Université de Bordeaux, Bordeaux, France; INSERM U1211, France; CHU de Bordeaux, Department of Medical Genetics, Bordeaux, France.
Université de Bordeaux, Bordeaux, France; INSERM U1211, France.
Brain Dev. 2022 Sep;44(8):567-570. doi: 10.1016/j.braindev.2022.05.001. Epub 2022 May 24.
Pathogenic variants in ATP1A3 cause various phenotypes of neurological disorders, including alternating hemiplegia of childhood 2, CAPOS syndrome (cerebellar ataxia, areflexia, pes cavus, optic atrophy, and sensorineural hearing loss) and rapid-onset dystonia-parkinsonism (RDP). Early developmental and epileptic encephalopathy has also been reported. Polymicrogyria has recently been added to the phenotypic spectrum of ATP1A3-related disorders.
We report here a male patient with early developmental delay who at 12 months presented dystonia of the right arm which evolved into hemidystonia at the age of 2. A cerebral MRI showed bilateral perisylvian polymicrogyria with intact basal ganglia. Whole-exome and whole-genome sequencing analyses identified a de novo new ATP1A3 missense variant (p.Arg914Lys) predicted pathogenic. Hemidystonia was thought not to be due to polymicrogyria, but rather a consequence of this variant.
This case expands the phenotypic spectrum of ATP1A3-related disorders with a new variant associated with hemidystonia and polymicrogyria and thereby, suggests a clinical continuum between the different phenotypes of this condition.
ATP1A3 中的致病变异可引起多种神经病变表型,包括儿童交替性偏瘫 2 型、CAPOS 综合征(小脑共济失调、反射消失、高弓足、视神经萎缩和感觉神经性听力损失)和快速进展性肌张力障碍-帕金森病(RDP)。也有报道称其与早发性发育和癫痫性脑病相关。最近,多小脑回畸形已被纳入 ATP1A3 相关疾病的表型谱中。
我们在此报告了一名男性患者,他有早期发育迟缓,在 12 个月大时出现右臂肌张力障碍,2 岁时发展为半身肌张力障碍。脑部 MRI 显示双侧侧脑室周围多小脑回畸形,基底节完整。全外显子组和全基因组测序分析确定了一个新的 ATP1A3 错义变异(p.Arg914Lys),预测为致病性变异。半身肌张力障碍并非由多小脑回畸形引起,而是该变异的结果。
该病例扩展了 ATP1A3 相关疾病的表型谱,发现了一个与半身肌张力障碍和多小脑回畸形相关的新变异,提示该疾病不同表型之间存在临床连续性。
Zotero 插件