10000 例 Gleason3+4 有利的中危前列腺癌患者升级和升期风险。
Risk of Upgrading and Upstaging Among 10 000 Patients with Gleason 3+4 Favorable Intermediate-risk Prostate Cancer.
机构信息
Harvard Medical School, Boston, MA, USA.
Harvard Radiation Oncology Program, Boston, MA, USA.
出版信息
Eur Urol Focus. 2019 Jan;5(1):69-76. doi: 10.1016/j.euf.2017.05.011. Epub 2017 Jun 17.
BACKGROUND
It is unknown whether active surveillance can be safely offered to patients with Gleason 3+4 favorable intermediate-risk (FIR) prostate cancer.
OBJECTIVE
To examine the incidence and predictors of upgrading and upstaging among patients with Gleason 3+4 FIR disease.
DESIGN, SETTING, AND PARTICIPANTS: The study involved 10 089 patients in the National Cancer Database diagnosed from 2010 to 2012 with Gleason 3+4 disease, prostate-specific antigen (PSA) <10ng/ml, and cT1c-2a prostate cancer with <50% positive biopsy cores (PBCs) who underwent radical prostatectomy.
OUTCOME MEASUREMENTS AND STATISTICAL ANALYSIS
Logistic regression was used to examine predictors of upgrading (pathologic Gleason ≥4+3 or tertiary Gleason 5 in a Gleason 7 tumor) or upstaging (pT3-4/N1).
RESULTS AND LIMITATIONS
Some 30.3% of Gleason 3+4 FIR patients were upgraded or upstaged. On multivariable analysis, predictors included higher PSA, percentage PBC, age, and cT2a versus cT1c (all p<0.001), but not black race (p=0.895). When stratified into ordinal variables, PSA 8.1-9.9 versus ≤4.0ng/ml (adjusted odds ratio [AOR] 1.93, 38.3% vs 24.4%), PBC 37.5-49.9% versus <12.5% (AOR 1.79, 37.8% vs 25.1%); highest age quartile (≥67 yr) versus lowest (≤55 yr; AOR 1.46, 35.7% vs 24.7%); and cT2a versus cT1c (AOR 1.33, 34.3% vs 29.8%) were associated with a higher risk of upgrading or upstaging (all p<0.001). Men with PBC <12.5% and PSA ≤4.0ng/ml had a 21.7% risk of more advanced disease. This increased to 44.3% for PBC 37.5-49.9% and PSA 8.1-9.9ng/ml. A limitation of the study is its retrospective nature.
CONCLUSIONS
Approximately one in three patients with Gleason 3+4 FIR harbored disease of higher grade or stage. Younger patients with low percentage PBC and PSA and cT1c disease have a lower risk and may be candidates for active surveillance. However, widely available clinical information is insufficient for predicting the risk of more advanced disease, and the development and incorporation of additional tools, including magnetic resonance imaging and genomic tests, are necessary.
PATIENT SUMMARY
Nearly one-third of patients with Gleason 3+4 favorable intermediate-risk prostate cancer harbor disease of higher grade or higher stage than their biopsy and clinical examination suggest. These patients would therefore be poor candidates for active surveillance.
背景
目前尚不清楚主动监测是否可以安全地应用于 Gleason 3+4 有利的中危(FIR)前列腺癌患者。
目的
研究 Gleason 3+4 FIR 疾病患者中升级和升级的发生率和预测因素。
设计、地点和参与者:这项研究涉及 2010 年至 2012 年间在国家癌症数据库中诊断为 Gleason 3+4 疾病、前列腺特异性抗原(PSA)<10ng/ml、cT1c-2a 前列腺癌且 PSA<10ng/ml 的 10089 例患者<50%的阳性活检核心(PBC),并接受了根治性前列腺切除术。
结果和局限性
约 30.3%的 Gleason 3+4 FIR 患者出现升级或升级。多变量分析显示,预测因素包括较高的 PSA、PBC 百分比、年龄和 cT2a 与 cT1c(均 p<0.001),但不包括黑人种族(p=0.895)。当分层为有序变量时,PSA 8.1-9.9 与≤4.0ng/ml(调整后的优势比[OR]1.93,38.3%比 24.4%),PBC 37.5-49.9%与<12.5%(OR 1.79,37.8%比 25.1%);最高年龄四分位数(≥67 岁)与最低年龄四分位数(≤55 岁;OR 1.46,35.7%比 24.7%)和 cT2a 与 cT1c(OR 1.33,34.3%比 29.8%)与升级或升级的风险增加相关(均 p<0.001)。PBC<12.5%和 PSA≤4.0ng/ml 的男性患更高级别疾病的风险为 21.7%。当 PBC 为 37.5-49.9%且 PSA 为 8.1-9.9ng/ml 时,这一比例上升至 44.3%。研究的一个局限性是其回顾性。
结论
大约三分之一的 Gleason 3+4 FIR 患者存在高级别或更高阶段的疾病。年轻患者,PBC 百分比和 PSA 低,cT1c 疾病的风险较低,可能是主动监测的候选者。然而,广泛可用的临床信息不足以预测更高级别疾病的风险,因此需要开发和纳入其他工具,包括磁共振成像和基因组检测。
患者总结
近三分之一的 Gleason 3+4 有利的中危前列腺癌患者的疾病分级或分期高于其活检和临床检查提示的水平。因此,这些患者不适合主动监测。
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