Retinal Damage and Visual Network Reconfiguration Defines Visual Function Recovery in Optic Neuritis.

IF 7.8 1区医学 Q1 CLINICAL NEUROLOGY

Neurology® Neuroimmunology & Neuroinflammation Pub Date : 2024-11-01 Epub Date: 2024-08-30 DOI:10.1212/NXI.0000000000200288

Pablo Villoslada, Elisabeth Solana, Salut Alba-Arbalat, Eloy Martinez-Heras, Francesc Vivo, Elisabet Lopez-Soley, Alberto Calvi, Anna Camos-Carreras, Marina Dotti-Boada, Rafel Alcubierre Bailac, Elena H Martinez-Lapiscina, Yolanda Blanco, Sara Llufriu, Bernardo F Sanchez Dalmau

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Abstract

Background and objectives: Recovery of vision after acute optic neuritis (AON) is critical to improving the quality of life of people with demyelinating diseases. The objective of the study was to prospectively assess the changes in visual acuity, retinal layer thickness, and cortical visual network in patients with AON to identify the predictors of permanent visual disability.

Methods: We studied a prospective cohort of 88 consecutive patients with AON with 6-month follow-up using high and low-contrast (2.5%) visual acuity, color vision, retinal thickness from optical coherence tomography, latencies and amplitudes of multifocal visual evoked potentials, mean deviation of visual fields, and diffusion-based structural (n = 53) and functional (n = 19) brain MRI to analyze the cortical visual network. The primary outcome was 2.5% low-contrast vision, and data were analyzed with mixed-effects and multivariate regression models.

Results: We found that after 6 months, low-contrast vision and quality of vision remained moderately impaired. The thickness of the ganglion cell layer at baseline was a predictor of low-contrast vision 6 months later (ß = 0.49 [CI 0.11-0.88], p = 0.012). The structural cortical visual network at baseline predicted low-contrast vision, the best predictors being the betweenness of the right parahippocampal cortex (ß = -036 [CI -0.66 to 0.06], p = 0.021), the node strength of the right V3 (ß = 1.72 [CI 0.29-3.15], p = 0.02), and the clustering coefficient of the left intraparietal sulcus (ß = 57.8 [CI 12.3-103.4], p = 0.015). The functional cortical visual network at baseline also predicted low-contrast vision, the best predictors being the betweenness of the left ventral occipital cortex (ß = 8.6 [CI: 4.03-13.3], p = 0.009), the node strength of the right intraparietal sulcus (ß = -2.79 [CI: -5.1-0.4], p = 0.03), and the clustering coefficient of the left superior parietal lobule (ß = 501.5 [CI 50.8-952.2], p = 0.03).

Discussion: The assessment of the visual pathway at baseline predicts permanent vision disability after AON, indicating that damage is produced early after disease onset and that it can be used for defining vision impairment and guiding therapy.

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视网膜损伤和视觉网络重构决定视神经炎的视觉功能恢复

背景和目的：急性视神经炎（AON）后视力的恢复对于改善脱髓鞘疾病患者的生活质量至关重要。本研究的目的是前瞻性地评估 AON 患者视力、视网膜层厚度和皮质视觉网络的变化，以确定永久性视力残疾的预测因素：我们对连续 88 例 AON 患者进行了为期 6 个月的前瞻性队列研究，采用高对比度和低对比度（2.5%）视力、色觉、光学相干断层扫描视网膜厚度、多焦点视觉诱发电位的潜伏期和振幅、视野平均偏差以及基于扩散的结构性（53 例）和功能性（19 例）脑磁共振成像来分析皮质视觉网络。主要结果为2.5%的低对比度视力，数据采用混合效应和多元回归模型进行分析：结果：我们发现，6 个月后，低对比度视力和视觉质量仍然受到中度损害。基线时神经节细胞层的厚度可预测 6 个月后的低对比度视力（ß = 0.49 [CI 0.11-0.88], p = 0.012）。基线时的皮层视觉网络结构可预测低对比度视力，其中预测效果最好的是右侧海马旁皮层（ß = -036 [CI -0.66 to 0.06], p = 0.021）、右侧 V3 的节点强度（ß = 1.72 [CI 0.29-3.15], p = 0.02）和左侧顶内沟的聚类系数（ß = 57.8 [CI 12.3-103.4], p = 0.015）。基线时的皮层视觉功能网络也能预测低对比度视觉，最佳预测因子是左侧腹枕叶皮层的间隔系数（ß = 8.6 [CI: 4.03-13.3], p = 0.009）、右顶内沟的节点强度（ß = -2.79 [CI：-5.1-0.4]，p = 0.03）和左顶上叶的聚类系数（ß = 501.5 [CI：50.8-952.2]，p = 0.03）：讨论：基线时的视觉通路评估可预测AON后的永久性视力残疾，表明损伤在发病后早期就已产生，可用于定义视力损伤和指导治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Neurology® Neuroimmunology & Neuroinflammation Neuroscience-Neurology

CiteScore

15.60

自引率

2.30%

发文量

219

审稿时长

8 weeks

期刊介绍： Neurology Neuroimmunology & Neuroinflammation is an official journal of the American Academy of Neurology. Neurology: Neuroimmunology & Neuroinflammation will be the premier peer-reviewed journal in neuroimmunology and neuroinflammation. This journal publishes rigorously peer-reviewed open-access reports of original research and in-depth reviews of topics in neuroimmunology & neuroinflammation, affecting the full range of neurologic diseases including (but not limited to) Alzheimer's disease, Parkinson's disease, ALS, tauopathy, and stroke; multiple sclerosis and NMO; inflammatory peripheral nerve and muscle disease, Guillain-Barré and myasthenia gravis; nervous system infection; paraneoplastic syndromes, noninfectious encephalitides and other antibody-mediated disorders; and psychiatric and neurodevelopmental disorders. Clinical trials, instructive case reports, and small case series will also be featured.