The Ken & Ruth Davee Department of Neurology, Northwestern University Feinberg School of Medicine, Chicago, Illinois.
Department of Pharmacology, Northwestern University Feinberg School of Medicine, Chicago, Illinois.
Hum Mutat. 2020 Jun;41(6):1138-1144. doi: 10.1002/humu.24017. Epub 2020 Apr 14.
CACNA1H genetic variants were originally reported in a childhood absence epilepsy cohort. Subsequently, genetic testing for CACNA1H became available and is currently offered by commercial laboratories. However, the current status of CACNA1H as a monogenic cause of epilepsy is controversial, highlighted by ClinGen's recent reclassification of CACNA1H as disputed. We analyzed published CACNA1H variants and those reported in ClinVar and found none would be classified as pathogenic or likely pathogenic per the American College of Medical Genetics classification criteria. Moreover, Cacna1h did not modify survival in a Dravet Syndrome mouse model. We observed a mild increase in susceptibility to hyperthermia-induced seizures in mice with reduced Cacna1h expression. Overall, we conclude that there is limited evidence that CACNA1H is a monogenic cause of epilepsy in humans and that this gene should be removed from commercial genetic testing panels to reduce the burden of variants of uncertain significance for healthcare providers, families and patients with epilepsy.
CACNA1H 基因突变最初是在儿童失神性癫痫队列中报道的。随后,CACNA1H 的基因检测开始普及,并由商业实验室提供。然而,CACNA1H 作为单基因癫痫病因的现状存在争议,ClinGen 最近将 CACNA1H 重新分类为有争议的证据就是证明。我们分析了已发表的 CACNA1H 变体以及 ClinVar 中报告的变体,发现根据美国医学遗传学学院的分类标准,没有一个会被归类为致病性或可能致病性。此外,Cacna1h 并未改变 Dravet 综合征小鼠模型的生存。我们观察到,在 Cacna1h 表达减少的小鼠中,对高热诱导的癫痫发作的敏感性略有增加。总的来说,我们得出结论,有有限的证据表明 CACNA1H 是人类癫痫的单基因病因,并且应该从商业基因检测面板中删除该基因,以减少对医疗保健提供者、癫痫患者及其家属的不确定意义的变异的负担。
