Department of Pediatrics, Osaka University Graduate School of Medicine, Osaka, Japan.
J Hum Genet. 2011 Dec;56(12):846-51. doi: 10.1038/jhg.2011.115. Epub 2011 Oct 20.
Glucose transporter 1 deficiency syndrome (Glut1-DS) is a congenital metabolic disorder characterized by refractory seizures with early infantile onset, developmental delay, movement disorders and acquired microcephaly. Glut1-DS is caused by heterozygous abnormalities of the SLC2A1 (Glut1) gene, whose product acts to transport glucose into the brain across the blood-brain barrier. We analyzed the SLC2A1 gene in 12 Japanese Glut1-DS patients who were diagnosed by characteristic clinical symptoms and hypoglycorrhachia as follows: all patients had infantile-onset seizures and mild to severe developmental delay, and ataxia was detected in 11 patients. For the 12 patients, we identified seven different mutations (three missense, one nonsense, two frameshift and one splice-site) in exons and exon-intron boundaries of the SLC2A1 gene by direct sequencing, of which six were novel mutations. Of the remaining five patients who had no point mutations and underwent investigation by multiplex ligation-dependent probe amplification, a complex abnormality with deletion and duplication was identified in one patient: this is the first case of such recombination of the SLC2A1 gene. Changes in regulatory sequences in the promoter region or genes other than SLC2A1 might be responsible for onset of Glut1-DS in the other four patients (33%) without SLC2A1 mutation.
葡萄糖转运蛋白 1 缺乏症(Glut1-DS)是一种先天性代谢紊乱,其特征为婴儿早期起病的难治性癫痫、发育迟缓、运动障碍和获得性小头症。Glut1-DS 是由 SLC2A1(Glut1)基因的杂合异常引起的,其产物作用是将葡萄糖穿过血脑屏障转运到大脑中。我们分析了 12 名日本 Glut1-DS 患者的 SLC2A1 基因,这些患者通过特征性临床表现和低血糖症确诊,具体如下:所有患者均有婴儿期起病的癫痫发作和轻至重度发育迟缓,11 名患者检测到共济失调。在这 12 名患者中,我们通过直接测序在 SLC2A1 基因的外显子和外显子-内含子边界上鉴定了七个不同的突变(三个错义突变,一个无义突变,两个移码突变和一个剪接位点突变),其中六个是新的突变。在另外五个没有点突变且接受多重连接依赖性探针扩增调查的患者中,一个患者中发现了缺失和重复的复杂异常:这是 SLC2A1 基因重组的首例病例。在另外四个没有 SLC2A1 突变的患者(33%)中,启动子区域或除 SLC2A1 之外的其他基因中的调节序列的变化可能导致 Glut1-DS 的发作。
