標題: | An Informatics-assisted Label-free Approach for Personalized Tissue Membrane Proteomics: Case Study on Colorectal Cancer |
作者: | Han, Chia-Li Chen, Jinn-Shiun Chan, Err-Cheng Wu, Chien-Peng Yu, Kun-Hsing Chen, Kuei-Tien Tsou, Chih-Chiang Tsai, Chia-Feng Chien, Chih-Wei Kuo, Yung-Bin Lin, Pei-Yi Yu, Jau-Song Hsueh, Chuen Chen, Min-Chi Chan, Chung-Chuan Chang, Yu-Sun Chen, Yu-Ju 生物科技學院 College of Biological Science and Technology |
公開日期: | 1-四月-2011 |
摘要: | We developed a multiplexed label-free quantification strategy, which integrates an efficient gel-assisted digestion protocol, high-performance liquid chromatography tandem MS analysis, and a bioinformatics alignment method to determine personalized proteomic profiles for membrane proteins in human tissues. This strategy provided accurate (6% error) and reproducible (34% relative S. D.) quantification of three independently purified membrane fractions from the same human colorectal cancer (CRC) tissue. Using CRC as a model, we constructed the personalized membrane protein atlas of paired tumor and adjacent normal tissues from 28 patients with different stages of CRC. Without fractionation, this strategy confidently quantified 856 proteins (>= 2 unique peptides) across different patients, including the first and robust detection (Mascot score: 22,074) of the well-documented CRC marker, carcinoembryonic antigen 5 by a discovery-type proteomics approach. Further validation of a panel of proteins, annexin A4, neutrophils defensin A1, and claudin 3, confirmed differential expression levels and high occurrences (48-70%) in 60 CRC patients. The most significant discovery is the overexpression of stomatin-like 2 (STOML2) for early diagnostic and prognostic potential. Increased expression of STOML2 was associated with decreased CRC-related survival; the mean survival period was 34.77 +/- 2.03 months in patients with high STOML2 expression, whereas 53.67 +/- 3.46 months was obtained for patients with low STOML2 expression. Further analysis by ELISA verified that plasma concentrations of STOML2 in early-stage CRC patients were elevated as compared with those of healthy individuals (p < 0.001), suggesting that STOML2 may be a noninvasive serological biomarker for early CRC diagnosis. The overall sensitivity of STOML2 for CRC detection was 71%, which increased to 87% when combined with CEA measurements. This study demonstrated a sensitive, label-free strategy for differential analysis of tissue membrane proteome, which may provide a roadmap for the subsequent identification of molecular target candidates of multiple cancer types. Molecular & Cellular Proteomics 10: 10.1074/mcp.M110.003087, 1-15, 2011. |
URI: | http://dx.doi.org/10.1074/mcp.M110.003087 http://hdl.handle.net/11536/9080 |
ISSN: | 1535-9476 |
DOI: | 10.1074/mcp.M110.003087 |
期刊: | MOLECULAR & CELLULAR PROTEOMICS |
Volume: | 10 |
Issue: | 4 |
結束頁: | |
顯示於類別: | 期刊論文 |