Literature DB >> 28664893

Preclinical radiotherapy at the Australian Synchrotron's Imaging and Medical Beamline: instrumentation, dosimetry and a small-animal feasibility study.

Jayde Livingstone1, Jean François Adam2, Jeffrey C Crosbie3, Chris J Hall1, Jessica E Lye4, Jonathan McKinlay1, Daniele Pelliccia3, Frédéric Pouzoulet5, Yolanda Prezado6, Andrew W Stevenson1, Daniel Häusermann1.   

Abstract

Therapeutic applications of synchrotron X-rays such as microbeam (MRT) and minibeam (MBRT) radiation therapy promise significant advantages over conventional clinical techniques for some diseases if successfully transferred to clinical practice. Preclinical studies show clear evidence that a number of normal tissues in animal models display a tolerance to much higher doses from MRT compared with conventional radiotherapy. However, a wide spread in the parameters studied makes it difficult to make any conclusions about the associated tumour control or normal tissue complication probabilities. To facilitate more systematic and reproducible preclinical synchrotron radiotherapy studies, a dedicated preclinical station including small-animal irradiation stage was designed and installed at the Imaging and Medical Beamline (IMBL) at the Australian Synchrotron. The stage was characterized in terms of the accuracy and reliability of the vertical scanning speed, as this is the key variable in dose delivery. The measured speed was found to be within 1% of the nominal speed for the range of speeds measured by an interferometer. Furthermore, dose measurements confirm the expected relationship between speed and dose and show that the measured dose is independent of the scan direction. Important dosimetric parameters such as peak dose, valley dose, the collimator output factor and peak-to-valley dose ratio are presented for 5 mm × 5 mm, 10 mm × 10 mm and 20 mm × 20 mm field sizes. Finally, a feasibility study on three glioma-bearing rats was performed. MRT and MBRT doses were prescribed to achieve an average dose of 65 Gy in the target, and magnetic resonance imaging follow-up was performed at various time points after irradiation to follow the tumour volume. Although it is impossible to draw conclusions on the different treatments with such a small number of animals, the feasibility of end-to-end preclinical synchrotron radiotherapy studies using the IMBL preclinical stage is demonstrated.

Entities:  

Keywords:  dosimetry; imaging; preclinical; radiotherapy

Mesh:

Year:  2017        PMID: 28664893     DOI: 10.1107/S1600577517006233

Source DB:  PubMed          Journal:  J Synchrotron Radiat        ISSN: 0909-0495            Impact factor:   2.616


  4 in total

1.  SyncMRT: a solution to image-guided synchrotron radiotherapy for quality assurance and pre-clinical trials.

Authors:  M J Barnes; J Paino; L R Day; D Butler; D Häusermann; D Pelliccia; J C Crosbie
Journal:  J Synchrotron Radiat       Date:  2022-06-07       Impact factor: 2.557

2.  Perspectives for microbeam irradiation at the SYRMEP beamline.

Authors:  Elisabeth Schültke; Stefan Fiedler; Ralf Hendrik Menk; Felix Jaekel; Diego Dreossi; Katia Casarin; Giuliana Tromba; Stefan Bartzsch; Stephan Kriesen; Guido Hildebrandt; Fulvia Arfelli
Journal:  J Synchrotron Radiat       Date:  2021-02-15       Impact factor: 2.616

3.  Evaluation of silicon strip detectors in transmission mode for online beam monitoring in microbeam radiation therapy at the Australian Synchrotron.

Authors:  Jeremy Davis; Andrew Dipuglia; Matthew Cameron; Jason Paino; Ashley Cullen; Susanna Guatelli; Marco Petasecca; Anatoly Rosenfeld; Michael Lerch
Journal:  J Synchrotron Radiat       Date:  2022-01-01       Impact factor: 2.616

4.  Comparative toxicity of synchrotron and conventional radiation therapy based on total and partial body irradiation in a murine model.

Authors:  Lloyd M L Smyth; Jacqueline F Donoghue; Jessica A Ventura; Jayde Livingstone; Tracy Bailey; Liam R J Day; Jeffrey C Crosbie; Peter A W Rogers
Journal:  Sci Rep       Date:  2018-08-13       Impact factor: 4.379

  4 in total

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