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阿尔茨海默病患者、疾病对照者及年龄匹配随机样本中的脑脊液tau蛋白和β-淀粉样蛋白

Cerebrospinal fluid tau and beta-amyloid in Alzheimer patients, disease controls and an age-matched random sample.

作者信息

Ibach Bernd, Binder Harald, Dragon Margarethe, Poljansky Stefan, Haen Ekkehard, Schmitz Eberhard, Koch Horst, Putzhammer Albert, Kluenemann Hans, Wieland Wolf, Hajak Goeran

机构信息

Department of Psychiatry, Psychosomatics and Psychotherapy, Geriatric Psychiatry Research Group, University of Regensburg at the Bezirksklinikum, Universitätsstrasse 84, D-93053 Regensburg, Germany.

出版信息

Neurobiol Aging. 2006 Sep;27(9):1202-11. doi: 10.1016/j.neurobiolaging.2005.06.005. Epub 2005 Aug 8.

Abstract

We prospectively evaluated the diagnostic accuracy of cerebrospinal fluid (CSF)-beta-amyloid1-42 (Abeta42), -total-tau (tau) and -phosphorylated-tau181 (p-tau181) as measured by sandwich ELISAs in the clinical routine of a community state hospital to discriminate between patients with Alzheimer's disease (AD), healthy controls (HC), non-AD-dementias, a group composed of various psychiatric disorders (non-AD-dementias, mental diseases) and an age-matched random sample (RS) (total N=219). By comparing patients with AD to HC as reference, tau revealed sensitivity (sens)/specificity (spec) of 88%/80%, p-tau(181) 88%/80%, tau/Abeta42-ratio 81%/85% and phospho-tau(181)/Abeta42-ratio 81%/78%. Discriminative power between HC and all dementias under investigation was estimated lower for tau (78%/77%) and p-tau(181) (73%/79%). Relative to patients with AD, ROC analysis for the RS revealed highest sens/spec for p-tau181 (79%/77%) and p-tau181/Abeta42 ratio (78%/75%). Differentiation between AD versus a group made of patients with various psychiatric disorders was optimised by using CSF-p-tau181 (80%/77%). Under clinical routine conditions current CSF-biomarkers show a substantial capacity to discriminate between AD and HC as reference and to mark off AD patients from RS and heterogeneous diagnostic groups composed of non-AD dementias and other psychiatric conditions. Despite a residual substantial overlap between the groups, we conclude that current CSF markers are well suited to support AD-related diagnostic procedures in every-day clinics.

摘要

我们前瞻性地评估了在一家社区公立医院的临床常规中,通过夹心酶联免疫吸附测定法(sandwich ELISAs)检测脑脊液(CSF)中β-淀粉样蛋白1-42(Aβ42)、总tau蛋白(tau)和磷酸化tau蛋白181(p-tau181)的诊断准确性,以区分阿尔茨海默病(AD)患者、健康对照(HC)、非AD痴呆、由各种精神疾病组成的一组(非AD痴呆、精神疾病)以及年龄匹配的随机样本(RS)(总N = 219)。通过将AD患者与作为对照的HC进行比较,tau蛋白的敏感性(sens)/特异性(spec)为88%/80%,p-tau(181)为88%/80%,tau/Aβ42比值为81%/85%,磷酸化tau(181)/Aβ42比值为81%/78%。tau蛋白(78%/77%)和p-tau(181)(73%/79%)对HC与所有被调查痴呆之间的鉴别能力估计较低。相对于AD患者,RS的ROC分析显示p-tau181(79%/77%)和p-tau181/Aβ42比值(78%/75%)的sens/spec最高。使用CSF-p-tau181(80%/77%)可优化AD与由各种精神疾病患者组成的一组之间的区分。在临床常规条件下,目前的CSF生物标志物显示出在区分AD与作为对照的HC以及将AD患者与RS和由非AD痴呆及其他精神疾病组成的异质性诊断组区分开来方面具有很大能力。尽管各组之间仍存在大量重叠,但我们得出结论,目前的CSF标志物非常适合在日常诊所中支持与AD相关的诊断程序。

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