Department of Radiation Oncology, Osaka University Graduate School of Medicine, Osaka, Japan.
Department of Medical Innovation, Osaka University Hospital, Osaka, Japan.
Acta Oncol. 2023 May;62(5):488-494. doi: 10.1080/0284186X.2023.2213443. Epub 2023 May 18.
This dose-escalation study evaluated the toxicity and efficacy of different stereotactic body radiation therapy (SBRT) doses for selecting an optimal dose for prostatic adenocarcinoma (PCa).
This clinical trial was registered at UMIN (UMIN000014328). Patients with low- or intermediate-risk PCa were equally assigned to 3 SBRT dose levels: 35, 37.5, and 40 Gy per 5 fractions. The primary endpoint was the occurrence rate of late grade ≥2 genitourinary (GU) and gastrointestinal (GI) adverse events at 2 years, while the secondary endpoint was the 2-year biochemical relapse-free (bRF) rate. Adverse events were evaluated using the Common Terminology Criteria for Adverse Events version 4.0.
Seventy-five patients (median age, 70 years) were enrolled from March 2014 to January 2018, of whom 10 (15%) and 65 (85%) had low- and intermediate-risk PCa, respectively. The median follow-up time was 48 months. Twelve (16%) patients received neoadjuvant androgen deprivation therapy. The 2-year occurrence rates of grade 2 late GU and GI toxicities were 34 and 7% in all cohorts, respectively (35 Gy: 21 and 4%; 37.5 Gy: 40 and 14%; 40 Gy: 42 and 5%). The occurrence risk of GU toxicities significantly increased with dose escalation ( = 0.0256). Grades 2 and 3 acute GU toxicities were observed in 19 (25%) and 1 (1%), respectively. Grade 2 acute GI toxicity was observed in 8 (11%) patients. No grade ≥3 GI or ≥4 GU acute toxicity or grade ≥3 late toxicity was observed. Clinical recurrence was detected in 2 patients.
An SBRT dose of 35 Gy per 5 fractions is less likely to cause adverse events in patients with PCa than 375- and 40-Gy SBRT doses. Higher doses of SBRT should be applied with caution.
本剂量递增研究旨在评估不同立体定向体放射治疗(SBRT)剂量治疗前列腺腺癌(PCa)的毒性和疗效,以选择最佳剂量。
本临床试验在 UMIN(UMIN000014328)注册。低危或中危 PCa 患者被平均分配到 3 个 SBRT 剂量水平:35、37.5 和 40Gy,共 5 个分数。主要终点是 2 年时晚期≥2 级泌尿生殖系统(GU)和胃肠道(GI)不良事件的发生率,次要终点是 2 年生化无复发生存率(bRF)。使用通用不良事件术语标准 4.0 评估不良事件。
2014 年 3 月至 2018 年 1 月共纳入 75 例患者(中位年龄 70 岁),其中 10 例(15%)和 65 例(85%)分别为低危和中危 PCa。中位随访时间为 48 个月。12 例(16%)患者接受了新辅助雄激素剥夺治疗。所有队列中,2 年时 2 级晚期 GU 和 GI 毒性的发生率分别为 34%和 7%(35Gy:21%和 4%;37.5Gy:40%和 14%;40Gy:42%和 5%)。GU 毒性的发生风险随剂量递增而显著增加(=0.0256)。19 例(25%)和 1 例(1%)分别出现 2 级和 3 级急性 GU 毒性。8 例(11%)患者出现 2 级急性 GI 毒性。未观察到≥3 级 GI 或≥4 级 GU 急性毒性或≥3 级晚期毒性。2 例患者检测到临床复发。
与 37.5 和 40Gy 的 SBRT 剂量相比,5 个分数 35Gy 的 SBRT 剂量不太可能导致 PCa 患者发生不良反应。应谨慎应用更高剂量的 SBRT。
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