大规模邻近延伸分析显示CSF中间因子和多巴脱羧酶是帕金森病的支持性诊断生物标志物。

IF 10.8 1区 医学 Q1 NEUROSCIENCES
Wojciech Paslawski, Shervin Khosousi, Ellen Hertz, Ioanna Markaki, Adam Boxer, Per Svenningsson
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引用次数: 0

摘要

背景:需要生物标志物来支持帕金森病(PD)的准确诊断。脑脊液(CSF)是一种成功发现神经退行性生物标志物的生物流体,现代高灵敏度的多路复用方法为进行发现研究提供了可能性。使用大规模多重邻近延伸分析(PEA)方法,我们旨在发现新的诊断蛋白生物标志物,从而准确区分PD与对照组和非典型帕金森病(APD)。方法:来自PD、皮质基底综合征(CBS)、进行性核上性麻痹(PSP)、多系统萎缩和对照组的CSF,使用Olink PEA面板进行分析。本研究使用了三个队列,分别包括192例、88例和36例。所有样本均在心血管II、肿瘤学II和代谢PEA面板上运行。结果:我们的分析显示,与对照组相比,测试和验证PD队列的CSF中分别有26和39种蛋白质差异表达。其中,6种蛋白质在两个队列中都发生了变化。Midkine(MK)在PD中以最强的效应大小增加,并用ELISA验证了结果。PD中另一种增加最多的蛋白质,DOPA脱羧酶(DDC),它催化DOPA(L-3,4-二羟基苯丙氨酸)脱羧为多巴胺,与多巴胺能治疗密切相关。此外,与PD和对照相比,激肽释放酶10在APD中发生了特异性变化,但在PD和对照之间没有变化。Wnt抑制因子1在两个独立队列中的CBS和PSP患者中持续下调。结论:使用大规模PEA方法,我们在PD患者的CSF中发现了潜在的新的PD诊断生物标志物,最显著的是MK和DDC。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Large-scale proximity extension assay reveals CSF midkine and DOPA decarboxylase as supportive diagnostic biomarkers for Parkinson's disease.

Large-scale proximity extension assay reveals CSF midkine and DOPA decarboxylase as supportive diagnostic biomarkers for Parkinson's disease.

Large-scale proximity extension assay reveals CSF midkine and DOPA decarboxylase as supportive diagnostic biomarkers for Parkinson's disease.

Large-scale proximity extension assay reveals CSF midkine and DOPA decarboxylase as supportive diagnostic biomarkers for Parkinson's disease.

Background: There is a need for biomarkers to support an accurate diagnosis of Parkinson's disease (PD). Cerebrospinal fluid (CSF) has been a successful biofluid for finding neurodegenerative biomarkers, and modern highly sensitive multiplexing methods offer the possibility to perform discovery studies. Using a large-scale multiplex proximity extension assay (PEA) approach, we aimed to discover novel diagnostic protein biomarkers allowing accurate discrimination of PD from both controls and atypical Parkinsonian disorders (APD).

Methods: CSF from patients with PD, corticobasal syndrome (CBS), progressive supranuclear palsy (PSP), multiple system atrophy and controls, were analysed with Olink PEA panels. Three cohorts were used in this study, comprising 192, 88 and 36 cases, respectively. All samples were run on the Cardiovascular II, Oncology II and Metabolism PEA panels.

Results: Our analysis revealed that 26 and 39 proteins were differentially expressed in the CSF of test and validation PD cohorts, respectively, compared to controls. Among them, 6 proteins were changed in both cohorts. Midkine (MK) was increased in PD with the strongest effect size and results were validated with ELISA. Another most increased protein in PD, DOPA decarboxylase (DDC), which catalyses the decarboxylation of DOPA (L-3,4-dihydroxyphenylalanine) to dopamine, was strongly correlated with dopaminergic treatment. Moreover, Kallikrein 10 was specifically changed in APD compared with both PD and controls, but unchanged between PD and controls. Wnt inhibitory factor 1 was consistently downregulated in CBS and PSP patients in two independent cohorts.

Conclusions: Using the large-scale PEA approach, we have identified potential novel PD diagnostic biomarkers, most notably MK and DDC, in the CSF of PD patients.

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来源期刊
Translational Neurodegeneration
Translational Neurodegeneration Neuroscience-Cognitive Neuroscience
CiteScore
19.50
自引率
0.80%
发文量
44
审稿时长
10 weeks
期刊介绍: Translational Neurodegeneration, an open-access, peer-reviewed journal, addresses all aspects of neurodegenerative diseases. It serves as a prominent platform for research, therapeutics, and education, fostering discussions and insights across basic, translational, and clinical research domains. Covering Parkinson's disease, Alzheimer's disease, and other neurodegenerative conditions, it welcomes contributions on epidemiology, pathogenesis, diagnosis, prevention, drug development, rehabilitation, and drug delivery. Scientists, clinicians, and physician-scientists are encouraged to share their work in this specialized journal tailored to their fields.
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