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Microcystic macular edema: Retrograde maculopathy caused by optic neuropathy

机译:黄斑微囊性水肿:视神经病变引起的逆行性黄斑病变

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Purpose To investigate retrograde axonal degeneration for its potential to cause microcystic macular edema (MME), a maculopathy that has been previously described in patients with demyelinating disease. To identify risk factors for MME and to expand the anatomic knowledge on MME. Design Retrospective case series. Participants We included 117 consecutive patients and 180 eyes with confirmed optic neuropathy of variable etiology. Patients with glaucoma were excluded. Methods We determined age, sex, visual acuity, etiology of optic neuropathy, and the temporal and spatial characteristics of MME. Eyes with MME were compared with eyes with optic neuropathy alone and to healthy fellow eyes. With retinal layer segmentation we quantitatively measured the intraretinal anatomy. Main Outcome Measures Demographic data, distribution of MME in the retina, and thickness of retinal layers were analyzed. Results We found MME in 16 eyes (8.8%) from 9 patients, none of whom had multiple sclerosis or neuromyelitis optica. The MME was restricted to the inner nuclear layer (INL) and had a characteristic perifoveal circular distribution. Compared with healthy controls, MME was associated with significant thinning of the ganglion cell layer and nerve fiber layer, as well as a thickening of the INL and the deeper retinal layers. Youth is a significant risk factor for MME. Conclusions Microcystic macular edema is not specific for demyelinating disease. It is a sign of optic neuropathy irrespective of its etiology. The distinctive intraretinal anatomy suggests that MME is caused by retrograde degeneration of the inner retinal layers, resulting in impaired fluid resorption in the macula.
机译:目的研究逆行轴突变性可能引起微囊性黄斑水肿(MME),黄斑病是一种先前已在脱髓鞘疾病患者中描述的黄斑病。识别MME的危险因素并扩展MME的解剖学知识。设计回顾案系列。参与者我们纳入了117例连续病患和180眼病因已证实的视神经病变。青光眼患者被排除在外。方法我们确定年龄,性别,视敏度,视神经病变的病因以及MME的时空特征。将患有MME的眼睛与仅患有视神经病变的眼睛以及健康的同龄人的眼睛进行了比较。使用视网膜层分割,我们定量测量了视网膜内解剖结构。主要结果指标分析了人口统计数据,MME在视网膜中的分布以及视网膜层的厚度。结果我们在9例患者的16眼(8.8%)中发现了MME,这些患者均没有多发性硬化症或视神经脊髓炎。 MME局限于核内层(INL),并具有特征性的小凹周围圆形分布。与健康对照组相比,MME与神经节细胞层和神经纤维层明显变薄以及INL和较深的视网膜层增厚有关。青年是MME的重要危险因素。结论微囊性黄斑水肿并非特异于脱髓鞘疾病。无论其病因如何,它都是视神经病变的标志。独特的视网膜内解剖结构表明MME是由视网膜内层的逆行变性引起的,从而导致黄斑中液体吸收受损。

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