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首页> 外文期刊>Seminars in Urologic Oncology >Pretreatment prostate-specific antigen and Gleason score predict the risk of extracapsular extension and the risk of failure following radiotherapy in patients with clinically localized prostate cancer.
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Pretreatment prostate-specific antigen and Gleason score predict the risk of extracapsular extension and the risk of failure following radiotherapy in patients with clinically localized prostate cancer.

机译:前列腺特异性抗原的预处理和Gleason评分可预测临床局限性前列腺癌患者放疗后囊外扩张的风险和失败的风险。

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摘要

The purpose of this study is to evaluate the use of a relatively simple equation for predicting the risk of extracapsular extension (ECE) based on the pretreatment prostate-specific antigen (PSA) and Gleason score (GS) in patients with clinically localized prostate cancer. Three hundred and seventy-four patients who underwent radical prostatectomy between 1988 and 1994 and 521 men undergoing definitive radiotherapy during a similar time period were eligible for this analysis. Surgically treated patients were considered eligible if the pathological stage, preoperative PSA, and GS were available. Among these patients, the median preoperative PSA was 8.1 ng/mL (range, 0 to 195 ng/mL), and the median preoperative GS was 6 (range, 2 to 10). The empirically derived equation tested was (1.5 x PSA + [GS - 3] x 10). For this equation, the range of calculated risk was limited to 0% to 100%. Using the empirically derived equation, patients with a low calculated risk (CR) of < or = 33% had an average calculated risk (ACR) of 21.9% and an observed incidence (OI) of ECE was 17.8%. Patients with a moderate CR of 34% to 66% had an ACR of 46.3%, and an OI of ECE was 46.7%. Patients with a CR of 67% to 100% had an ACR of 83.7% and an OI of ECE of 66.7%. Of the 21 patients who had a PSA < or = 4 and a GS < or = 4, only 1 patient (4.8%) was found to have ECE. Men with an estimated risk of ECE of <33%, 33% to 67%, and >67% had a 4-year risk of biochemical failure following radiotherapy of 29%, 56%, and 78% (P < .00001). This empirically derived data appears to be reasonably accurate at estimating the incidence of ECE in patients with at low or intermediate risk before surgery. The risk of biochemical failure following radiotherapy also correlated the risk of ECE. Future staging systems for prostate cancer should use similar approach for defining risk groups.
机译:这项研究的目的是评估在临床局部前列腺癌患者中基于治疗前前列腺特异性抗原(PSA)和格里森评分(GS)的相对简单的方程式,用于预测囊外扩张(ECE)风险的用途。 1988年至1994年间接受根治性前列腺切除术的374例患者和521例在相同时间段接受了明确放疗的男性符合此分析的条件。如果有病理分期,术前PSA和GS,则认为手术治疗的患者合格。在这些患者中,术前PSA的中位数为8.1 ng / mL(范围为0至195 ng / mL),术前GS的中位数为6(范围为2至10)。测试的根据经验得出的方程为(1.5 x PSA + [GS-3] x 10)。对于此等式,计算的风险范围限制为0%至100%。使用根据经验得出的方程式,低计算风险(CR)<或= 33%的患者的平均计算风险(ACR)为21.9%,观察到的ECE发生率(OI)为17.8%。中度CR为34%至66%的患者的ACR为46.3%,ECE的OI为46.7%。 CR为67%到100%的患者的ACR为83.7%,ECI的OI为66.7%。在21名PSA <或= 4和GS <或= 4的患者中,只有1例(4.8%)被发现患有ECE。估计ECE风险<33%,33%至67%和> 67%的男性在放疗后发生生化衰竭的4年风险为29%,56%和78%(P <.00001)。根据经验得出的数据似乎在估计术前低或中等风险患者的ECE发生率方面相当准确。放射治疗后生化失败的风险也与ECE的风险相关。未来的前列腺癌分期系统应使用类似的方法来定义风险组。

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