Assessing Retinal Structure in Patients with Parkinson's Disease.

Journal of neurology & neurophysiology Pub Date : 2019-01-01 Epub Date: 2019-03-07 DOI:10.4172/2155-9562.1000485
Jonathon B Young, Pooja Godara, Vesper Williams, Phyllis Summerfelt, Thomas B Connor, Sergey Tarima, Alexis Visotcky, Robert F Cooper, Karen Blindauer, Joseph Carroll
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引用次数: 7

Abstract

Objective: The retina is an extension of the central nervous system (CNS), and ocular symptoms can precede manifestations of CNS disorders. Given that several neurodegenerative conditions that affect the brain exhibit ocular symptoms, the retina may be an accessible biomarker to monitor disease progression. Dopamine, the key neurotransmitter related to Parkinson's disease (PD), is contained in amacrine and interplexiform cells, which reside in specific retinal layers. Understanding how loss of dopaminergic cells affects retinal anatomy could be relevant for monitoring disease progression. Here, our objective is to evaluate retinal structure (foveal pit morphology and thickness) in patients with PD.

Methods: Thirty-three Caucasian subjects diagnosed with PD and 40 age-matched Caucasian control subjects underwent retinal imaging with spectral-domain optical coherence tomography (SD-OCT). Axial length measurements were used to correct the lateral scale of each macular volume scan. From these corrected volumes, foveal morphology was quantified with previously described algorithms, and Early Treatment Diabetic Retinopathy Study (ETDRS) grids of retinal thickness were generated and incorporated into a logistic regression model to predict PD.

Results: Interocular foveal morphology measurements were highly symmetrical in PD patients and control subjects. There were no significant differences in foveal pit morphology between PD patients and control subjects. Using a model incorporating sex and axial length corrected ETDRS regions, we generated a receiver operating characteristic curve with a C-statistic of 0.80.

Conclusion: Our study, which to our knowledge is the first to properly scale OCT measurements when quantifying retinal thickness, demonstrates that PD patients retain foveal symmetry between eyes. When constructing a model to predict PD, sex, along with the center 1 mm and temporal outer ETDRS regions, were significant predictors of PD. In addition to proper scaling of OCT measures, gender and racial differences in retinal anatomy should be considered in building future predictive PD models when using OCT.

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帕金森病患者视网膜结构的评估。
目的:视网膜是中枢神经系统(CNS)的延伸,眼部症状可先于中枢神经系统疾病的表现。鉴于几种影响大脑的神经退行性疾病表现出眼部症状,视网膜可能是监测疾病进展的一种可获得的生物标志物。多巴胺是与帕金森病(PD)相关的关键神经递质,存在于特定视网膜层的无突细胞和丛状细胞中。了解多巴胺能细胞的丧失如何影响视网膜解剖结构,可能与监测疾病进展有关。在这里,我们的目的是评估PD患者的视网膜结构(中央凹的形态和厚度)。方法:33例诊断为帕金森病的白种人和40例年龄匹配的白种人对照,采用光谱域光学相干断层扫描(SD-OCT)进行视网膜成像。轴向长度测量用于校正每个黄斑体积扫描的横向刻度。根据这些校正后的体积,使用先前描述的算法对中央凹形态进行量化,并生成早期治疗糖尿病视网膜病变研究(ETDRS)视网膜厚度网格,并将其纳入逻辑回归模型以预测PD。结果:PD患者和对照组的眼间中央凹形态测量高度对称。PD患者与对照组在中央凹凹形态上无显著差异。使用包含性别和轴向长度校正的ETDRS区域的模型,我们生成了c统计量为0.80的受试者工作特性曲线。结论:据我们所知,我们的研究是第一个在量化视网膜厚度时适当缩放OCT测量的研究,表明PD患者保留了两眼中央凹对称性。在构建预测PD的模型时,性别、中心1mm和时间外ETDRS区域是PD的显著预测因子。除了OCT测量的适当比例外,在使用OCT时,在建立未来的预测PD模型时应考虑视网膜解剖学中的性别和种族差异。
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