首页> 美国卫生研究院文献>International Journal of Alzheimers Disease >Combined Analysis of CSF Tau Aβ42 Aβ1–42 and Aβ1–40ox in Alzheimers Disease Dementia with Lewy Bodies and Parkinsons Disease Dementia
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Combined Analysis of CSF Tau Aβ42 Aβ1–42 and Aβ1–40ox in Alzheimers Disease Dementia with Lewy Bodies and Parkinsons Disease Dementia

机译:阿尔茨海默氏病痴呆伴路易体和帕金森氏病痴呆的CSF TauAβ42Aβ1-42%和Aβ1-40ox%的综合分析

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摘要

We studied the diagnostic value of CSF Aβ42/tau versus low Aβ1–42% and high Aβ1–40ox% levels for differential diagnosis of Alzheimer's disease (AD) and dementia with Lewy bodies (DLB), respectively. CSF of 45 patients with AD, 15 with DLB, 21 with Parkinson's disease dementia (PDD), and 40 nondemented disease controls (NDC) was analyzed by Aβ-SDS-PAGE/immunoblot and ELISAs (Aβ42 and tau). Aβ42/tau lacked specificity in discriminating AD from DLB and PDD. Best discriminating biomarkers were Aβ1–42% and Aβ1–40ox% for AD and DLB, respectively. AD and DLB could be differentiated by both Aβ1–42% and Aβ1–40ox% with an accuracy of 80% at minimum. Thus, we consider Aβ1–42% and Aβ1–40ox% to be useful biomarkers for AD and DLB, respectively. We propose further studies on the integration of Aβ1–42% and Aβ1–40ox% into conventional assay formats. Moreover, future studies should investigate the combination of Aβ1–40ox% and CSF alpha-synuclein for the diagnosis of DLB.
机译:我们研究了脑脊液Aβ42/ tau与低Aβ1–42%和高Aβ1–40 ox %水平分别对阿尔茨海默氏病(AD)和路易体痴呆(DLB)的诊断价值。通过Aβ-SDS-PAGE/免疫印迹和ELISA(Aβ42和tau)分析了45例AD,15例DLB,21例帕金森氏病痴呆(PDD)和40例非痴呆疾病对照(NDC)患者的CSF。 Aβ42/ tau蛋白在区分AD与DLB和PDD方面缺乏特异性。最佳的生物标志物分别是AD和DLB的Aβ1–42%和Aβ1–40 ox %。 AD和DLB可由Aβ1–42%和Aβ1–40 ox %区分,最低准确度为80%。因此,我们认为Aβ1–42%和Aβ1–40 ox %分别是AD和DLB的有用生物标记。我们提议进一步研究将Aβ1-42%和Aβ1-40 ox %整合到常规测定形式中。此外,未来的研究应探讨Aβ1–40 ox %和CSFα-突触核蛋白的组合对DLB的诊断。

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