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Tau 种子扩增检测揭示了阿尔茨海默病脑中 tau 种与病理形式之间的关系。

Tau seed amplification assay reveals relationship between seeding and pathological forms of tau in Alzheimer's disease brain.

机构信息

AbbVie Deutschland GmbH & Co. KG, Neuroscience Research, Knollstrasse, 67061, Ludwigshafen, Germany.

Department of Neurology, Hannover Medical School, Hanover, Germany.

出版信息

Acta Neuropathol Commun. 2023 Nov 14;11(1):181. doi: 10.1186/s40478-023-01676-w.

Abstract

Tau seed amplification assays (SAAs) directly measure the seeding activity of tau and would therefore be ideal biomarkers for clinical trials targeting seeding-competent tau in Alzheimer's disease (AD). However, the precise relationship between tau seeding measured by SAA and the levels of pathological forms of tau in the AD brain remains unknown. We developed a new tau SAA based on full-length 0N3R tau with sensitivity in the low fg/ml range and used it to characterize 103 brain samples from three independent cohorts. Tau seeding clearly discriminated between AD and control brain samples. Interestingly, seeding was absent in Progressive Supranuclear Palsy (PSP) putamen, suggesting that our tau SAA did not amplify 4R tau aggregates from PSP brain. The specificity of our tau SAA for AD brain was further supported by analysis of matched hippocampus and cerebellum samples. While seeding was detected in hippocampus from Braak stages I-II, no seeding was present in AD cerebellum that is devoid of tau inclusions. Analysis of 40 middle frontal gyrus samples encompassing all Braak stages showed that tau SAA seeding activity gradually increased with Braak stage. This relationship between seeding activity and the presence of tau inclusions in AD brain was further supported by robust correlations between tau SAA results and the levels of phosphorylated tau212/214, phosphorylated tau181, aggregated tau, and sarkosyl-insoluble tau. Strikingly, we detected tau seeding in the middle frontal gyrus already at Braak stage II-III, suggesting that tau SAA can detect tau pathology earlier than conventional immunohistochemical staining. In conclusion, our data suggest a quantitative relationship between tau seeding activity and pathological forms of tau in the human brain and provides an important basis for further development of tau SAA for accessible human samples.

摘要

tau 种子扩增测定(SAA)直接测量 tau 的种子活性,因此是针对阿尔茨海默病(AD)中具有种子能力的 tau 的临床试验的理想生物标志物。然而,通过 SAA 测量的 tau 种子与 AD 大脑中病理形式的 tau 水平之间的确切关系尚不清楚。我们开发了一种基于全长 0N3R tau 的新型 tau SAA,其灵敏度在 fg/ml 低范围内,并使用它来表征来自三个独立队列的 103 个大脑样本。tau 种子明显区分了 AD 和对照大脑样本。有趣的是,在进行性核上性麻痹(PSP)壳核中不存在种子,这表明我们的 tau SAA 不会从 PSP 大脑中扩增 4R tau 聚集物。我们的 tau SAA 对 AD 大脑的特异性进一步通过匹配的海马体和小脑样本分析得到支持。虽然在 Braak 阶段 I-II 的海马体中检测到种子,但在没有 tau 包含物的 AD 小脑体中不存在种子。对包含所有 Braak 阶段的 40 个额中回样本的分析表明,tau SAA 种子活性随 Braak 阶段逐渐增加。AD 大脑中种子活性与 tau 包含物的存在之间的这种关系进一步得到 tau SAA 结果与磷酸化 tau212/214、磷酸化 tau181、聚集 tau 和 Sarkosyl 不溶性 tau 水平之间的强相关性的支持。引人注目的是,我们已经在 Braak 阶段 II-III 检测到额中回中的 tau 种子,这表明 tau SAA 可以比传统免疫组织化学染色更早地检测到 tau 病理学。总之,我们的数据表明 tau 种子活性与人类大脑中病理形式的 tau 之间存在定量关系,并为进一步开发用于可及人类样本的 tau SAA 提供了重要基础。

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