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Grey matter atrophy of basal forebrain and hippocampus in mild cognitive impairment.

机译:轻度认知障碍中基底前脑和海马的灰质萎缩。

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The basal forebrain area (BFA) is closely connected to the hippocampus by virtue of cholinergic neuronal projections. Structural neuroimaging studies have shown reduced volumes of both structures in Alzheimer's disease and its prodromal stage mild cognitive impairment (MCI), but generally not in the same investigation. By combining voxel based morphometry and region of interest methods, we measured the grey matter (GM) volumes of the two brain regions with the goal of elucidating their contributions to MCI and its two subtypes (amnestic MCI and non-amnestic MCI) in an elderly epidemiological sample. The results replicated previous findings that the atrophies of both brain regions were associated with an increased likelihood of MCI and its two subtypes. However, in a regression model for the prediction of MCI with GM volumes for both regions used as predictors, only hippocampal atrophy remained significant. Two possible interpretations for this pattern of results were discussed. One is that the observed correlation between BFA atrophy and MCI is spurious and due to the hippocampal atrophy correlated with both. Alternatively, our observation is consistent with the possibility that BFA atrophy has a causal effect on MCI, which is mediated via its influence on hippocampal atrophy. Furthermore, we found that the left hippocampal atrophy had a stronger effect than the right hippocampus and bilateral BFA in the prediction of amnestic MCI occurrence when the four unilateral areas were entered into one regression model. In addition, a slight but statistically significant difference was found in the left hippocampal volume between APOE epsilon4 allele carriers and non-carriers, consistent with prior studies.
机译:基底前脑区(BFA)通过胆碱能神经元投射与海马紧密相连。结构性神经影像学研究显示,阿尔茨海默氏病及其前驱阶段轻度认知障碍(MCI)两种结构的体积均减少,但通常不在同一研究中。通过结合基于体素的形态学和感兴趣区域方法,我们测量了两个大脑区域的灰质(GM)体积,目的是阐明它们对老年人的MCI及其两个亚型(记忆删除MCI和非记忆删除MCI)的贡献流行病学样本。结果重复了先前的发现,即两个大脑区域的萎缩与MCI及其两个亚型的可能性增加有关。但是,在用于预测MCI的回归模型中,两个区域的GM量均用作预测因子,仅海马萎缩仍然很明显。讨论了这种结果模式的两种可能的解释。一种是观察到的BFA萎缩与MCI之间的相关性是虚假的,并且是由于海马萎缩与这两者相关。另外,我们的观察结果与BFA萎缩对MCI有因果关系的可能性是一致的,这是通过其对海马萎缩的影响而介导的。此外,我们发现,当四个单侧区域进入一种回归模型时,在预测记忆MCI发生方面,左海马萎缩的作用比右海马和双侧BFA的作用强。此外,在APOE epsilon4等位基因携带者和非携带者之间,左侧海马体积发现了轻微但有统计学意义的差异,这与先前的研究一致。

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