Esomeprazole enhances the effect of ionizing radiation to improve tumor control

Kassidy A. Hebert; Sergio Jaramillo; Wangjie Yu; Min Wang; Ratna Veeramachaneni; Vlad C. Sandulache; Andrew G. Sikora; Mark D. Bonnen; Ananth V. Annapragada; David Corry; Farrah Kheradmand; Raj K. Pandita; Michelle S. Ludwig; Tej K. Pandita; Shixia Huang; Cristian Coarfa; Sandra L. Grimm; Dimuthu Perera; George Miles; Yohannes T. Ghebre

doi:10.18632/oncotarget.28008

Esomeprazole enhances the effect of ionizing radiation to improve tumor control

Kassidy A. Hebert, Sergio Jaramillo, Wangjie Yu, Min Wang, Ratna Veeramachaneni, Vlad C. Sandulache, Andrew G. Sikora, Mark D. Bonnen, Ananth V. Annapragada, David Corry, Farrah Kheradmand, Raj K. Pandita, Michelle S. Ludwig, Tej K. Pandita, Shixia Huang, Cristian Coarfa, Sandra L. Grimm, Dimuthu Perera, George Miles, Yohannes T. Ghebre

Head & Neck Surgery

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

The resistance of cancer cells to radiation-based treatment is a major clinical challenge confounding standard of care in cancer. This problem is particularly notable in many solid tumors where cancer cells are only partially responsive to radiation therapy. Combination of radiation with radiosensitizers is able to enhance tumor cell killing. However, currently available radiosensitizers are associated with significant normal tissue toxicity. Accordingly, there is an unmet need to develop safer and more effective radiosensitizers to improve tumor control. Here, we evaluated the radiosensitizing effect of the FDA-approved drug esomeprazole in normal and radioresistant human head and neck squamous cell carcinoma (HNSCC) cells in vitro, and in a mouse model of HNSCC. For the in vitro studies, we used cancer cell colony formation (clonogenicity) assay to compare cancer cell growth in the absence or presence of esomeprazole. To determine mechanism(s) of action, we assessed cell proliferation and profiled cell cycle regulatory proteins. In addition, we performed reverse phase protein array (RPPA) study to understand the global effect of esomeprazole on over 200 cancer-related proteins. For the in vivo study, we engrafted HNSCC in a mouse model and compared tumor growth in animals treated with radiation, esomeprazole, and combination of radiation with esomeprazole. We found that esomeprazole inhibits tumor growth and dose-dependently enhances the cell killing effect of ionizing radiation in wildtype and p53-mutant radioresistant cancer cells. Mechanistic studies demonstrate that esomeprazole arrests cancer cells in the G1 phase of the cell cycle through upregulation of p21 protein and inhibition of cyclin-dependent kinases (Cdks) type 1 (Cdk1) and type 2 (Cdk2). In vivo data showed greater tumor control in animals treated with combination of radiation and esomeprazole compared to either treatment alone, and that this was associated with inhibition of cell proliferation in vivo. In addition, combination of esomeprazole with radiation significantly impaired repair following radiation-induced DNA damage. Our studies indicate that esomeprazole sensitizes cancer cells to ionizing radiation, and is associated with upregulation of p21 to arrest cells in the G1 phase of the cell cycle. Our findings have significant therapeutic implications for the repurposing of esomeprazole as a radiosensitizer in HNSCC and other solid tumors.

Original language	English (US)
Pages (from-to)	1339-1353
Number of pages	15
Journal	Oncotarget
Volume	12
Issue number	14
DOIs	https://doi.org/10.18632/oncotarget.28008
State	Published - Jul 6 2021

Keywords

Esomeprazole
Ionizing radiation
Proton pump inhibitors
Radiosensitization
Tumor control

ASJC Scopus subject areas

Oncology

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10.18632/oncotarget.28008

Cite this

Hebert, K. A., Jaramillo, S., Yu, W., Wang, M., Veeramachaneni, R., Sandulache, V. C., Sikora, A. G., Bonnen, M. D., Annapragada, A. V., Corry, D., Kheradmand, F., Pandita, R. K., Ludwig, M. S., Pandita, T. K., Huang, S., Coarfa, C., Grimm, S. L., Perera, D., Miles, G., & Ghebre, Y. T. (2021). Esomeprazole enhances the effect of ionizing radiation to improve tumor control. Oncotarget, 12(14), 1339-1353. https://doi.org/10.18632/oncotarget.28008

Hebert, KA, Jaramillo, S, Yu, W, Wang, M, Veeramachaneni, R, Sandulache, VC, Sikora, AG, Bonnen, MD, Annapragada, AV, Corry, D, Kheradmand, F, Pandita, RK, Ludwig, MS, Pandita, TK, Huang, S, Coarfa, C, Grimm, SL, Perera, D, Miles, G & Ghebre, YT 2021, 'Esomeprazole enhances the effect of ionizing radiation to improve tumor control', Oncotarget, vol. 12, no. 14, pp. 1339-1353. https://doi.org/10.18632/oncotarget.28008

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title = "Esomeprazole enhances the effect of ionizing radiation to improve tumor control",

abstract = "The resistance of cancer cells to radiation-based treatment is a major clinical challenge confounding standard of care in cancer. This problem is particularly notable in many solid tumors where cancer cells are only partially responsive to radiation therapy. Combination of radiation with radiosensitizers is able to enhance tumor cell killing. However, currently available radiosensitizers are associated with significant normal tissue toxicity. Accordingly, there is an unmet need to develop safer and more effective radiosensitizers to improve tumor control. Here, we evaluated the radiosensitizing effect of the FDA-approved drug esomeprazole in normal and radioresistant human head and neck squamous cell carcinoma (HNSCC) cells in vitro, and in a mouse model of HNSCC. For the in vitro studies, we used cancer cell colony formation (clonogenicity) assay to compare cancer cell growth in the absence or presence of esomeprazole. To determine mechanism(s) of action, we assessed cell proliferation and profiled cell cycle regulatory proteins. In addition, we performed reverse phase protein array (RPPA) study to understand the global effect of esomeprazole on over 200 cancer-related proteins. For the in vivo study, we engrafted HNSCC in a mouse model and compared tumor growth in animals treated with radiation, esomeprazole, and combination of radiation with esomeprazole. We found that esomeprazole inhibits tumor growth and dose-dependently enhances the cell killing effect of ionizing radiation in wildtype and p53-mutant radioresistant cancer cells. Mechanistic studies demonstrate that esomeprazole arrests cancer cells in the G1 phase of the cell cycle through upregulation of p21 protein and inhibition of cyclin-dependent kinases (Cdks) type 1 (Cdk1) and type 2 (Cdk2). In vivo data showed greater tumor control in animals treated with combination of radiation and esomeprazole compared to either treatment alone, and that this was associated with inhibition of cell proliferation in vivo. In addition, combination of esomeprazole with radiation significantly impaired repair following radiation-induced DNA damage. Our studies indicate that esomeprazole sensitizes cancer cells to ionizing radiation, and is associated with upregulation of p21 to arrest cells in the G1 phase of the cell cycle. Our findings have significant therapeutic implications for the repurposing of esomeprazole as a radiosensitizer in HNSCC and other solid tumors.",

keywords = "Esomeprazole, Ionizing radiation, Proton pump inhibitors, Radiosensitization, Tumor control",

author = "Hebert, {Kassidy A.} and Sergio Jaramillo and Wangjie Yu and Min Wang and Ratna Veeramachaneni and Sandulache, {Vlad C.} and Sikora, {Andrew G.} and Bonnen, {Mark D.} and Annapragada, {Ananth V.} and David Corry and Farrah Kheradmand and Pandita, {Raj K.} and Ludwig, {Michelle S.} and Pandita, {Tej K.} and Shixia Huang and Cristian Coarfa and Grimm, {Sandra L.} and Dimuthu Perera and George Miles and Ghebre, {Yohannes T.}",

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doi = "10.18632/oncotarget.28008",

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AU - Hebert, Kassidy A.

AU - Jaramillo, Sergio

AU - Yu, Wangjie

AU - Wang, Min

AU - Veeramachaneni, Ratna

AU - Sandulache, Vlad C.

AU - Sikora, Andrew G.

AU - Bonnen, Mark D.

AU - Annapragada, Ananth V.

AU - Corry, David

AU - Kheradmand, Farrah

AU - Pandita, Raj K.

AU - Ludwig, Michelle S.

AU - Pandita, Tej K.

AU - Huang, Shixia

AU - Coarfa, Cristian

AU - Grimm, Sandra L.

AU - Perera, Dimuthu

AU - Miles, George

AU - Ghebre, Yohannes T.

PY - 2021/7/6

Y1 - 2021/7/6

N2 - The resistance of cancer cells to radiation-based treatment is a major clinical challenge confounding standard of care in cancer. This problem is particularly notable in many solid tumors where cancer cells are only partially responsive to radiation therapy. Combination of radiation with radiosensitizers is able to enhance tumor cell killing. However, currently available radiosensitizers are associated with significant normal tissue toxicity. Accordingly, there is an unmet need to develop safer and more effective radiosensitizers to improve tumor control. Here, we evaluated the radiosensitizing effect of the FDA-approved drug esomeprazole in normal and radioresistant human head and neck squamous cell carcinoma (HNSCC) cells in vitro, and in a mouse model of HNSCC. For the in vitro studies, we used cancer cell colony formation (clonogenicity) assay to compare cancer cell growth in the absence or presence of esomeprazole. To determine mechanism(s) of action, we assessed cell proliferation and profiled cell cycle regulatory proteins. In addition, we performed reverse phase protein array (RPPA) study to understand the global effect of esomeprazole on over 200 cancer-related proteins. For the in vivo study, we engrafted HNSCC in a mouse model and compared tumor growth in animals treated with radiation, esomeprazole, and combination of radiation with esomeprazole. We found that esomeprazole inhibits tumor growth and dose-dependently enhances the cell killing effect of ionizing radiation in wildtype and p53-mutant radioresistant cancer cells. Mechanistic studies demonstrate that esomeprazole arrests cancer cells in the G1 phase of the cell cycle through upregulation of p21 protein and inhibition of cyclin-dependent kinases (Cdks) type 1 (Cdk1) and type 2 (Cdk2). In vivo data showed greater tumor control in animals treated with combination of radiation and esomeprazole compared to either treatment alone, and that this was associated with inhibition of cell proliferation in vivo. In addition, combination of esomeprazole with radiation significantly impaired repair following radiation-induced DNA damage. Our studies indicate that esomeprazole sensitizes cancer cells to ionizing radiation, and is associated with upregulation of p21 to arrest cells in the G1 phase of the cell cycle. Our findings have significant therapeutic implications for the repurposing of esomeprazole as a radiosensitizer in HNSCC and other solid tumors.

AB - The resistance of cancer cells to radiation-based treatment is a major clinical challenge confounding standard of care in cancer. This problem is particularly notable in many solid tumors where cancer cells are only partially responsive to radiation therapy. Combination of radiation with radiosensitizers is able to enhance tumor cell killing. However, currently available radiosensitizers are associated with significant normal tissue toxicity. Accordingly, there is an unmet need to develop safer and more effective radiosensitizers to improve tumor control. Here, we evaluated the radiosensitizing effect of the FDA-approved drug esomeprazole in normal and radioresistant human head and neck squamous cell carcinoma (HNSCC) cells in vitro, and in a mouse model of HNSCC. For the in vitro studies, we used cancer cell colony formation (clonogenicity) assay to compare cancer cell growth in the absence or presence of esomeprazole. To determine mechanism(s) of action, we assessed cell proliferation and profiled cell cycle regulatory proteins. In addition, we performed reverse phase protein array (RPPA) study to understand the global effect of esomeprazole on over 200 cancer-related proteins. For the in vivo study, we engrafted HNSCC in a mouse model and compared tumor growth in animals treated with radiation, esomeprazole, and combination of radiation with esomeprazole. We found that esomeprazole inhibits tumor growth and dose-dependently enhances the cell killing effect of ionizing radiation in wildtype and p53-mutant radioresistant cancer cells. Mechanistic studies demonstrate that esomeprazole arrests cancer cells in the G1 phase of the cell cycle through upregulation of p21 protein and inhibition of cyclin-dependent kinases (Cdks) type 1 (Cdk1) and type 2 (Cdk2). In vivo data showed greater tumor control in animals treated with combination of radiation and esomeprazole compared to either treatment alone, and that this was associated with inhibition of cell proliferation in vivo. In addition, combination of esomeprazole with radiation significantly impaired repair following radiation-induced DNA damage. Our studies indicate that esomeprazole sensitizes cancer cells to ionizing radiation, and is associated with upregulation of p21 to arrest cells in the G1 phase of the cell cycle. Our findings have significant therapeutic implications for the repurposing of esomeprazole as a radiosensitizer in HNSCC and other solid tumors.

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KW - Ionizing radiation

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KW - Radiosensitization

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Esomeprazole enhances the effect of ionizing radiation to improve tumor control

Abstract

Keywords

ASJC Scopus subject areas

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