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血清 Tau 蛋白能否预测缺血性脑卒中患者的预后?

Does serum Tau protein predict the outcome of patients with ischemic stroke?

机构信息

Department of Neurology, Medical University of Lublin, Jaczewskiego 8, 20-954, Lublin, Poland.

出版信息

J Mol Neurosci. 2011 Mar;43(3):241-5. doi: 10.1007/s12031-010-9403-4. Epub 2010 Jun 12.

DOI:10.1007/s12031-010-9403-4
PMID:20549384
Abstract

The prediction of outcome after ischemic stroke (IS) is currently based on indirect data from clinical and radiological evaluation. We evaluated the usefulness of serum Tau protein as possible prognostic markers for IS. Fifty-six patients with computed tomography-confirmed IS were enrolled. Blood samples were obtained on days 1, 3, 5, and 10 after stroke onset. Tau and S100BB serum levels were measured by commercially available enzyme-linked immunosorbent assay. Neurological deficits were quantified by the National Institute of Health Stroke Scale on days 1, 3, 5, and 10 of stroke. Functional disability was rated with the Barthel Index and Rankin Scale on days 1, 3, 5, and 10 and additionally 3 months after the stroke. Computed tomography scan was performed to calculate infarct volume on admission to hospital and on day 10 from the diagnosis of IS onset. Tau protein was detected in the serum of 47.8% patients with IS. Patients in whom Tau protein was detected in serum, when compared with patients without Tau protein, developed more severe neurological deficits, had worse functional status measured in the early and late phase of IS, and were found to have larger volume of infarction. However, Tau protein concentrations measured within the early phase of IS did not correlate with degrees of neurological deficit and disability in the early phase and also after 3 months of IS. Detection of Tau protein in the serum of patients with IS but not its concentration can be considered as a bad prognostic factor for the clinical outcome in early and late phase of IS.

摘要

目前,缺血性中风(IS)预后的预测是基于临床和影像学评估的间接数据。我们评估了血清 Tau 蛋白作为 IS 预后标志物的有用性。共纳入 56 例经计算机断层扫描(CT)确诊的 IS 患者。在中风发病后第 1、3、5 和 10 天采集血液样本。采用商业上可用的酶联免疫吸附测定法测量 Tau 和 S100BB 血清水平。在中风发病第 1、3、5 和 10 天,采用国立卫生研究院中风量表(NIHSS)量化神经功能缺损。在中风发病第 1、3、5 和 10 天,采用巴氏指数(Barthel Index)和 Rankin 量表评估功能障碍,并在中风后 3 个月进行评估。进行 CT 扫描以计算入院时和中风发病后第 10 天的梗死体积。在 47.8%的 IS 患者血清中检测到 Tau 蛋白。与未检测到 Tau 蛋白的患者相比,在血清中检测到 Tau 蛋白的患者出现更严重的神经功能缺损,在 IS 的早期和晚期阶段功能状态更差,并且发现梗死体积更大。然而,IS 早期阶段测量的 Tau 蛋白浓度与早期和 IS 后 3 个月的神经功能缺损和残疾程度无关。在 IS 患者的血清中检测到 Tau 蛋白,但不检测其浓度,可被认为是 IS 早期和晚期临床结局的不良预后因素。

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