Substantial subpial cortical demyelination in progressive multiple sclerosis: have we underestimated the extent of cortical pathology?

Lauren Griffiths, R. Reynolds, Rhian Evans, Ryan J. Bevan, M. Rees, D. Gveric, J. Neal, O. Howell
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引用次数: 12

Abstract

Aim: Multiple sclerosis (MS) is an inflammatory demyelinating and neurodegenerative disease. Much of the complex symptomatology relates to pathology outside the classic white matter plaque, whereby lesions of the cortical grey matter, which are difficult to resolve by conventional clinical imaging, are in part predictive of outcome. We investigated the extent of grey matter pathology in whole coronal macrosections to reassess the contribution of cortical pathology to total demyelinating lesion area in progressive MS. Methods: Twenty-two cases of progressive MS were prepared as whole bi-hemispheric macrosections for histology, immunostaining and quantitative analysis of lesion number and relative area, leptomeningeal inflammation and microglial/macrophage activation. Results: Cortical grey matter demyelination was seen in all cases, which was more extensive than in white and deep grey matter (hippocampus, thalamus and basal ganglia) and accounted for 0.8%-60.2% of the entire measurable cortical ribbon. The pattern of cortical grey matter demyelination was predominantly subpial (mean 90.9%, range 60%-100%, of total cortical grey matter lesion area) and cases with the largest areas of subpial cortical lesions had more and larger deep grey matter lesions, greater numbers of activated microglia/macrophages, both in lesions as well as in normal cortical grey matter, together with elevated leptomeningeal inflammation and lymphoid-like structures. White matter lesion area was unchanged when compared with the progressive MS cases with little subpial cortical demyelination. Conclusion: Analysis of whole coronal macrosections reveals cortical demyelination is more extensive than reported by conventional histological methods. Cases of progressive MS with substantial subpial cortical demyelination that is independent of underlying white matter lesion area support the implications that these lesions may in-part arise through different pathogenetic mechanisms. Biomarkers and/or imaging correlates of this subpial pathology are required if we are to fully comprehend the clinical disease process.
进展性多发性硬化症的实质枕下皮质脱髓鞘:我们是否低估了皮质病理的程度?
目的:多发性硬化症(MS)是一种炎性脱髓鞘和神经退行性疾病。许多复杂的症状与典型白质斑块以外的病理有关,因此,常规临床成像难以解决的皮质灰质病变在一定程度上预测了结果。方法:将22例进展性多发性硬化症患者制作成双半球完整大切片,进行组织学、免疫染色、病变数量和相对面积、小脑膜炎症和小胶质/巨噬细胞活化的定量分析。结果:所有病例均可见皮质灰质脱髓鞘,其脱髓鞘范围较白质和深部灰质(海马、丘脑和基底节区)更为广泛,占整个可测皮质带的0.8% ~ 60.2%。皮层灰质脱髓鞘的模式主要是在枕下(平均90.9%,范围60%-100%,占皮质灰质总病变面积),枕下皮质病变面积最大的病例有更多更大的深部灰质病变,激活的小胶质细胞/巨噬细胞数量更多,病变和正常皮质灰质中都有,并伴有轻脑膜炎症和淋巴样结构升高。与进展性MS患者相比,白质病变面积没有变化,并伴有少量的枕下皮质脱髓鞘。结论:整个冠状动脉宏观切片分析显示皮质脱髓鞘比常规组织学方法报道的更广泛。进展性多发性硬化症伴枕下皮质脱髓鞘的病例与潜在的白质病变区域无关,这表明这些病变可能部分是由不同的发病机制引起的。如果我们要充分了解临床疾病过程,就需要这种基底下病理的生物标志物和/或影像学相关指标。
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