Castellani Daniele, Pace Gianna, Cecchini Sara, Franzese Carmine, Cicconofri Andrea, Romagnoli Daniele, Del Rosso Alessandro, Possanzini Marco, Paci Enrico, Dellabella Marco, Pierangeli Tiziana
Unit of Urology, IRCCS INRCA, Ancona, Italy; Ph.D. Program, Faculty of Medicine, School of Urology, Polytechnic University of the Marche Region, Ancona, Italy.
Unit of Urology, ULSS 3 Serenissima, Dolo, Italy.
Urol Oncol. 2022 Oct;40(10):452.e9-452.e16. doi: 10.1016/j.urolonc.2022.06.011. Epub 2022 Jul 21.
To assess predictors of clinically significant (cs) prostate cancer (PCa) in men who had a non-malignant Multiparametric magnetic resonance imaging (mpMRI)-targeted biopsy and persistent Prostate Imaging-Reporting Data System (PI-RADS) 3 to 5 lesions in subsequent mpMRI.
We retrospectively analyzed MRI-targeted biopsy database in three centers.
persistence of at least one PI-RADS ≥3 lesion found negative for cancer in a previous MRI-targeted plus systemic biopsy (baseline biopsy).
downgrading to PI-RADS 1-2. A logistic regression analysis was performed to estimate the predictors of csPCa.
Fifty-seven patients were included. Median interval between biopsies was 12.9(2.43) months. Median age was 68.0(12) years. Median PSA was 7.0(5.45) ng/ml. At follow-up, 24.6%, 54.4%, and 21% of patients had a PI-RADS score 3, 4, and 5 index lesion (IL), respectively. At re-biopsy, 28/57(49.1%) men were found to harbor PCa. Among these, 22(78.6%) had csPCa. csPCa was found outside the IL in only 2 patients. Eleven, 13, and 5 patients with PI-RADS 3, 4, and 5, respectively, had no cancer. Three patients with a PI-RADS 3 lesion had cancer (2 with Gleason score 3+3, 1 with Gleason score 3+4). 14/43 men with a PI-RADS 4/5 lesion harbored Gleason score ≥3+4 PCa. Logistic regression analysis found that PSA (HR 1.281, 95% CI: 1.013-1.619, P = 0.039) and IL size (HR 1.146, 95% CI: 1.018-1.268, P = 0.041) were the predictors of csPCa at re-biopsy.
Patients with non-malignant pathology from PI-RADS ≥3 lesions targeted biopsy should be follow-up with mpMRI, and those with persistent PI-RADS 4 to 5 lesions should repeat MRI-targeted and systematic biopsy.
评估在接受非恶性多参数磁共振成像(mpMRI)靶向活检且后续mpMRI中持续存在前列腺影像报告和数据系统(PI-RADS)3至5类病变的男性中,具有临床意义(cs)的前列腺癌(PCa)的预测因素。
我们回顾性分析了三个中心的MRI靶向活检数据库。
在先前的MRI靶向联合系统活检(基线活检)中发现至少一个PI-RADS≥3类病变为癌症阴性且持续存在。
病变降级为PI-RADS 1-2类。进行逻辑回归分析以评估csPCa的预测因素。
共纳入57例患者。两次活检之间的中位间隔时间为12.9(2.43)个月。中位年龄为68.0(12)岁。中位前列腺特异性抗原(PSA)为7.0(5.45)ng/ml。在随访中,分别有24.6%、54.4%和21%的患者的PI-RADS评分为3、4和5类索引病变(IL)。再次活检时,57例中有28例(49.1%)男性被发现患有PCa。其中,22例(78.6%)患有csPCa。仅2例患者在IL以外发现csPCa。分别有11例、13例和5例PI-RADS 3、4和5类病变的患者未患癌症。3例PI-RADS 3类病变的患者患有癌症(2例Gleason评分3+3,1例Gleason评分3+4)。14/43例PI-RADS 4/5类病变的男性患有Gleason评分≥3+4的PCa。逻辑回归分析发现,PSA(风险比[HR] 1.281,95%置信区间[CI]:1.013-1.619,P = 0.039)和IL大小(HR 1.146,95% CI:1.018-1.268,P = 0.041)是再次活检时csPCa的预测因素。
来自PI-RADS≥3类病变靶向活检且病理结果为非恶性的患者应接受mpMRI随访,而PI-RADS 4至5类病变持续存在的患者应重复进行MRI靶向和系统活检。
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