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MUC1 expression in incidental prostate cancer predicts staging and grading on the subsequent radical prostatectomy.

机译:MUC1在偶然的前列腺癌中的表达预示了随后的前列腺癌根治术的分期和分级。

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The behavior of Incidental prostate cancer (IPC) cannot be reliably predicted by means of conventional histomorphology. MUC1 (episialin) expression has been linked to poor outcome in peripheral prostate cancer (PC). We aimed to determine the so far neglected prognostic role of MUC1 expression in IPC which most commonly represents transition zone cancer. Using Tissue microarray (TMA), we assessed the association between MUC1 expression recorded in transurethral resection specimens of the prostate (TURP chips) and histopathologic outcome parameters (Gleason scores and histologic staging) performed on the subsequent radical prostatectomies (RPs) in a study cohort of 54 patients. Due to tissue loss during arraying and sectioning, a total of 44 (81.5%) tumor samples remained available for immunostaining which was dichotomized by two independent clinical pathologists as being absent or present. MUC1 expression was present in 7 (15.9%) of the 44 IPC immunohistochemically investigated with a striking over-representation in high stage tumors, and was significantly correlated with histopathologic staging (rho = 0.4; p = 0.02) and Gleason scores (rho = 0.3; p = 0.03) performed on the corresponding RPs. These data were confirmed by means of the McNemar test (staging: p = 0.01; grading: p = 0.04). Our findings suggest that MUC1 might become a valuable adjunct to enable individual prognostic ramification prior to radical surgery in prostate cancer histologically detected in TURP chips. This interesting observation clearly awaits validation by larger studies surveying clinical follow-up data.
机译:不能通过常规组织形态学可靠地预测偶然性前列腺癌(IPC)的行为。 MUC1(episialin)表达与外周前列腺癌(PC)不良预后相关。我们旨在确定迄今为止在IPC中MUC1表达被忽视的预后作用,而IPC最常代表过渡区癌。使用组织芯片(TMA),我们评估了研究队列中经尿道前列腺电切术标本(TURP芯片)中记录的MUC1表达与随后进行的根治性前列腺切除术(RPs)进行的组织病理学结果参数(格里森评分和组织学分期)之间的关联54位患者中。由于在排列和切片过程中组织损失,总共有44个(81.5%)肿瘤样品可用于免疫染色,由两名独立的临床病理学家将其分为或不存在。 MUC1表达存在于44个IPC免疫组织化学研究中的7个(15.9%)中,在晚期肿瘤中明显超标,并且与组织病理学分期(rho = 0.4; p = 0.02)和格里森评分(rho = 0.3)显着相关; p = 0.03)在相应的RP上执行。这些数据通过McNemar检验得到证实(阶段:p = 0.01;等级:p = 0.04)。我们的研究结果表明,MUC1可能成为有价值的辅助手段,以使根治性手术之前在TURP芯片中进行组织学检测的前列腺癌患者能够进行个体预后评估。这项有趣的观察显然等待大型研究的临床随访数据的验证。

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