Modulation of mTOR signaling by radiation and rapamycin treatment in canine mast cell cancer cells

Morla Phan; Changseok Kim; Anthony Mutsaers; Valerie Poirier; Brenda Coomber

Modulation of mTOR signaling by radiation and rapamycin treatment in canine mast cell cancer cells

Can J Vet Res. 2022 Jan;86(1):3-12.

Authors

Morla Phan¹, Changseok Kim¹, Anthony Mutsaers¹, Valerie Poirier¹, Brenda Coomber¹

Affiliation

¹ Department of Biomedical Sciences (Phan, Mutsaers, Coomber) and Department of Clinical Studies (Kim, Mutsaers, Poirier), Ontario Veterinary College, University of Guelph, Guelph, Ontario N1G 2W1.

PMID: 34975216
PMCID: PMC8697317

Abstract
in English, French

Rapamycin has been reported to reduce cancer cell survival in certain tumors following radiation therapy, but the mechanisms driving this phenomenon are unclear. Rapamycin inhibits mTOR signaling, a pathway responsible for several essential cell functions. The objective of this study was to investigate the effects of rapamycin and radiation on the activation and inhibition of mTOR signaling and the relationship between mTOR signaling and DNA damage response in vitro using canine mast cell tumor (MCT) cancer cell lines. Rapamycin rapidly inhibited S6K phosphorylation in a dose-dependent manner. Ionizing radiation (3, 6, or 10 Gy) was able to activate mTOR signalling, but the combination of radiation and rapamycin maintained mTOR inhibition. The comet assay revealed that co-treatment with rapamycin induced modest increases in the severity of DNA damage to MCT cells, but that these differences were not statistically significant. Although the relationship between mTOR and DNA damage response in MCT cancer cell lines remains unclear, our findings suggest the possibility of interaction, leading to enhancement of radiation response.

Il a été rapporté que la rapamycine réduisait la survie des cellules cancéreuses dans certaines tumeurs après une radiothérapie, mais les mécanismes à l’origine de ce phénomène ne sont pas clairs. La rapamycine inhibe la signalisation mTOR, une voie responsable de plusieurs fonctions cellulaires essentielles. L’objectif de cette étude était d’étudier les effets de la rapamycine et des radiations sur l’activation et l’inhibition de la signalisation mTOR et la relation entre la signalisation mTOR et la réponse aux dommages à l’ADN in vitro à l’aide de lignées cellulaires cancéreuses de tumeurs mastocytaires canines (MCT). La rapamycine a rapidement inhibé la phosphorylation de S6K de manière dose-dépendante. Le rayonnement ionisant (3, 6 ou 10 Gy) a pu activer la signalisation mTOR, mais la combinaison de rayonnement et de rapamycine a maintenu l’inhibition de mTOR. Le test des comètes a révélé que le co-traitement avec la rapamycine induisait des augmentations modestes de la gravité des dommages à l’ADN des cellules MCT, mais que ces différences n’étaient pas statistiquement significatives. Bien que la relation entre mTOR et la réponse aux dommages à l’ADN dans les lignées cellulaires cancéreuses MCT reste incertaine, nos résultats suggèrent la possibilité d’une interaction, conduisant à une amélioration de la réponse aux radiations.(Traduit par Docteur Serge Messier).

Copyright and/or publishing rights held by the Canadian Veterinary Medical Association.

MeSH terms

Animals
Cell Line, Tumor
Dog Diseases* / drug therapy
Dog Diseases* / radiotherapy
Dogs
Mast Cells* / drug effects
Mast Cells* / radiation effects
Signal Transduction* / drug effects
Signal Transduction* / radiation effects
Sirolimus* / pharmacology
TOR Serine-Threonine Kinases* / drug effects
TOR Serine-Threonine Kinases* / radiation effects

Substances

TOR Serine-Threonine Kinases
Sirolimus

Abstract in English, French

MeSH terms

Substances

Abstract
in English, French