Seminal plasma as a source of prostate cancer peptide biomarker

Plos One · Jan 2013

Seminal plasma as a source of prostate cancer peptide biomarker candidates for detection of indolent and advanced disease.

Extensive prostate specific antigen screening for prostate cancer generates a high number of unnecessary biopsies and over-treatment due to insufficient differentiation between indolent and aggressive tumours. We hypothesized that seminal plasma is a robust source of novel prostate cancer (PCa) biomarkers with the potential to improve primary diagnosis of and to distinguish advanced from indolent disease. ⋯ Seminal plasma represents a robust source of potential peptide makers for primary PCa diagnosis. Our findings warrant further prospective validation to confirm the diagnostic potential of identified seminal biomarker candidates.

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- Jochen Neuhaus, Eric Schiffer, Philine von Wilcke, Hartwig W Bauer, Hing Leung, Justyna Siwy, Wolfram Ulrici, Uwe Paasch, Lars-Christian Horn, and Jens-Uwe Stolzenburg.
- University of Leipzig, Department of Urology, Leipzig, Germany. jochen.neuhaus@medizin.uni-leipzig.de
- Plos One. 2013 Jan 1; 8 (6): e67514.
BackgroundExtensive prostate specific antigen screening for prostate cancer generates a high number of unnecessary biopsies and over-treatment due to insufficient differentiation between indolent and aggressive tumours. We hypothesized that seminal plasma is a robust source of novel prostate cancer (PCa) biomarkers with the potential to improve primary diagnosis of and to distinguish advanced from indolent disease.Methodology/Principal FindingsIn an open-label case/control study 125 patients (70 PCa, 21 benign prostate hyperplasia, 25 chronic prostatitis, 9 healthy controls) were enrolled in 3 centres. Biomarker panels a) for PCa diagnosis (comparison of PCa patients versus benign controls) and b) for advanced disease (comparison of patients with post surgery Gleason score <7 versus Gleason score >7) were sought. Independent cohorts were used for proteomic biomarker discovery and testing the performance of the identified biomarker profiles. Seminal plasma was profiled using capillary electrophoresis mass spectrometry. Pre-analytical stability and analytical precision of the proteome analysis were determined. Support vector machine learning was used for classification. Stepwise application of two biomarker signatures with 21 and 5 biomarkers provided 83% sensitivity and 67% specificity for PCa detection in a test set of samples. A panel of 11 biomarkers for advanced disease discriminated between patients with Gleason score 7 and organ-confined (Conclusions/SignificanceSeminal plasma represents a robust source of potential peptide makers for primary PCa diagnosis. Our findings warrant further prospective validation to confirm the diagnostic potential of identified seminal biomarker candidates.

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Seminal plasma as a source of prostate cancer peptide biomarker candidates for detection of indolent and advanced disease.

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