NPRL2 相关性癫痫的临床表型和基因型:4 例病例报告及文献复习。
Clinical phenotype and genotype of NPRL2-related epilepsy: Four cases reports and literature review.
机构信息
Department of Neurology, Beijing Children's Hospital, National Center for Children's Health, Capital Medical University, 56 Nanlishi Road, Xicheng District, Beijing 100045, China; Epilepsy Center, Children's Hospital Affiliated to Shandong University, Jinan, China; Epilepsy Center, Jinan Children's Hospital, Jinan, China.
Department of Neurology, Beijing Children's Hospital, National Center for Children's Health, Capital Medical University, 56 Nanlishi Road, Xicheng District, Beijing 100045, China.
出版信息
Seizure. 2024 Mar;116:100-106. doi: 10.1016/j.seizure.2023.09.003. Epub 2023 Sep 6.
BACKGROUND
NPRL2-related epilepsy, caused by pathogenic germline variants of the NPRL2 gene, is a newly discovered childhood epilepsy linked to enhanced mTORC1 signalling. However, the phenotype and genotype of NPRL2 variants are still poorly understood. Here, we summarize the association between the phenotype and genotype of NPRL2-related epilepsy.
METHODS
A retrospective analysis was conducted for four Chinese children with epilepsy due to likely pathogenic NPRL2 variants identified through whole-exome sequencing (WES). Previous reports of patients with NPRL2-related epilepsy were reviewed systematically.
RESULTS
One of our patients presented focal epilepsy involving the central region, which should be distinguished from self-limited epilepsy with centrotemporal spikes (SeLECTS). The four novel likely pathogenic NPRL2 variants consisted of two nonsense variants, one frameshift variant, and one copy number variant (CNV). Bioinformatics analysis revealed the two nonsense variants to be highly conserved and cause alterations in protein structure. Including our four cases, a total of 33 patients with NPRL2-related epilepsy have been identified to date. The most common presentation is focal epilepsy (70%), including sleep-related hypermotor epilepsy (SHE), temporal lobe epilepsy (TLE), and frontal lobe epilepsy (FLE). Infantile epileptic spasms syndrome (IESS) is also a notable feature of NPRL2-related epilepsy. Malformations of cortical development (MCD, 8/20), especially focal cortical dysplasia (FCD, 6/20), are common neuroimaging abnormalities. Two-thirds of the NPRL2 variants reported are loss of function (LoF) (14/21). Among these mutations, c.100C>T (p.Arg34*) and c.314T>C (p.Leu105Pro) have been detected in two families (likely due to a founder effect).
CONCLUSION
NPRL2-related epilepsy shows high phenotypic and genotypic heterogeneity. Our study expands the genotype spectrum of NPRL2-related epilepsy, and the phenotype of focal epilepsy involving the central region should be clearly distinguished with SeLECTS, with reference value for clinical diagnosis.
背景
由 NPRL2 基因的致病性种系变异引起的 NPRL2 相关癫痫是一种新发现的与增强的 mTORC1 信号相关的儿童癫痫。然而,NPRL2 变异的表型和基因型仍知之甚少。在此,我们总结了 NPRL2 相关癫痫的表型与基因型之间的关联。
方法
对通过全外显子组测序(WES)鉴定出的 4 例可能致病性 NPRL2 变异相关癫痫的中国儿童进行回顾性分析。系统回顾了 NPRL2 相关癫痫患者的既往报告。
结果
我们的 1 名患者表现为中央区局灶性癫痫,这应与具有中央颞区棘波的自限性癫痫(SELECTS)相区别。这 4 个新的可能致病性 NPRL2 变异包括 2 个无义变异、1 个移码变异和 1 个拷贝数变异(CNV)。生物信息学分析显示这 2 个无义变异高度保守,导致蛋白结构改变。包括我们的 4 例病例在内,迄今为止共发现 33 例 NPRL2 相关癫痫患者。最常见的表现是局灶性癫痫(70%),包括睡眠相关的过度运动性癫痫(SHE)、颞叶癫痫(TLE)和额叶癫痫(FLE)。婴儿癫痫性痉挛综合征(IESS)也是 NPRL2 相关癫痫的显著特征。皮质发育畸形(MCD,8/20),特别是局灶性皮质发育不良(FCD,6/20)是常见的神经影像学异常。报道的 NPRL2 变异中有三分之二为功能丧失(LoF)(14/21)。在这些突变中,c.100C>T(p.Arg34*)和 c.314T>C(p.Leu105Pro)已在两个家系中检出(可能由于一个奠基者效应)。
结论
NPRL2 相关癫痫表现出高度的表型和基因型异质性。我们的研究扩展了 NPRL2 相关癫痫的基因型谱,中央区局灶性癫痫的表型应与 SELECTS 明确区分,具有临床诊断参考价值。
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