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无标记、定量分泌组蛋白质组学在癌症生物标志物发现中的工作流程比较:方法评估、血清中的差异分析和验证。

Workflow comparison for label-free, quantitative secretome proteomics for cancer biomarker discovery: method evaluation, differential analysis, and verification in serum.

机构信息

OncoProteomics Laboratory, Department of Medical Oncology, VUmc-Cancer Center Amsterdam, VU University Medical Center, Amsterdam, The Netherlands.

出版信息

J Proteome Res. 2010 Apr 5;9(4):1913-22. doi: 10.1021/pr901072h.

DOI:10.1021/pr901072h
PMID:20085282
Abstract

The cancer cell secretome has emerged as an attractive subproteome for discovery of candidate blood-based biomarkers. To choose the best performing workflow, we assessed the performance of three first-dimension separation strategies prior to nanoLC-MS/MS analysis: (1) 1D gel electrophoresis (1DGE), (2) peptide SCX chromatography, and (3) tC2 protein reversed phase chromatography. 1DGE using 4-12% gradient gels outperformed the SCX and tC2 methods with respect to number of identified proteins (1092 vs 979 and 580, respectively), reproducibility of protein identification (80% vs 70% and 72%, respectively, assessed in biological N = 3). Reproducibility of protein quantitation based on spectral counting was similar for all 3 methods (CV: 26% vs 24% and 24%, respectively). As a proof-of-concept of secretome proteomics for blood-based biomarker discovery, the gradient 1DGE workflow was subsequently applied to identify IGF1R-signaling related proteins in the secretome of mouse embryonic fibroblasts transformed with human IGF1R (MEF/Toff/IGF1R). VEGF and osteopontin were differentially detected by LC-MS/MS and verified in secretomes by ELISA. Follow-up in serum of mice bearing MEF/Toff/IGF1R-induced tumors showed an increase of osteopontin levels paralleling tumor growth, and reduction in the serum of mice in which IGF1R expression was shut off and tumor regressed.

摘要

癌细胞分泌组作为候选血液生物标志物的发现,已经成为一个很有吸引力的亚蛋白组。为了选择性能最佳的工作流程,我们在进行纳升液相色谱-串联质谱分析之前,评估了三种一维分离策略的性能:(1) 一维凝胶电泳 (1DGE)、(2) 肽 SCX 色谱和 (3) tC2 蛋白质反相色谱。与 SCX 和 tC2 方法相比,使用 4-12%梯度凝胶的 1DGE 在鉴定的蛋白质数量方面表现更好(分别为 1092 对 979 和 580)、蛋白质鉴定的重现性(分别为 80%对 70%和 72%,在生物学上 N = 3 进行评估)。基于光谱计数的蛋白质定量的重现性对于所有 3 种方法都相似(CV:分别为 26%对 24%和 24%)。作为基于血液生物标志物发现的分泌组蛋白质组学的概念验证,随后将梯度 1DGE 工作流程应用于鉴定人 IGF1R 转化的小鼠胚胎成纤维细胞 (MEF/Toff/IGF1R) 分泌组中的 IGF1R 信号相关蛋白。LC-MS/MS 检测到 VEGF 和骨桥蛋白差异,并通过 ELISA 在分泌组中进行验证。携带 MEF/Toff/IGF1R 诱导肿瘤的小鼠血清中的后续研究显示,骨桥蛋白水平随着肿瘤生长而增加,而 IGF1R 表达关闭和肿瘤消退的小鼠血清中骨桥蛋白水平降低。

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