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两种新型血液生物标志物候选物可测量 tau 的降解,与痴呆相关:一项前瞻性研究。

Two novel blood-based biomarker candidates measuring degradation of tau are associated with dementia: A prospective study.

机构信息

Nordic Bioscience A/S, Herlev, Denmark.

DTU Bioengineering, Technical University of Denmark, Kgs, Lyngby, Denmark.

出版信息

PLoS One. 2018 Apr 11;13(4):e0194802. doi: 10.1371/journal.pone.0194802. eCollection 2018.

Abstract

BACKGROUND

Truncated tau appears to be specifically related to disease pathology and recent studies have shown the presence and elevation of several truncated tau species in Cerebrospinal fluid (CSF) of subjects with Alzheimer's disease (AD); however, the relevance of truncated Tau measurements in blood is still being studied.

OBJECTIVE

The aim of the current study was to assess the longitudinal associations between baseline levels of two novel blood biomarker candidates measuring truncated tau, Tau-A and Tau-C, and the risk of incident dementia and AD in elderly women.

METHODS

Using solid phase competitive ELISA, two tau fragments were detected in serum of 5,309 women from the Prospective Epidemiological Risk Factor study. The study was an observational, prospective study of Danish postmenopausal women. Subjects were followed with registry-linkage for up to 15 years (median follow-up time 13.7 years). Cox regression was used to assess the utility of the biomarker candidates in relation to dementia and AD.

RESULTS

High levels of Tau-A and Tau-C (above the median) in blood were associated with lower risk of dementia and AD (Tau-A: Dementia HR[95% CI] = 0.85[0.70-1.04]; AD 0.71[0.52-0.98] and Tau-C: Dementia 0.84[0.70-1.00]; AD 0.78[0.60-1.03]). Tau-C gave a very modest increase in the AUC in a 5-year prediction horizon as compared to a reference model with age and education, while a combination of the two did not improve their predictive capacity.

CONCLUSIONS

Measurement of tau in serum is feasible. The serological tau turnover profile may be related to the diagnosis and development of dementia and AD. The exact processing and profile in serum in relation to cognitive disorders remains to be further assessed to provide simple non-invasive tests to identify subjects with progressive cognitive disorders.

摘要

背景

截断的 tau 似乎与疾病病理学有特定的关系,最近的研究表明,阿尔茨海默病(AD)患者的脑脊液(CSF)中存在并升高了几种截断的 tau 物质;然而,血液中截断 Tau 的测量相关性仍在研究中。

目的

本研究旨在评估两种新型血液生物标志物候选物(测量截断 tau 的 Tau-A 和 Tau-C)在基线水平与老年女性发生痴呆和 AD 风险之间的纵向关联。

方法

使用固相竞争 ELISA 法,在来自前瞻性流行病学风险因素研究的 5309 名女性的血清中检测到两种 tau 片段。该研究是一项对丹麦绝经后女性的观察性、前瞻性研究。受试者通过登记链接进行了长达 15 年的随访(中位随访时间为 13.7 年)。使用 Cox 回归评估生物标志物候选物与痴呆和 AD 的相关性。

结果

血液中 Tau-A 和 Tau-C (高于中位数)水平较高与痴呆和 AD 的风险较低相关(Tau-A:痴呆 HR[95%CI] = 0.85[0.70-1.04];AD 0.71[0.52-0.98];Tau-C:痴呆 0.84[0.70-1.00];AD 0.78[0.60-1.03])。与年龄和教育相结合的参考模型相比,Tau-C 在 5 年预测期内对 AUC 的改善非常有限,而两者的结合并不能提高其预测能力。

结论

在血清中测量 tau 是可行的。血清中 tau 的周转率特征可能与痴呆和 AD 的诊断和发展有关。与认知障碍相关的血清中 tau 的具体处理和特征仍有待进一步评估,以提供简单的非侵入性测试来识别有进展性认知障碍的受试者。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/912f/5895005/258ab260e7d6/pone.0194802.g001.jpg

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