Uctepe Eyyup, Esen Fatma Nisa, Tümer Sait, Mancılar Hanifenur, Yeşilyurt Ahmet
Acıbadem Ankara Tissue Typing Laboratory, Ankara, Turkey.
Acibadem Labgen Genetic Diagnosis Center, İstanbul, Turkey.
Intractable Rare Dis Res. 2022 Nov;11(4):219-221. doi: 10.5582/irdr.2022.01096.
Potassium voltage-gated channel subfamily B member 1 () encodes Kv2.1 potassium channel. KCNB1 mutations are known to cause global developmental delay, behavioral disorders, and various epilepsies. Most variants occur de novo and are rarely inherited. Here, we report a 14-year-old male patient who was admitted to our clinic with seizures, developmental delay history, and intellectual disability. Brain magnetic resonance image (MRI) was normal and electroencephalogram (EEG) showed spike and sharp-wave complexes emerging in the left hemisphere parietooccipital areas, which were paroxysmally generalized. We performed whole exome sequence analysis (WES) and identified a heterozygous frameshift mutation c.522delA in exon 1 of (NM_004975.4) predicting a premature stop codon p.Lys174Asnfs*20 in the proband. Sanger sequencing confirmed the heterozygous c.522delA mutation in the proband and his mother who also had epilepsy and learning difficulties. His 45 year old mother had used antiepileptic drugs for 9 years after a seizure episode at 12 years old. Also, his mother's uncle's son is nonverbal and has developmental delay and epilepsy. Our study shows that frameshift mutation cytoplasmic domain of gene can cause intrafamilial phenotypic variability and relatively mild clinical findings in these patients.
钾离子电压门控通道亚家族B成员1()编码Kv2.1钾通道。已知KCNB1突变会导致全面发育迟缓、行为障碍和各种癫痫。大多数变异是新发的,很少遗传。在此,我们报告一名14岁男性患者,因癫痫发作、发育迟缓病史和智力残疾入住我院。脑部磁共振成像(MRI)正常,脑电图(EEG)显示左半球顶枕区出现棘波和尖慢复合波,并阵发性泛化。我们进行了全外显子组测序分析(WES),在(NM_004975.4)的外显子1中鉴定出一个杂合移码突变c.522delA,预测先证者中出现一个提前终止密码子p.Lys174Asnfs*20。桑格测序证实先证者及其同样患有癫痫和学习困难的母亲存在杂合c.522delA突变。他45岁的母亲在12岁癫痫发作后已服用抗癫痫药物9年。此外,他母亲的叔叔的儿子无语言能力,有发育迟缓和癫痫。我们的研究表明,基因的移码突变细胞质结构域可导致这些患者家族内表型变异和相对较轻的临床症状。
