Department of Medical Genetics, Karadeniz Technical University Faculty of Medicine, Ortahisar, 61100, Trabzon, Türkiye.
Department of Pediatric Neurology, Kartal Dr. Lütfi Kirdar City Hospital, Istanbul, Türkiye.
Neurogenetics. 2024 Apr;25(2):119-130. doi: 10.1007/s10048-024-00751-1. Epub 2024 Feb 22.
The terms developmental epileptic encephalopathy with spike-and-wave activation in sleep (DEE-SWAS) and epileptic encephalopathy with spike-and-wave activation in sleep (EE-SWAS) designate a spectrum of conditions that are typified by different combinations of motor, cognitive, language, and behavioral regression linked to robust spike-and-wave activity during sleep. In this study, we aimed at describing the clinical and molecular findings in "(developmental) epileptic encephalopathy with spike-and-wave activation in sleep" (D)EE-SWAS) patients as well as at contributing to the genetic etiologic spectrum of (D)EE-SWAS. Single nucleotide polymorphism (SNP) array and whole-exome sequencing (WES) techniques were used to determine the underlying genetic etiologies. Of the 24 patients included in the study, 8 (33%) were female and 16 (67%) were male. The median age at onset of the first seizure was 4 years and the median age at diagnosis of (D)EE-SWAS was 5 years. Of the 24 cases included in the study, 13 were compatible with the clinical diagnosis of DEE-SWAS and 11 were compatible with the clinical diagnosis of EE-SWAS. Abnormal perinatal history was present in four cases (17%), and two cases (8%) had a family history of epilepsy. Approximately two-thirds (63%) of all patients had abnormalities detected on brain computerized tomography/magnetic resonance (CT/MR) imaging. After SNP array and WES analysis, the genetic etiology was revealed in 7 out of 24 (29%) cases. Three of the variants detected were novel (SLC12A5, DLG4, SLC9A6). This study revealed for the first time that Smith-Magenis syndrome, SCN8A-related DEE type 13 and SLC12A5 gene variation are involved in the genetic etiology of (D)EE-SWAS. (D)EE-SWAS is a genetically diverse disorder with underlying copy number variations and single-gene abnormalities. In the current investigation, rare novel variations in genes known to be related to (D)EE-SWAS and not previously reported genes to be related to (D)EE-SWAS were discovered, adding to the molecular genetic spectrum. Molecular etiology enables the patient and family to receive thorough and accurate genetic counseling as well as a personalized medicine approach.
术语“睡眠中出现棘波和尖波的发育性癫痫性脑病(DEE-SWAS)”和“睡眠中出现棘波和尖波的癫痫性脑病(EE-SWAS)”用于描述一组不同的疾病,这些疾病的特征是不同的运动、认知、语言和行为退化组合,与睡眠中的强棘波和尖波活动有关。在这项研究中,我们旨在描述“睡眠中出现棘波和尖波的(发育性)癫痫性脑病(D)EE-SWAS)”患者的临床和分子发现,并为(D)EE-SWAS 的遗传病因谱做出贡献。我们使用单核苷酸多态性(SNP)阵列和全外显子组测序(WES)技术来确定潜在的遗传病因。在纳入研究的 24 名患者中,有 8 名(33%)为女性,16 名(67%)为男性。首次发作的中位年龄为 4 岁,(D)EE-SWAS 的中位诊断年龄为 5 岁。在纳入研究的 24 例中,有 13 例符合 DEE-SWAS 的临床诊断,11 例符合 EE-SWAS 的临床诊断。有 4 例(17%)存在异常围产期病史,有 2 例(8%)有癫痫家族史。大约三分之二(63%)的患者在脑计算机断层扫描/磁共振成像(CT/MR)上有异常。在 SNP 阵列和 WES 分析后,在 24 例中的 7 例(29%)发现了遗传病因。检测到的 3 种变异均为新变异(SLC12A5、DLG4、SLC9A6)。本研究首次发现,Smith-Magenis 综合征、SCN8A 相关 DEE 型 13 和 SLC12A5 基因突变与(D)EE-SWAS 的遗传病因有关。(D)EE-SWAS 是一种遗传异质性疾病,其潜在的拷贝数变异和单基因异常。在目前的研究中,发现了以前未报道的与(D)EE-SWAS 相关的基因中的罕见新变异,以及已知与(D)EE-SWAS 相关的基因中的新变异,增加了分子遗传谱。分子病因学使患者及其家属能够接受全面、准确的遗传咨询和个性化的药物治疗。
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