Neuropsychiatric symptoms: Risk factor or disease marker? A study of structural imaging biomarkers of Alzheimer's disease and incident cognitive decline

IF 3.5 2区 医学 Q1 NEUROIMAGING Human Brain Mapping Pub Date : 2024-09-10 DOI:10.1002/hbm.70016
Dylan X. Guan, Tanaeem Rehman, Santhosh Nathan, Romella Durrani, Olivier Potvin, Simon Duchesne, G. Bruce Pike, Eric E. Smith, Zahinoor Ismail
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Abstract

Neuropsychiatric symptoms (NPS) are risk factors for Alzheimer's disease (AD) but can also manifest secondary to AD pathology. Mild behavioral impairment (MBI) refers to later-life emergent and persistent NPS that may mark early-stage AD. To distinguish MBI from NPS that are transient or which represent psychiatric conditions (non-MBI NPS), we investigated the effect of applying MBI criteria on NPS associations with AD structural imaging biomarkers and incident cognitive decline. Data for participants (n = 1273) with normal cognition (NC) or mild cognitive impairment (MCI) in the National Alzheimer's Coordinating Center Uniform Data Set were analyzed. NPS status (MBI, non-MBI NPS) was derived from the Neuropsychiatric Inventory Questionnaire and psychiatric history. Normalized measures of bilateral hippocampal (HPC) and entorhinal cortex (EC) volume, and AD meta-region of interest (ROI) mean cortical thickness were acquired from T1-weighted magnetic resonance imaging scans. Multivariable linear and Cox regressions examined NPS associations with imaging biomarkers and incident cognitive decline, respectively. MBI was associated with lower volume and cortical thickness in all ROIs in both NC and MCI, except for EC volume in NC. Non-MBI NPS were only associated with lower HPC volume in NC. Although both of the NPS groups showed higher hazards for MCI/dementia than No NPS, MBI participants showed more rapid decline. Although both types of NPS were linked to HPC atrophy, only NPS that emerged and persisted in later-life, consistent with MBI criteria, were related to AD neurodegenerative patterns beyond the HPC. Moreover, MBI predicted faster progression to dementia than non-MBI NPS.

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神经精神症状:风险因素还是疾病标志物?阿尔茨海默病结构成像生物标志物与认知能力下降事件的研究
神经精神症状(NPS)是阿尔茨海默病(AD)的危险因素,但也可能继发于阿尔茨海默病的病理变化。轻度行为障碍(MBI)指的是晚年出现的和持续的 NPS,可能是早期 AD 的标志。为了将轻度行为障碍与瞬时性或代表精神疾病的非轻度行为障碍(非轻度行为障碍)区分开来,我们研究了轻度行为障碍标准的应用对非轻度行为障碍与 AD 结构成像生物标志物和认知能力下降事件之间关系的影响。我们对国家阿尔茨海默氏症协调中心统一数据集中认知正常(NC)或轻度认知障碍(MCI)的参与者(n = 1273)的数据进行了分析。NPS状态(MBI、非MBI NPS)由神经精神量表问卷和精神病史得出。双侧海马(HPC)和内侧皮质(EC)体积的归一化测量值以及AD感兴趣元区(ROI)平均皮质厚度均来自T1加权磁共振成像扫描。多变量线性回归和 Cox 回归分别检验了 NPS 与成像生物标志物和认知能力下降事件的关系。在NC和MCI中,MBI与所有ROI中较低的体积和皮质厚度有关,但NC中的EC体积除外。而非 MBI NPS 只与 NC 中较低的 HPC 体积有关。虽然两组非神经功能缺损患者患 MCI/痴呆症的危险性均高于无非神经功能缺损患者,但 MBI 参与者的衰退速度更快。虽然两种类型的NPS都与HPC萎缩有关,但只有在晚年出现并持续的NPS(符合MBI标准)才与HPC以外的AD神经退行性病变模式有关。此外,MBI 比非 MBI NPS 预测痴呆症的进展更快。
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来源期刊
Human Brain Mapping
Human Brain Mapping 医学-核医学
CiteScore
8.30
自引率
6.20%
发文量
401
审稿时长
3-6 weeks
期刊介绍: Human Brain Mapping publishes peer-reviewed basic, clinical, technical, and theoretical research in the interdisciplinary and rapidly expanding field of human brain mapping. The journal features research derived from non-invasive brain imaging modalities used to explore the spatial and temporal organization of the neural systems supporting human behavior. Imaging modalities of interest include positron emission tomography, event-related potentials, electro-and magnetoencephalography, magnetic resonance imaging, and single-photon emission tomography. Brain mapping research in both normal and clinical populations is encouraged. Article formats include Research Articles, Review Articles, Clinical Case Studies, and Technique, as well as Technological Developments, Theoretical Articles, and Synthetic Reviews. Technical advances, such as novel brain imaging methods, analyses for detecting or localizing neural activity, synergistic uses of multiple imaging modalities, and strategies for the design of behavioral paradigms and neural-systems modeling are of particular interest. The journal endorses the propagation of methodological standards and encourages database development in the field of human brain mapping.
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