ONE SHOT - single shot radiotherapy for localized prostate cancer: study protocol of a single arm, multicenter phase I/II trial

Total dose and dose per fraction play an important role in the curative treatment of prostate cancer with radiotherapy (RT). Modern image-guided external RT allows safe dose escalation for prostate cancer. Doses above 74 Gy with conventional fractionation (2 Gy/day) have been shown to be beneficial. There are strong radiobiological considerations that suggest that treatment with a small number of large fractions (hypofractionation) may increase the therapeutic ratio of RT for prostate cancer.

The “α/β” ratio (i.e., cell sensitivity/cell repair) is a key parameter of the cell-survival linear-quadratic (LQ) model that purportedly defines the sensitivity of each tissue (healthy or tumoral) to changes in treatment fractionation. Prostate cancer cells may have a low α/β ratio (i.e.,~ 1.5 Gy), lower than that of most tumors or even of the late-responding normal tissues surrounding the tumor, the rectum and the bladder (α/β ratio 3–5 Gy) [1]. Thus, hypofractionation may increase the tumor cell killing effect with relatively less toxic effect on the surrounding late responding normal tissues compared to conventional fractionation. Several authors have reported their respective experiences with moderate hypofractionation (i.e., dose per fraction 2.5 Gy to 4 Gy) for prostate cancer confirming the equivalence in terms of disease control and tolerance compared to standard fractionated treatments [2‐5].

Bio-mathematical models using large patient data sets have focused on external beam RT schedules using less than 4 Gy fractions. It deserves to be acknowledged that the LQ model may not be predictive of cell survival and isoeffects with doses per fraction above 3-4Gy. Indeed, the predictions of the LQ model at very high dose/fraction (extreme hypofractionation) may be somehow “ambivalent”, either overestimated (less repair of sublethal damage thus a lower value for “β”) or underestimated (increased indirect cell-death secondary to intravascular endothelial damage). Staring from this background, clinical research on extreme hypofractionation started some 15 years ago when stereotactic body RT (SBRT) technology appeared as a treatment option against localized prostate cancer competing with high-dose rate brachytherapy (HDR-BT).

Indeed, preliminary results on extreme hypofractionation with SBRT have been reported during the last few years mainly for low-risk patients in single-institution [6‐8] or multi-institutional [9] series. Most frequently, 5 fractions of 7.25 Gy have been delivered for a total equivalent dose to the tumor of 90 Gy in 2 Gy/fraction (LQ model) and a success rate of > 90%, 5-year biochemical relapse-free (bRFS) survival rates [10]. Data published so far for prostate SBRT have shown, although with a limited follow-up, late grade 3 toxicity rates for rectal and genitourinary (GU) toxicity lying within a ≤ 3% range [8, 11, 12]. Although, caution is recommended to avoid passing a too optimistic message regarding the potential biological benefits of extreme hypofractionation for prostate cancer (i.e., more cure with less side effects), financial and logistical advantages can undoubtedly be foreseen. In fact, a drop from 40 or more treatments to 5 or less sessions may reduce the cost of external beam RT, will increase the availability of treatment slots in otherwise busy departments (important issue in countries with limited resources), and significantly improve patient’s convenience.

The question of how far can the number of fractions with SBRT be reduced is an exciting research matter with an undoubtful goal, face the challenge of assessing the potential for cure of prostate cancer patients with a single and unique fraction of high dose irradiation similar to what is already undertaken with radiosurgery against brain, lung, and liver targets. Such type of effort has already been attempted with HDR-BT. Recently, Prada et al. [13] reported a relatively disappointing 66% 6-year bRFS survival though a very good tolerance after a single interstitial application of 19 Gy to the prostate. Reasons for this suboptimal result may be related, for instance, to a suboptimal dose-distribution with HDR-BT compared to SBRT. Hoskin et al. have recently published the results on 49 patients treated with a single fraction of HDR-BT to 19/20 Gy [14]. With 49 months median follow-up, the 4-year estimates of grade-3 GU and gastrointestinal (GI) toxicity was 2% and 0%, respectively, with no grade 4 events, while the 4-year bRFS was 94%. Similarly, Morton et al. confirmed with a median follow-up time of 20 months the good tolerance of a single 19 Gy single HDR-BT fraction in terms of toxicity and impact on quality of life (QoL) [15] and Krauss et al. reported a 3-year bRFS rate of 93% [16], similar to results observed by Hoskin et al. In conclusion, for the authors one single fraction HDR-BT is feasible, weakly toxic, and with promising preliminary results.

Although, the effects are mostly encouraging, only controlled studies are able to properly address the impact of single fraction SBRT in prostate cancer outcomes. Therefore, a phase I/II approach will be a properly controlled study to demonstrate early evidence of safety and efficacy of the intervention and substantiate further the role of a single-fraction SBRT approach. If positive, the results of ONE SHOT will help determine the design of subsequent phase III trials in the exclusive RT setting for the treatment of localized disease.

This study was approved by the Ethics committee of the Geneva University Hospital (2017–01236) and is registered on clinicaltrials.gov (NCT03294889). This is a phase I/II, prospective, multicenter, single-arm study.

Optimal management of localized low- or intermediate risk prostate cancer remains a challenging situation, with different treatment options available ranging from active surveillance to radical treatment [25]. Considering that patients under active surveillance have a greater risk of disease progression and metastases compared to definitive treatments [26], the choice of the more appropriate curative option is a crucial issue for clinicians.

SBRT represents a valid treatment option for these patients, combing a good toxicity profile, promising disease control rates, and limited impact on QoL. Recently reported, preliminary results of the Scandinavian phase III HYPO-RT-PC trial found in 1200 intermediate-risk prostate cancer patients similar biochemical control rates and toxicities results with extreme hypofractionation (42.7 Gy in seven fractions of 6.1 Gy over two and a half weeks) compared to standard fractionation 78 Gy [27]. However, the optimal SBRT fractionation schedule for curative treatment of patients with localized prostate cancer is, so far, unknown. Based on the promising results of HDR-BT monotherapy treatments [15, 28, 29], single-shot SBRT may represent an appealing treatment modality for prostate cancer patients.

To our knowledge, ONE SHOT is the first phase I/II trial assessing the efficacy and safety of a single-dose SBRT treatment for patients with localized prostate cancer in a multicenter setting. ONE SHOT proposes the same treatment technique under a strict RTQA protocol for all patients. By reducing significantly the beam-on time [30], our single shot linac-based FFF VMAT technique with intra-fractional control motion is expected to guarantee not only treatment reproducibility [31] but also minimize intra-fraction dose uncertainties [32]. Moreover, the implementation of patient-reported outcome using validated questionnaires will provide a reliable evaluation of the clinical impact of a single-dose SBRT by reporting a longitudinal follow-up on the long-term of radiation-induced side effects compared to physician-reported data.

While waiting for results of presently ongoing randomized phase III trials comparing SBRT with other fractionation or treatment, results of the ONE SHOT trial, if positive, may help to design subsequent studies exploring the role of SBRT monotherapy in the exclusive RT treatment of localized disease.