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阿尔茨海默病基于体素的灰质分析简史。

A brief history of voxel-based grey matter analysis in Alzheimer's disease.

机构信息

Herchel Smith Building for Brain and Mind Sciences, Department of Clinical Neurosciences, University of Cambridge School of Clinical Medicine, Cambridge, UK.

出版信息

J Alzheimers Dis. 2014;38(3):647-59. doi: 10.3233/JAD-130362.

DOI:10.3233/JAD-130362
PMID:24037033
Abstract

Voxel-based morphometry (VBM) and cortical thickness measurement are common techniques to identify regional atrophy in neurodegenerative diseases such as Alzheimer's disease (AD). Because studies employing these methods draw conclusions regarding patterns of regional cortical degeneration, it is important to be aware of their possible limitations. To evaluate the effect of different VBM versions, we performed voxel-based analyses through successive versions-from SPM99 to SPM8-as well as FSL-VBM on n = 20 AD patients and n = 20 controls. Reproducibility was assessed in an independent sample, again of n = 20 per group, from the Alzheimer's Disease Neuroimaging Initiative (ADNI) database. Further, we tested the hypothesis that VBM can sensitively detect hippocampal atrophy, but is relatively insensitive to changes in the cortical ribbon, by contrasting VBM with FreeSurfer cortical thickness measurements. The results with both datasets confirmed that VBM preferentially identifies grey matter lesions in the mesial temporal lobe but is largely insensitive to isocortical atrophy. In contrast, FreeSurfer identified thinning of cortical ribbon association cortex more significant in post- rather than pre-Rolandic areas and with relative preservation of primary sensory-motor regions-in other words precisely as would be expected in AD. The results highlight a bias that VBM has toward detecting mesial temporal lobe atrophy. This finding has important implications for interpretation of clinical and cognitive studies in AD.

摘要

体素形态计量学(VBM)和皮质厚度测量是识别神经退行性疾病(如阿尔茨海默病(AD))中区域性萎缩的常用技术。由于采用这些方法的研究得出了关于区域性皮质退化模式的结论,因此了解它们的可能局限性很重要。为了评估不同 VBM 版本的影响,我们通过连续的版本(从 SPM99 到 SPM8)以及 FSL-VBM 在 n = 20 名 AD 患者和 n = 20 名对照中进行了基于体素的分析。在来自 Alzheimer's Disease Neuroimaging Initiative (ADNI) 数据库的独立样本中(n = 20 名/组)再次评估了可重复性。此外,我们通过对比 VBM 与 FreeSurfer 皮质厚度测量来测试 VBM 能否敏感地检测出海马萎缩,但相对不能检测皮质带变化的假设。两个数据集的结果都证实,VBM 优先识别内侧颞叶的灰质病变,但对同型皮质萎缩基本不敏感。相比之下,FreeSurfer 识别出后 Rolandic 区而非前 Rolandic 区的皮质带联合皮质变薄更显著,且初级感觉运动区相对保留——换句话说,正是 AD 中所预期的情况。这些结果强调了 VBM 对检测内侧颞叶萎缩的偏向性。这一发现对 AD 中临床和认知研究的解释具有重要意义。

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