Disease control and late toxicity in Adaptive Dose Painting by Numbers vs. non-adaptive radiotherapy for head and neck cancer: a randomized controlled phase II trial.

De Bruycker, Aurélie; De Neve, Wilfried; Daisne, Jean-François; Vercauteren, Tom; De Gersem, Werner; Olteanu, Luiza; Berwouts, Dieter; Deheneffe, Stéphanie; Madani, Indira; Goethals, Ingeborg; Duprez, Fréderic

doi:10.1016/j.ijrobp.2024.01.012

Disease control and late toxicity in Adaptive Dose Painting by Numbers vs. non-adaptive radiotherapy for head and neck cancer: a randomized controlled phase II trial.

De Bruycker, Aurélie

;

De Neve, Wilfried

;

Daisne, Jean-François

;

Vercauteren, Tom

;

Duprez, Fréderic

;et.al.

(2024) International Journal of Radiation: Oncology - Biology - Physics — Vol. 120, n° 2, p. 516-527 (2024)

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Authors

De Bruycker, Aurélie
Author
De Neve, Wilfried
Author
Daisne, Jean-François
Author
Vercauteren, Tom
Author
Deheneffe, StéphanieUCLouvain
Author
Duprez, Fréderic
Author

Abstract

Local recurrence remains the main cause of death in stage III-IV non-metastatic head-and-neck cancer (HNC) with relapse-prone regions within high F-FDG-PET-signal gross tumor volume. We investigated if dose-escalation within this subvolume combined with a 3-phase treatment-adaptation could increase local (LC) and regional (RC) control at equal or minimized radiation-induced toxicity, by comparing adaptive F-FDG-PET-voxel-intensity-based dose-painting-by-numbers (A-DPBN) with non-adaptive standard intensity-modulated radiotherapy (S-IMRT). This two-center randomized controlled phase II trial assigned (1:1) patients to receive A-DPBN or S-IMRT (+/-chemotherapy). Eligibility: non-metastatic HNC of oral cavity, oro-/hypopharynx or larynx, needing radio(chemo)therapy; T1-4N0-3 (exception: T1-2N0 glottic); KPS≥70; ≥18 years and informed consent. 1-year LC and RC. The dose prescription for A-DPBN was intercurrently adapted in two steps to an absolute dose-volume limit (≤1.75cm can receive >84Gy and normalized isoeffective dose >96Gy) as a safety measure during the study course after 4/7 A-DPBN patients developed ≥G3 mucosal ulcers. Ninety-five patients were randomized (A-DPBN: 47; S-IMRT: 48). Median follow-up amounts 31 months (IQR: 14-48 months); 29 patients died (17 of cancer progression). A-DPBN results in superior LC compared to S-IMRT with 1- and 2-year LC of 91% and 88% vs. 78% and 75%, respectively (hazard ratio, 3.13; 95% confidence interval, 1.13-8.71; p=0.021). RC and overall survival are comparable between arms, as is overall grade (G) ≥3 late toxicity (36% vs. 20%, p=0.1). More ≥G3 late mucosal ulcers are observed in active smokers (29% vs. 3%, p=0.005) and alcohol users (33% vs. 13%, p=0.02), independent of treatment arm. Similarly, in the A-DPBN arm, significantly more patients that smoked at diagnosis developed ≥G3 (46% vs. 12%, p=0.005) and ≥G4 (29% vs. 8%, p=0.048) mucosal ulcers. One arterial blowout occurred following a G5 mucosal toxicity. A-DPBN resulted in superior 1- and 2-year LC for HNC compared to S-IMRT. This supports further exploration in multicenter phase III trials. It will however be challenging to recruit a substantial patient sample for such trials as concerns have arisen on the association of late mucosal ulcers when escalating the dose in continuing smokers.

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De Bruycker, A., De Neve, W., Daisne, J.-F., Vercauteren, T., De Gersem, W., Olteanu, L., Berwouts, D., Deheneffe, S., Madani, I., Goethals, I., & Duprez, F. (2024). Disease control and late toxicity in Adaptive Dose Painting by Numbers vs. non-adaptive radiotherapy for head and neck cancer: a randomized controlled phase II trial. International Journal of Radiation: Oncology - Biology - Physics, 120(2), 516-527. https://doi.org/10.1016/j.ijrobp.2024.01.012 (Original work published 2024)