良性家族性婴儿癫痫伴婴儿惊厥和阵发性舞蹈手足徐动症家系的表型和 PRRT2 突变。
Phenotypes and PRRT2 mutations in Chinese families with benign familial infantile epilepsy and infantile convulsions with paroxysmal choreoathetosis.
机构信息
Department of Pediatrics, Peking University First Hospital, No, 1 of Xian Men Street, , Beijing, Xicheng District 100034, China.
出版信息
BMC Neurol. 2013 Dec 26;13:209. doi: 10.1186/1471-2377-13-209.
BACKGROUND
Mutations in the PRRT2 gene have been identified as the major cause of benign familial infantile epilepsy (BFIE), paroxysmal kinesigenic dyskinesia (PKD) and infantile convulsions with paroxysmal choreoathetosis/dyskinesias (ICCA). Here, we analyzed the phenotypes and PRRT2 mutations in Chinese families with BFIE and ICCA.
METHODS
Clinical data were collected from 22 families with BFIE and eight families with ICCA. PRRT2 mutations were screened using PCR and direct sequencing.
RESULTS
Ninety-five family members were clinically affected in the 22 BFIE families. During follow-up, two probands had one seizure induced by diarrhea at the age of two years. Thirty-one family members were affected in the eight ICCA families, including 11 individuals with benign infantile epilepsy, nine with PKD, and 11 with benign infantile epilepsy followed by PKD. Two individuals in one ICCA family had PKD or ICCA co-existing with migraine. One affected member in another ICCA family had experienced a fever-induced seizure at 7 years old. PRRT2 mutations were detected in 13 of the 22 BFIE families. The mutation c.649_650insC (p.R217PfsX8) was found in nine families. The mutations c.649delC (p.R217EfsX12) and c.904_905insG (p.D302GfsX39) were identified in three families and one family, respectively. PRRT2 mutations were identified in all eight ICCA families, including c.649_650insC (p.R217PfsX8), c.649delC (p.R217EfsX12), c.514_517delTCTG (p.S172RfsX3) and c.1023A > T (X341C). c.1023A > T is a novel mutation predicted to elongate the C-terminus of the protein by 28 residues.
CONCLUSIONS
Our data demonstrated that PRRT2 is the major causative gene of BFIE and ICCA in Chinese families. Site c.649 is a mutation hotspot: c.649_650insC is the most common mutation, and c.649delC is the second most common mutation in Chinese families with BFIE and ICCA. As far as we know, c.1023A > T is the first reported mutation in exon 4 of PRRT2. c.649delC was previously reported in PKD, ICCA and hemiplegic migraine families, but we further detected it in BFIE-only families. c.904_905insG was reported in an ICCA family, but we identified it in a BFIE family. c.514_517delTCTG was previously reported in a PKD family, but we identified it in an ICCA family. Migraine and febrile seizures plus could co-exist in ICCA families.
背景
PRRT2 基因突变已被确定为良性家族性婴儿癫痫(BFIE)、阵发性运动诱发性运动障碍(PKD)和婴儿期癫痫伴阵发性舞蹈手足徐动症/运动障碍(ICCA)的主要病因。在此,我们分析了中国 BFIE 和 ICCA 家系的表型和 PRRT2 突变。
方法
收集了 22 个 BFIE 家系和 8 个 ICCA 家系的临床资料。采用 PCR 和直接测序法筛选 PRRT2 突变。
结果
在 22 个 BFIE 家系中,95 个家系成员出现临床症状。在随访中,2 个先证者在 2 岁时因腹泻诱发 1 次发作。8 个 ICCA 家系中有 31 个家系成员受累,包括 11 个良性婴儿癫痫患者、9 个 PKD 患者和 11 个良性婴儿癫痫后继发 PKD 患者。1 个 ICCA 家系中有 2 个患者同时患有 PKD 或 ICCA 和偏头痛。另 1 个 ICCA 家系中有 1 个受累成员在 7 岁时曾因发热诱发癫痫。在 22 个 BFIE 家系中发现了 13 个 PRRT2 突变。在 9 个家系中发现了 c.649_650insC(p.R217PfsX8)突变。在 3 个家系和 1 个家系中分别发现了 c.649delC(p.R217EfsX12)和 c.904_905insG(p.D302GfsX39)突变。在 8 个 ICCA 家系中均发现了 PRRT2 突变,包括 c.649_650insC(p.R217PfsX8)、c.649delC(p.R217EfsX12)、c.514_517delTCTG(p.S172RfsX3)和 c.1023A > T(X341C)。c.1023A > T 是一种新的突变,预计会使蛋白的 C 末端延长 28 个氨基酸残基。
结论
我们的数据表明 PRRT2 是中国 BFIE 和 ICCA 家系的主要致病基因。c.649 是一个突变热点:c.649_650insC 是最常见的突变,c.649delC 是中国 BFIE 和 ICCA 家系中第二常见的突变。据我们所知,c.1023A > T 是 PRRT2 外显子 4 中首次报道的突变。c.649delC 先前在 PKD、ICCA 和偏瘫性偏头痛家系中报道过,但我们在仅 BFIE 家系中也检测到了它。c.904_905insG 先前在 ICCA 家系中报道过,但我们在 BFIE 家系中也发现了它。c.514_517delTCTG 先前在 PKD 家系中报道过,但我们在 ICCA 家系中发现了它。偏头痛和热性惊厥伴发可在 ICCA 家系中共同存在。
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