R. This study provides the first evidence to suggest that SSP411 is overexpressed in bile from CC patients, suggesting that SSP411 may be a CC-associated biomarker. Promisingly, as a single biomarker, SSP411 could distinguish patients with CC from choledocholithiasis patients and normal individuals, suggesting that SSP411 may represent a potentially useful serum biomarker for the diagnosis of CC (Figure 6). Although the mean serum level of SSP411 in the SMER28 web benign group was higher than in the normal, there was no significant difference between the two groups. The ROC analysis also revealed that the serum level of SSP411 could not effectively differentiate benign disease from the normal individuals (Figure 6B). We speculated that this bias was attributed to the insufficient sample size, especially for the benign group. Similarly, no significant correlation was observed between the serum levels of SSP411 and lymph node metastasis or neural invasion in CC (data not shown), which may also be attributed to the small sample size of the negative patients. Further Rubusoside chemical information research is required to characterize the function of SSP411, which may also provide better understanding of the pathogenesis of CC. In conclusion, this study demonstrates that 2-DE-based quantitative proteomic approaches are feasible for the discovery of disease biomarkers in bile. SSP411 represents a novel promising potential serum biomarker for CC. A study with a larger series of CC patients, including early stage patients, with a longer follow-up is currently in progress at our center to confirm the diagnostic accuracy and prognostic value of SSP411.Proteomic Study Reveals SSP411 as a CC BiomarkerFigure 6. Validation of the diagnostic value of SSP411 in serum samples using an ELISA. (A). Distribution of the serum OD value in cholangiocarcinoma (CC) patients, patients with benign disease and healthy individuals. (B). Receiver operating characteristic (ROC) analysis for the optimal cut-off point for discrimination between between different groups (CC vs. benign; CC vs. benign+normal; benign vs. normal). (C). Distribution of the serum OD values in hepatocellular carcinoma (HCC) patients, patients with liver cirrhosis and healthy individuals. (D). ROC analysis of SSP411 for HCC. (E). ROC analysis results between different CC and HCC groups. doi:10.1371/journal.pone.0047476.gSupporting InformationFigure S1 BioGPS database analysis shows the tissue distribution of proteins identified by 2-DE. (A) Protein was uniquely expressed in the human liver; (B) another protein was highly expressed in the liver or fetal liver; (C) SSP411 was a male germ cell-enriched gene. (TIF) Figure S2 Immunohistochemical staining of PGAM-1,Table S1 Identification of differentiated proteins using MALDI-TOF/TOF. (XLSX)AcknowledgmentsThe authors thank Professor Jiahao Sha and Professor Zuomin Zhou (Laboratory of Reproductive Medicine, Nanjing Medical University, Nanjing, 210029, China) for their valuable advice in proteomic analysis.PDIA3, HSPD1 and SSP411 in intrahepatic cholangiocarcinoma (IHC) tissues. (TIF)Author 16574785 ContributionsConceived and designed the experiments: XCL XHW FC LYP. Performed the experiments: JS WZW JDW WC BF FQW QYT. Analyzed the data: JS JDW QYT. Contributed reagents/materials/analysis tools: MW JCT QYT. Wrote the paper: JS XCL.Proteomic Study Reveals SSP411 as a CC Biomarker
Ganoderma lucidum is a basidiomycete fungus and has been one of mostly widely used folk remedy in Asia for thousands years. P.R. This study provides the first evidence to suggest that SSP411 is overexpressed in bile from CC patients, suggesting that SSP411 may be a CC-associated biomarker. Promisingly, as a single biomarker, SSP411 could distinguish patients with CC from choledocholithiasis patients and normal individuals, suggesting that SSP411 may represent a potentially useful serum biomarker for the diagnosis of CC (Figure 6). Although the mean serum level of SSP411 in the benign group was higher than in the normal, there was no significant difference between the two groups. The ROC analysis also revealed that the serum level of SSP411 could not effectively differentiate benign disease from the normal individuals (Figure 6B). We speculated that this bias was attributed to the insufficient sample size, especially for the benign group. Similarly, no significant correlation was observed between the serum levels of SSP411 and lymph node metastasis or neural invasion in CC (data not shown), which may also be attributed to the small sample size of the negative patients. Further research is required to characterize the function of SSP411, which may also provide better understanding of the pathogenesis of CC. In conclusion, this study demonstrates that 2-DE-based quantitative proteomic approaches are feasible for the discovery of disease biomarkers in bile. SSP411 represents a novel promising potential serum biomarker for CC. A study with a larger series of CC patients, including early stage patients, with a longer follow-up is currently in progress at our center to confirm the diagnostic accuracy and prognostic value of SSP411.Proteomic Study Reveals SSP411 as a CC BiomarkerFigure 6. Validation of the diagnostic value of SSP411 in serum samples using an ELISA. (A). Distribution of the serum OD value in cholangiocarcinoma (CC) patients, patients with benign disease and healthy individuals. (B). Receiver operating characteristic (ROC) analysis for the optimal cut-off point for discrimination between between different groups (CC vs. benign; CC vs. benign+normal; benign vs. normal). (C). Distribution of the serum OD values in hepatocellular carcinoma (HCC) patients, patients with liver cirrhosis and healthy individuals. (D). ROC analysis of SSP411 for HCC. (E). ROC analysis results between different CC and HCC groups. doi:10.1371/journal.pone.0047476.gSupporting InformationFigure S1 BioGPS database analysis shows the tissue distribution of proteins identified by 2-DE. (A) Protein was uniquely expressed in the human liver; (B) another protein was highly expressed in the liver or fetal liver; (C) SSP411 was a male germ cell-enriched gene. (TIF) Figure S2 Immunohistochemical staining of PGAM-1,Table S1 Identification of differentiated proteins using MALDI-TOF/TOF. (XLSX)AcknowledgmentsThe authors thank Professor Jiahao Sha and Professor Zuomin Zhou (Laboratory of Reproductive Medicine, Nanjing Medical University, Nanjing, 210029, China) for their valuable advice in proteomic analysis.PDIA3, HSPD1 and SSP411 in intrahepatic cholangiocarcinoma (IHC) tissues. (TIF)Author 16574785 ContributionsConceived and designed the experiments: XCL XHW FC LYP. Performed the experiments: JS WZW JDW WC BF FQW QYT. Analyzed the data: JS JDW QYT. Contributed reagents/materials/analysis tools: MW JCT QYT. Wrote the paper: JS XCL.Proteomic Study Reveals SSP411 as a CC Biomarker
Ganoderma lucidum is a basidiomycete fungus and has been one of mostly widely used folk remedy in Asia for thousands years. P.