蛋白质组
生物标志物
仿形(计算机编程)
生物标志物发现
蛋白质组学
计算生物学
样品(材料)
血液蛋白质类
生物信息学
计算机科学
色谱法
医学
生物
化学
内科学
遗传学
基因
操作系统
作者
Philipp E. Geyer,Eugenia Voytik,Peter V. Treit,Sophia Doll,Alisa Kleinhempel,Lili Niu,Johannes Müller,Jakob M. Bader,Daniel Teupser,Lesca M. Holdt,Matthias Mann
摘要
Abstract Plasma and serum are rich sources of information regarding an individual’s health state and protein tests inform medical decision making. Despite major investments, few new biomarkers have reached the clinic. Mass spectrometry (MS)-based proteomics now allows highly specific and quantitative read-out of the plasma proteome. Here we employ Plasma Proteome Profiling to define contamination marker panels to assess plasma samples and the likelihood that suggested biomarkers are instead artifacts related to sample handling and processing. We acquire deep reference proteomes of erythrocytes, platelets, plasma and whole blood of 20 individuals (>6000 proteins), and compare serum and plasma proteomes. Based on spike-in experiments we determine contamination-associated proteins, many of which have been reported as biomarker candidates as revealed by a comprehensive literature survey. We provide sample preparation guidelines and an online resource ( www.plasmaproteomeprofiling.org ) to assess overall sample-related bias in clinical studies and to prevent costly miss-assignment of biomarker candidates.
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