Neurology Department, Dijon University Hospital, 14 rue Paul Gaffarel, 21000, Dijon, Burgundy, France.
Biochemistry of the Peroxisome, Inflammation and Lipid Metabolism, EA7270/Inserm, University of Burgundy and Franche-Comté, Dijon, Burgundy, France.
Cerebellum. 2024 Dec;23(6):2616-2621. doi: 10.1007/s12311-024-01725-7. Epub 2024 Jul 29.
Biallelic WARS2 pathogenic variants responsible for partial defect in aminoacylation, have recently been reported in subjects presenting with late-onset phenotypes combining dopa-responsive early-onset dystonia parkinsonism with altered DaTSCAN and progressive myoclonus ataxia. Here, we present the case of a 39-year-old male with childhood-onset progressive dopa-responsive dystonia parkinsonism, prominent psychiatric features and ataxia whose genome sequencing identified a p.(Arg36Ter) nonsense variant and a hypomorphic p.(Trp13Gly) missense variant, allowing the diagnosis of WARS2-related disease. The p.(Trp13Gly) missense variant has previously been reported in individuals with less severe phenotypes than those carrying biallelic WARS2 loss-of-function variants. Among these individuals, two subjects had similar genetic backgrounds and almost identical clinical history to our patient. Our report brings additional proof that the p.(Trp13Gly) variant acts as a hypomorphic allele, offering insight on a genotype-phenotype correlation in WARS2-related disorders.
最近有研究报道,在具有晚发性表型的患者中发现了WARTS2 双等位致病性变异,这些患者的表型组合为多巴胺反应性早发性肌张力障碍帕金森病,伴有 DaTSCAN 改变和进行性肌阵挛共济失调。在此,我们报告了一例 39 岁男性的病例,其具有儿童起病的进行性多巴胺反应性肌张力障碍帕金森病、突出的精神特征和共济失调,基因组测序发现了一个 p.(Arg36Ter)无义变异和一个功能降低的 p.(Trp13Gly)错义变异,从而诊断为 WARS2 相关疾病。先前已有报道称,携带 p.(Trp13Gly)错义变异的个体的表型比携带双等位 WARTS2 功能丧失变异的个体要轻。在这些个体中,有两名个体具有与我们患者相似的遗传背景和几乎相同的临床病史。我们的报告提供了额外的证据,证明 p.(Trp13Gly)变异是一个功能降低的等位基因,为 WARS2 相关疾病的基因型-表型相关性提供了新的见解。
