ESTRO 2022

Session Item

Sunday

May 08

16:55 - 17:55

Auditorium 12

Microenvironment

Chair: Kasper Rouschop, The Netherlands;

Co-Chair: Sissel Hauge, Norway

Session Code: 2500

Session Type: Proffered Papers

Track: Radiobiology

17:35 - 17:45

Fractionated radiotherapy and its effect on the tumour microenvironment: a small animal study.

Rebecca D'Alonzo, Australia

Presentation Number: OC-0597

Abstract

Abstract Title:

Fractionated radiotherapy and its effect on the tumour microenvironment: a small animal study.

Authors:

Rebecca D'Alonzo^1,2,3, Synat Keam^4,2,3, Kelly MacKinnon^1,2, Alistair Cook^2,3,5, Anna Nowak^2,3,4, Suki Gill⁶, Pejman Rowshanfarzad¹, Martin Ebert^1,7,8

¹University of Western Australia, School of Physics, Mathematics and Computing, Perth, Australia; ²University of Western Australia, National Centre for Asbestos Related Diseases, Perth, Australia; ³Institute for Respiratory Health, Institute for Respiratory Health, Perth, Australia; ⁴University of Western Australia, Medical School, Perth, Australia; ⁵University of Western Australia, School of Biomedical Sciences, Perth, Australia; ⁶Sir Charles Gairdner Hospital, Department of Radiation Oncology, Perth, Australia; ⁷Sir Charles Gairdner Hospital, Australia, Department of Radiation Oncology, Perth, Australia; ⁸5D Clinics, 5D Clinics, Perth, Australia

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Purpose or Objective

Malignant tumours have decreased oxygenation due to malformed blood vessels. Hypoxia decreases the effectiveness of radiotherapy (RT), and the abnormal vessels prevent both systemic therapies and immune cells from reaching some areas of the tumour. Tumour hypoxia is associated with poorer prognosis. This study was aimed at quantifying alterations of the tumour microenvironment (TME) that can be achieved with varying RT fractionation. The objective was to assess changes in vasculature normalisation and reoxygenation that can be achieved with localised RT in order to facilitate better tumour access for lymphocytes and systemic therapies.

Material and Methods

AB1-HA mesothelioma tumour cells were subcutaneously injected into BALB/cJAusbP mice. Mice with established tumours underwent RT fractionation with an X-RAD 225Cx small animal RT device, a pre-clinical translation of clinical linear accelerators. Starting 10 days post-inoculation, mice received one of the following fractionation schedules: 0 Gy, 2 Gy x 3, 2 Gy x 4, 2 Gy x 5, 6 Gy x 1 or 6 Gy x 2 fractions. Fractions were delivered on consecutive days. On day 15 mice underwent hybrid optical and Doppler ultrasound imaging with a LAZR-X photoacoustic imaging instrument, to assess the spatial oxygen saturation concentration and the vasculature within the tumour. Imaging continued every second day, until day 29 post-inoculation, when mice were euthanised, and tumours harvested. Harvested tumours were stained for markers of vasculature and hypoxia.

Results

Alterations to the TME were observed following different RT fractionation schedules. Imaging showed an increase in oxygen saturation and vascularisation for irradiated tumours. The changes were significant for 2 Gy x 4, 2 Gy x 5 and 6 Gy x 2 fractions compared to the control, with 2 Gy x 5 having the greatest increase and being extremely significant (p<0.1x10^-6) across all modalities. These results were supported by tissue stains, which showed both an overall absolute increase in vasculature and improved vessel normalisation.

Conclusion

RT fractionation can be used to modulate the TME. This has the potential to be exploited to prime the tumour for susceptibility to other treatments, for example immune checkpoint inhibitors.