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Should Pathologists Routinely Report Prostate Tumour Volume? The Prognostic Value of Tumour Volume in Prostate Cancer

机译:病理学家应常规报告前列腺肿瘤量吗?肿瘤体积在前列腺癌中的预后价值

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Background: The independent prognostic value of tumour volume in radical prostatectomy (RP) specimens is controversial, and it remains a matter of debate whether pathologists should report a measure of tumour volume. In addition, tumour volume might be of value in substaging of pathologic tumour stage (pT2) prostate cancer (PCa). Objective: To assess the prognostic value of PCa tumour volume. Design, setting, and participants: The cohort consisted of 344 participants in the European Randomised Study of Screening for Prostate Cancer (ERSPC), Rotterdam section, whose PCa was treated with RP. Mean time of follow-up was 96.2 mo. Measurements: Tumour volume was measured in totally embedded RP specimens with a morphometric, computer-assisted method and assessed as a continuous variable, as relative tumour volume (tumour volume divided by prostate volume), and in a binary fashion (>0.5 ml or <0.5 ml). These variables were related to prostate-specific antigen (PSA) progression, local recurrence, or distant metastasis and PCa-related mortality using univariate and multivariable Cox proportional hazards analyses. The analyses were repeated in the subgroup with pT2 tumours. Results and limitations: Tumour volume was related to tumour stage, Gleason score, seminal vesicle invasion (SVI), and surgical margin status. In univariate analyses, tumour volume and relative tumour volume were predictive for all outcome variables. In multivariable analyses, including age, tumour stage, Gleason score, SVI, and surgical margin status, neither tumour volume nor relative volume were independent predictors of progression or mortality. Tumour volume >0.5 ml was predictive for PSA recurrence and local and/or distant progression in univariate analyses but not in multivariable analyses. Tumour volume was not predictive for recurrence or mortality in univariate or multivariable analyses in the pT2 subgroup. Conclusions: Tumour volume did not add prognostic value to routinely assessed pathologic parameters. Therefore, there seems to be little reason to routinely measure tumour volume in RP specimens.
机译:背景:根治性前列腺切除术(RP)标本中肿瘤体积的独立预后价值存在争议,病理学家是否应报告肿瘤体积的测量值尚有争议。另外,肿瘤体积可能在病理性肿瘤分期(pT2)前列腺癌(PCa)的分期中具有价值。目的:评估PCa肿瘤体积的预后价值。设计,背景和参加者:该队列由344名参加欧洲鹿特丹前列腺癌筛查随机研究(ERSPC)的参与者组成,该研究的PCa经过RP治疗。平均随访时间为96.2 mo。测量:使用形态计量学,计算机辅助方法在完全包埋的RP标本中测量肿瘤体积,并以连续变量,相对肿瘤体积(肿瘤体积除以前列腺体积)和二进制形式(> 0.5 ml或< 0.5毫升)。使用单变量和多变量Cox比例风险分析,这些变量与前列腺特异性抗原(PSA)的进展,局部复发或远处转移以及PCa相关的死亡率有关。在患有pT2肿瘤的亚组中重复进行分析。结果与局限性:肿瘤体积与肿瘤分期,格里森评分,精囊浸润(SVI)和手术切缘状态有关。在单变量分析中,肿瘤体积和相对肿瘤体积可预测所有结果变量。在多变量分析中,包括年龄,肿瘤分期,格里森评分,SVI和手术切缘情况,肿瘤体积和相对体积均不是进展或死亡率的独立预测因子。 > 0.5 ml的肿瘤体积在单变量分析中可预测PSA复发以及局部和/或远处进展,但在多变量分析中则不可预测。在pT2亚组的单变量或多变量分析中,肿瘤体积不能预测复发或死亡。结论:肿瘤体积并未增加常规评估的病理学参数的预后价值。因此,似乎没有理由定期测量RP标本中的肿瘤体积。

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