Haas Anna-Lena, Olm Pauline, Utz Janine, Siegmann Eva-Maria, Spitzer Philipp, Florvaag Anna, Schmidt Manuel Alexander, Doerfler Arnd, Lewczuk Piotr, Kornhuber Johannes, Maler Juan Manuel, Oberstein Timo Jan
Department of Psychiatry and Psychotherapy, Friedrich-Alexander-Universität Erlangen-Nürnberg, Erlangen, Germany.
Institute of Neuroradiology, Friedrich-Alexander-Universität Erlangen-Nürnberg, Erlangen, Germany.
Front Aging Neurosci. 2023 Feb 22;15:1121500. doi: 10.3389/fnagi.2023.1121500. eCollection 2023.
Alzheimer's disease (AD) is indicated by a decrease in amyloid beta 42 (Aβ42) level or the Aβ42/Aβ40 ratio, and by increased levels of Tau with phosphorylated threonine at position 181 (pTau181) in cerebrospinal fluid (CSF) years before the onset of clinical symptoms. However, once only pTau181 is increased, cognitive decline in individuals with subjective or mild cognitive impairment is slowed compared to individuals with AD. Instead of a decrease in Aβ42 levels, an increase in Aβ42 was observed in these individuals, leading to the proposal to refer to them as nondemented subjects with increased pTau-levels and Aβ surge with subtle cognitive deterioration (PASSED). In this study, we determined the longitudinal atrophy rates of AD, PASSED, and Biomarker-negative nondemented individuals of two independent cohorts to determine whether these groups can be distinguished by their longitudinal atrophy patterns or rates.
Depending on their CSF-levels of pTau 181 (T), total Tau (tTau, N), Aβ42 or ratio of Aβ42/Aβ40 (A), 185 non-demented subjects from the Alzheimer's Disease Neuroimaging Initiative (ADNI) and 62 non-demented subjects from Erlangen AD cohort were assigned to an ATN group (A-T-N-, A-T+N±, A+T-N±and A+T+N±) and underwent T1-weighted structural magnetic resonance imaging (sMRI). Longitudinal grey matter (GM) atrophy patterns were assessed with voxel-based morphometry (VBM) using the cat12 toolbox on spm12 (statistical parametric mapping) of MRI scans from individuals in the ADNI cohort with a mean follow-up of 2 and 5 years, respectively. The annualized atrophy rate for individuals in the Erlangen cohort was determined using region of interest analysis (ROI) in terms of a confirmatory analysis.
In the A-T+N± group, VBM did not identify any brain region that showed greater longitudinal atrophy than the A+T+N±, A+T+N± or biomarker negative control group. In contrast, marked longitudinal atrophy in the temporal lobe was evident in the A+T-N± group compared with A+T-N± and biomarker-negative subjects. The ROI in the angular gyrus identified by VBM analysis of the ADNI cohort did not discriminate better than the hippocampal volume and atrophy rate between AD and PASSED in the confirmatory analysis.
In this study, nondemented subjects with PASSED did not show a unique longitudinal atrophy pattern in comparison to nondemented subjects with AD. The nonsignificant atrophy rate compared with controls suggests that increased pTau181-levels without concomitant amyloidopathy did not indicate a neurodegenerative disorder.
阿尔茨海默病(AD)在临床症状出现前数年,脑脊液(CSF)中β淀粉样蛋白42(Aβ42)水平或Aβ42/Aβ40比值降低,且苏氨酸181位点磷酸化的Tau(pTau181)水平升高。然而,一旦仅pTau181升高,与AD患者相比,主观认知障碍或轻度认知障碍个体的认知衰退会减缓。这些个体中未观察到Aβ42水平降低,反而出现Aβ42升高,因此有人提议将他们称为pTau水平升高且伴有轻微认知衰退的Aβ激增的非痴呆受试者(PASSED)。在本研究中,我们确定了两个独立队列中AD、PASSED和生物标志物阴性的非痴呆个体的纵向萎缩率,以确定这些组是否可以通过其纵向萎缩模式或速率来区分。
根据阿尔茨海默病神经影像学倡议(ADNI)的185名非痴呆受试者和埃尔朗根AD队列的62名非痴呆受试者的脑脊液pTau 181(T)、总Tau(tTau,N)、Aβ42或Aβ42/Aβ40比值(A)水平,将他们分配到一个ATN组(A-T-N-、A-T+N±、A+T-N±和A+T+N±),并接受T1加权结构磁共振成像(sMRI)。使用cat12工具箱在ADNI队列个体的MRI扫描的spm12(统计参数映射)上通过基于体素的形态计量学(VBM)评估纵向灰质(GM)萎缩模式,平均随访时间分别为2年和5年。通过感兴趣区域分析(ROI)确定埃尔朗根队列个体的年化萎缩率,作为验证性分析。
在A-T+N±组中,VBM未发现任何脑区的纵向萎缩比A+T+N±、A+T+N±或生物标志物阴性对照组更严重。相比之下,与A+T-N±和生物标志物阴性受试者相比,A+T-N±组颞叶明显存在明显的纵向萎缩。在验证性分析中,通过对ADNI队列的VBM分析确定的角回ROI在区分AD和PASSED方面并不比海马体积和萎缩率更好。
在本研究中,与AD非痴呆受试者相比,PASSED非痴呆受试者未表现出独特的纵向萎缩模式。与对照组相比无显著萎缩率表明,pTau181水平升高而无淀粉样病变并不表明存在神经退行性疾病。
