Frequency of the D620N mutation in VPS35 in Parkinson disease.

Kishore R Kumar, Anne Weissbach, Marcus Heldmann, Meike Kasten, Sinem Tunc, Carolyn M Sue, Marina Svetel, Vladimir S Kostić, Juan Segura-Aguilar, Alfredo Ramirez, David K Simon, Peter Vieregge, Thomas F Münte, Johann Hagenah, Christine Klein, Katja Lohmann
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引用次数: 82

Abstract

Objective: To evaluate the frequency and clinical spectrum of the recently identified p.D620N mutation in the VPS35 gene in Parkinson disease (PD) in an international sample.

Design: Genetic analysis by DNA sequencing and detailed clinical and neuropsychiatric assessment as well as neuroimaging in mutation carriers.

Setting: Tertiary referral centers in Germany, Serbia, Chile, and the United States.

Patients: One thousand seven hundred seventy-four patients with PD.

Main outcome measure: Frequency of the p.D620N mutation.

Results: A single mutation carrier was identified. The mutation carrier was a 60-year-old German man who had tremor-dominant PD since the age of 45 years. Longitudinal follow-up over 13 years revealed a disease progression from Hoehn and Yahr stage 1 to 3. There was evidence of mild cognitive impairment on the Montreal Cognitive Assessment. No abnormalities were observed by multimodal neuroimaging. He had a family history consistent with autosomal dominant inheritance. An affected paternal aunt and 3 reportedly unaffected siblings were also found to be mutation carriers.

Conclusion: VPS35 mutations are a rare cause of PD in different populations. The clinical phenotype may be indistinguishable from idiopathic PD with the possible exception of an earlier age at onset. Genetic analysis of the extended family revealed incomplete penetrance of the p.D620N mutation.

帕金森病VPS35中D620N突变的频率
目的:评价最近在国际样本中发现的帕金森病(PD) VPS35基因p.D620N突变的频率和临床谱。设计:通过DNA测序和详细的临床和神经精神评估以及突变携带者的神经影像学进行遗传分析。地点:德国、塞尔维亚、智利和美国的三级转诊中心。患者:一千七百七十四名PD患者。主要观察指标:p.D620N突变频率。结果:鉴定出单个突变载体。突变携带者是一名60岁的德国男性,他从45岁起就患有震颤型PD。13年的纵向随访显示,从Hoehn和Yahr阶段1到3的疾病进展。在蒙特利尔认知评估中有轻度认知障碍的证据。多模态神经影像学检查未见异常。他的家族史符合常染色体显性遗传。一位受影响的姑姑和3名据报道未受影响的兄弟姐妹也被发现是突变携带者。结论:在不同人群中,VPS35突变是一种罕见的PD病因。临床表型可能与特发性PD难以区分,可能的例外是发病年龄较早。家族遗传分析显示p.D620N突变不完全外显。
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来源期刊
Archives of neurology
Archives of neurology 医学-临床神经学
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