位于钠通道核心区域之外的SCN1A错义变异导致的严重癫痫表型:功能结果与临床表型之间的关系
Severe epilepsy phenotype with SCN1A missense variants located outside the sodium channel core region: Relationship between functional results and clinical phenotype.
作者信息
Fang Zhixu, Xie Lingling, Li Xue, Gui Jianxiong, Yang Xiaoyue, Han Ziyao, Luo Hanyu, Huang Dishu, Chen Hengsheng, Cheng Li, Jiang Li
机构信息
Department of Neurology, Children's Hospital of Chongqing Medical University, National Clinical Research Center for Child Health and Disorders, Ministry of Education Key Laboratory of Child Development and Disorders, Chongqing Key Laboratory of Pediatrics, No. 136, Zhongshan Er Road, Yuzhong District, Chongqing 400014, China.
Department of Neurology, Children's Hospital of Chongqing Medical University, National Clinical Research Center for Child Health and Disorders, Ministry of Education Key Laboratory of Child Development and Disorders, Chongqing Key Laboratory of Pediatrics, No. 136, Zhongshan Er Road, Yuzhong District, Chongqing 400014, China.
出版信息
Seizure. 2022 Oct;101:109-116. doi: 10.1016/j.seizure.2022.07.018. Epub 2022 Aug 3.
PURPOSE
Most SCN1A missense variants located outside the sodium channel core region show a mild phenotype. However, there are exceptions, because of which it is challenging to determine the correlation between genotype and phenotype. In this study, we aimed to determine whether functional study could be used to determine disease severity in cases with such variants, and elucidate possible genotype-phenotype relationships.
METHODS
Forty-seven patients with SCN1A missense variants were recruited, and one with a Dravet syndrome phenotype with an SCN1A missense variant (c.3811T>C/ p.W1271R) located outside the core region was screened with electrophysiological tests. We also reviewed functional SCN1A studies on patients with inconsistent phenotypes and genotypes, and studied the relationship between electrophysiological measurements and clinical phenotype.
RESULTS
Patch clamp experiments showed that the W1271R variant caused significantly reduced sodium current, decreased channel voltage sensitivity, loss of channel availability, and prolonged recovery time from inactivation compared with wild type (WT), which ultimately caused a change in loss of function (LOF). Twelve cases of severe SCN1A-related epilepsy with missense variants located outside the channel core region were also included from the functional studies. Nine patients with missense SCN1A variants showed complete (3/9) or partial (6/9) physiological LOF. Two missense SCN1A variants caused physiological gain-and-loss of function (G-LOF), and one caused decreased excitability (DE).
CONCLUSIONS
Not all missense variants located outside the core region cause a mild phenotype. Although current functional studies in heterologous expression systems do not accurately reflect disease severity caused by SCN1A missense variants, they could be an effective model for generation of data to study the initial effects of SCN1A missense variants.
目的
大多数位于钠通道核心区域之外的SCN1A错义变体表现出轻度表型。然而,也有例外情况,因此确定基因型与表型之间的相关性具有挑战性。在本研究中,我们旨在确定功能研究是否可用于确定具有此类变体的病例的疾病严重程度,并阐明可能的基因型-表型关系。
方法
招募了47例具有SCN1A错义变体的患者,并对1例患有Dravet综合征表型且SCN1A错义变体(c.3811T>C/p.W1271R)位于核心区域之外的患者进行了电生理测试筛查。我们还回顾了关于表型和基因型不一致的患者的SCN1A功能研究,并研究了电生理测量与临床表型之间的关系。
结果
膜片钳实验表明,与野生型(WT)相比,W1271R变体导致钠电流显著降低、通道电压敏感性降低、通道可用性丧失以及失活后恢复时间延长,最终导致功能丧失(LOF)改变。功能研究还纳入了12例严重的SCN1A相关癫痫病例,其错义变体位于通道核心区域之外。9例具有SCN1A错义变体的患者表现出完全(3/9)或部分(6/9)生理性LOF。2个SCN1A错义变体导致生理性功能得失(G-LOF),1个导致兴奋性降低(DE)。
结论
并非所有位于核心区域之外的错义变体都会导致轻度表型。尽管目前在异源表达系统中的功能研究不能准确反映SCN1A错义变体引起的疾病严重程度,但它们可能是生成数据以研究SCN1A错义变体初始效应的有效模型。
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