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高分辨率弥散张量成像在 Pelizaeus-Merzbacher 病小鼠模型固定脑组织中的应用:与白质病理的定量测量比较。

High-resolution diffusion tensor imaging of fixed brain in a mouse model of Pelizaeus-Merzbacher disease: comparison with quantitative measures of white matter pathology.

机构信息

Institute of Neuroscience and Psychology and Glasgow Experimental Magnetic Resonance Imaging Centre, College of Medical, Veterinary and Life Sciences, University of Glasgow, Glasgow, UK.

出版信息

NMR Biomed. 2011 Dec;24(10):1369-79. doi: 10.1002/nbm.1700. Epub 2011 Mar 24.

Abstract

Diffusion tensor imaging (DTI) is a powerful technique for the noninvasive assessment of the central nervous system. To facilitate the application of this technique to in vivo studies, we characterised a mouse model of the leukodystrophy, Pelizaeus-Merzbacher disease (PMD), comparing high-resolution ex vivo DTI findings with quantitative histological analysis of selected areas of the brain. The mice used in this study (Plp1-transgenic) carry transgenic copies of the Plp1 gene and are models for PMD as a result of gene duplication. Plp1 transgenic mice display a mild ataxia and experience frequent seizures around the time at which they were imaged. Axial (λ(1) ) and radial (RD) diffusivities and fractional anisotropy (FA) data were analysed using an exploratory whole-brain voxel-based method, a voxel-based approach using tract-based spatial statistics (TBSS), and by application of conventional region of interest (ROI) analyses to selected white matter tracts. Raw t value maps and TBSS analyses indicated widespread changes throughout the brain of Plp1-transgenic mice compared with the wild-type. ROI analyses of the corpus callosum, anterior commissure and hippocampal fimbria showed that FA was reduced significantly, whereas λ(1) and RD were increased significantly, in Plp1-transgenic mice compared with the wild-type. The DTI data derived from ROI analyses were subsequently compared with histological measures taken in the same regions. These revealed an almost complete absence of myelin, preservation of axons, marked astrocytosis and increased or unchanged cell densities. These data contribute to our growing understanding of the basis of anisotropic water diffusion in the normal and diseased nervous system.

摘要

弥散张量成像(DTI)是一种用于评估中枢神经系统的非侵入性技术。为了促进该技术在体内研究中的应用,我们对一种脑白质营养不良(Pelizaeus-Merzbacher 病,PMD)的小鼠模型进行了特征描述,将高分辨率离体 DTI 结果与脑内选定区域的定量组织学分析进行了比较。本研究中使用的小鼠(Plp1-转基因)携带 Plp1 基因的转基因拷贝,由于基因重复,成为 PMD 的模型。Plp1 转基因小鼠表现出轻微的共济失调,并在成像时经常发生癫痫发作。使用基于体素的全脑探索性方法、基于束的空间统计学(TBSS)的体素方法以及对选定的白质束进行常规感兴趣区域(ROI)分析,对轴向(λ(1))和径向(RD)扩散率和各向异性分数(FA)数据进行了分析。原始 t 值图和 TBSS 分析表明,与野生型相比,Plp1 转基因小鼠的大脑广泛发生了变化。胼胝体、前连合和海马伞 ROI 分析显示,与野生型相比,FA 显著降低,而 λ(1) 和 RD 显著增加。ROI 分析得出的 DTI 数据随后与同一区域的组织学测量值进行了比较。这些结果显示,几乎完全没有髓鞘,保留了轴突,星形胶质细胞明显增生,细胞密度增加或不变。这些数据有助于我们加深对正常和病态神经系统各向异性水扩散基础的理解。

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