由反复出现的 c.892C>T NACC1 变异引起的多动障碍。
Hyperkinetic Movement Disorder Caused by the Recurrent c.892C>T NACC1 Variant.
机构信息
Research Unit of Clinical Medicine, University of Oulu, Oulu, Finland.
Medical Research Center, Oulu University Hospital, University of Oulu, Oulu, Finland.
出版信息
Mov Disord Clin Pract. 2024 Jun;11(6):708-715. doi: 10.1002/mdc3.14051. Epub 2024 May 2.
BACKGROUND
Genetic syndromes of hyperkinetic movement disorders associated with epileptic encephalopathy and intellectual disability are becoming increasingly recognized. Recently, a de novo heterozygous NACC1 (nucleus accumbens-associated 1) missense variant was described in a patient cohort including one patient with a combined mitochondrial oxidative phosphorylation (OXPHOS) deficiency.
OBJECTIVES
The objective is to characterize the movement disorder in affected patients with the recurrent c.892C>T NACC1 variant and study the NACC1 protein and mitochondrial function at the cellular level.
METHODS
The movement disorder was analyzed on four patients with the NACC1 c.892C>T (p.Arg298Trp) variant. Studies on NACC1 protein and mitochondrial function were performed on patient-derived fibroblasts.
RESULTS
All patients had a generalized hyperkinetic movement disorder with chorea and dystonia, which occurred cyclically and during sleep. Complex I was found altered, whereas the other OXPHOS enzymes and the mitochondria network seemed intact in one patient.
CONCLUSIONS
The movement disorder is a prominent feature of NACC1-related disease.
背景
与癫痫性脑病和智力障碍相关的多动障碍的遗传综合征正越来越受到关注。最近,在一个包括一名线粒体氧化磷酸化(OXPHOS)缺陷合并患者的患者队列中,描述了一种新的杂合 NACC1(伏隔核相关 1)错义变体。
目的
本研究的目的是对携带反复发生的 NACC1 c.892C>T 变异体的受影响患者的运动障碍进行特征描述,并在细胞水平上研究 NACC1 蛋白和线粒体功能。
方法
对 4 名 NACC1 c.892C>T(p.Arg298Trp)变异体患者的运动障碍进行分析。对患者来源的成纤维细胞进行 NACC1 蛋白和线粒体功能的研究。
结果
所有患者均出现全身性多动障碍,伴有舞蹈症和肌张力障碍,且周期性发生,在睡眠中也会出现。在一名患者中发现复合物 I 改变,而其他 OXPHOS 酶和线粒体网络似乎完好无损。
结论
运动障碍是 NACC1 相关疾病的一个突出特征。
Zotero 插件