中国 PCDH19 簇状癫痫患儿的表型和基因型特征。
Phenotypic and genotypic characteristics of children with PCDH19 clustering epilepsy in China.
机构信息
Neurology Department, National Center for Children's Health China, Beijing Children Hospital affiliated to Capital Medical University, Beijing, 100045, China.
Department of Medical Genetics and Developmental Biology, School of Basic Medical Sciences, Capital Medical University, Beijing, 10069, China.
出版信息
Seizure. 2024 Oct;121:95-104. doi: 10.1016/j.seizure.2024.07.023. Epub 2024 Jul 31.
PURPOSE
PCDH19 gene variants, termed PCDH19 clustering epilepsy, represent a distinct etiology of epilepsy. This study aimed to elucidate the clinical manifestations and explore the genotypes and phenotypes of children affected by PCDH19 clustering epilepsy.
METHODS
This retrospective study included medical history, magnetic resonance imaging, video-electroencephalography, and genetic analysis of patients diagnosed with PCDH19 Clustering Epilepsy at the Neurology Department of Beijing Children's Hospital from 2015 to 2023. Chi-square tests and logistic regression analyses were conducted to study the factors associated with developmental delay in patients.
RESULTS
The age at seizure onset ranged from 5 to 61 months among all 30 patients (median 14 months; IQR 9.25-22.5 months). Among the 30 patients, 29 were female and 1 was male. Clusters of seizures and fever-triggered seizures were observed, with the most prevalent seizure types being focal to bilateral tonic-clonic seizures (FBTCS). Seizures were successfully controlled in 15 patients. Unfortunately, one patient experienced a sudden unexpected death in epilepsy (SUDEP). Additionally, 14 patients had hereditary mutations, 14 had de novo mutations, 1 had both hereditary and de novo mutations, and 1 male patient had a mosaic component mutation of 0.64 due to a somatic mutation. Developmental delays were identified in 17 patients (56.7 %), and 6 patients (20 %) were diagnosed with autism spectrum disorder (ASD). Among the 17 patients, 9 experienced developmental delays before the onset of epilepsy, while 8 were initially normal but later developed developmental delays during disease progression. Statistical analysis revealed that the presence of drug-resistant epilepsy was an independent risk factor for the occurrence of developmental delays (P = 0.020, OR = 9.758, 95 % CI (1.440-66.111)).
CONCLUSION
In this study, 13 new potential rare pathogenic variations in PCDH19 clustering epilepsy were identified. The clinical features observed in patients are consistent with known phenotypic features, and we found that patients with drug-resistant epilepsy are more likely to have developmental delays. The severity of the phenotype in patients with PCDH19 variants ranged from drug-responsive seizures to refractory epilepsy.
目的
PCDH19 基因突变,称为 PCDH19 簇状癫痫,代表一种独特的癫痫病因。本研究旨在阐明患儿的临床表现,并探讨 PCDH19 簇状癫痫患儿的基因型和表型。
方法
本回顾性研究纳入了 2015 年至 2023 年在北京儿童医院神经内科诊断为 PCDH19 簇状癫痫的患者的病史、磁共振成像、视频脑电图和基因分析。采用卡方检验和 logistic 回归分析研究与患者发育迟缓相关的因素。
结果
30 例患者的癫痫发作年龄为 5 至 61 个月(中位数 14 个月;IQR 9.25-22.5 个月)。30 例患者中,29 例为女性,1 例为男性。观察到癫痫发作簇和发热诱发的癫痫发作,最常见的癫痫发作类型为局灶性双侧强直阵挛发作(FBTCS)。15 例患者癫痫发作得到控制。不幸的是,1 例患者发生癫痫猝死(SUDEP)。此外,14 例患者有遗传性突变,14 例有新生突变,1 例既有遗传性又有新生突变,1 例男性患者因体细胞突变存在 0.64 的嵌合体突变。17 例患者(56.7%)存在发育迟缓,6 例(20%)被诊断为自闭症谱系障碍(ASD)。在 17 例发育迟缓患者中,9 例在癫痫发作前存在发育迟缓,8 例最初正常,但在疾病进展过程中出现发育迟缓。统计分析显示,耐药性癫痫的存在是发育迟缓发生的独立危险因素(P = 0.020,OR = 9.758,95%CI(1.440-66.111))。
结论
本研究发现了 13 种新的潜在罕见致病性 PCDH19 簇状癫痫变异。患者的临床特征与已知表型特征一致,我们发现耐药性癫痫患者更有可能出现发育迟缓。PCDH19 变异患者的表型严重程度从药物反应性癫痫发作到难治性癫痫发作不等。
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