FLASH Proton Radiation Therapy Mitigates Inflammatory and Fibrotic Pathways and Preserves Cardiac Function in a Preclinical Mouse Model of Radiation-Induced Heart Disease

Kyle Kim; Michele M Kim; Giorgos Skoufos; Eric S Diffenderfer; Seyyedeh Azar Oliaei Motlagh; Michail Kokkorakis; Ilektra Koliaki; George Morcos; Khayrullo Shoniyozov; Joanna Griffin; Artemis G Hatzigeorgiou; James M Metz; Alexander Lin; Steven J Feigenberg; Keith A Cengel; Bonnie Ky; Constantinos Koumenis; Ioannis I Verginadis

doi:10.1016/j.ijrobp.2024.01.224

FLASH Proton Radiation Therapy Mitigates Inflammatory and Fibrotic Pathways and Preserves Cardiac Function in a Preclinical Mouse Model of Radiation-Induced Heart Disease

Int J Radiat Oncol Biol Phys. 2024 Feb 15:S0360-3016(24)00301-8. doi: 10.1016/j.ijrobp.2024.01.224. Online ahead of print.

Authors

Kyle Kim¹, Michele M Kim¹, Giorgos Skoufos², Eric S Diffenderfer¹, Seyyedeh Azar Oliaei Motlagh¹, Michail Kokkorakis³, Ilektra Koliaki³, George Morcos¹, Khayrullo Shoniyozov¹, Joanna Griffin⁴, Artemis G Hatzigeorgiou⁵, James M Metz¹, Alexander Lin¹, Steven J Feigenberg¹, Keith A Cengel¹, Bonnie Ky⁶, Constantinos Koumenis⁷, Ioannis I Verginadis⁸

Affiliations

¹ Department of Radiation Oncology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania.
² Department of Electrical & Computer Engineering, University of Thessaly, Greece; Hellenic Pasteur Institute, Athens, Greece.
³ Department of Radiation Oncology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania; Department of Clinical Pharmacy and Pharmacology, University of Groningen, University Medical Center Groningen, Groningen, The Netherlands.
⁴ Department of Medicine, Cardiovascular Institute, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania.
⁵ Department of Electrical & Computer Engineering, University of Thessaly, Greece; Hellenic Pasteur Institute, Athens, Greece; DIANA-Laboratory, Department of Computer Science and Biomedical Informatics, University of Thessaly, Thessaly, Greece.
⁶ Department of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania.
⁷ Department of Radiation Oncology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania. Electronic address: costas.koumenis@pennmedicine.upenn.edu.
⁸ Department of Radiation Oncology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania. Electronic address: vioannis@pennmedicine.upenn.edu.

PMID: 38364948
DOI: 10.1016/j.ijrobp.2024.01.224

Abstract

Purpose: Studies during the past 9 years suggest that delivering radiation at dose rates exceeding 40 Gy/s, known as "FLASH" radiation therapy, enhances the therapeutic index of radiation therapy (RT) by decreasing normal tissue damage while maintaining tumor response compared with conventional (or standard) RT. This study demonstrates the cardioprotective benefits of FLASH proton RT (F-PRT) compared with standard (conventional) proton RT (S-PRT), as evidenced by reduced acute and chronic cardiac toxicities.

Methods and materials: Mice were imaged using cone beam computed tomography to precisely determine the heart's apex as the beam isocenter. Irradiation was conducted using a shoot-through technique with a 5-mm diameter circular collimator. Bulk RNA-sequencing was performed on nonirradiated samples, as well as apexes treated with F-PRT or S-PRT, at 2 weeks after a single 40 Gy dose. Inflammatory responses were assessed through multiplex cytokine/chemokine microbead assay and immunofluorescence analyses. Levels of perivascular fibrosis were quantified using Masson's Trichrome and Picrosirius red staining. Additionally, cardiac tissue functionality was evaluated by 2-dimensional echocardiograms at 8- and 30-weeks post-PRT.

Results: Radiation damage was specifically localized to the heart's apex. RNA profiling of cardiac tissues treated with PRT revealed that S-PRT uniquely upregulated pathways associated with DNA damage response, induction of tumor necrosis factor superfamily, and inflammatory response, and F-PRT primarily affected cytoplasmic translation, mitochondrion organization, and adenosine triphosphate synthesis. Notably, F-PRT led to a milder inflammatory response, accompanied by significantly attenuated changes in transforming growth factor β1 and α smooth muscle actin levels. Critically, F-PRT decreased collagen deposition and better preserved cardiac functionality compared with S-PRT.

Conclusions: This study demonstrated that F-PRT reduces the induction of an inflammatory environment with lower expression of inflammatory cytokines and profibrotic factors. Importantly, the results indicate that F-PRT better preserves cardiac functionality, as confirmed by echocardiography analysis, while also mitigating the development of long-term fibrosis.

Grants and funding

P01 CA257904/CA/NCI NIH HHS/United States