Department of Radiation Oncology, University of Miami Miller School of Medicine and Sylvester Comprehensive Cancer Center, Miami, FL, USA.
Department of Public Health Sciences, University of Chicago, Chicago, IL, USA; NRG Oncology, Philadelphia, PA, USA.
Lancet. 2022 May 14;399(10338):1886-1901. doi: 10.1016/S0140-6736(21)01790-6.
In men with a detectable prostate-specific antigen (PSA) level after prostatectomy for prostate cancer, salvage prostate bed radiotherapy (PBRT) results in about 70% of patients being free of progression at 5 years. A three-group randomised trial was designed to determine whether incremental gains in patient outcomes can be achieved by adding either 4-6 months of short-term androgen deprivation therapy (ADT) to PBRT, or both short-term ADT and pelvic lymph node radiotherapy (PLNRT) to PBRT.
The international, multicentre, randomised, controlled SPPORT trial was done at 283 radiation oncology cancer treatment centres in the USA, Canada, and Israel. Eligible patients (aged ≥18 years) were those who after prostatectomy for adenocarcinoma of the prostate had a persistently detectable or an initially undetectable and rising PSA of between 0·1 and 2·0 ng/mL. Patients with and without lymphadenectomy (N0/Nx) were eligible if there was no clinical or pathological evidence of lymph node involvement. Other eligibility criteria included pT2 or pT3 disease, prostatectomy Gleason score of 9 or less, and a Zubrod performance status of 0-1. Eligible patients were randomly assigned to receive PBRT alone at a dose of 64·8-70·2 Gy at 1·8 Gy per fraction daily (group 1), PBRT plus short-term ADT (group 2), or PLNRT (45 Gy at 1·8 Gy per fraction, and then a volume reduction made to the planning target volume for the remaining 19·8-25 ·2 Gy) plus PBRT plus short-term ADT (group 3). The primary endpoint was freedom from progression, in which progression was defined as biochemical failure according to the Phoenix definition (PSA ≥2 ng/mL over the nadir PSA), clinical failure (local, regional, or distant), or death from any cause. A planned interim analysis of 1191 patents with minimum potential follow-up time of 5 years applied a Haybittle-Peto boundary of p<0·001 (one sided) for comparison of 5-year freedom from progression rates between the treatment groups. This trial is registered with ClinicalTrials.gov, NCT00567580. The primary objectives of the trial have been completed, although long-term follow-up is continuing.
Between March 31, 2008, and March 30, 2015, 1792 eligible patients were enrolled and randomly assigned to the three treatment groups (592 to group 1 [PBRT alone], 602 to group 2 [PBRT plus short-term ADT], and 598 to group 3 [PLNRT plus PBRT plus short-term ADT]). 76 patients subsequently found to be ineligible were excluded from the analyses; thus, the evaluable patient population comprised 1716 patients. At the interim analysis (n=1191 patients; data cutoff May 23, 2018), the Haybittle-Peto boundary for 5-year freedom from progression was exceeded when group 1 was compared with group 3 (difference 17·9%, SE 2·9%; p<0·0001). The difference between groups 2 and 3 did not exceed the boundary (p=0·0063). With additional follow-up beyond the interim analysis (the final planned analysis; data cutoff May 26, 2021), at a median follow-up among survivors of 8·2 years (IQR 6·6-9·4), the 5-year freedom from progression rates in all 1716 eligible patients were 70·9% (95% CI 67·0-74·9) in group 1, 81·3% (78·0-84·6) in group 2, and 87·4% (84·7-90·2) in group 3. Per protocol criteria, freedom from progression in group 3 was superior to groups 1 and 2. Acute (≤3 months after radiotherapy) grade 2 or worse adverse events were significantly more common in group 3 (246 [44%] of 563 patients) than in group 2 (201 [36%] of 563; p=0·0034), which, in turn, were more common than in group 1 (98 [18%] of 547; p<0·0001). Similar findings were observed for grade 3 or worse adverse events. However, late toxicity (>3 months after radiotherapy) did not differ significantly between the groups, apart from more late grade 2 or worse blood or bone marrow events in group 3 versus group 2 (one-sided p=0·0060) attributable to the addition of PLNRT in this group.
The results of this randomised trial establish the benefit of adding short-term ADT to PBRT to prevent progression in prostate cancer. To our knowledge, these are the first such findings to show that extending salvage radiotherapy to treat the pelvic lymph nodes when combined with short-term ADT results in meaningful reductions in progression after prostatectomy in patients with prostate cancer.
National Cancer Institute.
对于前列腺癌根治术后前列腺特异性抗原(PSA)水平持续升高的患者,挽救性前列腺床放疗(PBRT)可使约 70%的患者在 5 年内无进展。本研究旨在设计一项三分组随机试验,以确定在 PBRT 基础上分别加用 4-6 个月短期雄激素剥夺治疗(ADT)、加用短期 ADT 联合盆腔淋巴结放疗(PLNRT)是否能够进一步提高患者的治疗效果。
本国际多中心随机对照 SPORT 试验在加拿大、以色列和美国的 283 个放疗中心开展。符合条件的患者(年龄≥18 岁)为前列腺腺癌根治术后持续或初始未检测到 PSA 水平升高(0.1-2.0ng/ml)的患者。行或不行淋巴结清扫术(N0/Nx)的患者均符合条件,其标准为无临床或病理证据提示淋巴结受累。其他入选标准包括 pT2 或 pT3 疾病、前列腺切除术 Gleason 评分为 9 分及以下、Zubrod 体能状态评分为 0-1 分。合格患者被随机分配接受单纯 PBRT(剂量 64.8-70.2Gy,1.8Gy/次,1 天 1 次)(组 1)、PBRT 联合短期 ADT(组 2)或 PLNRT(45Gy,1.8Gy/次,然后将计划靶区体积缩小至 19.8-25.2Gy 剩余剂量)联合 PBRT 联合短期 ADT(组 3)。主要终点是无进展生存,其中进展定义为根据 Phoenix 定义(PSA 高于最低 PSA 水平的 2ng/ml)的生化失败、临床失败(局部、区域或远处)或任何原因导致的死亡。一项对 1191 例患者的中位潜在随访时间至少为 5 年的计划中期分析应用了 Haybittle-Peto 边界(单侧 p<0.001),以比较各组 5 年无进展生存率。本试验在 ClinicalTrials.gov 注册,编号为 NCT00567580。该试验的主要目标已经完成,尽管正在进行长期随访。
2008 年 3 月 31 日至 2015 年 3 月 30 日期间,纳入了 1792 例符合条件的患者,并随机分为三组治疗(组 1:592 例患者接受单纯 PBRT;组 2:602 例患者接受 PBRT 联合短期 ADT;组 3:598 例患者接受 PLNRT 联合 PBRT 联合短期 ADT)。之后有 76 例患者被排除出分析,因此可评估的患者人群包括 1716 例。在中期分析(n=1191 例患者;数据截止日期为 2018 年 5 月 23 日)时,与组 3 相比,组 1 的 5 年无进展生存 Haybittle-Peto 边界被突破(差异 17.9%,SE 2.9%;p<0.0001)。组 2 与组 3 之间的差异未超过边界(p=0.0063)。在中期分析后(最终计划分析;数据截止日期为 2021 年 5 月 26 日),幸存者的中位随访时间为 8.2 年(IQR 6.6-9.4),1716 例合格患者的 5 年无进展生存率在组 1 中为 70.9%(95%CI 67.0-74.9),在组 2 中为 81.3%(78.0-84.6),在组 3 中为 87.4%(84.7-90.2)。根据方案标准,组 3 的无进展生存率优于组 1 和组 2。在组 3(563 例患者中有 246 例[44%])中,3 个月内发生的急性(放疗后≤3 个月)2 级或更严重不良事件显著多于组 2(563 例患者中有 201 例[36%];p=0.0034),而组 2 又显著多于组 1(547 例患者中有 98 例[18%];p<0.0001)。3 级或更严重不良事件也观察到类似的发现。然而,各组之间晚期毒性(放疗后>3 个月)差异无统计学意义,除了组 3 中晚期 2 级或更严重的血液或骨髓事件发生率高于组 2(单侧 p=0.0060),这归因于该组中添加了 PLNRT。
这项随机试验的结果证实了在 PBRT 中加用短期 ADT 以预防前列腺癌进展的益处。据我们所知,这些是首次表明在前列腺癌根治术后,将挽救性放疗扩展至治疗盆腔淋巴结,同时联合短期 ADT,可显著降低前列腺癌患者术后的进展率。
美国国立癌症研究所。
