首页> 美国卫生研究院文献>Asian Journal of Andrology >Utility of tissue microarrays for profiling prognostic biomarkers in clinically localized prostate cancer: the expression of BCL-2 E-cadherin Ki-67 and p53 as predictors of biochemical failure after radical prostatectomy with nested control for clinical and pathological risk factors
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Utility of tissue microarrays for profiling prognostic biomarkers in clinically localized prostate cancer: the expression of BCL-2 E-cadherin Ki-67 and p53 as predictors of biochemical failure after radical prostatectomy with nested control for clinical and pathological risk factors

机译:组织芯片在临床局限性前列腺癌中预测预后生物标志物的实用性:BCL-2E-钙粘着蛋白Ki-67和p53的表达可作为根治性前列腺切除术后巢式控制临床和病理风险因素的生化失败的预测指标

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摘要

A cure cannot be assured for all men with clinically localized prostate cancer undergoing radical treatment. Molecular markers would be invaluable if they could improve the prediction of occult metastatic disease. This study was carried out to investigate the expression of BCL-2, Ki-67, p53 and E-cadherin in radical prostatectomy specimens. We sought to assess their ability to predict early biochemical relapse in a specific therapeutic setting. Eighty-two patients comprising 41 case pairs were matched for pathological stage, Gleason grade and preoperative prostate-specific antigen (PSA) concentration. One patient in each pair had biochemical recurrence (defined as PSA ≥ 0.2 ng mL−1 within 2 years of surgery) and the other remained biochemically free of disease (defined as undetectable PSA at least 3 years after surgery). Immunohistochemical analysis was performed to assess marker expression on four replicate tissue microarrays constructed with benign and malignant tissue from each radical prostatectomy specimen. Ki-67, p53 and BCL-2, but not E-cadherin, were significantly upregulated in prostate adenocarcinoma compared with benign prostate tissue (P < 0.01). However, no significant differences in expression of any of the markers were observed when comparing patients who developed early biochemical relapse with patients who had no biochemical recurrence. This study showed that expression of p53, BCL-2 and Ki-67 was upregulated in clinically localized prostate cancer compared with benign prostate tissue, with no alteration in E-cadherin expression. Biomarker upregulation had no prognostic value for biochemical recurrence after radical prostatectomy, even after considering pathological stage, whole tumour Gleason grade and preoperative serum PSA level.
机译:不能保证所有接受根治性治疗的临床局限性前列腺癌男性均能治愈。如果分子标记物可以改善隐匿性转移性疾病的预测,那么它们将是无价的。本研究旨在探讨前列腺癌根治术标本中BCL-2,Ki-67,p53和E-cadherin的表达。我们试图评估他们预测在特定治疗环境中早期生化复发的能力。对包括41个病例对的82例患者进行病理分期,格里森分级和术前前列腺特异性抗原(PSA)浓度匹配。每对中的一名患者发生了生化复发(定义为在手术后2年内PSA≥0.2 ng mL −1 ),另一名患者在生化方面没有疾病(定义为术后至少3年未检测到PSA) )。进行了免疫组织化学分析,以评估由每个前列腺癌根治术标本的良性和恶性组织构成的四个重复组织微阵列上的标志物表达。与良性前列腺组织相比,前列腺腺癌中Ki-67,p53和BCL-2,但不是E-钙黏着蛋白显着上调(P <0.01)。但是,将发生早期生化复发的患者与未发生生化复发的患者进行比较时,未观察到任何标志物的表达差异。这项研究表明,与良性前列腺组织相比,在临床上局限性前列腺癌中p53,BCL-2和Ki-67的表达上调,而E-钙粘蛋白的表达没有改变。即使在考虑病理分期,整个肿瘤的Gleason分级和术前血清PSA水平之后,生物标志物上调对于根治性前列腺切除术后的生化复发没有预后价值。

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