Clinical value of plasma brain-derived tau and p-tau217 in acute ischemic stroke

IF 1.9 Q3 CLINICAL NEUROLOGY Cerebral circulation - cognition and behavior Pub Date : 2024-01-01 DOI:10.1016/j.cccb.2024.100291

Julia K. Gundersen , Fernando Gonzalez-Ortiz , Thomas Karikari , Bjørn-Eivind Kirsebom , Katrin Mertes , Henrik Zetterberg , Hlin Kvartsberg , Ole Morten Rønning , Berglind Gísladóttir , Kaj Blennow , Tormod Fladby

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Abstract

Introduction

Diagnosis of acute ischemic stroke (AIS) as based on clinical examination and neuroimaging has limitations in determining subgroup aetiology and subsequent long-term motor and cognitive impairment. Identification of high-risk patients enables personalised prophylaxis and rehabilitation strategies. This study explores the clinical value of plasma brain-derived tau (BD-tau) and phosphorylated-tau217 (p-tau217), primarily associated with neurodegeneration, in identifying patients at risk of sequela after AIS.

Methods

We analysed a cohort of 193 patients admitted to the stroke unit at Akershus University Hospital in Oslo, Norway. Each patient received a diagnosis of AIS (n=102), transient ischemic attack (TIA, n=63) or stroke mimic (n=31). Patient characteristics were collected from hospital records. Biomarkers were quantified using Simoa HDX in venous blood sampled obtained the day after admission. Inpatient short-term outcomes, including stroke diameter on magnetic resonance imaging (MRI, n=134) and mini mental state examination (MMSE, n=153), were assessed prior to discharge. Non-parametric statistics, including Kruskal-Wallis and Kendall´s tau-b correlation tests were applied. Backwards stepwise linear regression analysis was used to determine the association between stroke diameter or MMSE and the biomarkers. A full model was fitted with explanatory variables as listen in table 1.

Results

BD-tau was significantly increased in AIS patients as compared to mimics (p=.004), whereas p- tau217 did not differentiate between the diagnostic groups. MRIs were available for 66 (64.7%) of AIS patients, of whom n=36 were diagnosed with cortical and n=30 with subcortical stroke. Cortical stroke diameter showed a strong correlation with BD-tau (fig. 1, <.001) and p-tau217 (=.003). In regression analysis, only BD-tau was found to be significantly associated with stroke diameter (table 1). Subcortical strokes were mot associated with any of the biomarkers. Furthermore, MMSE score correlated with BD-tau (fig. 2, <.001) and p-tau217 (<.001). In regression analysis, age was the strongest predictor of MMSE score, followed by p-tau217.

Discussion

Our findings suggest that blood-based BD-tau and p-tau217 have clinical potential in determining AIS subgroup aetiology and provide insights into cognitive impairment in AIS patients. These findings may have implications for rehabilitation and secondary prophylaxis after stroke.

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血浆脑源性 tau 和 p-tau217 在急性缺血性脑卒中中的临床价值

导言根据临床检查和神经影像学诊断急性缺血性卒中（AIS）在确定亚组病因及随后的长期运动和认知障碍方面存在局限性。高危患者的识别有助于制定个性化的预防和康复策略。本研究探讨了血浆脑源性 tau（BD-tau）和磷酸化 tau217（p-tau217）（主要与神经变性有关）在识别 AIS 后遗症高危患者方面的临床价值。每位患者均被诊断为 AIS（102 人）、短暂性脑缺血发作（TIA，63 人）或中风模拟（31 人）。患者特征由医院记录收集。使用 Simoa HDX 对入院次日采集的静脉血样本中的生物标记物进行量化。出院前对住院患者的短期疗效进行评估，包括磁共振成像（MRI，134 人）和迷你精神状态检查（MMSE，153 人）显示的卒中直径。采用非参数统计，包括 Kruskal-Wallis 和 Kendall´s tau-b 相关性检验。逆向逐步线性回归分析用于确定中风直径或 MMSE 与生物标志物之间的关系。结果BD-tau在AIS患者中明显高于模拟患者（p=.004），而p- tau217在诊断组之间没有差异。有 66 名（64.7%）AIS 患者接受了核磁共振成像检查，其中 36 人被诊断为皮质中风，30 人被诊断为皮质下中风。皮质卒中直径与 BD-tau （图 1，<.001）和 p-tau217 （=.003）密切相关。在回归分析中，发现只有 BD-tau 与中风直径显著相关（表 1）。皮层下中风与任何生物标志物均无相关性。此外，MMSE 评分与 BD-tau 相关（图 2，<.001），与 p-tau217 相关（< .001）。我们的研究结果表明，基于血液的 BD-tau 和 p-tau217 在确定 AIS 亚组病因方面具有临床潜力，并为 AIS 患者的认知障碍提供了见解。这些发现可能对脑卒中后的康复和二级预防有意义。

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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