Epilepsy and Neurogenetics Program, Ruber Internacional Hospital, La Masó 34, 28034, Madrid, Spain.
Initiative for Neuroscience (INCE) Foundation, Madrid, Spain.
Neurotherapeutics. 2023 Sep;20(5):1294-1304. doi: 10.1007/s13311-023-01395-z. Epub 2023 Jun 6.
MOGHE is defined as mild malformation of cortical development with oligodendroglial hyperplasia in epilepsy. Approximately half of the patients with histopathologically confirmed MOGHE carry a brain somatic variant in the SLC35A2 gene encoding a UDP-galactose transporter. Previous research showed that D-galactose supplementation results in clinical improvement in patients with a congenital disorder of glycosylation due to germline variants in SLC35A2. We aimed to evaluate the effects of D-galactose supplementation in patients with histopathologically confirmed MOGHE, with uncontrolled seizures or cognitive impairment and epileptiform activity at the EEG after epilepsy surgery (NCT04833322). Patients were orally supplemented with D-galactose for 6 months in doses up to 1.5 g/kg/day and monitored for seizure frequency including 24-h video-EEG recording, cognition and behavioral scores, i.e., WISC, BRIEF-2, SNAP-IV, and SCQ, and quality of life measures, before and 6 months after treatment. Global response was defined by > 50% improvement of seizure frequency and/or cognition and behavior (clinical global impression of "much improved" or better). Twelve patients (aged 5-28 years) were included from three different centers. Neurosurgical tissue samples were available in all patients and revealed a brain somatic variant in SLC35A2 in six patients (non-present in the blood). After 6 months of supplementation, D-galactose was well tolerated with just two patients presenting abdominal discomfort, solved after dose spacing or reduction. There was a 50% reduction or higher of seizure frequency in 3/6 patients, with an improvement at EEG in 2/5 patients. One patient became seizure-free. An improvement of cognitive/behavioral features encompassing impulsivity (mean SNAP-IV - 3.19 [- 0.84; - 5.6]), social communication (mean SCQ - 2.08 [- 0.63; - 4.90]), and executive function (BRIEF-2 inhibit - 5.2 [- 1.23; - 9.2]) was observed. Global responder rate was 9/12 (6/6 in SLC35A2-positive). Our results suggest that supplementation with D-galactose in patients with MOGHE is safe and well tolerated and, although the efficacy data warrant larger studies, it might build a rationale for precision medicine after epilepsy surgery.
MOGHE 被定义为癫痫伴少突胶质细胞增生的皮质发育轻度畸形。约一半经组织病理学证实的 MOGHE 患者携带编码 UDP-半乳糖转运蛋白的 SLC35A2 基因的脑体细胞变异。先前的研究表明,D-半乳糖补充剂可改善因 SLC35A2 种系变异导致的先天性糖基化障碍患者的临床症状。我们旨在评估 D-半乳糖补充剂对组织病理学证实的 MOGHE 患者的影响,这些患者在癫痫手术后仍有癫痫发作或认知障碍和 EEG 上的癫痫样活动(NCT04833322)。患者接受 D-半乳糖口服补充治疗,剂量高达 1.5g/kg/天,持续 6 个月,并在治疗前和治疗后 6 个月监测癫痫发作频率,包括 24 小时视频脑电图记录、认知和行为评分,即 WISC、BRIEF-2、SNAP-IV 和 SCQ,以及生活质量评估。总体反应定义为癫痫发作频率和/或认知和行为改善超过 50%(临床总体印象为“明显改善”或更好)。从三个不同的中心共纳入 12 名患者(年龄 5-28 岁)。所有患者均有神经外科组织样本,其中 6 名患者(不在血液中)发现 SLC35A2 脑体细胞变异。补充 6 个月后,D-半乳糖耐受性良好,仅 2 名患者出现腹部不适,通过调整剂量或减少剂量后得到解决。6 名患者中有 3 名癫痫发作频率降低 50%或更高,5 名患者中有 2 名脑电图改善。1 名患者无癫痫发作。认知/行为特征改善,包括冲动性(平均 SNAP-IV-3.19[-0.84;-5.6])、社会交流(平均 SCQ-2.08[-0.63;-4.90])和执行功能(BRIEF-2 抑制-5.2[-1.23;-9.2])。总体应答率为 9/12(SLC35A2 阳性者 6/6)。我们的结果表明,在 MOGHE 患者中补充 D-半乳糖是安全且耐受良好的,尽管疗效数据需要更大的研究,但它可能为癫痫手术后的精准医学提供依据。
