优化中危前列腺癌的治疗:一项随机 3 期试验的二次分析。
Optimizing Treatment in Intermediate-Risk Prostate Cancer: Secondary Analysis of a Randomized Phase 3 Trial.
机构信息
Service de radio-oncologie, Centre Hospitalier Universitaire de Sherbrooke, Sherbrooke, Canada.
Centre de recherche clinique, Centre Hospitalier Universitaire de Sherbrooke, Sherbrooke, Canada.
出版信息
Int J Radiat Oncol Biol Phys. 2021 Nov 1;111(3):732-740. doi: 10.1016/j.ijrobp.2021.04.013. Epub 2021 Apr 24.
PURPOSE
To identify patients with intermediate-risk prostate cancer (IRPC) benefiting from de-escalation of androgen deprivation therapy (ADT) and/or dose escalated radiation therapy (DERT), we performed a secondary analysis of a phase 3 trial by measuring biochemical failure (BF), distant metastases, prostate cancer-specific mortality, overall survival (OS), and distant metastases-free survival (DMFS) rates according to prognostic intermediate risk factors (IRF).
METHODS AND MATERIALS
The initial trial randomized 600 patients with IRPC to a 3-arm trial with 200 patients per arm, consisting of 6 months of ADT plus 70 Gy radiation therapy (ADT + RT70) versus ADT plus a DERT of 76 Gy (ADT + DERT76) versus DERT of 76 Gy alone (DERT76). We performed an analysis based on IRF: clinical stage, prostate-specific antigen level, Gleason score, percentage of positive biopsy cores (PBC) ≥50%, and Gleason pattern. Patients were allocated to 2 groups: favorable intermediate risk (FIR), defined as patients with only 1 IRF without Gleason pattern 4 + 3 or PBC ≥50%; and unfavorable intermediate risk (UIR), defined as all other patients. BF, distant metastases, prostate cancer-specific mortality, OS, and DMFS were compared between FIR and UIR.
RESULTS
The median follow-up was 11.3 years (interquartile range, 10.9-11.7). In the FIR cohort, BF and OS were not significantly different between arms. UIR patients had significantly worse DMFS (hazard ratio [95% confidence interval], 1.61 [1.20-2.15]; P = .026) and OS (1.51 [1.12-2.04]; P = .0495) and a nonsignificant higher cumulative incidence of BF rate (1.55 [0.98-2.47]; P = .08). In UIR patients, a significant improvement in BF was seen in the arms receiving ADT compared to DERT76 alone. On multivariable analysis, Gleason pattern 4 + 3 and prostate-specific antigen >10 ng/mL independently affected BF and OS, regardless of the treatment arm.
CONCLUSIONS
In IRPC, therapeutic optimization appears possible. To avoid ADT side effects, DERT76 alone appears sufficient in patients harboring only 1 risk factor without Gleason pattern 4 + 3 and PBC ≥50% (FIR). All other UIR patients seem to benefit from ADT + DERT76.
目的
通过测量生化失败(BF)、远处转移、前列腺癌特异性死亡率、总生存(OS)和远处无转移生存(DMFS)率,根据预后中间风险因素(IRF),确定从中度风险前列腺癌(IRPC)中获益于去势治疗(ADT)和/或剂量递增放疗(DERT)下调的患者,我们对一项 3 期试验进行了二次分析。
方法和材料
初始试验将 600 名 IRPC 患者随机分为 3 臂试验,每臂 200 名患者,包括 6 个月 ADT 加 70 Gy 放疗(ADT+RT70)与 ADT 加 76 Gy DERT(ADT+DERT76)与 76 Gy 单独 DERT(DERT76)。我们根据 IRF 进行了分析:临床分期、前列腺特异性抗原水平、Gleason 评分、阳性活检核心百分比(PBC)≥50%和 Gleason 模式。患者被分为 2 组:有利中间风险(FIR),定义为无 Gleason 模式 4+3 或 PBC≥50%的 1 个 IRF 的患者;和不利中间风险(UIR),定义为所有其他患者。比较 FIR 和 UIR 之间的 BF、远处转移、前列腺癌特异性死亡率、OS 和 DMFS。
结果
中位随访时间为 11.3 年(四分位距,10.9-11.7)。在 FIR 队列中,各臂之间 BF 和 OS 无显著差异。UIR 患者的 DMFS(危险比[95%置信区间],1.61[1.20-2.15];P=0.026)和 OS(1.51[1.12-2.04];P=0.0495)显著更差,且 BF 累积发生率也存在非显著升高(1.55[0.98-2.47];P=0.08)。在 UIR 患者中,与单独接受 DERT76 治疗相比,接受 ADT 治疗的患者 BF 显著改善。多变量分析显示,无论治疗臂如何,Gleason 模式 4+3 和前列腺特异性抗原>10ng/mL 均独立影响 BF 和 OS。
结论
在 IRPC 中,似乎可以进行治疗优化。为避免 ADT 的副作用,单独接受 DERT76 治疗似乎足以治疗仅携带 1 个风险因素且无 Gleason 模式 4+3 和 PBC≥50%(FIR)的患者。所有其他 UIR 患者似乎都受益于 ADT+DERT76。
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