Shin Minyoung, Simkin Dina, Suyeoka Genn M, Chetkovich Dane M
Davee Department of Neurology and Clinical Neurosciences, Northwestern University Medical School, 303 East Chicago Avenue, Ward Building 10-201, Chicago, IL 60611-3008, USA.
Brain Res. 2006 Apr 14;1083(1):14-20. doi: 10.1016/j.brainres.2006.01.102. Epub 2006 Mar 20.
Epilepsy is an often-debilitating disease with many etiologies. Genetic predisposition is common for many of the generalized epilepsy syndromes, and mutations in genes encoding neuronal ion channels are causative in many cases. We previously identified a locus for juvenile audiogenic monogenic seizures (jams1) in the Black Swiss mouse strain, delimited by the gene basigin (Bsg) and the marker D10Mit140. This region includes Hcn2, the gene encoding the hyperpolarization-activated cyclic nucleotide-gated channel subunit 2 (HCN2), an ion channel implicated in epilepsy. By sequencing genomic DNA, we found that Black Swiss mice have a single polymorphism in exon 2 within the Hcn2 gene. This single G/C to A/T base change alters the third position of a codon specifying alanine residue 293, without changing the predicted amino acid sequence. Furthermore, we found no detectable differences in HCN2 protein expression in the brains of Black Swiss mice, compared to control mice. We therefore reason that juvenile audiogenic seizures in Black Swiss mice are unlikely to be due to abnormalities of HCN2 channel function.
癫痫是一种病因多样、常使人衰弱的疾病。遗传易感性在许多全身性癫痫综合征中很常见,编码神经元离子通道的基因突变在许多情况下是致病原因。我们之前在黑瑞士小鼠品系中确定了一个青少年听源性单基因癫痫(jams1)的基因座,其范围由基底膜蛋白(Bsg)基因和标记D10Mit140界定。该区域包括Hcn2,即编码超极化激活的环核苷酸门控通道亚基2(HCN2)的基因,这是一种与癫痫有关的离子通道。通过对基因组DNA进行测序,我们发现黑瑞士小鼠在Hcn2基因的第2外显子中有一个单核苷酸多态性。这个单一的G/C到A/T碱基变化改变了指定丙氨酸残基293的密码子的第三位,而没有改变预测的氨基酸序列。此外,与对照小鼠相比,我们在黑瑞士小鼠的大脑中未发现可检测到的HCN2蛋白表达差异。因此,我们推断黑瑞士小鼠的青少年听源性癫痫不太可能是由于HCN2通道功能异常所致。
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