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解析肌萎缩侧索硬化症中 MRI 信号改变的病理生物学机制:超高场 MRI 和定量神经病理学整合的全脑取样策略。

Dissecting the pathobiology of altered MRI signal in amyotrophic lateral sclerosis: A post mortem whole brain sampling strategy for the integration of ultra-high-field MRI and quantitative neuropathology.

机构信息

Nuffield Department of Clinical Neurosciences, University of Oxford, Oxford, UK.

Wellcome Centre for Integrative Neuroimaging, FMRIB, Nuffield Department of Clinical Neurosciences, University of Oxford, Oxford, UK.

出版信息

BMC Neurosci. 2018 Mar 13;19(1):11. doi: 10.1186/s12868-018-0416-1.

Abstract

BACKGROUND

Amyotrophic lateral sclerosis (ALS) is a clinically and histopathologically heterogeneous neurodegenerative disorder, in which therapy is hindered by the rapid progression of disease and lack of biomarkers. Magnetic resonance imaging (MRI) has demonstrated its potential for detecting the pathological signature and tracking disease progression in ALS. However, the microstructural and molecular pathological substrate is poorly understood and generally defined histologically. One route to understanding and validating the pathophysiological correlates of MRI signal changes in ALS is to directly compare MRI to histology in post mortem human brains.

RESULTS

The article delineates a universal whole brain sampling strategy of pathologically relevant grey matter (cortical and subcortical) and white matter tracts of interest suitable for histological evaluation and direct correlation with MRI. A standardised systematic sampling strategy that was compatible with co-registration of images across modalities was established for regions representing phosphorylated 43-kDa TAR DNA-binding protein (pTDP-43) patterns that were topographically recognisable with defined neuroanatomical landmarks. Moreover, tractography-guided sampling facilitated accurate delineation of white matter tracts of interest. A digital photography pipeline at various stages of sampling and histological processing was established to account for structural deformations that might impact alignment and registration of histological images to MRI volumes. Combined with quantitative digital histology image analysis, the proposed sampling strategy is suitable for routine implementation in a high-throughput manner for acquisition of large-scale histology datasets. Proof of concept was determined in the spinal cord of an ALS patient where multiple MRI modalities (T1, T2, FA and MD) demonstrated sensitivity to axonal degeneration and associated heightened inflammatory changes in the lateral corticospinal tract. Furthermore, qualitative comparison of R2* and susceptibility maps in the motor cortex of 2 ALS patients demonstrated varying degrees of hyperintense signal changes compared to a control. Upon histological evaluation of the same region, intensity of signal changes in both modalities appeared to correspond primarily to the degree of microglial activation.

CONCLUSION

The proposed post mortem whole brain sampling methodology enables the accurate intraindividual study of pathological propagation and comparison with quantitative MRI data, to more fully understand the relationship of imaging signal changes with underlying pathophysiology in ALS.

摘要

背景

肌萎缩侧索硬化症(ALS)是一种临床和组织病理学上表现出异质性的神经退行性疾病,其治疗受到疾病快速进展和缺乏生物标志物的阻碍。磁共振成像(MRI)已显示出其在检测 ALS 中的病理特征和跟踪疾病进展方面的潜力。然而,其微观结构和分子病理学基础仍知之甚少,通常通过组织学进行定义。理解和验证 ALS 中 MRI 信号变化的病理生理学相关性的一种方法是直接将 MRI 与死后人脑的组织学进行比较。

结果

本文描述了一种普遍适用于病理性相关灰质(皮质和皮质下)和白质感兴趣区域的全脑采样策略,适用于组织学评估和与 MRI 的直接相关性。建立了一种标准化的系统采样策略,该策略与跨模态图像配准兼容,适用于具有明确神经解剖学标志的磷酸化 43kDa TAR DNA 结合蛋白(pTDP-43)模式的区域。此外,基于轨迹的采样有助于准确描绘感兴趣的白质束。建立了一个数字摄影工作流程,涵盖了采样和组织学处理的各个阶段,以解决可能影响组织学图像与 MRI 体积配准和对齐的结构变形问题。结合定量数字组织学图像分析,该采样策略适用于以高通量方式常规实施,以获取大规模的组织学数据集。在一名 ALS 患者的脊髓中进行了概念验证,其中多种 MRI 模态(T1、T2、FA 和 MD)均显示出对轴突变性的敏感性,以及对侧皮质脊髓束中升高的炎症变化的敏感性。此外,对 2 名 ALS 患者的运动皮层中的 R2*和磁化率图进行定性比较表明,与对照相比,信号变化的程度存在不同程度的高亮。对同一区域进行组织学评估后,两种模态的信号变化强度似乎主要与小胶质细胞激活程度相对应。

结论

所提出的死后全脑采样方法能够实现对病理性传播的个体化研究,并与定量 MRI 数据进行比较,以更全面地理解 ALS 中成像信号变化与潜在病理生理学之间的关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1505/5848544/d1f40794664d/12868_2018_416_Fig1_HTML.jpg

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