首页> 外文期刊>Journal of the Neurological Sciences: Official Bulletin of the World Federation of Neurology >Human brain atlas-based multimodal MRI analysis of volumetry, diffusimetry, relaxometry and lesion distribution in multiple sclerosis patients and healthy adult controls: Implications for understanding the pathogenesis of multiple sclerosis and consolidation of quantitative MRI results in MS
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Human brain atlas-based multimodal MRI analysis of volumetry, diffusimetry, relaxometry and lesion distribution in multiple sclerosis patients and healthy adult controls: Implications for understanding the pathogenesis of multiple sclerosis and consolidation of quantitative MRI results in MS

机译:基于人脑图谱的多模式MRI分析多发性硬化症患者和健康成人对照患者的容量,扩散测定,张弛度测定和病变分布:对于了解多发性硬化的发病机理和MS定量MRI结果巩固的意义

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摘要

Multiple sclerosis (MS) is the most common immune-mediated disabling neurological disease of the central nervous system. The pathogenesis of MS is not fully understood. Histopathology implicates both demyelination and axonal degeneration as the major contributors to the accumulation of disability. The application of several in vivo quantitative magnetic resonance imaging (MRI) methods to both lesioned and normal-appearing brain tissue has not yet provided a solid conclusive support of the hypothesis that MS might be a diffuse disease. In this work, we adopted FreeSurfer to provide standardized macrostructure or volumetry of lesion free normal-appearing brain tissue in combination with multiple quantitative MRI metrics (T 2 relaxation time, diffusion tensor anisotropy and diffusivities) that characterize tissue microstructural integrity. By incorporating a large number of healthy controls, we have attempted to separate the natural age-related change from the disease-induced effects. Our work shows elevation in diffusivity and relaxation times and reduction in volume in a number of normal-appearing white matter and gray matter structures in relapsing-remitting multiple sclerosis patients. These changes were related in part with the spatial distribution of lesions. The whole brain lesion load and age-adjusted expanded disability status score showed strongest correlations in regions such as corpus callosum with qMRI metrics that are believed to be specific markers of axonal dysfunction, consistent with histologic data of others indicating axonal loss that is independent of focal lesions. Our results support that MS at least in part has a neurodegenerative component.
机译:多发性硬化症(MS)是中枢神经系统最常见的免疫介导的致残性神经疾病。 MS的发病机理尚未完全了解。组织病理学表明脱髓鞘和轴突变性是导致残疾累积的主要因素。几种体内定量磁共振成像(MRI)方法在病变和正常出现的脑组织中的应用尚未为MS可能是弥漫性疾病的假说提供坚实的结论性支持。在这项工作中,我们采用FreeSurfer结合了表征组织微结构完整性的多个定量MRI指标(T 2弛豫时间,弥散张量各向异性和弥散性),提供了无损伤,正常出现的正常脑组织的标准化宏观结构或容积。通过纳入大量健康对照,我们试图将与年龄相关的自然变化与疾病引起的影响区分开。我们的工作表明,在复发缓解型多发性硬化症患者中,许多正常出现的白质和灰质结构的扩散和舒张时间升高,体积减小。这些变化部分与病变的空间分布有关。全脑病变负荷和年龄调整后的扩展残疾状态评分在诸如体与qMRI指标等区域显示出最强的相关性,qMRI指标被认为是轴突功能障碍的特定标志物,与其他组织学数据一致,表明轴突损失与局灶性无关病变。我们的结果支持MS至少部分具有神经退行性成分。

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