Hypersynchronization in mild cognitive impairment: the 'X' model.

Sandra Pusil, M. E. López, P. Cuesta, R. Bruña, E. Pereda, F. Maestú
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引用次数: 54

Abstract

Hypersynchronization has been proposed as a synaptic dysfunction biomarker in the Alzheimer's disease continuum, reflecting the alteration of the excitation/inhibition balance. While animal models have verified this idea extensively, there is still no clear evidence in humans. Here we test this hypothesis, evaluating the risk of conversion from mild cognitive impairment (MCI) to Alzheimer's disease in a longitudinal study. We compared the functional resting state eyes-closed magnetoencephalographic networks of 54 patients with MCI who were followed-up every 6 months. According to their clinical outcome, they were split into: (i) the 'progressive' MCI (n = 27) group; and (ii) the 'stable' MCI group (n = 27). They did not differ in gender or educational level. For all participants, two magnetoencephalographic recordings were acquired. Functional connectivity was evaluated using the phase locking value. To extract the functional connectivity network with significant changes between both magnetoencephalographic recordings, we evaluated the functional connectivity ratio, defined as functional connectivity post-/pre-condition, in a network-based statistical model with an ANCOVA test with age as covariate. Two significant networks were found in the theta and beta bands, involving fronto-temporal and fronto-occipital connections, and showing a diminished functional connectivity ratio in the progressive MCI group. These topologies were then evaluated at each condition showing that at baseline, patients with progressive MCI showed higher synchronization than patients with stable MCI, while in the post-condition this pattern was reversed. These results may be influenced by two main factors in the post-condition: the increased synchrony in the stable MCI patients and the network failure in the progressive MCI patients. These findings may be explained as an 'X' form model where the hypersynchrony predicts conversion, leading subsequently to a network breakdown in progressive MCI. Patients with stable MCI showed an opposite phenomenon, which could indicate that they were a step beyond in the Alzheimer's disease continuum. This model would be able to predict the risk for the conversion to dementia in MCI patients.
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轻度认知障碍的超同步:“X”模型。
超同步已被认为是阿尔茨海默病连续体中突触功能障碍的生物标志物,反映了兴奋/抑制平衡的改变。虽然动物模型已经广泛证实了这一观点,但在人类身上仍然没有明确的证据。在这里,我们检验了这一假设,在一项纵向研究中评估了从轻度认知障碍(MCI)转变为阿尔茨海默病的风险。我们比较了每6个月随访的54例轻度认知损伤患者的静息状态闭眼脑磁图网络。根据临床结果,他们被分为:(i)“进行性”轻度认知损伤组(n = 27);(ii)“稳定”MCI组(n = 27)。他们在性别和教育水平上没有差别。所有参与者均获得两次脑磁图记录。使用相位锁定值评估功能连通性。为了提取两种脑磁图记录之间显著变化的功能连接网络,我们在基于网络的统计模型中评估了功能连接比率,定义为功能连接后/前条件,并使用ANCOVA检验,以年龄为协变量。在theta和beta波段发现了两个重要的网络,涉及额颞叶和额枕叶连接,并且在进行性MCI组显示功能连接比率降低。然后在每种情况下对这些拓扑结构进行评估,显示在基线时,进行性MCI患者比稳定型MCI患者表现出更高的同步性,而在后一种情况下,这种模式被逆转。这些结果可能受到两个主要因素的影响:稳定型MCI患者的同步性增加和进展型MCI患者的网络失效。这些发现可以解释为“X”型模型,其中超同步预测转换,随后导致进行性MCI的网络崩溃。稳定型轻度认知障碍患者表现出相反的现象,这可能表明他们在阿尔茨海默病的连续体中超越了一步。该模型将能够预测MCI患者转化为痴呆的风险。
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