A Systematic Review of the Association between Amyloid-β and τ Pathology with Functional Connectivity Alterations in the Alzheimer Dementia Spectrum Utilizing PET Scan and rsfMRI.
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引用次数: 8
Abstract
The association between functional connectivity (FC) alterations with amyloid-β (Aβ) and τ protein depositions in Alzheimer dementia is a subject of debate in the current literature. Although many studies have suggested a declining FC accompanying increased Aβ and τ concentrations, some investigations have contradicted this hypothesis. Therefore, this systematic review was conducted to sum up the current literature in this regard. The PROSPERO guideline for systematic reviews was applied for development of a research protocol, and this study was initiated after getting the protocol approval. Studies were screened, and those investigating FC measured by resting-state functional MRI and Aβ and τ protein depositions using amyloid and τ positron emission tomography were included. We categorized the included studies into 3 groups methodologically, addressing the question using global connectivity analysis (examining all regions of interest across the brain based on a functional atlas), seed-based connectivity analysis, or within-networks connectivity analysis. The quality of the studies was assessed using the Newcastle-Ottawa Scale. Among 31 included studies, 14 found both positive and negative correlations depending on the brain region and stage of the investigated disease, while 7 showed an overall negative correlation, 8 indicated an overall positive correlation, and 2 found a nonsignificant association between protein deposition and FC. The investigated regions were illustrated using tables. The posterior default mode network, one of the first regions of amyloid accumulation, and the temporal lobe, the early τ deposition region, are the 2 most investigated regions where inconsistencies exist. In conclusion, our study indicates that transneuronal spreading of τ and the amyloid hypothesis can justify higher FC related to higher protein depositions when global connectivity analysis is applied. However, the discrepancies observed when investigating the brain locally could be due to the varying manifestations of the amyloid and τ overload compensatory mechanisms in the brain at different stages of the disease with hyper- and hypoconnectivity cycles that can occur repeatedly. Nevertheless, further studies investigating both amyloid and τ deposition simultaneously while considering the stage of Alzheimer dementia are required to assess the accuracy of this hypothesis.
阿尔茨海默氏症中功能连接(FC)改变与淀粉样蛋白-β (a β)和τ蛋白沉积之间的关系是当前文献中争论的主题。尽管许多研究表明,随着a β和τ浓度的增加,FC下降,但一些研究反驳了这一假设。因此,本文对这方面的现有文献进行了系统的综述。应用PROSPERO系统评价指南制定研究方案,并在获得方案批准后启动本研究。筛选研究,包括通过静息状态功能MRI测量的FC和使用淀粉样蛋白和τ正电子发射断层扫描测量的Aβ和τ蛋白沉积的研究。我们将纳入的研究在方法上分为三组,使用全局连通性分析(基于功能图谱检查大脑中所有感兴趣的区域)、基于种子的连通性分析或网络内连通性分析来解决问题。研究的质量采用纽卡斯尔-渥太华量表进行评估。在纳入的31项研究中,14项研究发现与所研究疾病的脑区和阶段呈正相关和负相关,7项研究发现总体负相关,8项研究发现总体正相关,2项研究发现蛋白质沉积与FC之间无显著相关性。调查区域用表格表示。后默认模式网络是淀粉样蛋白最早积累的区域之一,而颞叶是早期τ沉积区域,这是两个研究最多的存在不一致性的区域。总之,我们的研究表明,当应用全局连通性分析时,τ的跨神经元扩散和淀粉样蛋白假说可以证明更高的FC与更高的蛋白质沉积相关。然而,在局部研究大脑时观察到的差异可能是由于在疾病的不同阶段大脑中淀粉样蛋白和τ过载代偿机制的不同表现,具有可重复发生的超连接和低连接周期。然而,需要进一步的研究同时调查淀粉样蛋白和τ沉积,同时考虑阿尔茨海默病的阶段,以评估这一假设的准确性。
期刊介绍:
This open access and online-only journal publishes original articles covering the entire spectrum of cognitive dysfunction such as Alzheimer’s and Parkinson’s disease, Huntington’s chorea and other neurodegenerative diseases. The journal draws from diverse related research disciplines such as psychogeriatrics, neuropsychology, clinical neurology, morphology, physiology, genetic molecular biology, pathology, biochemistry, immunology, pharmacology and pharmaceutics. Strong emphasis is placed on the publication of research findings from animal studies which are complemented by clinical and therapeutic experience to give an overall appreciation of the field. Dementia and Geriatric Cognitive Disorders Extra provides additional contents based on reviewed and accepted submissions to the main journal Dementia and Geriatric Cognitive Disorders Extra .