Preclinical dosimetry in proton minibeam radiation therapy: Robustness analysis and guidelines

Ramon Ortiz; Ludovic De Marzi; Yolanda Prezado

doi:10.1002/mp.15780

Preclinical dosimetry in proton minibeam radiation therapy: Robustness analysis and guidelines

Med Phys. 2022 Aug;49(8):5551-5561. doi: 10.1002/mp.15780. Epub 2022 Jun 8.

Authors

Ramon Ortiz^{1

2}, Ludovic De Marzi^{3

4}, Yolanda Prezado^{1

2}

Affiliations

¹ Institut Curie, Université PSL, CNRS UMR3347, Inserm U1021, Signalisation Radiobiologie et Cancer, Orsay, France.
² Université Paris-Saclay, CNRS UMR3347, Inserm U1021, Signalisation Radiobiologie et Cancer, Orsay, France.
³ Centre de Protonthérapie d'Orsay, Radiation Oncology Department, Campus Universitaire, Institut Curie, PSL Research University, Orsay, France.
⁴ Institut Curie, Campus Universitaire, PSL Research University, University Paris Saclay, INSERM LITO, Orsay, France.

Abstract

Purpose: Proton minibeam radiation therapy (pMBRT) is a new radiotherapy approach that has shown a significant increase in the therapeutic window in glioma-bearing rats compared to conventional proton therapy. The dosimetry of pMBRT is challenging and error prone due to the submillimetric beamlet sizes used. The aim of this study was to perform a robustness analysis on the setup parameters utilized in current preclinical trials and provide guidelines for reproducible dosimetry. The results of this work are intended to guide upcoming implementations of pMBRT worldwide, as well as pave the way for future clinical implementations.

Methods: Monte Carlo simulations and experimental data were used to evaluate the impact of variations in setup parameters and uncertainties in collimator specifications on lateral pMBRT dose distributions. The value of each parameter was modified individually to evaluate their effect on dose distributions. Experimental dosimetry was performed by means of high-resolution detectors, that is, radiochromic films, the IBA Razor and the Microdiamond detector. New guidelines were proposed to optimize the experimental setup in pMBRT studies and perform reproducible dosimetry.

Results: The sensitivity of dose distributions to uncertainties and variations in setup parameters was quantified. Quantities that define pMBRT lateral profiles (i.e., the peak-to-valley dose ratio [PVDR], peak and valley doses, and peak width) are significantly influenced by small-scale fluctuations in several of those parameters. The setup implemented at the Orsay proton therapy center for pMBRT irradiation was optimized to increase PVDRs and peak symmetry. In addition, we proposed guidelines to perform accurate and reproducible dosimetry in preclinical studies.

Conclusions: This study revealed the importance of adopting guidelines and protocols tailored to the distinct dose delivery method and dose distributions in pMBRT. This new methodology leads to reproducible dosimetry, which is imperative in preclinical trials. The results and guidelines presented in this manuscript can ease the initiation of pMBRT investigations in other centers.

Keywords: Monte Carlo simulations; dosimetry; proton minibeam radiation therapy; spatial fractionation of the dose.

MeSH terms

Animals
Glioma*
Monte Carlo Method
Proton Therapy* / methods
Protons
Radiometry / methods
Radiotherapy Dosage
Rats

Substances

Protons

Abstract

MeSH terms

Substances

Grants and funding