Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum.

Timo Piironen; Alexander Haese; Hartwig Huland; Thomas Steuber; Ib Jarle Christensen; Nils Brünner; Keld Danø; Gunilla Høyer-Hansen; Hans Lilja

Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum.

Standard

Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum. / Piironen, Timo; Haese, Alexander; Huland, Hartwig; Steuber, Thomas; Christensen, Ib Jarle; Brünner, Nils; Danø, Keld; Høyer-Hansen, Gunilla; Lilja, Hans.

in: CLIN CHEM, Jahrgang 52, Nr. 5, 5, 2006, S. 838-844.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Piironen, T, Haese, A, Huland, H, Steuber, T, Christensen, IJ, Brünner, N, Danø, K, Høyer-Hansen, G & Lilja, H 2006, 'Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum.', CLIN CHEM, Jg. 52, Nr. 5, 5, S. 838-844. <http://www.ncbi.nlm.nih.gov/pubmed/16543389?dopt=Citation>

APA

Piironen, T., Haese, A., Huland, H., Steuber, T., Christensen, I. J., Brünner, N., Danø, K., Høyer-Hansen, G., & Lilja, H. (2006). Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum. CLIN CHEM, 52(5), 838-844. [5]. http://www.ncbi.nlm.nih.gov/pubmed/16543389?dopt=Citation

Vancouver

Piironen T, Haese A, Huland H, Steuber T, Christensen IJ, Brünner N et al. Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum. CLIN CHEM. 2006;52(5):838-844. 5.

Bibtex

@article{2b6bf138ec3140fe8a942a8a9c539ca0,

title = "Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum.",

abstract = "BACKGROUND: Early detection of prostate cancer (PCa) centers on measurements of prostate-specific antigen (PSA), but current testing practices suffer from lack of specificity and generate many unnecessary prostate biopsies. Soluble urokinase plasminogen activator receptor (uPAR) is present in blood in both intact and cleaved forms. Increased uPAR in blood is correlated with poor prognosis in various cancers, but uPAR has not been shown to be useful in PCa diagnostics. We assessed the ability of immunoassays for specific uPAR forms to discriminate PCa from benign conditions. METHODS: We measured total PSA (tPSA), free PSA (fPSA), intact uPAR [uPAR(I-III)], intact uPAR + cleaved uPAR domains II+III [uPAR(I-III) + uPAR(II-III)], and cleaved uPAR domain I [uPAR(I)] in sera from 224 men with and 166 men without PCa. We assessed differences in serum concentrations between the PCa and noncancer groups within the entire cohort and in men with tPSA concentrations of 2-10 microg/L. The diagnostic accuracy of individual analytes and analyte combinations was explored by logistic regression and ROC analyses and evaluations of sensitivity and specificity pairs. RESULTS: Serum uPAR(I) and uPAR(II-III) were higher in PCa than in benign disease. In men with tPSA between 2 and 10 microg/L, the combination of %fPSA with the ratio uPAR(I)/uPAR(I-III) had a greater area under the ROC curve (0.73) than did %fPSA (0.68). CONCLUSIONS: Specific measurements of different uPAR forms in serum improve the specificity of PCa detection. The uPAR forms may therefore be complementary to PSA for PCa detection, most importantly in men with moderately increased PSA.",

author = "Timo Piironen and Alexander Haese and Hartwig Huland and Thomas Steuber and Christensen, {Ib Jarle} and Nils Br{\"u}nner and Keld Dan{\o} and Gunilla H{\o}yer-Hansen and Hans Lilja",

year = "2006",

language = "Deutsch",

volume = "52",

pages = "838--844",

journal = "CLIN CHEM",

issn = "0009-9147",

publisher = "American Association for Clinical Chemistry Inc.",

number = "5",

}

RIS

TY - JOUR

T1 - Enhanced discrimination of benign from malignant prostatic disease by selective measurements of cleaved forms of urokinase receptor in serum.

AU - Piironen, Timo

AU - Haese, Alexander

AU - Huland, Hartwig

AU - Steuber, Thomas

AU - Christensen, Ib Jarle

AU - Brünner, Nils

AU - Danø, Keld

AU - Høyer-Hansen, Gunilla

AU - Lilja, Hans

PY - 2006

Y1 - 2006

N2 - BACKGROUND: Early detection of prostate cancer (PCa) centers on measurements of prostate-specific antigen (PSA), but current testing practices suffer from lack of specificity and generate many unnecessary prostate biopsies. Soluble urokinase plasminogen activator receptor (uPAR) is present in blood in both intact and cleaved forms. Increased uPAR in blood is correlated with poor prognosis in various cancers, but uPAR has not been shown to be useful in PCa diagnostics. We assessed the ability of immunoassays for specific uPAR forms to discriminate PCa from benign conditions. METHODS: We measured total PSA (tPSA), free PSA (fPSA), intact uPAR [uPAR(I-III)], intact uPAR + cleaved uPAR domains II+III [uPAR(I-III) + uPAR(II-III)], and cleaved uPAR domain I [uPAR(I)] in sera from 224 men with and 166 men without PCa. We assessed differences in serum concentrations between the PCa and noncancer groups within the entire cohort and in men with tPSA concentrations of 2-10 microg/L. The diagnostic accuracy of individual analytes and analyte combinations was explored by logistic regression and ROC analyses and evaluations of sensitivity and specificity pairs. RESULTS: Serum uPAR(I) and uPAR(II-III) were higher in PCa than in benign disease. In men with tPSA between 2 and 10 microg/L, the combination of %fPSA with the ratio uPAR(I)/uPAR(I-III) had a greater area under the ROC curve (0.73) than did %fPSA (0.68). CONCLUSIONS: Specific measurements of different uPAR forms in serum improve the specificity of PCa detection. The uPAR forms may therefore be complementary to PSA for PCa detection, most importantly in men with moderately increased PSA.

AB - BACKGROUND: Early detection of prostate cancer (PCa) centers on measurements of prostate-specific antigen (PSA), but current testing practices suffer from lack of specificity and generate many unnecessary prostate biopsies. Soluble urokinase plasminogen activator receptor (uPAR) is present in blood in both intact and cleaved forms. Increased uPAR in blood is correlated with poor prognosis in various cancers, but uPAR has not been shown to be useful in PCa diagnostics. We assessed the ability of immunoassays for specific uPAR forms to discriminate PCa from benign conditions. METHODS: We measured total PSA (tPSA), free PSA (fPSA), intact uPAR [uPAR(I-III)], intact uPAR + cleaved uPAR domains II+III [uPAR(I-III) + uPAR(II-III)], and cleaved uPAR domain I [uPAR(I)] in sera from 224 men with and 166 men without PCa. We assessed differences in serum concentrations between the PCa and noncancer groups within the entire cohort and in men with tPSA concentrations of 2-10 microg/L. The diagnostic accuracy of individual analytes and analyte combinations was explored by logistic regression and ROC analyses and evaluations of sensitivity and specificity pairs. RESULTS: Serum uPAR(I) and uPAR(II-III) were higher in PCa than in benign disease. In men with tPSA between 2 and 10 microg/L, the combination of %fPSA with the ratio uPAR(I)/uPAR(I-III) had a greater area under the ROC curve (0.73) than did %fPSA (0.68). CONCLUSIONS: Specific measurements of different uPAR forms in serum improve the specificity of PCa detection. The uPAR forms may therefore be complementary to PSA for PCa detection, most importantly in men with moderately increased PSA.

M3 - SCORING: Zeitschriftenaufsatz

VL - 52

SP - 838

EP - 844

JO - CLIN CHEM

JF - CLIN CHEM

SN - 0009-9147

IS - 5

M1 - 5

ER -