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Prediction of the risk of harboring prostate cancer by a prebiopsy nomogram based on extended biopsy protocol

机译:基于扩展活检方案的活检前诺模图预测患有前列腺癌的风险

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Objective: We aimed to build a nomogram allowing to predict the probability of prostate cancer (PC) after an initial 21-core biopsy and with readily available clinical data. Methods: 1,490 screened men who underwent an initial 21-core biopsy protocol were included. A multivariate logistic regression was realized including age, prostate volume, prostate-specific antigen (PSA) level, digital rectal examination (DRE) and transrectal ultrasonography (TRUS). Receiver-operating characteristic estimates were used to quantify accuracy of each model. Results: PC was detected in 41.3% of the patients. Median PSA, age and prostate volume were 6.2 ng/ml (range 0.2-50), 64.6 years (range 33-87) and 40 ml (range 10-270), respectively. Abnormal TRUS findings were detected in 14.7% of patients. Age, PSA level, prostate volume, DRE and TRUS were significantly associated with PC (all p ≤ 0.004) in univariable logistic regression analysis. In multivariate logistic regression analysis, significant associations were found for age, PSA level, prostate volume and DRE. Predictive accuracy estimate of this model was equal to 0.70. TRUS was not an independent predictor of PC. Conclusions: We constructed the first prebiopsy predictive nomogram based on an extended 21-core biopsy procedure with age, PSA level, DRE and prostate volume which are readily available clinical data to urologists.
机译:目的:我们旨在建立一个诺模图,以预测最初的21芯活检后的前列腺癌(PC)的可能性,并提供现成的临床数据。方法:纳入1,490名接受初次21芯活检的筛查男性。实现了多元logistic回归,包括年龄,前列腺体积,前列腺特异性抗原(PSA)水平,直肠指检(DRE)和经直肠超声检查(TRUS)。接收者操作特征估计用于量化每个模型的准确性。结果:在41.3%的患者中检测到PC。 PSA中位数,年龄和前列腺体积分别为6.2 ng / ml(范围0.2-50),64.6岁(范围33-87)和40 ml(范围10-270)。在14.7%的患者中发现了TRUS异常发现。在单变量logistic回归分析中,年龄,PSA水平,前列腺体积,DRE和TRUS与PC显着相关(所有p≤0.004)。在多元逻辑回归分析中,发现年龄,PSA水平,前列腺体积和DRE有显着相关性。该模型的预测精度估计等于0.70。 TRUS不是PC的独立预测因子。结论:我们基于年龄,PSA水平,DRE和前列腺体积的扩展的21芯活检程序,构建了第一份活检前预测诺模图,这是泌尿科医师可轻易获得的临床数据。

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