Department of Psychiatry, Nagasaki University Hospital, Sakamoto 1-7-1, Nagasaki, Japan.
J Hum Genet. 2012 May;57(5):338-41. doi: 10.1038/jhg.2012.23. Epub 2012 Mar 8.
Paroxysmal kinesigenic dyskinesia (PKD (MIM128000)) is a neurological disorder characterized by recurrent attacks of involuntary movements. Benign familial infantile convulsion (BFIC) is also one of a neurological disorder characterized by clusters of epileptic seizures. The BFIC1 (MIM601764), BFIC2 (MIM605751) and BFIC4 (MIM612627) loci have been mapped to chromosome 19q, 16p and 1p, respectively, while BFIC3 (MIM607745) is caused by mutations in SCN2A on chromosome 2q24. Furthermore, patients with BFIC have been observed in a family concurrently with PKD. Both PKD and BFIC2 are heritable paroxysmal disorders and map to the same region on chromosome 16. Recently, the causative gene of PKD, the protein-rich transmembrane protein 2 (PRRT2), has been detected using whole-exome sequencing. We performed mutation analysis of PRRT2 by direct sequencing in 81 members of 17 families containing 15 PKD families and two BFIC families. Direct sequencing revealed that two mutations, c.649dupC and c.748C>T, were detected in all members of the PKD and BFIC families. Our results suggest that BFIC2 is caused by a truncated mutation that also causes PKD. Thus, PKD and BFIC2 are genetically identical and may cause convulsions and involuntary movements via a similar mechanism.
发作性运动诱发性运动障碍 (PKD (MIM128000)) 是一种以反复出现的不自主运动为特征的神经系统疾病。良性家族性婴儿惊厥 (BFIC) 也是一种以癫痫发作群集为特征的神经系统疾病。BFIC1 (MIM601764)、BFIC2 (MIM605751) 和 BFIC4 (MIM612627) 位点分别定位在 19q、16p 和 1p 染色体上,而 BFIC3 (MIM607745) 是由 2q24 染色体上 SCN2A 的突变引起的。此外,还观察到一个家族中同时存在 BFIC 和 PKD 的患者。PKD 和 BFIC2 都是遗传性阵发性疾病,定位于 16 号染色体的同一区域。最近,使用全外显子组测序检测到 PKD 的致病基因,富含蛋白的跨膜蛋白 2 (PRRT2)。我们通过对包含 15 个 PKD 家族和 2 个 BFIC 家族的 17 个家族的 81 名成员进行 PRRT2 突变分析。直接测序显示,PKD 和 BFIC 家族的所有成员均检测到 c.649dupC 和 c.748C>T 两种突变。我们的结果表明,BFIC2 是由一种截断突变引起的,该突变也导致 PKD。因此,PKD 和 BFIC2 在遗传上是相同的,可能通过类似的机制引起惊厥和不自主运动。
