Predicting dose response to prostate cancer radiotherapy: validation of a radiation signature in the randomized phase III NRG/RTOG 0126 and SAKK 09/10 trials

A. Dal Pra; P. Ghadjar; H. M. Ryu; J. A. Proudfoot; S. Hayoz; J. M. Michalski; D. E. Spratt; Y. Liu; C. Schär; A. M. Berlin; D. R. Zwahlen; J. P. Simko; T. Hölscher; J. A. Efstathiou; B. Polat; H. M. Sandler; G. Hildebrandt; M. B. Parliament; A. C. Mueller; I. S. Dayes; L. Plasswilm; R. J.M. Correa; J. M. Robertson; T. G. Karrison; E. Davicioni; W. A. Hall; F. Y. Feng; A. Pollack; G. N. Thalmann; P. L. Nguyen; D. M. Aebersold; P. T. Tran; S. G. Zhao

doi:10.1016/j.annonc.2025.01.017

Predicting dose response to prostate cancer radiotherapy: validation of a radiation signature in the randomized phase III NRG/RTOG 0126 and SAKK 09/10 trials

A. Dal Pra
, P. Ghadjar
, H. M. Ryu
, J. A. Proudfoot
, S. Hayoz
, J. M. Michalski
, D. E. Spratt
, Y. Liu
, C. Schär
, A. M. Berlin
, D. R. Zwahlen
, J. P. Simko
, T. Hölscher
, J. A. Efstathiou
, B. Polat
, H. M. Sandler
, G. Hildebrandt
, M. B. Parliament
, A. C. Mueller
, I. S. Dayes

L. Plasswilm, R. J.M. Correa, J. M. Robertson, T. G. Karrison, E. Davicioni, W. A. Hall, F. Y. Feng, A. Pollack, G. N. Thalmann, P. L. Nguyen, D. M. Aebersold, P. T. Tran, S. G. Zhao

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

Background: The SAKK 09/10 trial randomized biochemically recurrent prostate cancer patients to salvage radiation 64 Gy versus 70 Gy, and the NRG/RTOG 0126 randomized intermediate-risk prostate cancer patients to definitive radiation 70.2 Gy versus 79.2 Gy. We investigated a previously developed Post-Operative Radiation Therapy Outcomes Score (PORTOS) to identify preferential benefit from radiation dose escalation (DE). Materials and methods: PORTOS was evaluated in patients enrolled in SAKK 09/10 and NRG/RTOG 0126 with available tissue that passed quality control (n = 226, 215). PORTOS was evaluated in the published post-operative groups in SAKK 09/10 and in tertiles in NRG/RTOG 0126 as cut-offs had not been established for biopsy samples and definitive radiation patients. Clinical and molecular correlates in a real-world dataset of 42 407 prostatectomy and 31 107 biopsy samples were also analyzed. Results: In SAKK 09/10, the biomarker-treatment interaction was statistically significant between PORTOS (lower versus higher) and treatment arm for clinical progression-free survival. Only patients in the higher PORTOS group benefited from DE. In NRG/RTOG 0126, in patients with a lower tertile PORTOS, there was no difference in Phoenix biochemical failure (BF). However, for patients in the average and higher tertile PORTOS range, there was a significant benefit for DE for Phoenix BF. An interaction test indicated a significant difference in benefit for DE between higher and lower PORTOS groups. PORTOS was not strongly associated with clinicopathological variables in either trial or the large real-world dataset. In the latter, PORTOS was modestly associated with hypoxia signatures and strongly associated with immune signatures and subtypes. Conclusion: In the SAKK 09/10 and RTOG 0126 randomized controlled trials, we demonstrated that PORTOS can potentially identify a subset of patients who benefit from DE, a subgroup that cannot be identified using clinicopathological or prognostic variables. These results suggest that PORTOS could be used clinically as a predictor of radiation response.

Original language	English
Pages (from-to)	572-582
Number of pages	11
Journal	Annals of Oncology
Volume	36
Issue number	5
DOIs	https://doi.org/10.1016/j.annonc.2025.01.017
State	Published - May 2025

Keywords

biomarkers
prostate cancer
radiation dose response

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10.1016/j.annonc.2025.01.017

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Dal Pra, A., Ghadjar, P., Ryu, H. M., Proudfoot, J. A., Hayoz, S., Michalski, J. M., Spratt, D. E., Liu, Y., Schär, C., Berlin, A. M., Zwahlen, D. R., Simko, J. P., Hölscher, T., Efstathiou, J. A., Polat, B., Sandler, H. M., Hildebrandt, G., Parliament, M. B., Mueller, A. C., ... Zhao, S. G. (2025). Predicting dose response to prostate cancer radiotherapy: validation of a radiation signature in the randomized phase III NRG/RTOG 0126 and SAKK 09/10 trials. Annals of Oncology, 36(5), 572-582. https://doi.org/10.1016/j.annonc.2025.01.017

@article{ae004148de67443480f9ca3895dc02b7,

title = "Predicting dose response to prostate cancer radiotherapy: validation of a radiation signature in the randomized phase III NRG/RTOG 0126 and SAKK 09/10 trials",

abstract = "Background: The SAKK 09/10 trial randomized biochemically recurrent prostate cancer patients to salvage radiation 64 Gy versus 70 Gy, and the NRG/RTOG 0126 randomized intermediate-risk prostate cancer patients to definitive radiation 70.2 Gy versus 79.2 Gy. We investigated a previously developed Post-Operative Radiation Therapy Outcomes Score (PORTOS) to identify preferential benefit from radiation dose escalation (DE). Materials and methods: PORTOS was evaluated in patients enrolled in SAKK 09/10 and NRG/RTOG 0126 with available tissue that passed quality control (n = 226, 215). PORTOS was evaluated in the published post-operative groups in SAKK 09/10 and in tertiles in NRG/RTOG 0126 as cut-offs had not been established for biopsy samples and definitive radiation patients. Clinical and molecular correlates in a real-world dataset of 42 407 prostatectomy and 31 107 biopsy samples were also analyzed. Results: In SAKK 09/10, the biomarker-treatment interaction was statistically significant between PORTOS (lower versus higher) and treatment arm for clinical progression-free survival. Only patients in the higher PORTOS group benefited from DE. In NRG/RTOG 0126, in patients with a lower tertile PORTOS, there was no difference in Phoenix biochemical failure (BF). However, for patients in the average and higher tertile PORTOS range, there was a significant benefit for DE for Phoenix BF. An interaction test indicated a significant difference in benefit for DE between higher and lower PORTOS groups. PORTOS was not strongly associated with clinicopathological variables in either trial or the large real-world dataset. In the latter, PORTOS was modestly associated with hypoxia signatures and strongly associated with immune signatures and subtypes. Conclusion: In the SAKK 09/10 and RTOG 0126 randomized controlled trials, we demonstrated that PORTOS can potentially identify a subset of patients who benefit from DE, a subgroup that cannot be identified using clinicopathological or prognostic variables. These results suggest that PORTOS could be used clinically as a predictor of radiation response.",

keywords = "biomarkers, prostate cancer, radiation dose response",

author = "\{Dal Pra\}, A. and P. Ghadjar and Ryu, \{H. M.\} and Proudfoot, \{J. A.\} and S. Hayoz and Michalski, \{J. M.\} and Spratt, \{D. E.\} and Y. Liu and C. Sch{\"a}r and Berlin, \{A. M.\} and Zwahlen, \{D. R.\} and Simko, \{J. P.\} and T. H{\"o}lscher and Efstathiou, \{J. A.\} and B. Polat and Sandler, \{H. M.\} and G. Hildebrandt and Parliament, \{M. B.\} and Mueller, \{A. C.\} and Dayes, \{I. S.\} and L. Plasswilm and Correa, \{R. J.M.\} and Robertson, \{J. M.\} and Karrison, \{T. G.\} and E. Davicioni and Hall, \{W. A.\} and Feng, \{F. Y.\} and A. Pollack and Thalmann, \{G. N.\} and Nguyen, \{P. L.\} and Aebersold, \{D. M.\} and Tran, \{P. T.\} and Zhao, \{S. G.\}",

note = "Publisher Copyright: {\textcopyright} 2025 The Authors",

year = "2025",

month = may,

doi = "10.1016/j.annonc.2025.01.017",

language = "English",

volume = "36",

pages = "572--582",

journal = "Annals of Oncology",

issn = "0923-7534",

number = "5",

}

Dal Pra, A, Ghadjar, P, Ryu, HM, Proudfoot, JA, Hayoz, S, Michalski, JM, Spratt, DE, Liu, Y, Schär, C, Berlin, AM, Zwahlen, DR, Simko, JP, Hölscher, T, Efstathiou, JA, Polat, B, Sandler, HM, Hildebrandt, G, Parliament, MB, Mueller, AC, Dayes, IS, Plasswilm, L, Correa, RJM, Robertson, JM, Karrison, TG, Davicioni, E, Hall, WA, Feng, FY, Pollack, A, Thalmann, GN, Nguyen, PL, Aebersold, DM, Tran, PT & Zhao, SG 2025, 'Predicting dose response to prostate cancer radiotherapy: validation of a radiation signature in the randomized phase III NRG/RTOG 0126 and SAKK 09/10 trials', Annals of Oncology, vol. 36, no. 5, pp. 572-582. https://doi.org/10.1016/j.annonc.2025.01.017

TY - JOUR

T1 - Predicting dose response to prostate cancer radiotherapy

T2 - validation of a radiation signature in the randomized phase III NRG/RTOG 0126 and SAKK 09/10 trials

AU - Dal Pra, A.

AU - Ghadjar, P.

AU - Ryu, H. M.

AU - Proudfoot, J. A.

AU - Hayoz, S.

AU - Michalski, J. M.

AU - Spratt, D. E.

AU - Liu, Y.

AU - Schär, C.

AU - Berlin, A. M.

AU - Zwahlen, D. R.

AU - Simko, J. P.

AU - Hölscher, T.

AU - Efstathiou, J. A.

AU - Polat, B.

AU - Sandler, H. M.

AU - Hildebrandt, G.

AU - Parliament, M. B.

AU - Mueller, A. C.

AU - Dayes, I. S.

AU - Plasswilm, L.

AU - Correa, R. J.M.

AU - Robertson, J. M.

AU - Karrison, T. G.

AU - Davicioni, E.

AU - Hall, W. A.

AU - Feng, F. Y.

AU - Pollack, A.

AU - Thalmann, G. N.

AU - Nguyen, P. L.

AU - Aebersold, D. M.

AU - Tran, P. T.

AU - Zhao, S. G.

PY - 2025/5

Y1 - 2025/5

N2 - Background: The SAKK 09/10 trial randomized biochemically recurrent prostate cancer patients to salvage radiation 64 Gy versus 70 Gy, and the NRG/RTOG 0126 randomized intermediate-risk prostate cancer patients to definitive radiation 70.2 Gy versus 79.2 Gy. We investigated a previously developed Post-Operative Radiation Therapy Outcomes Score (PORTOS) to identify preferential benefit from radiation dose escalation (DE). Materials and methods: PORTOS was evaluated in patients enrolled in SAKK 09/10 and NRG/RTOG 0126 with available tissue that passed quality control (n = 226, 215). PORTOS was evaluated in the published post-operative groups in SAKK 09/10 and in tertiles in NRG/RTOG 0126 as cut-offs had not been established for biopsy samples and definitive radiation patients. Clinical and molecular correlates in a real-world dataset of 42 407 prostatectomy and 31 107 biopsy samples were also analyzed. Results: In SAKK 09/10, the biomarker-treatment interaction was statistically significant between PORTOS (lower versus higher) and treatment arm for clinical progression-free survival. Only patients in the higher PORTOS group benefited from DE. In NRG/RTOG 0126, in patients with a lower tertile PORTOS, there was no difference in Phoenix biochemical failure (BF). However, for patients in the average and higher tertile PORTOS range, there was a significant benefit for DE for Phoenix BF. An interaction test indicated a significant difference in benefit for DE between higher and lower PORTOS groups. PORTOS was not strongly associated with clinicopathological variables in either trial or the large real-world dataset. In the latter, PORTOS was modestly associated with hypoxia signatures and strongly associated with immune signatures and subtypes. Conclusion: In the SAKK 09/10 and RTOG 0126 randomized controlled trials, we demonstrated that PORTOS can potentially identify a subset of patients who benefit from DE, a subgroup that cannot be identified using clinicopathological or prognostic variables. These results suggest that PORTOS could be used clinically as a predictor of radiation response.

AB - Background: The SAKK 09/10 trial randomized biochemically recurrent prostate cancer patients to salvage radiation 64 Gy versus 70 Gy, and the NRG/RTOG 0126 randomized intermediate-risk prostate cancer patients to definitive radiation 70.2 Gy versus 79.2 Gy. We investigated a previously developed Post-Operative Radiation Therapy Outcomes Score (PORTOS) to identify preferential benefit from radiation dose escalation (DE). Materials and methods: PORTOS was evaluated in patients enrolled in SAKK 09/10 and NRG/RTOG 0126 with available tissue that passed quality control (n = 226, 215). PORTOS was evaluated in the published post-operative groups in SAKK 09/10 and in tertiles in NRG/RTOG 0126 as cut-offs had not been established for biopsy samples and definitive radiation patients. Clinical and molecular correlates in a real-world dataset of 42 407 prostatectomy and 31 107 biopsy samples were also analyzed. Results: In SAKK 09/10, the biomarker-treatment interaction was statistically significant between PORTOS (lower versus higher) and treatment arm for clinical progression-free survival. Only patients in the higher PORTOS group benefited from DE. In NRG/RTOG 0126, in patients with a lower tertile PORTOS, there was no difference in Phoenix biochemical failure (BF). However, for patients in the average and higher tertile PORTOS range, there was a significant benefit for DE for Phoenix BF. An interaction test indicated a significant difference in benefit for DE between higher and lower PORTOS groups. PORTOS was not strongly associated with clinicopathological variables in either trial or the large real-world dataset. In the latter, PORTOS was modestly associated with hypoxia signatures and strongly associated with immune signatures and subtypes. Conclusion: In the SAKK 09/10 and RTOG 0126 randomized controlled trials, we demonstrated that PORTOS can potentially identify a subset of patients who benefit from DE, a subgroup that cannot be identified using clinicopathological or prognostic variables. These results suggest that PORTOS could be used clinically as a predictor of radiation response.

KW - biomarkers

KW - prostate cancer

KW - radiation dose response

UR - https://www.scopus.com/pages/publications/85219073953

U2 - 10.1016/j.annonc.2025.01.017

DO - 10.1016/j.annonc.2025.01.017

M3 - Article

C2 - 39986927

AN - SCOPUS:85219073953

SN - 0923-7534

VL - 36

SP - 572

EP - 582

JO - Annals of Oncology

JF - Annals of Oncology

IS - 5

ER -

Predicting dose response to prostate cancer radiotherapy: validation of a radiation signature in the randomized phase III NRG/RTOG 0126 and SAKK 09/10 trials

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Keywords

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