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Predicting biochemical recurrence after radical prostatectomy for patients with organ-confined disease using p27 expression.

机译:使用p27表达预测前列腺癌根治术后器官受限疾病患者的生化复发。

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OBJECTIVES: It is unclear why men who undergo radical prostatectomy (RP) and are found to have pathologically organ-confined disease develop prostate-specific antigen (PSA) recurrences. We previously found that patients with less than 45% of cells in the prostate needle biopsy specimen (PNBx) staining positive for the cell cycle regulator p27 had a significantly increased risk of biochemical recurrence after RP. We sought to determine whether p27 staining in the PNBx specimen might serve as a molecular marker for PSA failure in the subset of patients who develop PSA recurrence despite organ-confined disease at RP. METHODS: The PNBx specimens of 161 men treated with RP between 1991 and 2000 were examined for p27 expression using immunohistochemistry. The p27 cutpoint of less than 45% expression was used to define the high and low-risk categories. Patients were separated into two groups for analysis: organ-confined (pT2 and negative surgical margins) and non-organ-confined (pT2 with positive surgical margins, pT3, pT4, or lymph node involvement). The mean and median follow-up for patients with organ-confined and non-organ-confined disease was 47 and 43 months and 42 and 38 months, respectively. Multivariate Cox proportional hazards analysis was used to examine the preoperative clinical variables that were the strongest predictors of biochemical recurrence after RP among each group. RESULTS: Among organ-confined patients, p27 expression was the only significant independent predictor of the time to biochemical recurrence after RP (hazard ratio 5.15, 95% confidence interval 1.41 to 18.83, P = 0.013). Among patients with non-organ-confined disease, the percentage of biopsy tissue with cancer, biopsy Gleason score, and PSA level were independent predictors of PSA recurrence. p27 expression was not a significant independent predictor of PSA recurrence among men with non-organ-confined disease. CONCLUSIONS: p27 expression in the PNBx was a significant independent predictor of PSA failure for patients with pathologically organ-confined disease, but not for those with non-organ-confined disease. Patients with organ-confined disease but low p27 expression had a greater than fivefold risk of developing PSA recurrence than were men with high p27 expression, suggesting that p27 may be a molecular marker associated with micrometastatic disease at the time of RP.
机译:目的:目前尚不清楚为什么进行根治性前列腺切除术(RP)并被发现患有病理器官受限疾病的男性会发展为前列腺特异性抗原(PSA)复发。我们先前发现前列腺细胞穿刺活检标本(PNBx)中细胞周期调节剂p27染色阳性的细胞少于45%的患者,RP后生化复发的风险显着增加。我们试图确定PNBx标本中的p27染色是否可作为RP的器官受限疾病而发生PSA复发的患者亚组中PSA失败的分子标记。方法:采用免疫组织化学方法检测了1991年至2000年间接受RP治疗的161名男性的PNBx标本中p27的表达。小于45%表达的p27临界点用于定义高风险和低风险类别。将患者分为两组进行分析:器官受限(pT2和手术切缘阴性)和非器官受限(pT2且手术切缘阳性,pT3,pT4或淋巴结受累)。器官合并和非器官合并疾病患者的平均随访和中位随访分别为47个月和43个月,42个月和38个月。多变量Cox比例风险分析用于检查术前临床变量,这些变量是各组中RP后生化复发的最强预测因子。结果:在器官受限患者中,p27表达是RP后生化复发时间的唯一重要独立预测因子(危险比5.15,95%置信区间1.41至18.83,P = 0.013)。在非器官受限疾病患者中,癌症活检组织百分比,活检格里森评分和PSA水平是PSA复发的独立预测因子。在非器官受限疾病男性中,p27表达不是PSA复发的重要独立预测因子。结论:PNBx中的p27表达是病理性器官受限疾病患者的PSA衰竭的重要独立预测因子,但对于非器官受限疾病患者则不是。患有器官受限疾病但p27表达低的患者发生PSA复发的风险比具有高p27表达的男性高五倍,这表明p27可能是RP时与微转移性疾病相关的分子标记。

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