Department of Neurology with Institute of Translational Neurology, Münster University Hospital, Münster, Germany.
Movement Disorders, Imaging and Neurostimulation, Biomedical Statistics and Multimodal Signal Processing Unit, Department of Neurology, University Medical Center of the Johannes Gutenberg University, Mainz, Germany.
J Neuroinflammation. 2020 Jun 12;17(1):186. doi: 10.1186/s12974-020-01827-z.
Multiple sclerosis (MS) is an autoimmune disease of the central nervous system (CNS), characterized by inflammatory and neurodegenerative processes. Despite demyelination being a hallmark of the disease, how it relates to neurodegeneration has still not been completely unraveled, and research is still ongoing into how these processes can be tracked non-invasively. Magnetic resonance imaging (MRI) derived brain network characteristics, which closely mirror disease processes and relate to functional impairment, recently became important variables for characterizing immune-mediated neurodegeneration; however, their histopathological basis remains unclear.
In order to determine the MRI-derived correlates of myelin dynamics and to test if brain network characteristics derived from diffusion tensor imaging reflect microstructural tissue reorganization, we took advantage of the cuprizone model of general demyelination in mice and performed longitudinal histological and imaging analyses with behavioral tests. By introducing cuprizone into the diet, we induced targeted and consistent demyelination of oligodendrocytes, over a period of 5 weeks. Subsequent myelin synthesis was enabled by reintroduction of normal food.
Using specific immune-histological markers, we demonstrated that 2 weeks of cuprizone diet induced a 52% reduction of myelin content in the corpus callosum (CC) and a 35% reduction in the neocortex. An extended cuprizone diet increased myelin loss in the CC, while remyelination commenced in the neocortex. These histologically determined dynamics were reflected by MRI measurements from diffusion tensor imaging. Demyelination was associated with decreased fractional anisotropy (FA) values and increased modularity and clustering at the network level. MRI-derived modularization of the brain network and FA reduction in key anatomical regions, including the hippocampus, thalamus, and analyzed cortical areas, were closely related to impaired memory function and anxiety-like behavior.
Network-specific remyelination, shown by histology and MRI metrics, determined amelioration of functional performance and neuropsychiatric symptoms. Taken together, we illustrate the histological basis for the MRI-driven network responses to demyelination, where increased modularity leads to evolving damage and abnormal behavior in MS. Quantitative information about in vivo myelination processes is mirrored by diffusion-based imaging of microstructural integrity and network characteristics.
多发性硬化症(MS)是一种中枢神经系统(CNS)自身免疫性疾病,其特征为炎症和神经退行性过程。尽管脱髓鞘是该疾病的标志之一,但它与神经退行性变的关系尚未完全阐明,并且仍在研究如何通过非侵入性方法跟踪这些过程。磁共振成像(MRI)衍生的脑网络特征与疾病过程密切相关,并与功能障碍相关,最近已成为描述免疫介导的神经退行性变的重要变量;然而,其组织病理学基础仍不清楚。
为了确定 MRI 衍生的髓鞘动力学相关性,并测试从弥散张量成像中得出的脑网络特征是否反映微观结构组织重组,我们利用杯状朊病毒模型中的普遍脱髓鞘在小鼠中进行了纵向组织学和成像分析,并结合行为测试。通过在饮食中引入杯状朊病毒,我们在 5 周的时间内诱导了少突胶质细胞的靶向和一致脱髓鞘。随后通过引入正常食物来促进髓鞘合成。
使用特定的免疫组织化学标记,我们证明了 2 周的杯状朊病毒饮食会导致胼胝体(CC)的髓鞘含量减少 52%,新皮层减少 35%。延长的杯状朊病毒饮食会增加 CC 中的髓鞘丢失,而新皮层中的髓鞘再生开始。这些通过扩散张量成像的 MRI 测量反映的组织学确定的动态变化。脱髓鞘与分数各向异性(FA)值降低以及网络水平的模块性和聚类增加有关。大脑网络的 MRI 衍生模块化和关键解剖区域(包括海马体、丘脑和分析皮质区域)的 FA 降低与记忆功能受损和焦虑样行为密切相关。
通过组织学和 MRI 指标显示的网络特异性再髓鞘,决定了功能表现和神经精神症状的改善。综上所述,我们展示了 MRI 驱动的网络对脱髓鞘反应的组织学基础,其中模块性增加导致 MS 中不断发展的损伤和异常行为。体内髓鞘形成过程的定量信息通过基于弥散的微观结构完整性和网络特征的成像来反映。
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