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精神分裂症和心境障碍患者外周血单个核细胞蛋白质组学分析:用于发现有鉴别能力的生物标志物的概念验证研究。

Profiling of the Peripheral Blood Mononuclear Cell Proteome in Schizophrenia and Mood Disorders for the Discovery of Discriminatory Biomarkers: A Proof-of-Concept Study.

机构信息

Scientific Initiative for Neuropsychiatric and Psychopharmacological Studies (SINAPS), Collaborative Antwerp Psychiatric Research Institute (CAPRI), University of Antwerp, Antwerp, Belgium,

Scientific Initiative for Neuropsychiatric and Psychopharmacological Studies (SINAPS), University Psychiatric Center Duffel, Duffel, Belgium,

出版信息

Neuropsychobiology. 2020;79(4-5):324-334. doi: 10.1159/000507631. Epub 2020 May 11.

DOI:10.1159/000507631
PMID:32392557
Abstract

INTRODUCTION

Current diagnoses in psychiatry are solely based on the evaluation of clinical presentation by the treating psychiatrist. This results in a high percentage of misdiagnosis and consequential inefficient treatment; especially regarding major depressive disorder (MDD), depression in the context of bipolar disorder (BD-D), bipolar disorder with manic symptoms (BD-M), and psychosis in the context of schizophrenia (SZ). Objective biomarkers allowing for accurate discriminatory diagnostics are therefore urgently needed.

METHODS

Peripheral blood mononuclear cell (PBMC) proteomes of patients with MDD (n = 5) , BD-D (n = 3), BD-M (n = 4), and SZ (n = 4), and also of healthy controls (HC; n = 6) were analyzed by state-of-the-art mass spectrometry. Proteins with a differential expression of a >2 standard deviation (SD) expression fold change from that of the HC and between either MDD versus BD-D or BD-M versus SZ were subsequently identified as potential discriminatory biomarkers.

RESULTS

In total, 4,271 individual proteins were retrieved from the HC. Of these, about 2,800 were detected in all patient and HC samples. For objective discrimination between MDD and BD-D, 66 candidate biomarkers were found. In parallel, 72 proteins might harbor a biomarker capacity for differential diagnostics of BD-M and SZ. A single biomarker was contraregulated versus HC in each pair of comparisons.

DISCUSSION

With this work, we provide a register of candidate biomarkers with the potential to objectively discriminate MDD from BD-D, and BD-M from SZ. Although concerning a proof-of-concept study with limited sample size, these data provide a stepping-stone for follow-up research on the validation of the true discriminatory potential and feasibility of clinical implementation of the discovered biomarker candidates.

摘要

简介

目前的精神病学诊断仅基于治疗精神病医生对临床表现的评估。这导致了误诊的高比例和随之而来的低效治疗;特别是在重度抑郁症(MDD)、双相情感障碍中的抑郁(BD-D)、伴有躁狂症状的双相情感障碍(BD-M)和精神分裂症中的精神病(SZ)的情况下。因此,迫切需要能够进行准确鉴别诊断的客观生物标志物。

方法

通过最先进的质谱分析了 MDD(n=5)、BD-D(n=3)、BD-M(n=4)和 SZ(n=4)患者以及健康对照者(HC;n=6)的外周血单核细胞(PBMC)蛋白质组。随后鉴定了差异表达>2 个标准差(SD)表达倍数的蛋白,并与 HC 进行比较,或者与 MDD 与 BD-D 或 BD-M 与 SZ 进行比较,将其鉴定为潜在的鉴别生物标志物。

结果

总共从 HC 中获取了 4271 种个体蛋白。其中约 2800 种在所有患者和 HC 样本中均有检出。为了客观地区分 MDD 和 BD-D,发现了 66 个候选生物标志物。同时,72 种蛋白可能具有区分 BD-M 和 SZ 的诊断生物标志物的能力。在每一对比较中,都有一个单一的生物标志物与 HC 呈相反的调控。

讨论

通过这项工作,我们提供了一份候选生物标志物的清单,这些标志物有可能客观地区分 MDD 与 BD-D,以及 BD-M 与 SZ。尽管这是一项样本量有限的概念验证研究,但这些数据为后续研究提供了一个起点,以验证发现的生物标志物候选物的真正鉴别潜力和临床实施的可行性。

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