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载脂蛋白Eε4:轻度认知障碍帕金森病患者执行功能障碍的生物标志物。

Apolipoprotein Eε4: A Biomarker for Executive Dysfunction among Parkinson's Disease Patients with Mild Cognitive Impairment.

作者信息

Samat Nor A, Abdul Murad Nor A, Mohamad Khairiyah, Abdul Razak Mohd R, Mohamed Ibrahim Norlinah

机构信息

Department of Medicine, UKM Medical Centre, Chancellor Tuanku Muhriz Hospital & Universiti Kebangsaan Malaysia Medical Centre, Kuala Lumpur, Malaysia.

Universiti Kebangsaan Malaysia Medical Molecular Biology Institute, Kuala Lumpur, Malaysia.

出版信息

Front Neurosci. 2017 Dec 20;11:712. doi: 10.3389/fnins.2017.00712. eCollection 2017.

DOI:10.3389/fnins.2017.00712
PMID:29326545
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5742342/
Abstract

Cognitive impairment is prevalent in Parkinson's disease (PD), affecting 15-20% of patients at diagnosis. α-synuclein expression and genetic polymorphisms of Apolipoprotein E () have been associated with the presence of cognitive impairment in PD although data have been inconsistent. To determine the prevalence of cognitive impairment in patients with PD using Montreal Cognitive Assessment (MoCA), Comprehensive Trail Making Test (CTMT) and Parkinson's disease-cognitive rating scale (PDCRS), and its association with plasma α-synuclein and genetic polymorphisms. This was across-sectional study involving 46 PD patients. Patients were evaluated using Montreal cognitive assessment test (MoCA), and detailed neuropsychological tests. The Parkinson's disease cognitive rating scale (PDCRS) was used for cognitive function and comprehensive trail making test (CTMT) for executive function. Blood was drawn for plasma α-synuclein measurements and genetic analysis. polymorphism was detected using MutaGEL from ImmunDiagnostik. Plasma α-synuclein was detected using the ELISA Technique (USCN Life Science Inc.) according to the standard protocol. Based on MoCA, 26 (56.5%) patients had mild cognitive impairment (PD-MCI) and 20 (43.5%) had normal cognition (PD-NC). Based on the PDCRS, 18 (39.1%) had normal cognition (PDCRS-NC), 17 (37%) had mild cognitive impairment (PDCRS-MCI), and 11 (23.9%) had dementia (PDCRS-PDD). In the PDCRS-MCI group, 5 (25%) patients were from PD-NC group and all PDCRS-PDD patients were from PD-MCI group. CTMT scores were significantly different between patients with MCI and normal cognition on MoCA ( = 0.003). Twenty one patients (72.4%) with executive dysfunction were from the PD-MCI group; 17 (77.3%) with severe executive dysfunction and 4 (57.1%) had mild to moderate executive dysfunction. There were no differences in the plasma α-synuclein concentration between the presence or types of cognitive impairment based on MoCA, PDCRS, and CTMT. The allele carrier frequency was significantly higher in patients with executive dysfunction ( = 0.014). MCI was prevalent in our PD population. PDCRS appeared to be more discriminatory in detecting MCI and PDD than MoCA. Plasma α-synuclein level was not associated with presence nor type of cognitive impairment, but the allele carrier status was significantly associated with executive dysfunction in PD.

摘要

认知障碍在帕金森病(PD)中很常见,在诊断时影响15%-20%的患者。α-突触核蛋白表达和载脂蛋白E()的基因多态性与PD中认知障碍的存在有关,尽管数据并不一致。本研究旨在使用蒙特利尔认知评估量表(MoCA)、综合连线测验(CTMT)和帕金森病认知评定量表(PDCRS)来确定PD患者认知障碍的患病率,及其与血浆α-突触核蛋白和基因多态性的关系。这是一项涉及46例PD患者的横断面研究。使用蒙特利尔认知评估测试(MoCA)和详细的神经心理学测试对患者进行评估。帕金森病认知评定量表(PDCRS)用于评估认知功能,综合连线测验(CTMT)用于评估执行功能。采集血液用于测量血浆α-突触核蛋白并进行基因分析。使用免疫诊断公司的MutaGEL检测基因多态性。根据标准方案,使用酶联免疫吸附测定技术(武汉优尔生科技股份有限公司)检测血浆α-突触核蛋白。基于MoCA,26例(56.5%)患者有轻度认知障碍(PD-MCI),20例(43.5%)认知正常(PD-NC)。基于PDCRS,18例(39.1%)认知正常(PDCRS-NC),17例(37%)有轻度认知障碍(PDCRS-MCI),11例(23.9%)有痴呆(PDCRS-PDD)。在PDCRS-MCI组中,5例(25%)患者来自PD-NC组,所有PDCRS-PDD患者均来自PD-MCI组。MoCA评估中,MCI患者和认知正常患者的CTMT评分有显著差异(=0.003)。21例(72.4%)执行功能障碍患者来自PD-MCI组;17例(77.3%)有严重执行功能障碍,4例(57.1%)有轻度至中度执行功能障碍。基于MoCA、PDCRS和CTMT,认知障碍的存在或类型不同,血浆α-突触核蛋白浓度无差异。执行功能障碍患者的等位基因携带频率显著更高(=0.014)。MCI在我们的PD患者群体中很普遍。与MoCA相比,PDCRS在检测MCI和PDD方面似乎更具鉴别力。血浆α-突触核蛋白水平与认知障碍的存在或类型无关,但等位基因携带状态与PD患者的执行功能障碍显著相关。

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