Flannery Kyle P, Safwat Sylvia, Matsell Eli, Battula Namarata, Hamed Ahlam A A, Mohamed Inaam N, Elseed Maha A, Koko Mahmoud, Abubaker Rayan, Abozar Fatima, Elsayed Liena E O, Bhise Vikram, Molday Robert S, Salih Mustafa A, Yahia Ashraf, Manzini M Chiara
Department of Neuroscience & Cell Biology, Rutgers-Robert Wood Johnson Medical School, New Brunswick, NJ 08901.
Department of Human Genetics, Medical Research Institute, Alexandria University, Alexandria, Egypt.
medRxiv. 2024 May 15:2024.05.15.24306843. doi: 10.1101/2024.05.15.24306843.
ATPase, class 1, type 8A, member 2 (ATP8A2) is a P4-ATPase with a critical role in phospholipid translocation across the plasma membrane. Pathogenic variants in are known to cause cerebellar ataxia, mental retardation, and disequilibrium syndrome 4 (CAMRQ4) which is often associated with encephalopathy, global developmental delay, and severe motor deficits. Here, we present a family with two siblings presenting with global developmental delay, intellectual disability, spasticity, ataxia, nystagmus, and thin corpus callosum. Whole exome sequencing revealed a homozygous missense variant in the nucleotide binding domain of ATP8A2 (p.Leu538Pro) that results in near complete loss of protein expression. This is in line with other missense variants in the same domain leading to protein misfolding and loss of ATPase function. In addition, by performing diffusion-weighted imaging, we identified bilateral hyperintensities in the posterior limbs of the internal capsule suggesting possible microstructural changes in axon tracts that had not been appreciated before and could contribute to the sensorimotor deficits in these individuals.
1类8A型2成员ATP酶(ATP8A2)是一种P4-ATP酶,在磷脂跨质膜转运中起关键作用。已知其致病变体会导致小脑共济失调、智力迟钝和失衡综合征4(CAMRQ4),该综合征常与脑病、全面发育迟缓及严重运动缺陷相关。在此,我们报告一个家庭,有两名兄弟姐妹表现出全面发育迟缓、智力残疾、痉挛、共济失调、眼球震颤和胼胝体变薄。全外显子组测序揭示ATP8A2核苷酸结合域存在一个纯合错义变体(p.Leu538Pro),导致蛋白质表达近乎完全丧失。这与同一结构域中导致蛋白质错误折叠和ATP酶功能丧失的其他错义变体一致。此外,通过进行扩散加权成像,我们在内囊后肢发现双侧高信号,提示轴突束可能存在此前未被认识到的微观结构变化,这可能导致这些个体出现感觉运动缺陷。
