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定量蛋白质生物标志物的统计检测为急性髓系白血病中失调的信号网络提供了见解。

Statistical detection of quantitative protein biomarkers provides insights into signaling networks deregulated in acute myeloid leukemia.

作者信息

Elo Laura L, Karjalainen Riikka, Ohman Tiina, Hintsanen Petteri, Nyman Tuula A, Heckman Caroline A, Aittokallio Tero

机构信息

Department of Mathematics and Statistics, University of Turku, Turku, Finland; Turku Centre for Biotechnology, Turku, Finland.

出版信息

Proteomics. 2014 Nov;14(21-22):2443-53. doi: 10.1002/pmic.201300460. Epub 2014 Oct 15.

DOI:10.1002/pmic.201300460
PMID:25211154
Abstract

The increasing coverage and sensitivity of LC-MS/MS-based proteomics have expanded its applications in systems medicine. In particular, label-free quantitation approaches are enabling biomarker discovery in terms of statistical comparison of proteomic profiles across large numbers of clinical samples. However, it still remains poorly understood how much protein markers can add novel insights compared to markers derived from mRNA transcriptomic profiling. Using paired label-free LC-MS/MS and gene expression microarray measurements from primary samples of patients with acute myeloid leukemia (AML), we demonstrate here that while the quantitative proteomic and transcriptomic profiles were highly correlated, in general, the marker panels showing statistically significant expression changes across the disease and healthy groups were profoundly different between protein and mRNA levels. In particular, the proteomic assay enabled unique links to known leukemic processes, which were missed when using the transcriptomic profiling alone, as well as identified additional links to metabolic regulators and chromatin remodelers, such as GPX1, fumarate hydratase, and SET oncogene, which have subsequently been evaluated in independent AML samples. Overall, these results highlighted the complementary and informative view obtained from the quantitative LC-MS/MS approach into the AML deregulated signaling networks.

摘要

基于液相色谱-串联质谱(LC-MS/MS)的蛋白质组学技术在覆盖范围和灵敏度方面的不断提高,已拓展了其在系统医学中的应用。特别是,无标记定量方法能够通过对大量临床样本的蛋白质组图谱进行统计比较来发现生物标志物。然而,与源自mRNA转录组分析的标志物相比,蛋白质标志物能提供多少新见解仍知之甚少。我们利用急性髓系白血病(AML)患者原代样本的配对无标记LC-MS/MS和基因表达微阵列测量,在此证明,虽然定量蛋白质组学和转录组学图谱高度相关,但总体而言,在疾病组和健康组中显示出统计学显著表达变化的标志物组在蛋白质和mRNA水平上存在深刻差异。特别是,蛋白质组学分析能够建立与已知白血病过程的独特联系,而仅使用转录组分析时会遗漏这些联系,并且还能识别与代谢调节因子和染色质重塑因子的其他联系,如谷胱甘肽过氧化物酶1(GPX1)、延胡索酸水合酶和SET癌基因,随后在独立的AML样本中对它们进行了评估。总体而言,这些结果突出了从定量LC-MS/MS方法中获得的关于AML失调信号网络的互补且信息丰富的观点。

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