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基于体素的轻度阿尔茨海默病白质异常检测

Voxel-based detection of white matter abnormalities in mild Alzheimer disease.

作者信息

Xie S, Xiao J X, Gong G L, Zang Y F, Wang Y H, Wu H K, Jiang X X

机构信息

Radiology Department, Peking University First Hospital, 8 Xishiku St, Xicheng District, Beijing, 100034, China.

出版信息

Neurology. 2006 Jun 27;66(12):1845-9. doi: 10.1212/01.wnl.0000219625.77625.aa.

Abstract

OBJECTIVE

To detect white matter abnormalities in patients with mild Alzheimer disease (AD) by diffusion tensor imaging and to determine their topographic relationship with gray matter atrophy.

METHODS

Thirteen patients with mild AD and 16 normal age-matched volunteers underwent diffusion tensor imaging and three-dimensional spoiled gradient-recalled sequence scanning. Voxel-based morphometry was conducted to detect regions of gray matter atrophy in the AD group relative to the control group. Fractional anisotropy (FA) maps were processed using SPM2 to make voxel-wise comparison of anisotropy in whole brain between the two groups. The relationship between locations of abnormalities in the white and gray matter was examined.

RESULTS

Significant reductions in anisotropy were found in the white matter of both medial temporal lobes, bilateral temporal stems, bilateral superior longitudinal fasciculi, bilateral internal capsules, and cerebral peduncles, as well as the white matter of left middle temporal gyrus and right superior parietal lobule, the body and genu of the corpus callosum, and the right lateral capsule in patients with AD. Although the decrease in FA was consistent with cortical volumetric reduction in both temporal lobes, the widespread involvement of bilateral superior longitudinal fasciculi was dominant in these white matter findings.

CONCLUSIONS

Voxel-wise comparison of whole-brain anisotropy revealed widely distributed disintegration of white matter in mild Alzheimer disease (AD). The white matter shows a different pattern of degeneration from gray matter and may be an independent factor in the progress of AD.

摘要

目的

通过弥散张量成像检测轻度阿尔茨海默病(AD)患者的白质异常,并确定其与灰质萎缩的拓扑关系。

方法

13例轻度AD患者和16名年龄匹配的正常志愿者接受了弥散张量成像和三维扰相梯度回波序列扫描。采用基于体素的形态学测量方法检测AD组相对于对照组的灰质萎缩区域。使用SPM2处理分数各向异性(FA)图,以对两组全脑各向异性进行逐体素比较。研究白质和灰质异常位置之间的关系。

结果

AD患者双侧内侧颞叶、双侧颞叶茎、双侧上纵束、双侧内囊、大脑脚以及左侧颞中回、右侧顶上小叶、胼胝体膝部和体部、右侧外囊的白质各向异性显著降低。虽然FA的降低与双侧颞叶皮质体积减少一致,但双侧上纵束的广泛受累在这些白质表现中占主导地位。

结论

全脑各向异性的逐体素比较显示,轻度阿尔茨海默病(AD)患者白质存在广泛分布的破坏。白质呈现出与灰质不同的退化模式,可能是AD进展中的一个独立因素。

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