脑脊液中的突触蛋白作为前驱期阿尔茨海默病预后的潜在新型生物标志物。

Synaptic proteins in CSF as potential novel biomarkers for prognosis in prodromal Alzheimer's disease.

机构信息

Alzheimer Center and Department of Neurology, Amsterdam Neuroscience, VU University Medical Center, P.O. Box 7057, 1007MB, Amsterdam, The Netherlands.

Institute of Neuroscience and Physiology, Department of Psychiatry and Neurochemistry, Sahlgrenska Academy at the University of Gothenburg, Mölndal, Sweden.

出版信息

Alzheimers Res Ther. 2018 Jan 15;10(1):5. doi: 10.1186/s13195-017-0335-x.

DOI:10.1186/s13195-017-0335-x

PMID:29370833

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6389073/

Abstract

BACKGROUND

We investigated whether a panel of 12 potential novel biomarkers consisting of proteins involved in synapse functioning and immunity would be able to distinguish patients with Alzheimer's disease (AD) and patients with mild cognitive impairment (MCI) from control subjects.

METHODS

We included 40 control subjects, 40 subjects with MCI, and 40 subjects with AD from the Amsterdam Dementia Cohort who were matched for age and sex (age 65 ± 5 years, 19 [48%] women). The mean follow-up of patients with MCI was 3 years. Two or three tryptic peptides per protein were analyzed in cerebrospinal fluid using parallel reaction monitoring mass spectrometry. Corresponding stable isotope-labeled peptides were added and used as reference peptides. Multilevel generalized estimating equations (GEEs) with peptides clustered per subject and per protein (as within-subject variables) were used to assess differences between diagnostic groups. To assess differential effects of individual proteins, we included the diagnosis × protein interaction in the model. Separate GEE analyses were performed to assess differences between stable patients and patients with progressive MCI (MCI-AD).

RESULTS

There was a main effect for diagnosis (p < 0.01) and an interaction between diagnosis and protein (p < 0.01). Analysis stratified according to protein showed higher levels in patients with MCI for most proteins, especially in patients with MCI-AD. Chromogranin A, secretogranin II, neurexin 3, and neuropentraxin 1 showed the largest effect sizes; β values ranged from 0.53 to 0.78 for patients with MCI versus control subjects or patients with AD, and from 0.67 to 0.98 for patients with MCI-AD versus patients with stable MCI. In contrast, neurosecretory protein VGF was lower in patients with AD than in patients with MCI (ß = -0.93 [SE 0.22]) and control subjects (ß = 0.46 [SE 0.19]).

CONCLUSIONS

Our results suggest that several proteins involved in vesicular transport and synaptic stability are elevated in patients with MCI, especially in patients with MCI progressing to AD dementia. This may reflect early events in the AD pathophysiological cascade. These proteins may be valuable as disease stage or prognostic markers in an early symptomatic stage of the disease.

摘要

背景

我们研究了由涉及突触功能和免疫的蛋白质组成的 12 种潜在新型生物标志物组成的面板是否能够区分阿尔茨海默病（AD）患者和轻度认知障碍（MCI）患者与对照受试者。

方法

我们纳入了来自阿姆斯特丹痴呆队列的 40 名对照受试者、40 名 MCI 受试者和 40 名 AD 受试者，他们在年龄和性别上相匹配（年龄 65±5 岁，19 [48%] 名女性）。MCI 患者的平均随访时间为 3 年。使用平行反应监测质谱法分析脑脊液中的两种或三种胰蛋白酶肽。加入相应的稳定同位素标记肽作为参考肽。使用多水平广义估计方程（GEE），每个受试者和每个蛋白质（作为个体内变量）聚类肽，以评估诊断组之间的差异。为了评估个体蛋白的差异效应，我们在模型中包含了诊断×蛋白相互作用。分别进行 GEE 分析以评估稳定患者与进展性 MCI（MCI-AD）患者之间的差异。

结果

诊断存在主要影响（p<0.01），并且诊断与蛋白之间存在交互作用（p<0.01）。根据蛋白进行分层分析显示，MCI 患者的大多数蛋白水平升高，尤其是 MCI-AD 患者。嗜铬粒蛋白 A、分泌颗粒蛋白 II、神经连接蛋白 3 和神经五肽素 1 显示出最大的效应大小；β值在 MCI 患者与对照受试者或 AD 患者相比为 0.53 至 0.78，在 MCI-AD 患者与稳定 MCI 患者相比为 0.67 至 0.98。相比之下，AD 患者的神经分泌蛋白 VGF 水平低于 MCI 患者（β=-0.93 [SE 0.22]）和对照受试者（β=0.46 [SE 0.19]）。

结论

我们的结果表明，参与囊泡转运和突触稳定性的几种蛋白在 MCI 患者中升高，尤其是在进展为 AD 痴呆的 MCI 患者中。这可能反映了 AD 病理生理级联的早期事件。这些蛋白可能作为疾病阶段或疾病早期症状阶段的预后标志物有价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f7eb/6389073/a619bc227e0e/13195_2017_335_Fig1_HTML.jpg

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脑脊液中的突触蛋白作为前驱期阿尔茨海默病预后的潜在新型生物标志物。

Synaptic proteins in CSF as potential novel biomarkers for prognosis in prodromal Alzheimer's disease.

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