Ngoh Adeline, Clark Maria, Greenaway Rebecca, Chen Xiumin, Reid Kimberley M, Barwick Katy, Meyer Esther, Moulding Dale, Trump Natalie, Cross J Helen, Fraser Sean D, de Hayr Lachlan, Kullmann Dimitri M, Lynch Joseph W, Harvey Robert J, Kurian Manju A
Developmental Neurosciences, UCL Great Ormond Street Institute of Child Health, Zayed Centre for Research into Rare Disease in Children, London, UK.
Paediatric Neurology, KK Women's and Children's Hospital, Singapore, Singapore.
Ann Neurol. 2025 Nov;98(5):951-966. doi: 10.1002/ana.27306. Epub 2025 Sep 13.
Landau-Kleffner syndrome (LKS), is a rare, poorly-understood epileptic encephalopathy with spike-wave activation in sleep associated with mutations in GRIN2A, encoding the N-Methyl-D-Aspartate receptor (NMDAR) GluN2A subunit. Physicians rely on empirical treatments, with scarce information on treatment efficacy and outcomes. This study aims to improve the understanding and clinical management of LKS.
Fifty-two patients with LKS were recruited via one quaternary referral center. Case-notes review delineated clinical features, long-term outcomes, and prognostic factors. Generalized estimating equations were used to determine the longitudinal association among electroencephalogram abnormalities, steroid therapy, and neuropsychological findings. After genetic screening, the impact of identified GRIN2A missense variants on NMDAR function was assessed using homology modeling, cell-surface trafficking assays, and electrophysiology in artificial synapses. Whole exome/genome sequencing was performed on GRIN2A-negative patients to identify novel gene associations.
LKS is complex with significant clinical and genetic heterogeneity. Besides speech and language impairment, many patients had other co-morbidities and almost half have long-term disability. Early age at disease onset was associated with worse outcomes. There was no reliable correlation between electroencephalogram findings and developmental scores. Steroid therapy improved language outcomes independently of electroencephalogram findings. GRIN2A mutations were identified in 15.5% of the cohort. Likely pathogenic variants in GABBR2, SCN1A, TRPC1, ERRFI1, CTXN3, IRX6, and IQCA1 were identified in 7 GRIN2A-negative individuals.
For LKS, early intervention is important for long-term outcomes. Furthermore, management should not be based solely on electroencephalogram findings. Genetic and functional investigations offer insights into disease pathophysiology and facilitate development of future targeted therapies. ANN NEUROL 2025;98:951-966.
Landau-Kleffner综合征(LKS)是一种罕见的、了解甚少的癫痫性脑病,睡眠中棘波激活,与编码N-甲基-D-天冬氨酸受体(NMDAR)GluN2A亚基的GRIN2A基因突变有关。医生依靠经验性治疗,关于治疗效果和结果的信息匮乏。本研究旨在提高对LKS的认识和临床管理水平。
通过一家四级转诊中心招募了52例LKS患者。病历回顾明确了临床特征、长期预后和预后因素。使用广义估计方程来确定脑电图异常、类固醇治疗和神经心理学结果之间的纵向关联。在进行基因筛查后,使用同源建模、细胞表面转运分析和人工突触电生理学评估已鉴定的GRIN2A错义变体对NMDAR功能的影响。对GRIN2A阴性患者进行全外显子组/基因组测序,以确定新的基因关联。
LKS情况复杂,具有显著的临床和遗传异质性。除言语和语言障碍外,许多患者还有其他合并症,近一半患者有长期残疾。疾病发病年龄早与预后较差相关。脑电图结果与发育评分之间没有可靠的相关性。类固醇治疗独立于脑电图结果改善了语言预后。在该队列的15.5%中鉴定出GRIN2A突变。在7名GRIN2A阴性个体中鉴定出GABBR2、SCN1A、TRPC1、ERRFI1、CTXN3、IRX6和IQCA1中可能的致病变体。
对于LKS,早期干预对长期预后很重要。此外,管理不应仅基于脑电图结果。基因和功能研究有助于深入了解疾病病理生理学,并促进未来靶向治疗的开发。《神经病学年鉴》2025年;98:951 - 966。
