Identification of Clinically Significant Prostate Cancer by Combined PCA3 and AMACR mRNA Detection in Urine Samples

Elena S Kotova; Yulia A Savochkina; Yuriy V Doludin; Alexander O Vasilyev; Elena A Prilepskay; Natalia V Potoldykova; Konstantin A Babalyan; Alexandra V Kanygina; Andrey O Morozov; Alexander V Govorov; Dmitry V Enikeev; Elena S Kostryukova; Elena N Ilina; Vadim M Govorun; Dmitry Y Pushkar; Elena I Sharova

摘要

Purpose: Preclinical evaluation of PCA3 and AMACR transcript simultaneous detection in urine to diagnose clinical significant prostate cancer (prostate cancer with Gleason score ≥ 7) in a Russian cohort. Patients and Methods: We analyzed urine samples of patients with a total serum PSA ≥ 2 ng/mL: 31 men with prostate cancer scheduled for radical prostatectomy, 128 men scheduled for first diagnostic biopsy (prebiopsy cohort). PCA3 , AMACR , PSA and GPI transcripts were detected by multiplex reverse transcription quantitative polymerase chain reaction, and the results were used for scores for calculation and statistical analysis. Results: There was no significant difference between clinically significant and nonsignificant prostate cancer PCA3 scores. However, there was a significant difference in the AMACR score (patients scheduled for radical prostatectomy p =0.0088, prebiopsy cohort p =0.029). We estimated AUCs, optimal cutoffs, sensitivities and specificities for PCa and csPCa detection in the prebiopsy cohort by tPSA, PCA3 score, PCPT Risk Calculator and classification models based on tPSA, PCA3 score and AMACR score. In the clinically significant prostate cancer ROC analysis, the PCA3 score AUC was 0.632 (95%CI: 0.511– 0.752), the AMACR score AUC was 0.711 (95%CI: 0.617– 0.806) and AUC of classification model based on the PCA3 score, the AMACR score and total PSA was 0.72 (95%CI: 0.58– 0.83). In addition, the correlation of the AMACR score with the ratio of total RNA and RNA of prostate cells in urine was shown (tau=0.347, p =6.542e– 09). Significant amounts of nonprostate RNA in urine may be a limitation for the AMACR score use. Conclusion: The AMACR score is a good predictor of clinically significant prostate cancer. Significant amounts of nonprostate RNA in urine may be a limitation for the AMACR score use. Evaluation of the AMACR score and classification models based on it for clinically significant prostate cancer detection with larger samples and a follow-up analysis is promising.

机译：目的：PCA3和AMACR转录物同时检测尿液中的临床前评价，以诊断俄罗斯队列中临床显着的前列腺癌（GROSEASE评分≥7）。患者及方法：我们分析了总血清PSA≥2ng/ ml的患者尿液样本：31名男性预定用于自由基前列腺切除术的前列腺癌，128名调度用于第一次诊断活检（PREBIOPSY COHORT）。通过多重逆转录定量聚合酶链反应检测PCA3，amacR，PSA和GPI转录物，结果用于计算和统计分析的分数。结果：临床显着和无情的前列腺癌PCA3分数之间没有显着差异。然而，AMACR评分存在显着差异（预定自由基前列腺切除术的患者P = 0.0088，P6 = 0.029）。通过TPSA，PCA3得分，PCPT风险计算器和基于TPSA，PCA3得分和AMACR评分，我们估计了PCA和CSPCA检测的AUC，PCA和CSPCA检测特异性，PCAT风险计算器和分类模型。在临床显着的前列腺癌ROC分析中，PCA3得分AUC为0.632（95％CI：0.511- 0.752），AMACR得分AUC为0.711（95％CI：0.617- 0.806）和基于PCA3得分的分类模型的AUC ，AMACR得分和总PSA为0.72（95％CI：0.58- 0.83）。此外，显示了尿液中前列腺细胞总RNA和RNA比率的相关性的相关性（Tau = 0.347，P = 6.542E-09）。尿液中大量的未突出量RNA可能是AMACR评分使用的限制。结论：AMACR评分是临床显着的前列腺癌的良好预测因子。尿液中大量的未突出量RNA可能是AMACR评分使用的限制。基于较大样本的临床显着的前列腺癌检测的基于临床显着的前列腺癌检测的评估和随访分析是有前途的。

Identification of Clinically Significant Prostate Cancer by Combined PCA3 and AMACR mRNA Detection in Urine Samples

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