Phosphorylated tau in Alzheimer's disease.

Advances in clinical chemistry Pub Date : 2023-01-01 Epub Date: 2023-06-09 DOI:10.1016/bs.acc.2023.05.001
Julia Telser, Kirsten Grossmann, Niklas Wohlwend, Lorenz Risch, Christoph H Saely, Philipp Werner
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Abstract

There is a need for blood biomarkers to detect individuals at different Alzheimer's disease (AD) stages because obtaining cerebrospinal fluid-based biomarkers is invasive and costly. Plasma phosphorylated tau proteins (p-tau) have shown potential as such biomarkers. This systematic review was conducted according to the PRISMA guidelines and aimed to determine whether quantification of plasma tau phosphorylated at threonine 181 (p-tau181), threonine 217 (p-tau217) and threonine 231 (p-tau231) is informative in the diagnosis of AD. All p-tau isoforms increase as a function of Aβ-accumulation and discriminate healthy individuals from those at preclinical AD stages with high accuracy. P-tau231 increases earliest, followed by p-tau181 and p-tau217. In advanced stages, all p-tau isoforms are associated with the clinical classification of AD and increase with disease severity, with the greatest increase seen for p-tau217. This is also reflected by a better correlation of p-tau217 with Aβ scans, whereas both, p-tau217 and p-tau181 correlated equally with tau scans. However, at the very advanced stages, p-tau181 begins to plateau, which may mirror the trajectory of the Aβ pathology and indicate an association with a more intermediate risk of AD. Across the AD continuum, the incremental increase in all biomarkers is associated with structural changes in widespread brain regions and underlying cognitive decline. Furthermore, all isoforms differentiate AD from non-AD neurodegenerative disorders, making them specific for AD. Incorporating p-tau181, p-tau217 and p-tau231 in clinical use requires further studies to examine ideal cut-points and harmonize assays.

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阿尔茨海默病中磷酸化的tau。
需要血液生物标志物来检测不同阿尔茨海默病(AD)阶段的个体,因为获得基于脑脊液的生物标志物具有侵入性且成本高昂。血浆磷酸化tau蛋白(p-tau)已显示出作为此类生物标志物的潜力。这项系统综述是根据PRISMA指南进行的,旨在确定苏氨酸181(p-tau181)、苏氨酸217(p-tau217)和苏氨酸231(p-tau231)磷酸化的血浆tau的定量是否对AD的诊断有帮助。所有p-au亚型都作为aβ-积累的函数而增加,并以高精度将健康个体与临床前AD阶段的个体区分开来。P-tau231增加最早,其次是P-tau181和P-tau217。在晚期,所有p-tau亚型都与AD的临床分类有关,并随着疾病严重程度的增加而增加,其中p-tau217的增加最大。这也反映在p-tau217与aβ扫描的更好相关性上,而p-tau218和p-tau181与tau扫描的相关性相等。然而,在非常晚期,p-tau181开始趋于平稳,这可能反映了Aβ病理学的轨迹,并表明与AD的中等风险有关。在整个AD连续体中,所有生物标志物的增量增加与广泛的大脑区域的结构变化和潜在的认知能力下降有关。此外,所有亚型都将AD与非AD神经退行性疾病区分开来,使其对AD具有特异性。在临床应用中结合p-tau181、p-tau217和p-tau231需要进一步的研究来检查理想的分界点并协调测定。
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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