4.1 Article

Discovery and validation of urinary biomarkers for propstate cancer

Journal

PROTEOMICS CLINICAL APPLICATIONS
Volume 2, Issue 4, Pages 556-570

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/prca.200780082

Keywords

capillary electrophoresis; diagnosis; mass spectrometry; prostate carcinoma; urine

Funding

  1. NCI NIH HHS [P01 CA104106-02, P01 CA104106-01A2, P01 CA104106-04, P01 CA104106-03, P01 CA104106] Funding Source: Medline
  2. NIGMS NIH HHS [R01 GM080148-02, R01 GM080148, T32 GM008349, T32 GM008349-20, R01 GM080148-01A1] Funding Source: Medline

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Only 30% of patients with elevated serum prostate specific antigen (PSA) levels who undergo prostate biopsy are diagnosed with prostate cancer (PCa). Novel methods are needed to reduce the number of unnecessary biopsies. We report on the identification and validation of a panel of 12 novel biomarkers for prostate cancer (PCaP), using CE coupled MS. The biomarkers could be defined by comparing first void urine of 51 men with PCa and.35 with negative prostate biopsy. In contrast, midstream urine samples did not allow the identification of discriminatory molecules, suggesting that prostatic fluids may be the source of the defined biomarkers. Consequently, first void urine samples were tested for sufficient amounts of prostatic fluid, using a prostatic fluid indicative panel (informative polypeptide panel; IPP). A combination of IPP and PCaP to predict positive prostate biopsy was evaluated in a blinded prospective study. Two hundred thirteen of 264 samples matched the IPP criterion. PCa was detected with 89% sensitivity, 5 1% specificity. Including age and percent free PSAto the proteomic signatures resulted in 91% sensitivity, 69% specificity.

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