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早期帕金森病视网膜变化的动态研究

Dynamics of retinal changes in early-stage Parkinson's disease.

作者信息

Murueta-Goyena Ane, Teijeira-Portas Sara, Blanco Martín Elisa, Vázquez-Picón Raquel, Ruiz Bajo Blanca, Bocos Jone, Sánchez-Molina Jorge, Alves Dias Patricia, Croitoru Ioana, Rodríguez Agirretxe Iñaki, Del Pino Rocío, Acera Marian, Tijero Beatriz, Sáez-Atxukarro Oihane, Romero-Bascones David, Gómez-Esteban Juan Carlos, Urcola Javier Aritz, Ruiz Martínez Javier, Gabilondo Iñigo

机构信息

Department of Neurosciences, Faculty of Medicine and Nursery, University of the Basque Country (UPV/EHU), Leioa, Spain.

Neurodegenerative Diseases Group, Biobizkaia Health Research Institute, Barakaldo, Bizkaia, Spain.

出版信息

Acta Neuropathol Commun. 2025 Jan 31;13(1):20. doi: 10.1186/s40478-025-01936-x.

Abstract

Parkinson's disease (PD) is a neurodegenerative disorder primarily characterized by motor symptoms, with emerging evidence suggesting retinal pathology, particularly in the ganglion cell-inner plexiform layer (GCIPL), detectable via optical coherence tomography (OCT). This study aimed to characterize early retinal dynamics in PD using OCT. We conducted a prospective one-year longitudinal multicenter study involving 53 early-stage PD patients with a disease duration of 5 years or less and 52 controls. The participants underwent retinal spectral-domain OCT, primary visual function and cognitive examinations. We examined baseline retinal measures and short-term longitudinal differences between groups via linear mixed effects models. In PD patients, the baseline GCIPL thickness in central regions was increased by up to 4 μm, and the rate of thinning in the parafoveal GCIPL was - 0.61 [0.29] µm/year faster over a one-year follow-up period than in controls in the 2- to 3-mm ring (p = 0.039). In PD patients, greater central GCIPL thickness was associated with poorer contrast sensitivity and reduced performance on the Farnsworth D15 color vision test. It also predicted subsequent thinning in both the GCIPL (2- to 3-mm ring) and the inner nuclear layer (2- to 5-mm rings). However, this increased thickness was not linked to prevalent or progressive motor or cognitive manifestations. In conclusion, this study provides the first detailed topographical description of early retinal dynamics in PD patients, revealing increased central GCIPL thickness and accelerated parafoveal GCIPL thinning in PD. However, the macular region shows complex and variable dynamics among PD patients, but these changes precede detectable progression in clinical scales.

摘要

帕金森病(PD)是一种主要以运动症状为特征的神经退行性疾病,越来越多的证据表明存在视网膜病变,特别是在神经节细胞 - 内丛状层(GCIPL),可通过光学相干断层扫描(OCT)检测到。本研究旨在利用OCT对帕金森病早期视网膜动态变化进行特征描述。我们进行了一项为期一年的前瞻性纵向多中心研究,纳入了53例疾病病程在5年及以内的早期帕金森病患者和52例对照者。参与者接受了视网膜光谱域OCT、主要视觉功能和认知检查。我们通过线性混合效应模型检查了基线视网膜测量值以及组间的短期纵向差异。在帕金森病患者中,中央区域的基线GCIPL厚度增加了多达4μm,在为期一年的随访期内,旁中央凹GCIPL的变薄速率比2至3毫米环内的对照组快 -0.61[0.29]μm/年(p = 0.039)。在帕金森病患者中,中央GCIPL厚度越大,对比敏感度越差,在 Farnsworth D15 色觉测试中的表现也越差。它还预测了GCIPL(2至3毫米环)和内核层(2至5毫米环)随后的变薄情况。然而,这种厚度增加与普遍或进行性的运动或认知表现无关。总之,本研究首次详细描述了帕金森病患者早期视网膜动态变化的地形图,揭示了帕金森病患者中央GCIPL厚度增加和旁中央凹GCIPL变薄加速。然而,黄斑区域在帕金森病患者中表现出复杂多变的动态变化,但这些变化在临床量表可检测到的进展之前就已出现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5cff/11784094/067a35fe5516/40478_2025_1936_Fig1_HTML.jpg

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