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Subcortical Shape Changes Hippocampal Atrophy and Cortical Thinning in Future Alzheimers Disease Patients

机译:未来阿尔茨海默氏病患者的皮质下形状变化海马萎缩和皮质变薄

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摘要

Efficacy of future treatments depends on biomarkers identifying patients with mild cognitive impairment at highest risk for transitioning to Alzheimer's disease. Here, we applied recently developed analysis techniques to investigate cross-sectional differences in subcortical shape and volume alterations in patients with stable mild cognitive impairment (MCI) (n = 23, age range 59–82, 47.8% female), future converters at baseline (n = 10, age range 66–84, 90% female) and at time of conversion (age range 68–87) compared to group-wise age and gender matched healthy control subjects (n = 23, age range 61–81, 47.8% female; n = 10, age range 66–82, 80% female; n = 10, age range 68–82, 70% female). Additionally, we studied cortical thinning and global and local measures of hippocampal atrophy as known key imaging markers for Alzheimer's disease. Apart from bilateral striatal volume reductions, no morphometric alterations were found in cognitively stable patients. In contrast, we identified shape alterations in striatal and thalamic regions in future converters at baseline and at time of conversion. These shape alterations were paralleled by Alzheimer's disease like patterns of left hemispheric morphometric changes (cortical thinning in medial temporal regions, hippocampal total and subfield atrophy) in future converters at baseline with progression to similar right hemispheric alterations at time of conversion. Additionally, receiver operating characteristic curve analysis indicated that subcortical shape alterations may outperform hippocampal volume in identifying future converters at baseline. These results further confirm the key role of early cortical thinning and hippocampal atrophy in the early detection of Alzheimer's disease. But first and foremost, and by distinguishing future converters but not patients with stable cognitive abilities from cognitively normal subjects, our results support the value of early subcortical shape alterations and reduced hippocampal subfield volumes as potential markers for the early detection of Alzheimer's disease.
机译:未来治疗的有效性取决于生物标记物,这些标记物可识别出轻度认知障碍患者中最有可能转变为阿尔茨海默氏病的风险。在这里,我们应用了最新开发的分析技术,以研究稳定的轻度认知障碍(MCI)(n = 23,年龄范围59-82,女性47.8%),基线时的未来转换者的皮质下形状和体积变化的横截面差异。 (n = 10,年龄在66-84岁,女性占90%),并且在转换时(年龄在68-87岁之间)与按年龄段和性别匹配的健康对照受试者(n = 23,年龄在61-81岁之间,女性47.8%; n = 10,年龄范围66-82,女性80%; n = 10,年龄范围68-82,70%女性)。此外,我们研究了皮质变薄以及海马萎缩的整体和局部测量,将其作为阿尔茨海默氏病的关键成像标志。除了双侧纹状体体积减少之外,在认知稳定的患者中未发现形态学改变。相反,我们在基线和转换时发现了未来转换器中纹状体和丘脑区域的形状变化。这些形状改变与阿尔茨海默氏病类似,例如在未来的转换器中,左半球形态变化的模式(内侧颞叶区域的皮质变薄,海马总区和亚视野萎缩),在转换时逐渐发展为类似的右半球改变。此外,接收机的工作特性曲线分析表明,在确定基线处的未来转换器时,皮层下的形状变化可能胜过海马体积。这些结果进一步证实了早期皮层变薄和海马萎缩在阿尔茨海默氏病的早期检测中的关键作用。但最重要的是,通过将未来的转换者与具有稳定的认知能力的患者与认知正常的受试者区分开,我们的结果支持早期皮层下形状改变和海马亚视野体积减小的价值,作为早期发现阿尔茨海默氏病的潜在标志。

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