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日间过度嗜睡可能与帕金森病的尾状核去神经支配有关。

Excessive daytime sleepiness may be associated with caudate denervation in Parkinson disease.

机构信息

Neurodegeneration Imaging Group, Institute of Psychiatry, Psychology and Neuroscience (IoPPN), King's College London, London, UK.

出版信息

J Neurol Sci. 2018 Apr 15;387:220-227. doi: 10.1016/j.jns.2018.02.032. Epub 2018 Feb 21.

Abstract

Excessive daytime sleepiness (EDS) is one of the earliest and most common non-motor symptoms of PD, substantially impacting on patient's quality of life. Using the Parkinson's Progression Markers Initiative database, we performed a case-control study to investigate whether dopaminergic deficit is associated with the development of EDS using dopaminergic specific single photon emission computed tomography (SPECT) molecular imaging of dopamine transporters (DAT). We enrolled 84 early de novo PD patients with EDS and 84 without EDS, who were matched for age, gender, age of diagnosis, years of education and disease duration. We assessed and compared semi-quantified [I]FP-CIT SPECT, and motor and non-motor features among these two groups, alongside exploring the clinical and imaging correlates of EDS and the predictive significance of these markers in the development of EDS. PD patients with EDS had worse non-motor (MDS-UPDRS Part-I, P < 0.001) and motor (MDS-UPRDS Part-II, P = 0.005) experiences of daily living, as well as worse autonomic (SCOPA-AUT, P < 0.0001) and cognitive (MoCA P = 0.05) function, depression (GDS, P = 0.002), and reduced caudate DAT ([I]FP-CIT, P = 0.024) compared to PD patients without EDS. Lower caudate [I]FP-CIT values correlated with higher EDS scores (r = -0.192, P = 0.013). Among patients without EDS, 47 PD patients (56%) developed EDS over a median follow-up of 36 months. Cox multivariate analysis, including all clinical and imaging data available, revealed that abnormal caudate [I]FP-CIT uptake (P = 0.030) and disease duration (P = 0.018) were predictors for the development of EDS. Although our findings indicate that dopaminergic deficits in the caudate may be associated to EDS in patients with PD, the pathophysiological causality is debateable, given that dopamine caudate denervation may covary with dopaminergic involvement at other targets and with non-dopaminergic involvement.

摘要

日间过度嗜睡(EDS)是 PD 的最早和最常见的非运动症状之一,极大地影响了患者的生活质量。我们使用帕金森进展标志物倡议数据库进行了一项病例对照研究,使用多巴胺转运体(DAT)的多巴胺能特异性单光子发射计算机断层扫描(SPECT)分子成像来研究多巴胺能缺陷是否与 EDS 的发展有关。我们招募了 84 名患有 EDS 的早期初发 PD 患者和 84 名无 EDS 的患者,他们在年龄、性别、诊断年龄、受教育年限和病程方面相匹配。我们评估和比较了这两组患者的半定量[I]FP-CIT SPECT,以及运动和非运动特征,同时探讨了 EDS 的临床和影像学相关性以及这些标志物在 EDS 发展中的预测意义。患有 EDS 的 PD 患者的非运动(MDS-UPDRS 第一部分,P<0.001)和运动(MDS-UPDRS 第二部分,P=0.005)日常生活体验更差,自主功能(SCOPA-AUT,P<0.0001)和认知功能(MoCA P=0.05)更差,抑郁(GDS,P=0.002),以及尾状核 DAT([I]FP-CIT,P=0.024)减少。较低的尾状核[I]FP-CIT 值与更高的 EDS 评分相关(r=-0.192,P=0.013)。在没有 EDS 的患者中,47 名 PD 患者(56%)在中位随访 36 个月后出现 EDS。Cox 多变量分析包括所有可用的临床和影像学数据,结果显示异常的尾状核[I]FP-CIT 摄取(P=0.030)和疾病持续时间(P=0.018)是 EDS 发展的预测因素。尽管我们的研究结果表明,PD 患者尾状核中的多巴胺能缺陷可能与 EDS 有关,但由于多巴胺能尾状核去神经支配可能与其他靶点的多巴胺能参与以及非多巴胺能参与相关,因此其病理生理因果关系仍存在争议。

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