Detecting differential protein expression in large-scale population proteomics

被引:12
|
作者
Ryu, So Young [1 ,4 ]
Qian, Wei-Jun [2 ,3 ]
Camp, David G. [2 ,3 ]
Smith, Richard D. [2 ,3 ]
Tompkins, Ronald G. [4 ]
Davis, Ronald W. [1 ]
Xiao, Wenzhong [1 ,4 ]
机构
[1] Stanford Univ, Stanford Genome Technol Ctr, Stanford, CA 94305 USA
[2] Pacific NW Natl Lab, Div Biol Sci, Richland, WA 99352 USA
[3] Pacific NW Natl Lab, Environm Mol Sci Lab, Richland, WA 99352 USA
[4] Harvard Univ, Sch Med, Massachusetts Gen Hosp, Boston, MA 02114 USA
基金
美国国家卫生研究院;
关键词
MASS-SPECTROMETRY DATA; V-PROTEIN; BINDING-PROTEIN; QUANTIFICATION; SIMIAN-VIRUS-5; DDB1; COMPLEX; INJURY; RATES; STAT1;
D O I
10.1093/bioinformatics/btu341
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
Motivation: Mass spectrometry (MS)-based high-throughput quantitative proteomics shows great potential in large-scale clinical biomarker studies, identifying and quantifying thousands of proteins in biological samples. However, there are unique challenges in analyzing the quantitative proteomics data. One issue is that the quantification of a given peptide is often missing in a subset of the experiments, especially for less abundant peptides. Another issue is that different MS experiments of the same study have significantly varying numbers of peptides quantified, which can result in more missing peptide abundances in an experiment that has a smaller total number of quantified peptides. To detect as many biomarker proteins as possible, it is necessary to develop bioinformatics methods that appropriately handle these challenges. Results: We propose a Significance Analysis for Large-scale Proteomics Studies (SALPS) that handles missing peptide intensity values caused by the two mechanisms mentioned above. Our model has a robust performance in both simulated data and proteomics data from a large clinical study. Because varying patients' sample qualities and deviating instrument performances are not avoidable for clinical studies performed over the course of several years, we believe that our approach will be useful to analyze large-scale clinical proteomics data.
引用
收藏
页码:2741 / 2746
页数:6
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