In Vitro Evaluation of Notch Inhibition to Enhance Efficacy of Radiation Therapy in Melanoma

Kamalram Thippu Jayaprakash, MSc, MRCP (UK), FRCR, MD; Mohammad Hussein, BSc, MSc, PhD; Richard Shaffer, MRCP (UK), FRCR; Agnieszka Michael, PhD; Andrew Nisbet, MSc, PhD; Mazhar Ajaz, MRCP (UK), FRCR, PhD

Advances in Radiation Oncology (Mar 2021)

In Vitro Evaluation of Notch Inhibition to Enhance Efficacy of Radiation Therapy in Melanoma

Kamalram Thippu Jayaprakash, MSc, MRCP (UK), FRCR, MD,
Mohammad Hussein, BSc, MSc, PhD,
Richard Shaffer, MRCP (UK), FRCR,
Agnieszka Michael, PhD,
Andrew Nisbet, MSc, PhD,
Mazhar Ajaz, MRCP (UK), FRCR, PhD

Affiliations

Kamalram Thippu Jayaprakash, MSc, MRCP (UK), FRCR, MD: Department of Clinical and Experimental Medicine, Faculty of Health and Medical Sciences, The Leggett Building, Manor Park, University of Surrey, Guildford, United Kingdom; Department of Oncology, St. Luke’s Cancer Centre, Royal Surrey Hospital, Egerton Road, Guildford, United Kingdom; Oncology Centre, Addenbrooke’s Hospital, Cambridge University Hospitals NHS Foundation Trust, Cambridge, United Kingdom; Department of Oncology, The Queen Elizabeth Hospital King’s Lynn NHS Foundation Trust, King’s Lynn, United Kingdom; Corresponding author: Kamalram Thippu Jayaprakash, MSc, MRCP (UK), FRCR, MD
Mohammad Hussein, BSc, MSc, PhD: Department of Medical Physics, St. Luke’s Cancer Centre, Royal Surrey Hospital, Guildford, United Kingdom
Richard Shaffer, MRCP (UK), FRCR: GenesisCare UK, Mount Alvernia Hospital, Guildford, United Kingdom
Agnieszka Michael, PhD: Department of Clinical and Experimental Medicine, Faculty of Health and Medical Sciences, The Leggett Building, Manor Park, University of Surrey, Guildford, United Kingdom; Department of Oncology, St. Luke’s Cancer Centre, Royal Surrey Hospital, Egerton Road, Guildford, United Kingdom
Andrew Nisbet, MSc, PhD: Department of Medical Physics and Biomedical Engineering, University College London, Malet Place Engineering Building, London, United Kingdom
Mazhar Ajaz, MRCP (UK), FRCR, PhD: Department of Clinical and Experimental Medicine, Faculty of Health and Medical Sciences, The Leggett Building, Manor Park, University of Surrey, Guildford, United Kingdom; Department of Oncology, St. Luke’s Cancer Centre, Royal Surrey Hospital, Egerton Road, Guildford, United Kingdom

Journal volume & issue: Vol. 6, no. 2
p. 100622

Abstract

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Purpose: The scope of radiation therapy is limited in melanoma. Using in vitro melanoma models, we investigated a Notch signaling inhibitor as a radiosensitizer to explore its potential to improve the efficacy of radiation therapy to widen the clinical application of radiation therapy in melanoma. Methods and Materials: Melanoma cell lines A375, SKMEL28, and G361 were grown using standard tissue culture methods. Radiation was delivered with a clinical x-ray unit, and a gamma secretase inhibitor RO4929097 was used to inhibit Notch signaling. Cell viability signal was used to calculate Loewe’s combination index to assess the interaction between radiation and RO4929097 and also the effect of scheduling of radiation and RO4929097 on synergy. Clonogenic assays were used to assess the clonogenic potential. An in vitro 3-dimensional culture model, γ-H2AX, and notch intracellular domain assays were used to interrogate potential underlying biological mechanisms of this approach. Scratch and transwell migration assays were used to assess cell migration. Results: A375 and SKMEL28 cell lines showed consistent synergy for most single radiation doses examined, with a tendency for better synergy with the radiation-first schedule (irradiation performed 24 hours before RO4929097 exposure). Clonogenic assays showed dose-dependent reduction in colony numbers. Both radiation and RO4929097 reduced the size of melanospheres grown in 3-dimensional culture in vitro, where RO4929097 demonstrated a significant effect on the size of A375 and SKMEL28 melanospheres, indicating potential modulation of stem cell phenotype. Radiation induced γ-H2AX foci signal levels were reduced after exposure to RO4929097 with a tendency toward reduction in notch intracellular domain levels for all 3 cell lines. RO4929097 impaired both de novo and radiation-enhanced cell migration. Conclusions: We demonstrate Notch signaling inhibition with RO4929097 as a promising strategy to potentially improve the efficacy of radiation therapy in melanoma. This strategy warrants further validation in vivo.

Published in Advances in Radiation Oncology

ISSN: 2452-1094 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Medicine (General): Medical physics. Medical radiology. Nuclear medicine; Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: http://www.journals.elsevier.com/advances-in-radiation-oncology/

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