Targeted and non-targeted proteomics to identify the urinary protein biomarkers for Wilson disease.

IF 3.2 3区 医学 Q2 MEDICAL LABORATORY TECHNOLOGY Clinica Chimica Acta Pub Date : 2024-12-12 DOI:10.1016/j.cca.2024.120090
Simin Dong, Xixi Wang, Huiling Zhou, Huan Xu, Liqian Su, Linshen Xie, Yongxin Li
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Abstract

Background: Wilson disease (WD) is a genetic disorder of copper metabolism. Early diagnosis of WD is inherently challenging due to the absence of typical symptoms. This study aimed to identify urinary protein biomarkers for WD using targeted and nontargeted mass spectrometry-based approaches.

Methods: Exploratory urinary proteomic research on WD patients was initially conducted and revealed some potential biomarkers (alpha-2-macroglobulin, alpha-1-antitrypsin, complement C3, prothrombin, and complement factor B). A multiple reaction monitoring (MRM) assay was subsequently developed and applied to an independent WD cohort for protein candidate validation. Finally, a Random Forest (RF) model constructed with five proteins was evaluated for its diagnostic capacity.

Results: The linear range of the MRM assay extended from 0.025 ng/L to 155 ng/L and the limit of quantification (LOQ) ranged from 0.0095 ng/L to 9.2308 ng/L. Alpha-2-macroglobulin, alpha-1-antitrypsin, and complement C3 exhibited significant increases (p < 0.05) in WD patients compared to the controls, whereas prothrombin and complement factor B only showed variations in concentration. The physiology reference intervals (RIs) for alpha-2-macroglobulin, alpha-1-antitrypsin, complement C3, prothrombin, and complement factor B were estimated as 0-12.50, 0-123.08, 0-5.20, 0-16.59, 0-4.85 ng/mol Cr, while the pathology RIs were 0-114.86, 0-600.98, 0-12.62, 0-22.16, and 0-10.83 ng/mol Cr, respectively. The RF model demonstrated an area under the curve (AUC) of 0.99 for the training data and 0.83 for the testing data.

Conclusions: Based on the proteomic results, the quantitative method was successfully applied for the validation of protein candidates in WD. Using supervised machine learning, the five-protein panel exhibited excellent accuracy in non-invasive diagnosis of WD.

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通过靶向和非靶向蛋白质组学鉴定威尔逊氏病的尿蛋白生物标志物。
背景介绍威尔逊病(WD)是一种铜代谢遗传性疾病。由于没有典型症状,WD 的早期诊断本身就具有挑战性。本研究旨在利用基于靶向和非靶向质谱的方法确定 WD 的尿蛋白生物标志物:方法:最初对WD患者进行了探索性尿液蛋白质组学研究,发现了一些潜在的生物标记物(α-2-巨球蛋白、α-1-抗胰蛋白酶、补体C3、凝血酶原和补体因子B)。随后开发了一种多反应监测(MRM)测定法,并将其应用于一个独立的 WD 队列,以验证候选蛋白质。最后,评估了用五种蛋白质构建的随机森林(RF)模型的诊断能力:MRM测定的线性范围为0.025纳克/升至155纳克/升,定量限(LOQ)为0.0095纳克/升至9.2308纳克/升。α-2-巨球蛋白、α-1-抗胰蛋白酶和补体 C3 显著增加(p 结论):根据蛋白质组学结果,定量方法成功地应用于验证 WD 中的候选蛋白质。利用监督机器学习,五种蛋白面板在无创诊断 WD 方面表现出了极高的准确性。
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来源期刊
Clinica Chimica Acta
Clinica Chimica Acta 医学-医学实验技术
CiteScore
10.10
自引率
2.00%
发文量
1268
审稿时长
23 days
期刊介绍: The Official Journal of the International Federation of Clinical Chemistry and Laboratory Medicine (IFCC) Clinica Chimica Acta is a high-quality journal which publishes original Research Communications in the field of clinical chemistry and laboratory medicine, defined as the diagnostic application of chemistry, biochemistry, immunochemistry, biochemical aspects of hematology, toxicology, and molecular biology to the study of human disease in body fluids and cells. The objective of the journal is to publish novel information leading to a better understanding of biological mechanisms of human diseases, their prevention, diagnosis, and patient management. Reports of an applied clinical character are also welcome. Papers concerned with normal metabolic processes or with constituents of normal cells or body fluids, such as reports of experimental or clinical studies in animals, are only considered when they are clearly and directly relevant to human disease. Evaluation of commercial products have a low priority for publication, unless they are novel or represent a technological breakthrough. Studies dealing with effects of drugs and natural products and studies dealing with the redox status in various diseases are not within the journal''s scope. Development and evaluation of novel analytical methodologies where applicable to diagnostic clinical chemistry and laboratory medicine, including point-of-care testing, and topics on laboratory management and informatics will also be considered. Studies focused on emerging diagnostic technologies and (big) data analysis procedures including digitalization, mobile Health, and artificial Intelligence applied to Laboratory Medicine are also of interest.
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