Phase II Multi-institutional Clinical Trial on a New Mixed Beam RT Scheme of IMRT on Pelvis Combined with a Carbon Ion Boost for High-risk Prostate Cancer Patients

Marvaso, Giulia; Jereczek‐Fossa, Barbara Alicja; Vischioni, Barbara; Ciardo, D.; Giandini, T.; Hasegawa, Azusa; Cattani, Federica; Carrara, M.; Ciocca, Mario; Bedini, N.; Villa, Sergio; Morlino, S.; Russo, Stefania; Zerini, Dario; Colangione, Sarah Pia; Panaino, C.M.V.; Fodor, C.; Santoro, Luigi; Pignoli, E.; Valvo, Francesca; Valdagni, Riccardo; Cobelli, Ottavio De; Orecchia, Roberto

doi:10.5301/tj.5000587

Cited by 13 publications

(17 citation statements)

References 23 publications

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“…The inclusion criteria were men with pathologically confirmed localized prostate cancer who received CIRT as the radical treatment. Patients with visceral or bone metastases [10], pelvic nodes metastases [11], postoperative radiotherapy [4], and recurrence after either surgery or radiotherapy [7] were excluded. Finally, 64 eligible patients participated in this study.…”

Section: Methodsmentioning

confidence: 99%

Preliminary exploration of clinical factors affecting acute toxicity and quality of life after carbon ion therapy for prostate cancer

Zhang

Li²,

et al. 2019

Radiat Oncol

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Purpose To assess toxicity and quality-of-life (QOL) after carbon ion radiotherapy (CIRT) at the Shanghai Proton and Heavy Ion Center (SPHIC) and identify clinical factors that correlate with urinary, bowel and sexual function. Methods Sixty-four patients with localized prostate cancer admitted from July 2015 to January 2018 underwent CIRT. At baseline and 5 time-points after radiotherapy, we assessed patients’ QOL using the 26-item edition of the Expanded Prostate Cancer Index-Composite (EPIC-26) Chinese version. Logistic regression was performed to identify clinical factors associated with acute genitourinary (GU) toxicity and relative QOL. Results By the end of CIRT, urinary irritation/obstruction temporarily declined (− 7.92 ± 1.76, p < .001). For urinary incontinence, bowel and sexual QOL, the scores remained stable at 2-year follow-up. The occurrences of acute Grade 1 and 2 GU toxicity were 20.3 and 10.9%, respectively, and of late Grade 1 and 2 GU toxicity were 3.1 and 1.6%, respectively. No acute or late gastrointestinal (GI) toxicity occurred. Transurethral resection of the prostate (TURP) was a risk factor that predicted a decline in urinary related QOL, and age made a difference to bowel-related QOL. For sexual QOL, castration status was a remarkable risk factor. An international prostate symptom score (IPSS) ≥8 increased the risk of Grade 1–2 acute GU toxicity 5.3-fold. Conclusion Patients with prostate cancer had favorable QOL after CIRT. IPSS ≥8 was a risk factor to acute GU toxicity, and TURP predicted a decline in urinary QOL. Age was related to bowel QOL, and castration status was associated with sexual QOL. Trial registration Carbon Ion Radiotherapy for the Treatment of Localized Prostate Cancer, NCT02739659 . Registered April 15, 2016.

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Section: Methodsmentioning

confidence: 99%

Preliminary exploration of clinical factors affecting acute toxicity and quality of life after carbon ion therapy for prostate cancer

Zhang

Li²,

et al. 2019

Radiat Oncol

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“…The NCT02672449 is a prospective, multicentric, phase II open-label trial that might provide novel insights on a new mixed beam RT scheme of a carbon ion boost followed by pelvic photon RT ( 76 ), and details about this ongoing trial are reported in Table 1 . Overall, data about CIRT in HR setting seems encouraging and could provide novel insight for the treatment of these patients.…”

Section: New Scenariosmentioning

confidence: 99%

Therapeutic Sequences in the Treatment of High-Risk Prostate Cancer: Paving the Way Towards Multimodal Tailored Approaches

et al. 2021

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Various definitions are currently in use to describe high-risk prostate cancer. This variety in definitions is important for patient counseling, since predicted outcomes depend on which classification is applied to identify patient’s prostate cancer risk category. Historically, strategies for the treatment of localized high-risk prostate cancer comprise local approaches such as surgery and radiotherapy, as well as systemic approaches such as hormonal therapy. Nevertheless, since high-risk prostate cancer patients remain the group with higher-risk of treatment failure and mortality rates, nowadays, novel treatment strategies, comprising hypofractionated-radiotherapy, second-generation antiandrogens, and hadrontherapy, are being explored in order to improve their long-term oncological outcomes. This narrative review aims to report the current management of high-risk prostate cancer and to explore the future perspectives in this clinical setting.

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“…4) The higher RBE and sharper lateral fields of CIRT, permitting biologic and physical dose escalation, should improve local control more than might be expected with photon‐based or proton‐based SBRT . 5) Hypoxia and other mechanisms of radiation resistance thought to confer resistance to photon‐based EBRT may be overcome with CIRT . And 6) intermediate endpoints, such as prostate‐specific antigen nadir and/or time to metastatic disease, could be used to support the viability of CIRT …”

Section: Challenges and Future Directionsmentioning

confidence: 99%

“…40 5) Hypoxia and other mechanisms of radiation resistance thought to confer resistance to photon-based EBRT may be overcome Cancer December 1, 2018 with CIRT. 27,[49][50][51] And 6) intermediate endpoints, such as prostate-specific antigen nadir and/or time to metastatic disease, could be used to support the viability of CIRT. 38,40,52,53 Patients with prostate cancer (including those from the United States) initially would receive treatment with 4 or 5 fractions of SBRT using photons (x-rays) versus protons versus CIRT (with photons considered the standard to which the others are compared), as noted above.…”

Section: Cancer Sites Suitable For Clinical Trialsmentioning

confidence: 99%

“…One site under discussion by our own group (NAPTA), in collaboration with the leadership of a number of centers with CIRT capability involves the design of a large phase II/III clinical trial for unfavorable intermediate and high-risk prostate cancer. The rationale for choosing this cancer site is as follows: (1) prostate cancer is one of the most common cancers treated definitively with radiation in the world, and is the most common cancer treated with CIRT 3,29 ; (2) increasingly SBRT is being used to treat both intermediate and high grade prostate cancer either as a monotherapy in 4 to 5 fractions or as a boost with 2 fractions after pelvic radiotherapy and recently a number of investigators have begun studying the feasibility of treating prostate cancer with a single fraction 39 (ClinicalTrials.gov Identifier: NCT03294889); (3) there are theoretical reasons to believe that CIRT, due to the tighter penumbra, should allow increased sparing of neurovascular structures and the penile bulb resulting in improved erectile function and favorably impacting quality of life 45–47 ; (4) the higher RBE and sharper lateral fields of CIRT, permitting biological and physical dose escalation, should improve local control more than might be expected with photon or proton based SBRT 43,44 ; (5) hypoxia and other mechanisms of radiation resistance thought to confer resistance to photon based EBRT may be overcome with CIRT 26,48–50 ; (6) intermediate endpoints such as PSA nadir and /or time to metastatic disease could be used to support the viability of CIRT 37,39,51,52 .…”

Section: Challenges and Future Directionsmentioning

confidence: 99%

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Clinical trials involving carbon‐ion radiation therapy and the path forward

Lazar

Schulte

Faddegon

et al. 2018

Cancer

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To describe the international landscape of clinical trials in carbon ion radiotherapy (CIRT), we reviewed the current status of 63 ongoing clinical trials (median: 47 subjects) involving CIRT identified from the clinicaltrials.gov trial registry and World Health Organization International Clinical Trials Platform Registry. We evaluated the potential for these trials to define the role of this modality in the treatment of specific cancer types, and to identify major challenges and opportunities to advance this technology. A significant body of literature suggests the potential for advantageous dose distributions and in preclinical biologic studies the enhanced effectiveness for CIRT compared to photons and protons. Additionally, clinical evidence, though limited, from phase I/II trials indicates the potential for CIRT to improve cancer outcomes. However, at present, high level phase III randomized clinical trial evidence does not exist. While there has been an increase in the number of trials investigating CIRT since 2010, and the number of countries and sites offering CIRT is slowly growing, this progress has excluded other countries. We propose several recommendations to study this modality in order to accelerate progress in the field, including to (1) increase the number of multi-national randomized clinical trials (2) leveraging existing CIRT facilities to launch larger multi-national trials directed at common cancers combined with high level quality assurance; and (3) developing more compact and less expensive “next generation” treatment systems integrated with radiobiological research and pre-clinical testing.

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Phase II Multi-institutional Clinical Trial on a New Mixed Beam RT Scheme of IMRT on Pelvis Combined with a Carbon Ion Boost for High-risk Prostate Cancer Patients

Cited by 13 publications

References 23 publications

Preliminary exploration of clinical factors affecting acute toxicity and quality of life after carbon ion therapy for prostate cancer

Preliminary exploration of clinical factors affecting acute toxicity and quality of life after carbon ion therapy for prostate cancer

Therapeutic Sequences in the Treatment of High-Risk Prostate Cancer: Paving the Way Towards Multimodal Tailored Approaches

Clinical trials involving carbon‐ion radiation therapy and the path forward

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