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Diagnostic performance of new and classic CSF biomarkers in age-related dementias

机译:新的和经典的CSF生物标志物在老年性痴呆中的诊断性能

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摘要

The identification of diagnostic-prognostic biomarkers of dementia has become a global priority due to the prevalence of neurodegenerative diseases in aging populations. The objective of this study was to assess the diagnostic performance of cerebrospinal fluid (CSF) biomarkers across patients affected by either Alzheimer’s disease (AD), tauopathies other than AD (TP), or vascular dementia (VD), and cognitively normal subjects (CNS). One hundred fifty-three patients were recruited and tested for classical AD CSF biomarkers- Amyloid-ß42 and tau proteins - and novel candidate biomarkers - neurofilament (NF-) light and microRNA (miR) -21, -125b, -146a, and -222.All dementia patients had significantly higher concentrations of NF-light compared to CNS, with the TP group displaying the highest NF-light values. A significant inverse correlation was also observed between NF-light and cognitive impairment. Of the four miRNAs analyzed, miR-222 levels were significantly increased in VD patients compared to both CNS and AD. In addition, while NF-light showed a better diagnostic performance than miR-222 and classical AD biomarkers in differentiating TP and VD from CNS, classical AD biomarkers revealed higher performance in discriminating AD from non-AD disorders.Overall, our results suggest that CSF NF-light and miR-222 are promising biomarkers that may help to diagnose non-AD disorders.
机译:由于衰老人群中神经退行性疾病的流行,对痴呆症的诊断和预后生物标志物的鉴定已成为全球优先考虑的问题。这项研究的目的是评估脑脊髓液(CSF)生物标志物在阿尔茨海默氏病(AD),除AD(TP)或血管性痴呆(VD)以外的其他疾病以及认知正常受试者(CNS)的患者中的诊断性能)。招募了153位患者,并测试了其经典AD CSF生物标志物-淀粉样蛋白-ß42和tau蛋白-以及新型候选生物标志物-神经丝(NF-)轻和微RNA(miR)-21,-125b,-146a和- 222.与中枢神经系统相比,所有痴呆患者的NF-光浓度均显着较高,而TP组显示出最高的NF-光值。在NF-光和认知障碍之间也观察到显着的负相关。与CNS和AD相比,在分析的四个miRNA中,VD患者的miR-222水平显着升高。此外,尽管NF-light在区分TP和VD与中枢神经系统方面表现出比miR-222和经典AD生物标志物更好的诊断性能,但经典AD生物标志物在区分AD和非AD疾病方面显示出更高的性能。总体而言,我们的结果表明CSF NF-light和miR-222是有前途的生物标志物,可能有助于诊断非AD疾病。

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