils A
University Department of Human Genetics, Bonn, Germany.
Neuroreport. 2000 Aug 21;11(12):2687-9. doi: 10.1097/00001756-200008210-00016.
Recent identification of ion channel gene mutations in Mendelian epilepsies suggests that genetically driven neuronal hyperexcitability plays an important role in epileptogenesis. In this study, we tested the hypothesis that genetic variation in the human SCN2B gene confers liability to common subtypes of idiopathic generalized epilepsies (IGE). A systematic search for mutations was performed in 92 IGE patients. We detected a novel single nucleotide polymorphism (SNP), however, allele frequencies did not differ between IGE patients and controls (chi2 = 0.19, df = 1, p = 0.744). Furthermore, a missense mutation in codon 209 (Asn209Pro) was identified in one patient, but was found to be absent in an affected sibling of the index patient. Thus, our results do not suggest a major role of the SCN2B gene in the etiology of common IGE subtypes.
最近在孟德尔癫痫中发现离子通道基因突变,这表明基因驱动的神经元过度兴奋在癫痫发生中起重要作用。在本研究中,我们检验了以下假设:人类SCN2B基因的遗传变异会导致特发性全身性癫痫(IGE)常见亚型的易感性。对92例IGE患者进行了系统的突变搜索。我们检测到一个新的单核苷酸多态性(SNP),然而,IGE患者和对照组之间的等位基因频率没有差异(χ2 = 0.19,自由度 = 1,p = 0.744)。此外,在一名患者中鉴定出密码子209处的错义突变(Asn209Pro),但在索引患者的一名患病同胞中未发现该突变。因此,我们的结果并不表明SCN2B基因在常见IGE亚型的病因中起主要作用。