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在阿尔茨海默病的TgF344-AD大鼠模型中,静息脑网络状态转换的早期方向性改变。

Early altered directionality of resting brain network state transitions in the TgF344-AD rat model of Alzheimer's disease.

作者信息

De Waegenaere Sam, van den Berg Monica, Keliris Georgios A, Adhikari Mohit H, Verhoye Marleen

机构信息

Department of Biomedical Sciences, Bio-Imaging Lab, University of Antwerp, Antwerp, Belgium.

μNEURO Research Centre of Excellence, University of Antwerp, Antwerp, Belgium.

出版信息

Front Hum Neurosci. 2024 Apr 5;18:1379923. doi: 10.3389/fnhum.2024.1379923. eCollection 2024.

Abstract

INTRODUCTION

Alzheimer's disease (AD) is a progressive neurodegenerative disease resulting in memory loss and cognitive decline. Synaptic dysfunction is an early hallmark of the disease whose effects on whole-brain functional architecture can be identified using resting-state functional MRI (rsfMRI). Insights into mechanisms of early, whole-brain network alterations can help our understanding of the functional impact of AD's pathophysiology.

METHODS

Here, we obtained rsfMRI data in the TgF344-AD rat model at the pre- and early-plaque stages. This model recapitulates the major pathological and behavioral hallmarks of AD. We used co-activation pattern (CAP) analysis to investigate if and how the dynamic organization of intrinsic brain functional networks states, undetectable by earlier methods, is altered at these early stages.

RESULTS

We identified and characterized six intrinsic brain states as CAPs, their spatial and temporal features, and the transitions between the different states. At the pre-plaque stage, the TgF344-AD rats showed reduced co-activation of hub regions in the CAPs corresponding to the default mode-like and lateral cortical network. Default mode-like network activity segregated into two distinct brain states, with one state characterized by high co-activation of the basal forebrain. This basal forebrain co-activation was reduced in TgF344-AD animals mainly at the pre-plaque stage. Brain state transition probabilities were altered at the pre-plaque stage between states involving the default mode-like network, lateral cortical network, and basal forebrain regions. Additionally, while the directionality preference in the network-state transitions observed in the wild-type animals at the pre-plaque stage had diminished at the early-plaque stage, TgF344-AD animals continued to show directionality preference at both stages.

DISCUSSION

Our study enhances the understanding of intrinsic brain state dynamics and how they are impacted at the early stages of AD, providing a nuanced characterization of the early, functional impact of the disease's neurodegenerative process.

摘要

引言

阿尔茨海默病(AD)是一种进行性神经退行性疾病,会导致记忆丧失和认知衰退。突触功能障碍是该疾病的早期标志,其对全脑功能结构的影响可通过静息态功能磁共振成像(rsfMRI)来识别。深入了解早期全脑网络改变的机制有助于我们理解AD病理生理学的功能影响。

方法

在此,我们在TgF344-AD大鼠模型的斑块前期和早期阶段获取了rsfMRI数据。该模型概括了AD的主要病理和行为特征。我们使用共激活模式(CAP)分析来研究内在脑功能网络状态的动态组织在这些早期阶段是否以及如何发生改变,而早期方法无法检测到这种改变。

结果

我们将六种内在脑状态识别并表征为CAPs,以及它们的空间和时间特征,以及不同状态之间的转换。在斑块前期,TgF344-AD大鼠在与默认模式样和外侧皮质网络相对应的CAPs中枢纽区域的共激活减少。默认模式样网络活动分离为两种不同的脑状态,其中一种状态的特征是基底前脑的高共激活。这种基底前脑共激活在TgF344-AD动物中主要在斑块前期减少。在涉及默认模式样网络、外侧皮质网络和基底前脑区域的状态之间,斑块前期的脑状态转换概率发生了改变。此外,虽然在斑块前期野生型动物中观察到的网络状态转换中的方向性偏好在斑块早期有所减弱,但TgF344-AD动物在两个阶段都继续表现出方向性偏好。

讨论

我们的研究增进了对内在脑状态动态变化以及它们在AD早期阶段如何受到影响的理解,为该疾病神经退行性过程的早期功能影响提供了细致入微的表征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c60/11026683/869ae91c6d65/fnhum-18-1379923-g0001.jpg

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