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多发性硬化症的眼部病变:不论疾病持续时间如何,均存在视网膜萎缩和炎症。

Ocular pathology in multiple sclerosis: retinal atrophy and inflammation irrespective of disease duration.

机构信息

Multiple Sclerosis Center, Department of Neurology, University of California San Francisco, San Francisco, CA 94143, USA.

出版信息

Brain. 2010 Jun;133(Pt 6):1591-601. doi: 10.1093/brain/awq080. Epub 2010 Apr 21.

Abstract

There has been growing interest in the use of retinal imaging for tracking disease progression in multiple sclerosis. However, systematic and detailed pathological descriptions of retinal tissue in multiple sclerosis are lacking. Graded, histological evaluations on eyes from 82 patients with multiple sclerosis and 10 subjects with other neurological diseases, with immunohistochemistry on a subset, were performed and correlated with clinical and pathological findings. Multiple sclerosis cases demonstrated evidence of retinal atrophy and inflammation even in late-stage disease. Retinal ganglion cell loss was significant and remaining neurons appeared shrunken and were partially engulfed by human leukocyte antigen-DR positive cells with the phenotype of microglia in samples subjected to immunohistochemistry. Neurofilament staining revealed variable but prominent degrees of axonal loss and injury. Neuronal loss was noted in the inner nuclear layer with focal reduction in cell density. Foamy-appearing human leukocyte antigen-DR positive cells were evident near vessels and periphlebitis was found in a small but significant number of multiple sclerosis cases. Glial fibrillary acidic protein staining showed extensive astrocyte hypertrophy and proliferation with prominent gliosis in multiple sclerosis cases. Frequent but previously unreported abnormalities in the iris were documented in the majority of chronic multiple sclerosis cases. The injury to both iris and retina could be seen at all stages of disease. Severity of retinal atrophy was correlated with overall brain weight at time of autopsy (P = 0.04) and a trend for increased atrophy was seen with longer disease duration (P = 0.13). This study provides the first large-scale pathological description of retinas in multiple sclerosis, including patients with different subtypes of disease at all stages, and with variable clinical severity. Changes were seen not only in the retinal nerve fibre layer and ganglion cell layer, but also in the inner nuclear layer, suggesting that retinal injury is more widespread than previously appreciated. Furthermore, the human retina is devoid of myelin, but inflammation was demonstrated to be prominent in multiple sclerosis and to persist in the retina at late stages of disease. The prominent gliosis and inflammation surrounding vessels of the inner retina could potentially impact optical coherence tomography evaluations in multiple sclerosis-as standard techniques exploit presumed differences in tissue reflectivity and utilize automated edge detection algorithms to judge axon loss in the nerve fibre layer. Deciphering the relationships between the different types of retinal pathology may aid us in understanding the factors that drive both inflammation and tissue atrophy in multiple sclerosis.

摘要

人们对使用视网膜成像来跟踪多发性硬化症的疾病进展越来越感兴趣。然而,多发性硬化症视网膜组织的系统和详细的病理学描述仍然缺乏。对 82 例多发性硬化症患者和 10 例其他神经疾病患者的眼部进行了分级、组织学评估,并对其中一部分进行了免疫组织化学检查,同时将其与临床和病理发现进行了相关性分析。多发性硬化症患者的视网膜甚至在晚期疾病中也显示出萎缩和炎症的证据。视网膜神经节细胞的损失是显著的,剩余的神经元出现萎缩,并被部分吞噬,在接受免疫组织化学检查的样本中,这些神经元被 HLA-DR 阳性细胞吞噬,其表型为小胶质细胞。神经丝染色显示轴突丢失和损伤程度不同,但很明显。在内核层中可见神经元丢失,细胞密度局灶性降低。在血管附近可见泡沫状 HLA-DR 阳性细胞,在一小部分多发性硬化症患者中发现了小但有意义的血管周围炎。胶质纤维酸性蛋白染色显示星形胶质细胞肥大和增生广泛,多发性硬化症病例中有明显的神经胶质增生。在大多数慢性多发性硬化症病例中,都记录到虹膜的频繁但以前未报道的异常。在疾病的所有阶段都可以看到虹膜和视网膜的损伤。视网膜萎缩的严重程度与尸检时的大脑总重量相关(P=0.04),并且随着疾病持续时间的延长,萎缩程度有增加的趋势(P=0.13)。这项研究首次对多发性硬化症的视网膜进行了大规模的病理学描述,包括不同疾病亚型的各个阶段的患者,以及不同的临床严重程度。不仅在视网膜神经纤维层和神经节细胞层,而且在内核层都观察到了变化,这表明视网膜损伤比以前认为的更为广泛。此外,人类视网膜不含髓磷脂,但在多发性硬化症中炎症明显,并在疾病的晚期持续存在。内层视网膜血管周围的明显神经胶质增生和炎症可能会影响多发性硬化症的光学相干断层扫描评估——标准技术利用组织反射率的假定差异,并利用自动边缘检测算法来判断神经纤维层中的轴突丢失。阐明不同类型的视网膜病理学之间的关系,可能有助于我们理解驱动多发性硬化症中炎症和组织萎缩的因素。

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