Stereotactic prostate radiotherapy with or without androgen deprivation therapy, study protocol for a phase III, multi-institutional randomized-controlled trial.

BJR open Pub Date : 2022-11-29 eCollection Date: 2022-01-01 DOI:10.1259/bjro.20220032
Marco Lorenzo Bonù, Alessandro Magli, Davide Tomasini, Francesco Frassine, Domenico Albano, Stefano Arcangeli, Alessio Bruni, Stefano Ciccarelli, Martina De Angeli, Giulio Francolini, Ciro Franzese, Paolo Ghirardelli, Luigi Grazioli, Andrea Guerini, Andrea Lancia, Giulia Marvaso, Matteo Sepulcri, Luca Eolo Trodella, Vittorio Morelli, Andrea Georgopulos, Anastasiya Oleksandrivna Domina, Lorenzo Granello, Eneida Mataj, Fernando Barbera, Luca Triggiani
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引用次数: 0

Abstract

Objective: The therapeutic landscape for localized prostate cancer (PC) is evolving. Stereotactic radiotherapy (SRT) has been reported to be at least not inferior to standard radiotherapy, but the effect of androgen deprivation therapy (ADT) in this setting is still unknown and its use is left to clinical judgment. There is therefore the need to clarify the role of ADT in association with SRT, which is the aim of the present study.

Methods: We present a study protocol for a randomized, multi-institutional, Phase III clinical trial, designed to study SRT in unfavorable intermediate and a subclass of high-risk localized PC. Patients (pts) will be randomized 1:1 to SRT + ADT or SRT alone. SRT will consists in 36.25 Gy in 5 fractions, ADT will be a single administration of Triptorelin 22.5 mg concurrent to SRT. Primary end point will be biochemical disease-free survival. Secondary end points will be disease-free survival, freedom from local recurrence, freedom from regional recurrence, freedom from distant metastasis and overall survival (OS); quality of life QoL and patient reported outcomes will be an exploratory end point and will be scored with EPIC-26, EORTC PR 25, IPSS, IIEF questionnaires in SRT + ADT and SRT alone arms. Moreover, clinician reported acute and late toxicity, assessed with CTCAE v. 5.0 scales will be safety end points.

Results: Sample size is estimated of 310 pts. For acute toxicity and quality of life results are awaited after 6 months since last patient in, whereas, for efficacy end points and late toxicity mature results will be available 3-5 years after last patient in.

Conclusion: Evidence is insufficient to guide decision making concerning ADT administration in the new scenario of prostate ultra-hypofractionation. Hence, the need to investigate the ADT role in SRT specific setting.

Advances in knowledge: The stereotactic prostate radiotherapy with or without ADT trial (SPA Trial) has been designed to establish a new standard of care for SRT in localized unfavorable intermediate and a subclass of localized high risk PC.

立体定向前列腺放疗伴或不伴雄激素剥夺治疗,III期多机构随机对照试验研究方案
局限性前列腺癌(PC)的治疗前景正在发展。立体定向放疗(SRT)至少不逊于标准放疗,但雄激素剥夺疗法(ADT)在这种情况下的效果尚不清楚,其使用尚待临床判断。因此,有必要澄清ADT与SRT相关的作用,这是本研究的目的。我们提出了一项随机、多机构、三期临床试验的研究方案,旨在研究SRT在不利的中间和高风险局部PC的亚类中的应用。患者(pts)将按1:1随机分配到SRT + ADT或单独SRT。SRT将分为五个部分,共36.25 Gy, ADT将是在SRT的同时单次给予Triptorelin 22.5 mg。主要终点为生化无病生存期(bDFS)。次要终点将是无病生存期(DFS)、无局部复发(FFLR)、无区域复发(FFRR)、无远处转移(FFDM)和总生存期(OS);生活质量(QoL)和患者报告结果(PRO)将是一个探索性终点,并将在SRT + ADT和SRT单独组中使用EPIC-26、EORTC PR 25、IPSS和IIEF问卷进行评分。此外,临床医生报告的急性和晚期毒性,用CTCAE v5.0量表评估将是安全终点。样本量估计为310分。对于急性毒性和生活质量的结果要在最后一位患者入院后6个月后才能得到,而对于疗效终点和晚期毒性的成熟结果要在最后一位患者入院后3至5年才能得到。证据不足,指导决策有关ADT给药的新情况下,前列腺超低分割。因此,有必要研究ADT在SRT特定环境中的作用。立体定向前列腺放疗加或不加雄激素剥夺治疗试验(SPA试验)的目的是为局部不良中度和局部高危前列腺癌的SRT治疗建立一个新的标准。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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