High‑Resolution T2 MRI Volumetry of Medial Temporal Lobe Subregions Predicts Cognitive Decline Across the Alzheimer's Disease Continuum.

IF 1.5 4区心理学 Q4 CLINICAL NEUROLOGY

Applied Neuropsychology-Adult Pub Date : 2025-08-21 DOI:10.1080/23279095.2025.2546951

Mehrdad Mozafar, Sahba Shahbazi, Mohammad Amir Amirian, Kosar Shekari, Neshat Sepahvand, Melika Esmaeili, AmirAbbas Amini, Shayan Shakeri, Hanieh Mirhosseini, Mahsa Mayeli

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Abstract

Atrophy of medial temporal lobe (MTL) subregions is an early biomarker of Alzheimer's disease (AD). This study aimed to examine the relationship between MTL subregion volumes and cognitive performance in patients across the AD continuum. We analyzed data from 276 participants using the Alzheimer's Disease Neuroimaging Initiative (ADNI), including 74 cognitively normal (CN), 110 subjective memory complaints (SMC), 37 early mild cognitive impairment (EMCI), 35 late mild cognitive impairment (LMCI), and 20 AD participants. MTL subregions volumes were measusing high-resolution T2-weighted MRI, and analyses were adjusted for age, education, APOE ε4 status, and intracranial volume (ICV). Significant atrophy in regions such as the cornu ammonis (CA), dentate gyrus (DG), subiculum (SUB), entorhinal cortex (ERC), and Brodmann area 35 (BA35) was found in AD participants compared with other groups. In AD, poorer Alzheimer's Disease Assessment Scale - Cognitive Subscale 13 (ADAS-13) performance was associated with reduced CA, DG, BA35, and parahippocampal cortex (PHC) volumes. In LMCI, lower Mini-Mental State Examination (MMSE) scores were associated with atrophy in CA and SUB. Diminished Montreal Cognitive Assessment (MoCA) scores were linked to reduced ERC volumes in CN, as well as with atrophy in BA35, ERC and CA subfields among AD patients. In LMCI, poorer Trail Making Test, Part B performance (i.e., longer completion time) was related to smaller Brodmann area 36 (BA36), collateral sulcus (CS), and PHC subregion volumes, whereas in the AD, it was related to BA36 only. Poorer immediate memory recall in AD was associated with atrophy in CA, DG, while in early stages of MCI, poorer verbal learning scores correlated with atrophy in the CA, DG, BA35, SUB, and CS regions. Moreover, diminished Logical Memory Delayed Recall was associated with atrophy in the CA, BA35, and PHC subfields among AD subjects. These findings support the value of atrophy in MTL subregions as potential imaging markers for detecting and monitoring cognitive decline across the AD continuum.

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内侧颞叶亚区高分辨率T2 MRI体积测量预测阿尔茨海默病连续体的认知能力下降。

内侧颞叶（MTL）亚区萎缩是阿尔茨海默病（AD）的早期生物标志物。本研究旨在检查跨AD患者MTL亚区容量与认知表现之间的关系。我们使用阿尔茨海默病神经影像学倡议（ADNI）分析了276名参与者的数据，包括74名认知正常（CN）， 110名主观记忆投诉（SMC）， 37名早期轻度认知障碍（EMCI）， 35名晚期轻度认知障碍（LMCI）和20名AD参与者。MTL亚区体积测量高分辨率t2加权MRI，并根据年龄、教育程度、APOE ε4状态和颅内容积（ICV）调整分析结果。与其他组相比，AD参与者的锥体（CA）、齿状回（DG）、耻骨下（SUB）、内嗅皮质（ERC）和Brodmann区35 （BA35）等区域明显萎缩。在AD患者中，较差的阿尔茨海默病评估量表-认知亚量表13 （ADAS-13）表现与CA、DG、BA35和海马旁皮质（PHC）体积减少有关。在LMCI中，较低的迷你精神状态检查（MMSE）评分与CA和SUB的萎缩有关。蒙特利尔认知评估（MoCA）评分降低与CN的ERC体积减少以及AD患者BA35、ERC和CA子区萎缩有关。在LMCI中，较差的Trail Making Test， B部分性能（即较长的完成时间）与较小的Brodmann area 36 (BA36)，侧支沟（CS）和PHC分区域体积有关，而在AD中，仅与BA36有关。AD患者较差的即时记忆回忆与CA、DG的萎缩有关，而在MCI的早期阶段，较差的言语学习得分与CA、DG、BA35、SUB和CS区域的萎缩有关。此外，在AD受试者中，逻辑记忆延迟回忆的减少与CA、BA35和PHC子区萎缩有关。这些发现支持MTL亚区萎缩作为检测和监测AD连续体认知能力下降的潜在成像标记的价值。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Applied Neuropsychology-Adult CLINICAL NEUROLOGY-PSYCHOLOGY

CiteScore

4.50

自引率

11.80%

发文量

134

期刊介绍： pplied Neuropsychology-Adult publishes clinical neuropsychological articles concerning assessment, brain functioning and neuroimaging, neuropsychological treatment, and rehabilitation in adults. Full-length articles and brief communications are included. Case studies of adult patients carefully assessing the nature, course, or treatment of clinical neuropsychological dysfunctions in the context of scientific literature, are suitable. Review manuscripts addressing critical issues are encouraged. Preference is given to papers of clinical relevance to others in the field. All submitted manuscripts are subject to initial appraisal by the Editor-in-Chief, and, if found suitable for further considerations are peer reviewed by independent, anonymous expert referees. All peer review is single-blind and submission is online via ScholarOne Manuscripts.