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PSGR and PCA3 as biomarkers for the detection of prostate cancer in urine.

机译:PSGR和PCA3作为检测尿液中前列腺癌的生物标志物。

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摘要

BACKGROUND: Several studies have demonstrated the usefulness of monitoring an RNA transcript in urine, such as PCA3, for prostate cancer (PCa) diagnosis. PCa screening would benefit from additional biomarkers of higher specificity and could be used in conjunction with prostate-specific antigen (PSA) testing, in order to better determine biopsy candidates. METHODS: We used urine sediments after prostate massage (PM) from 215 consecutive patients, who presented for prostate biopsy. We tested whether prostate-specific G-protein coupled receptor (PSGR), a biomarker previously described to be over-expressed in PCa tissue, could also be detected by quantitative real-time PCR in post-PM urine sediment. We combined these findings with prostate cancer gene 3 (PCA3), the current gold standard for PCa diagnosis in urine, to test if a combination of both biomarkers could improve the sensitivity of PCA3 alone. RESULTS: By univariate analysis we found that PSGR and PCA3 were significant predictors of PCa. Receiver operator characteristic curve analysis and its multivariate extension, multivariate ROC (MultiROC), were used to assess the outcome predictive values of the individual and the paired biomarkers. We obtained the following area under the curve values: PSA (0.602), PSGR (0.681), PCA3 (0.656), and PSGRvPCA3 (0.729). Then, we tested whether a combination of PSGR and PCA3 could improve specificity by fixing the sensitivity at 95%. We obtained specificities of 15% (PSGR), 17% (PCA3), and 34% (PSGRvPCA3). CONCLUSIONS: A multiplexed model including PSGR and PCA3 improves the specificity for the detection of PCa, especially in the area of high sensitivity. This could be clinically useful for determining which patients should undergo biopsy.
机译:背景:多项研究表明,监测尿液中PCA3等RNA转录本对前列腺癌(PCa)诊断的有用性。 PCa筛查将受益于更高特异性的其他生物标志物,并可与前列腺特异性抗原(PSA)测试结合使用,以更好地确定活检候选物。方法:我们对215例连续进行前列腺穿刺活检的患者进行了前列腺按摩(PM)后使用了尿沉渣。我们测试了前列腺特异性G蛋白偶联受体(PSGR)(一种先前描述在PCa组织中过表达的生物标记)是否也可以通过定量实时PCR在PM后尿液沉积物中检测到。我们将这些发现与前列腺癌基因3(PCA3)(目前尿液中PCa诊断的金标准)结合起来,以测试两种生物标记物的组合是否可以单独改善PCA3的敏感性。结果:通过单因素分析,我们发现PSGR和PCA3是PCa的重要预测因子。接收者操作者特征曲线分析及其多元扩展,多元ROC(MultiROC)被用于评估个体和配对生物标志物的结果预测值。我们在曲线值下获得了以下区域:PSA(0.602),PSGR(0.681),PCA3(0.656)和PSGRvPCA3(0.729)。然后,我们测试了PSGR和PCA3的组合能否通过将灵敏度固定在95%来提高特异性。我们获得了15%(PSGR),17%(PCA3)和34%(PSGRvPCA3)的特异性。结论:PSGR和PCA3的多重模型提高了PCa检测的特异性,特别是在高灵敏度领域。这对于确定哪些患者应进行活检可能在临床上有用。

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