The Spinal Cord as Organ of Risk: Assessment for Acute and Subacute Neurological Adverse Effects after Microbeam Radiotherapy in a Rodent Model

Author:

Jaekel Felix1ORCID,Paino Jason2ORCID,Engels Elette2ORCID,Klein Mitzi3,Barnes Micah3ORCID,Häusermann Daniel3,Hall Christopher3,Zheng Gang4,Wang Hongxin4,Hildebrandt Guido1,Lerch Michael2ORCID,Schültke Elisabeth1

Affiliation:

1. Department of Radiooncology, Rostock University Medical Center, 18059 Rostock, Germany

2. Centre of Medical Radiation Physics, University of Wollongong, Wollongong 2522, Australia

3. Australian Synchrotron, ANSTO, Clayton 3168, Australia

4. Monash Biomedical Imaging, Clayton 3168, Australia

Abstract

Microbeam radiotherapy (MRT), a high dose rate radiotherapy technique using spatial dose fractionation at the micrometre range, has shown a high therapeutic efficacy in vivo in different tumour entities, including lung cancer. We have conducted a toxicity study for the spinal cord as organ of risk during irradiation of a target in the thoracic cavity. In young adult rats, the lower thoracic spinal cord was irradiated over a length of 2 cm with an array of quasi-parallel microbeams of 50 µm width, spaced at a centre-to-centre distance of 400 µm, with MRT peak doses up to 800 Gy. No acute or subacute adverse effects were observed within the first week after irradiation up to MRT peak doses of 400 Gy. No significant differences were seen between irradiated animals and non-irradiated controls in motor function and sensitivity, open field test and somatosensory evoked potentials (SSEP). After irradiation with MRT peak doses of 450–800 Gy, dose-dependent neurologic signs occurred. Provided that long-term studies do not reveal significant morbidity due to late toxicity, an MRT dose of 400 Gy can be considered safe for the spinal cord in the tested beam geometry and field size.

Funder

DAAD

DFG

ANSTO

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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