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当前对阿尔茨海默病中磁共振成像生物标志物与记忆的理解。

Current understanding of magnetic resonance imaging biomarkers and memory in Alzheimer's disease.

作者信息

Bayram Ece, Caldwell Jessica Z K, Banks Sarah J

机构信息

Department of Neurology, Cleveland Clinic Lou Ruvo Center for Brain Health, Las Vegas, NV, USA.

出版信息

Alzheimers Dement (N Y). 2018 Jun 14;4:395-413. doi: 10.1016/j.trci.2018.04.007. eCollection 2018.

Abstract

Alzheimer's disease (AD) is caused by a cascade of changes to brain integrity. Neuroimaging biomarkers are important in diagnosis and monitoring the effects of interventions. As memory impairments are among the first symptoms of AD, the relationship between imaging findings and memory deficits is important in biomarker research. The most established magnetic resonance imaging (MRI) finding is hippocampal atrophy, which is related to memory decline and currently used as a diagnostic criterion for AD. While the medial temporal lobes are impacted early by the spread of neurofibrillary tangles, other networks and regional changes can be found quite early in the progression. Atrophy in several frontal and parietal regions, cortical thinning, and white matter alterations correlate with memory deficits in early AD. Changes in activation and connectivity have been detected by functional MRI (fMRI). Task-based fMRI studies have revealed medial temporal lobe hypoactivation, parietal hyperactivation, and frontal hyperactivation in AD during memory tasks, and activation patterns of these regions are also altered in preclinical and prodromal AD. Resting state fMRI has revealed alterations in default mode network activity related to memory in early AD. These studies are limited in part due to the historic inclusion of patients who had suspected AD but likely did not have the disorder. Modern biomarkers allow for more diagnostic certainty, allowing better understanding of neuroimaging markers in true AD, even in the preclinical stage. Larger patient cohorts, comparison of candidate imaging biomarkers to more established biomarkers, and inclusion of more detailed neuropsychological batteries to assess multiple aspects of memory are needed to better understand the memory deficit in AD and help develop new biomarkers. This article reviews MRI findings related to episodic memory impairments in AD and introduces a new study with multimodal imaging and comprehensive neuropsychiatric evaluation to overcome current limitations.

摘要

阿尔茨海默病(AD)是由一系列影响大脑完整性的变化所引起的。神经影像生物标志物在AD的诊断以及监测干预效果方面具有重要意义。由于记忆障碍是AD最早出现的症状之一,因此在生物标志物研究中,影像结果与记忆缺陷之间的关系至关重要。最明确的磁共振成像(MRI)表现是海马萎缩,它与记忆衰退相关,目前已被用作AD的诊断标准。虽然内侧颞叶会较早受到神经原纤维缠结扩散的影响,但在疾病进展过程中,其他神经网络和区域变化也能在相当早期就被发现。早期AD患者的几个额叶和顶叶区域萎缩、皮质变薄以及白质改变都与记忆缺陷相关。功能磁共振成像(fMRI)已检测到激活和连接性的变化。基于任务的fMRI研究显示,AD患者在记忆任务期间内侧颞叶激活不足、顶叶激活过度以及额叶激活过度,而且在临床前和前驱期AD患者中,这些区域的激活模式也发生了改变。静息态fMRI显示,早期AD患者与记忆相关的默认模式网络活动存在改变。这些研究存在一定局限性,部分原因在于以往纳入了疑似患有AD但可能并非患有该疾病的患者。现代生物标志物能够提高诊断的确定性,有助于更好地了解真正AD患者(甚至在临床前阶段)的神经影像标志物。为了更好地理解AD患者的记忆缺陷并帮助开发新的生物标志物,需要更大规模的患者队列、将候选影像生物标志物与更成熟的生物标志物进行比较,以及纳入更详细的神经心理测试组合来评估记忆的多个方面。本文综述了与AD情景记忆障碍相关的MRI表现,并介绍了一项采用多模态成像和全面神经精神评估的新研究,以克服当前的局限性。

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