高剂量放疗联合或不联合雄激素剥夺治疗中危前列腺癌:肿瘤控制和毒性反应结果。
High-dose radiotherapy with or without androgen deprivation therapy for intermediate-risk prostate cancer: cancer control and toxicity outcomes.
机构信息
Department of Radiation Oncology and Winship Cancer Institute, Emory University, Atlanta, GA, USA.
出版信息
Int J Radiat Oncol Biol Phys. 2012 Aug 1;83(5):1473-9. doi: 10.1016/j.ijrobp.2011.10.036. Epub 2012 Jan 13.
PURPOSE
To evaluate the impact of short-course androgen deprivation therapy (ADT) on cancer control outcomes and toxicity in intermediate-risk prostate cancer treated with dose-escalated external beam radiotherapy (high-dose radiotherapy [HDRT]).
METHODS AND MATERIALS
Demographic, disease, and treatment characteristics of prostate cancer patients at 2 institution consortiums were charted. Of 296 men with intermediate-risk prostate cancer (defined as ≥T2b, prostate-specific antigen level >10 ng/mL, or Gleason score [GS] of 7, with none of the following: ≥T3, prostate-specific antigen level >20 ng/mL, GS ≥8, or positive nodes) treated with HDRT to a dose of 72 Gy or greater, 123 received short-course ADT and 173 did not. Univariate and multivariate analyses on biochemical failure-free survival (BFFS) (including subset analysis by disease factors) and on overall survival (OS) were performed, as were comparisons of gastrointestinal (GI) and genitourinary (GU) toxicity rates.
RESULTS
For the whole group, the median dose was 75.6 Gy; the minimum follow-up was 2 years, and the median follow-up was 47.4 months. For ADT vs. no ADT, the 5-year BFFS rate was 86% vs. 79% (p = 0.138) and the 5-year OS rate was 87% vs. 80% (p = 0.159). On multivariate analysis, percent positive cores (PPC) (p = 0.002) and GS (p = 0.008) were significantly associated with BFFS, with ADT showing a trend (p = 0.055). The impact of ADT was highest in the subsets with PPC greater than 50% (p = 0.019), GS 4+3 (p = 0.078), and number of risk factors greater than 1 (p = 0.022). Only intensity-modulated radiotherapy use (p = 0.012) and GS (p = 0.023) reached significance for OS, and there were no significant differences in GU or GI toxicity.
CONCLUSIONS
Although the use of ADT with HDRT did not influence BFFS, our study suggests a benefit in patients with PPC greater than 50%, GS 4+3, or multiple risk factors. No OS benefit was shown, and ADT was not associated with additional radiotherapy-related GI or GU toxicity.
目的
评估短程雄激素剥夺疗法(ADT)对接受剂量递增外照射放疗(高剂量放疗[HDRT])治疗的中危前列腺癌患者的癌症控制结果和毒性的影响。
方法和材料
对 2 个机构联盟的前列腺癌患者的人口统计学、疾病和治疗特征进行图表记录。在 296 名患有中危前列腺癌(定义为≥T2b、前列腺特异性抗原水平>10ng/mL 或 Gleason 评分[GS]为 7,且无以下任何一种情况:≥T3、前列腺特异性抗原水平>20ng/mL、GS≥8 或阳性淋巴结)的患者中,123 名接受 HDRT 治疗,剂量为 72Gy 或更高,173 名未接受 ADT。对生化无失败生存率(BFFS)(包括按疾病因素进行的亚组分析)和总生存率(OS)进行单变量和多变量分析,并比较胃肠道(GI)和泌尿生殖系统(GU)毒性发生率。
结果
对于整个组,中位剂量为 75.6Gy;最低随访时间为 2 年,中位随访时间为 47.4 个月。对于 ADT 与无 ADT,5 年 BFFS 率分别为 86%和 79%(p=0.138),5 年 OS 率分别为 87%和 80%(p=0.159)。多变量分析显示,阳性核心百分比(PPC)(p=0.002)和 GS(p=0.008)与 BFFS 显著相关,ADT 呈趋势(p=0.055)。ADT 的影响在 PPC>50%(p=0.019)、GS 4+3(p=0.078)和危险因素大于 1 个(p=0.022)的亚组中最高。仅调强放疗的使用(p=0.012)和 GS(p=0.023)对 OS 有显著影响,且在 GU 或 GI 毒性方面无显著差异。
结论
尽管 HDRT 联合 ADT 并未影响 BFFS,但本研究表明,对于 PPC>50%、GS 4+3 或多个危险因素的患者,可能有益。未显示 OS 获益,ADT 与放疗相关的额外 GI 或 GU 毒性无关。
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