A Phase 1 Trial of Image Guided Risk Volume-Adapted Postprostatectomy Radiation Therapy.

Krishnan R Patel, Esther Mena, Lindsay S Rowe, Holly Ning, Jason Cheng, Kilian Salerno, Erica Schott, Debbie-Ann Nathan, Erich P Huang, Liza Lindenberg, Peter Choyke, Baris Turkbey, Deborah E Citrin
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Abstract

Purpose: This was a phase 1 trial with the primary objective of identifying the most compressed dose schedule (DS) tolerable using risk volume-adapted, hypofractionated, postoperative radiation therapy (PORT) for biochemically recurrent prostate cancer. Secondary endpoints included biochemical progression-free survival and quality of life (QOL).

Methods and materials: Patients were treated with 1 of 3 isoeffective DSs (DS1: 20 fractions, DS2: 15 fractions, and DS3: 10 fractions) that escalated the dose to the imaging-defined local recurrence (73 Gy3 equivalent dose in 2Gy fractions) and de-escalated the dose to the remainder of the prostate bed (48 Gy3 equivalent dose in 2Gy fractions). Escalation followed a standard 3 + 3 design with a 6-patient expansion at the maximally tolerated hypofractionated DS. Dose-limiting toxicity was defined as Common Terminology Criteria for Adverse Events v.4.0 grade (G) 3 toxicity lasting >4 days within 21 days of PORT completion or G4 gastrointestinal (GI) or genitourinary toxicities thereafter. QOL was assessed longitudinally through 24 months with the Expanded Prostate Cancer Index Composite short form.

Results: Between January 2018 and December 2023, 15 patients were treated (3 with DS1, 3 with DS2, and 9 with DS3). The median follow-up was 48 months. No dose-limiting toxicities were observed on any DS, and thus, expansion occurred at DS3. The cumulative incidence of G3 GI and genitourinary toxicity was 7% and 9% at 24 months, respectively, with no G4 events observed. Transient, acute G2+ GI toxicity was the most common. QOL worsened transiently during study follow-up in urinary incontinence, GI, and sexual subdomains but was similar to baseline by 24 months. The biochemical progression-free survival was 91% at both 24 and 60 months.

Conclusions: The maximally tolerated hypofractionated DS for hypofractionated, risk volume-adapted PORT was determined to be DS3 (36.4 Gy to the prostate bed and 47.1 Gy to the imaging-defined recurrence in 10 daily fractions). No >G3 events were observed. Transient declines in QOL did not persist through 24 months.

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前列腺切除术后图像引导、风险量适应性放疗的一期试验
目的:这是一项 I 期试验,主要目的是确定可耐受的最紧凑剂量表 (DS),使用风险容量适应性、低分量、术后放疗 (PORT) 治疗生化复发前列腺癌。次要终点包括无生化进展生存期(bPFS)和生活质量(QOL):患者接受3种等效剂量方案(DS1:20个疗程,DS2:15个疗程,DS3:10个疗程)中的一种,剂量升级至影像学定义的局部复发(73Gy3 EQD2),剂量降级至前列腺床的其余部分(48Gy3 EQD2)。升级遵循标准的 3+3 设计,在最大耐受低分次剂量表 (MTHDS) 上扩增 6 名患者。剂量限制性毒性(DLT)的定义是:PORT 完成后 21 天内持续 4 天以上的 CTCAE v.4.0 3 级(G)毒性或之后的 4 级胃肠道(GI)或泌尿生殖系统(GU)毒性。使用 EPIC-26 对 24 个月的 QOL 进行纵向评估:结果:在2018年1月至2023年12月期间,15名患者接受了治疗(3名DS1患者、3名DS2患者和9名DS3患者)。中位随访时间为 48 个月。在任何 DS 上都未观察到 DLT,因此在 DS3 上进行了扩增。24 个月时,G3 消化道和泌尿道毒性的累积发生率分别为 7% 和 9%,未观察到 G4 事件。一过性、急性 G2+ 消化道毒性最为常见。研究随访期间,尿失禁、消化道和性生活等子领域的 QOL 出现短暂恶化,但在 24 个月时与基线相似。24个月和60个月的bPFS均为91%:经研究确定,低分量、风险体积适应性PORT的最大耐受低分量剂量表为DS3(前列腺床36.4Gy,影像学定义的复发部位47.1Gy,每天10次)。未观察到 >G3 事件。QOL 的短暂下降并未持续 24 个月。
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来源期刊
CiteScore
11.00
自引率
7.10%
发文量
2538
审稿时长
6.6 weeks
期刊介绍: International Journal of Radiation Oncology • Biology • Physics (IJROBP), known in the field as the Red Journal, publishes original laboratory and clinical investigations related to radiation oncology, radiation biology, medical physics, and both education and health policy as it relates to the field. This journal has a particular interest in original contributions of the following types: prospective clinical trials, outcomes research, and large database interrogation. In addition, it seeks reports of high-impact innovations in single or combined modality treatment, tumor sensitization, normal tissue protection (including both precision avoidance and pharmacologic means), brachytherapy, particle irradiation, and cancer imaging. Technical advances related to dosimetry and conformal radiation treatment planning are of interest, as are basic science studies investigating tumor physiology and the molecular biology underlying cancer and normal tissue radiation response.
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