Song Dandan, Peng Xiaoyi, Wang Yao, Cai Aojie, Tamang Sapana, Wang Huaili, Zhuo Zhihong
Department of Pediatrics, the First Affiliated Hospital of Zhengzhou University, Zhengzhou, Henan 450020, China.
Zhonghua Yi Xue Yi Chuan Xue Za Zhi. 2025 Mar 10;42(3):292-299. doi: 10.3760/cma.j.cn511374-20240919-00498.
To investigate the clinical phenotypic and genetic characteristics of three children with Paroxysmal kinesigenic dyskinesia (PKD) and Self-limited familial infantile epilepsy (SeLIE) caused by PRRT2 gene mutation.
Three children with PKD and SeLIE caused by PRRT2 gene mutation (children 1-3) who were treated in the First Affiliated Hospital of Zhengzhou University from November 2022 to August 2023 were selected as the research subjects. A retrospective study was conducted to collect the clinical and family history data of the three children. 2 mL of peripheral venous blood from children 1-3 and parents of children 1-2 were collected (parents of children refused to undergo genetic testing and no blood samples were collected), genomic DNA was extracted, whole exome sequencing (WES) was performed, and Sanger sequencing method was used for verification. According to the Classification Standards and Guidelines for Genetic Variants formulated by the American Society of Medical Genetics and Genomics (ACMG) (hereinafter referred to as the "ACMG Guidelines"), the pathogenicity of the variant loci detected in three children was rated, and the detrimental loci of the variant loci were analyzed by multiple bioinformatics software. This study has been approved by the Ethics Committee of the First Affiliated Hospital of Zhengzhou University (Ethics No. 2024-KY-0881-002).
The clinical data and genetic test results of the three children in this study are as follows. Child 1: female, age of onset of 4 months and 10 days, with seizures, manifested as sudden cessation of movements, staring in both eyes, cyanosis of the lips, paleness, and stiffness and shaking of limbs. The results of genetic testing showed that child 1 had maternal PRRT2 gene c.583_584dup (p.P196Afs34) frameshift variant, which was rated as a pathogenic variant (PVS1 PM2_Supporting PP4) according to ACMG guidelines. According to the clinical manifestations and genetic test results of child 1, he was diagnosed with SeLIE and took oral sodium valproate [0.5 mL/(kg.d)], and was still taking medication at the follow-up of 2 years old, and did not have seizures again after 5 months of age. Child 2: male, age of onset of 10 years old, manifested as dystonia after sudden movement. The results of genetic testing showed that child 2 had PRRT2 gene mutations: paternal c.649dupC (p.R217Pfs8) frameshift variant and maternal c.445C>A (p.Q149K) mutation. Among them, c.649dupC was a reported pathogenic variant, and according to ACMG guidelines, c.445C>A variant was rated as a variant of unknown clinical significance (PM2_Supporting), with a high probability of benignness. According to the clinical manifestations and genetic test results of the child 2, he was diagnosed with PKD, and was followed up with oral oxcarbazepine 9 mg/(kg.d) until 12 years and 2 months, and was still on the drug, and there was no recurrence of the seizure of the form of dyskinesia after taking the drug. Child 3: male, age of onset of 11 years old, manifested by dystonia after sudden exercise. The results of genetic testing showed that child 3 had a missense variant of PRRT2 gene c.904G>C (p.D302H), and his parents refused genetic testing, and the source of the mutation was unknown, and the variant was rated as a variant of unknown clinical significance (PM2_Supporting+PP3_Moderate+PP4) according to ACMG guidelines. According to the clinical manifestations and genetic test results of child 3, he was diagnosed with PKD, and was treated with oral oxcarbazepine 10 mg/(kg.d) for 1 year and then discontinued on his own, and was followed up at the age of 17, and there was no recurrence of the seizure of the form of movement disorder after taking the drug.
One case of SeLIE and two cases of PKD caused by PRRT2 gene mutations responded well to anti-seizure drugs. In this study, four variant loci of PRRT2 gene were found: c.583_584dup, c.904G>C, c.649dupC, c.445C>A, among which c.583_584dup were new variants, enriching the variant spectrum of PRRT2 gene.
探讨3例由PRRT2基因突变引起的发作性运动诱发性运动障碍(PKD)和自限性家族性婴儿癫痫(SeLIE)患儿的临床表型及遗传特征。
选取2022年11月至2023年8月在郑州大学第一附属医院就诊的3例由PRRT2基因突变引起的PKD和SeLIE患儿(患儿1 - 3)作为研究对象。进行回顾性研究,收集3例患儿的临床及家族史资料。采集患儿1 - 3及患儿1 - 2父母的外周静脉血2 mL(患儿3父母拒绝行基因检测,未采集血样),提取基因组DNA,进行全外显子组测序(WES),并采用Sanger测序法进行验证。根据美国医学遗传学与基因组学学会(ACMG)制定的《遗传变异分类标准与指南》(以下简称“ACMG指南”)对3例患儿检测到的变异位点的致病性进行评级,并通过多个生物信息学软件分析变异位点的有害性。本研究已获得郑州大学第一附属医院伦理委员会批准(伦理号:2024 - KY - 0881 - 002)。
本研究中3例患儿的临床资料及基因检测结果如下。患儿1:女,发病年龄4个月10天,发作时表现为运动突然停止、双眼凝视、口唇发绀、面色苍白、四肢强直抖动。基因检测结果显示患儿1存在母亲PRRT2基因c.583_584dup(p.P196Afs34)移码变异,根据ACMG指南评为致病性变异(PVS1 PM2_Supporting PP4)。根据患儿1的临床表现及基因检测结果,诊断为SeLIE,口服丙戊酸钠[0.5 mL/(kg·d)],2岁随访时仍在服药,5月龄后未再发作。患儿2:男,发病年龄10岁,表现为运动后突发肌张力障碍。基因检测结果显示患儿2存在PRRT2基因突变:父亲c.649dupC(p.R217Pfs8)移码变异和母亲c.445C>A(p.Q149K)突变。其中c.649dupC为已报道的致病性变异,根据ACMG指南,c.445C>A变异评为临床意义未明变异(PM2_Supporting),良性可能性大。根据患儿2的临床表现及基因检测结果,诊断为PKD,口服奥卡西平9 mg/(kg·d)随访至12岁2个月,仍在服药,服药后运动障碍形式发作未再复发。患儿3:男,发病年龄11岁,表现为运动后突发肌张力障碍。基因检测结果显示患儿3存在PRRT2基因c.904G>C(p.D302H)错义变异,其父母拒绝基因检测,突变来源不明,根据ACMG指南该变异评为临床意义未明变异(PM2_Supporting+PP3_Moderate+PP4)。根据患儿3的临床表现及基因检测结果,诊断为PKD,口服奥卡西平10 mg/(kg·d)治疗1年后自行停药,17岁随访,服药后运动障碍形式发作未再复发。
PRRT2基因突变所致1例SeLIE和2例PKD患儿对抗癫痫药物反应良好。本研究发现PRRT2基因4个变异位点:c.583_584dup、c.904G>C、c.649dupC、c.445C>A,其中c.583_584dup为新变异,丰富了PRRT2基因的变异谱。
