Department of Neurology, University of Pennsylvania, Philadelphia, Pennsylvania, USA.
Department of Radiology, University of Pennsylvania, Philadelphia, Pennsylvania, USA.
Ann Clin Transl Neurol. 2024 Mar;11(3):673-685. doi: 10.1002/acn3.51988. Epub 2024 Jan 23.
Alzheimer's disease neuropathologic change and alpha-synucleinopathy commonly co-exist and contribute to the clinical heterogeneity of dementia. Here, we examined tau epitopes marking various stages of tangle maturation to test the hypotheses that tau maturation is more strongly associated with beta-amyloid compared to alpha-synuclein, and within the context of mixed pathology, mature tau is linked to Alzheimer's disease clinical phenotype and negatively associated with Lewy body dementia.
We used digital histology to measure percent area-occupied by pathology in cortical regions among individuals with pure Alzheimer's disease neuropathologic change, pure alpha-synucleinopathy, and a co-pathology group with both Alzheimer's and alpha-synuclein pathologic diagnoses. Multiple tau monoclonal antibodies were used to detect early (AT8, MC1) and mature (TauC3) epitopes of tangle progression. We used linear/logistic regression to compare groups and test the association between pathologies and clinical features.
There were lower levels of tau pathology (β = 1.86-2.96, p < 0.001) across all tau antibodies in the co-pathology group compared to the pure Alzheimer's pathology group. Among individuals with alpha-synucleinopathy, higher alpha-synuclein was associated with greater early tau (AT8 β = 1.37, p < 0.001; MC1 β = 1.2, p < 0.001) but not mature tau (TauC3 p = 0.18), whereas mature tau was associated with beta-amyloid (β = 0.21, p = 0.01). Finally, lower tau, particularly TauC3 pathology, was associated with lower frequency of both core clinical features and categorical clinical diagnosis of dementia with Lewy bodies.
Mature tau may be more closely related to beta-amyloidosis than alpha-synucleinopathy, and pathophysiological processes of tangle maturation may influence the clinical features of dementia in mixed Lewy-Alzheimer's pathology.
阿尔茨海默病神经病理改变和α-突触核蛋白病通常共存,并导致痴呆的临床异质性。在这里,我们检查了标记神经原纤维缠结成熟各个阶段的tau 表位,以检验以下假设:与α-突触核蛋白相比,tau 成熟与β-淀粉样蛋白的相关性更强,并且在混合病理学的情况下,成熟的 tau 与阿尔茨海默病的临床表型相关,与路易体痴呆呈负相关。
我们使用数字组织学测量皮质区域中单纯阿尔茨海默病神经病理改变、单纯α-突触核蛋白病以及具有阿尔茨海默病和α-突触核蛋白病理诊断的共病组个体的病理区域百分比。使用多种 tau 单克隆抗体检测神经原纤维缠结进展的早期(AT8、MC1)和成熟(TauC3)表位。我们使用线性/逻辑回归比较组,并检验病理与临床特征之间的关联。
与单纯阿尔茨海默病病理学组相比,共病组中所有 tau 抗体的 tau 病理学水平较低(β=1.86-2.96,p<0.001)。在有α-突触核蛋白病的个体中,较高的α-突触核蛋白与较高的早期 tau(AT8 β=1.37,p<0.001;MC1 β=1.2,p<0.001)但不是成熟 tau(TauC3 p=0.18)相关,而成熟 tau 与β-淀粉样蛋白相关(β=0.21,p=0.01)。最后,较低的 tau,特别是 TauC3 病理学与 Lewy 体相关痴呆的核心临床特征和分类临床诊断的频率较低有关。
成熟的 tau 可能与β-淀粉样蛋白病的关系比α-突触核蛋白病更密切,并且神经原纤维缠结成熟的病理生理过程可能影响混合 Lewy-阿尔茨海默病病理学中的痴呆临床特征。
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