Department of Neurology, Mayo Clinic, Jacksonville, FL, USA; Division of Neurological and Psychiatric Nursing, Faculty of Health Sciences, Medical University of Gdansk, Gdansk, Poland; Neurology Department, St Adalbert Hospital, Copernicus PL Ltd., Gdansk, Poland.
Department of Neuroscience, Mayo Clinic, Jacksonville, FL, USA.
Parkinsonism Relat Disord. 2023 Jul;112:105481. doi: 10.1016/j.parkreldis.2023.105481. Epub 2023 Jun 13.
Perry syndrome (PS) is a hereditary neurodegenerative disorder caused by mutations in the DCTN1 gene and characterized by TDP-43 pathology. As the diagnosis is usually made at the advanced stages of the disease, there are no studies on the asymptomatic mutation carriers and their conversion to overt disease.
We personally examined 27 members of the large kindred of 104 individuals with familial parkinsonism. We evaluated each case with clinical (neurological examination; motor and non-motor scales), genetic testing (whole-exome or Sanger sequencing), and laboratory (neurofilament light, NFL; glial fibrillary acidic protein, GFAP) measures. Autopsy study was done on two individuals.
The mean age at evaluation was 49 years. Comorbidities were present in 20 cases, including sleep problems (n = 15 total, sleep apnea in 7), dysautonomia (n = 10), weight loss (n = 8), and anxiety/depression (n = 8). Neurological abnormalities were present in 18, including parkinsonism (n = 7), isolated tremor (n = 2), and varied isolated signs in individual cases. Cognition and smell were preserved. Genetic testing revealed a novel c.200G > T (Gly67Val) mutation in the DCTN1 gene in 10 individuals. The mutation, segregated with the PS phenotype (n = 4), was absent in gnomAD, and in silico predictions indicated it was pathogenic. Three young mutation carriers were monosymptomatic (prodromal), and three were asymptomatic. Plasma NFL and GFAP values were similar among the cases. Autopsy studies showed typical PS neuropathological findings.
We identified a novel pathogenic Gly67Val DCTN1 mutation. We report prodromal disease of PS in some mutation carriers; however, more investigation is necessary to confirm this observation.
佩里综合征(PS)是一种遗传性神经退行性疾病,由 DCTN1 基因突变引起,其特征是 TDP-43 病理学改变。由于该病的诊断通常在疾病的晚期进行,因此尚无关于无症状突变携带者及其向显性疾病转化的研究。
我们亲自检查了 104 例家族性帕金森病患者的大型家族中的 27 名成员。我们通过临床(神经检查;运动和非运动量表)、基因检测(全外显子或 Sanger 测序)和实验室(神经丝轻链,NFL;神经胶质纤维酸性蛋白,GFAP)评估每个病例。对两名个体进行了尸检研究。
评估时的平均年龄为 49 岁。20 例存在合并症,包括睡眠问题(共 15 例,其中 7 例为睡眠呼吸暂停)、自主神经功能障碍(n=10)、体重减轻(n=8)和焦虑/抑郁(n=8)。18 例存在神经系统异常,包括帕金森病(n=7)、孤立性震颤(n=2)和个别病例的各种孤立体征。认知和嗅觉保存完好。基因检测在 10 名个体中发现了 DCTN1 基因的 novel c.200G>T (Gly67Val) 突变。该突变与 PS 表型(n=4)分离,在 gnomAD 中不存在,并且计算机预测表明它是致病性的。3 名年轻的突变携带者为单症状性(前驱期),3 名无症状。病例之间的血浆 NFL 和 GFAP 值相似。尸检研究显示出典型的 PS 神经病理学发现。
我们发现了一种新的致病性 Gly67Val DCTN1 突变。我们报告了一些突变携带者中前驱期 PS 疾病;然而,需要更多的研究来证实这一观察结果。
