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Ιδρυματικό Αποθετήριο Πανεπιστημίου Θεσσαλίας
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Flash proton radiotherapy spares normal epithelial and mesenchymal tissues while preserving sarcoma response

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Συγγραφέας
Velalopoulou A., Karagounis I.V., Cramer G.M., Kim M.M., Skoufos G., Goia D., Hagan S., Verginadis I.I., Shoniyozov K., Chiango J., Cerullo M., Varner K., Yao L., Qin L., Hatzigeorgiou A.G., Minn A.J., Putt M., Lanza M., Assenmacher C.-A., Radaelli E., Huck J., Diffenderfer E., Dong L., Metz J., Koumenis C., Cengel K.A., Maity A., Busch T.M.
Ημερομηνία
2021
Γλώσσα
en
DOI
10.1158/0008-5472.CAN-21-1500
Λέξη-κλειδί
animal experiment
animal model
animal tissue
apoptosis
Article
bone development
bone injury
cell differentiation
chondrocyte
controlled study
epithelium
female
flash proton therapy
inflammation
keratinocyte
lymphedema
mesenchyme
mouse
muscle injury
nonhuman
osteoclast
osteolysis
proton therapy
sarcoma
signal transduction
skin defect
stem cell
adverse event
animal
bone
conservative treatment
disease model
dog
epithelium
gene expression profiling
human
metabolism
morbidity
muscle
pathology
procedures
radiation injury
radiation response
radiotherapy dosage
sarcoma
skin
treatment outcome
Animals
Bone and Bones
Disease Models, Animal
Dogs
Epithelium
Female
Gene Expression Profiling
Humans
Mice
Morbidity
Muscles
Organ Sparing Treatments
Proton Therapy
Radiation Injuries
Radiotherapy Dosage
Sarcoma
Skin
Treatment Outcome
American Association for Cancer Research Inc.
Εμφάνιση Μεταδεδομένων
Επιτομή
In studies of electron and proton radiotherapy, ultrahigh dose rates of FLASH radiotherapy appear to produce fewer toxicities than standard dose rates while maintaining local tumor control. FLASHproton radiotherapy (F-PRT) brings the spatial advantages of PRT to FLASH dose rates (>40 Gy/second), making it important to understand if and how F-PRT spares normal tissues while providing antitumor efficacy that is equivalent to standard-proton radiotherapy (S-PRT). Here we studied PRT damage to skin and mesenchymal tissues of muscle and bone and found that F-PRT of the C57BL/6 murine hind leg produced fewer severe toxicities leading to death or requiring euthanasia than S-PRT of the same dose. RNA-seq analyses of murine skin and bone revealed pathways upregulated by S-PRT yet unaltered by F-PRT, such as apoptosis signaling and keratinocyte differentiation in skin, as well as osteoclast differentiation and chondrocyte development in bone. Corroborating these findings, F-PRT reduced skin injury, stem cell depletion, and inflammation, mitigated late effects including lymphedema, and decreased histopathologically detected myofiber atrophy, bone resorption, hair follicle atrophy, and epidermal hyperplasia. F-PRT was equipotent to S-PRT in control of two murine sarcoma models, including at an orthotopic intramuscular site, thereby establishing its relevance to mesenchymal cancers. Finally, S-PRT produced greater increases in TGFb1 in murine skin and the skin of canines enrolled in a phase I study of F-PRT versus S-PRT. Collectively, these data provide novel insights into F-PRT-mediated tissue sparing and support its ongoing investigation in applications that would benefit fromthis sparing of skin and mesenchymal tissues. © 2021 The Authors.
URI
http://hdl.handle.net/11615/80553
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