Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors

BACKGROUND: The high incidence of cardiovascular events in cancer survivors has long been noted, but the mechanistic insights of cardiovascular toxicity of cancer treatments, especially for vessel diseases, remain unclear. It is well known that atherosclerotic plaque formation begins in the area exp...

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Autores principales: Ko, Kyung Ae, Wang, Yin, Kotla, Sivareddy, Fujii, Yuka, Vu, Hang Thi, Venkatesulu, Bhanu P., Thomas, Tamlyn N., Medina, Jan L., Gi, Young Jin, Hada, Megumi, Grande-Allen, Jane, Patel, Zarana S., Milgrom, Sarah A., Krishnan, Sunil, Fujiwara, Keigi, Abe, Jun-Ichi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Cardiovascular Medicine
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5896304/
https://www.ncbi.nlm.nih.gov/pubmed/29675417
http://dx.doi.org/10.3389/fcvm.2018.00026
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author Ko, Kyung Ae
Wang, Yin
Kotla, Sivareddy
Fujii, Yuka
Vu, Hang Thi
Venkatesulu, Bhanu P.
Thomas, Tamlyn N.
Medina, Jan L.
Gi, Young Jin
Hada, Megumi
Grande-Allen, Jane
Patel, Zarana S.
Milgrom, Sarah A.
Krishnan, Sunil
Fujiwara, Keigi
Abe, Jun-Ichi
author_facet Ko, Kyung Ae
Wang, Yin
Kotla, Sivareddy
Fujii, Yuka
Vu, Hang Thi
Venkatesulu, Bhanu P.
Thomas, Tamlyn N.
Medina, Jan L.
Gi, Young Jin
Hada, Megumi
Grande-Allen, Jane
Patel, Zarana S.
Milgrom, Sarah A.
Krishnan, Sunil
Fujiwara, Keigi
Abe, Jun-Ichi
author_sort Ko, Kyung Ae
collection PubMed
description BACKGROUND: The high incidence of cardiovascular events in cancer survivors has long been noted, but the mechanistic insights of cardiovascular toxicity of cancer treatments, especially for vessel diseases, remain unclear. It is well known that atherosclerotic plaque formation begins in the area exposed to disturbed blood flow, but the relationship between cancer therapy and disturbed flow in regulating plaque formation has not been well studied. Therefore, we had two goals for this study; (1) Generate an affordable, reliable, and reproducible mouse model to recapitulate the cancer therapy-induced cardiovascular events in cancer survivors, and (2) Establish a mouse model to investigate the interplay between disturbed flow and various cancer therapies in the process of atherosclerotic plaque formation. METHODS AND RESULTS: We examined the effects of two cancer drugs and ionizing radiation (IR) on disturbed blood flow-induced plaque formation using a mouse carotid artery partial ligation (PCL) model of atherosclerosis. We found that doxorubicin and cisplatin, which are commonly used anti-cancer drugs, had no effect on plaque formation in partially ligated carotid arteries. Similarly, PCL-induced plaque formation was not affected in mice that received IR (2 Gy) and PCL surgery performed one week later. In contrast, when PCL surgery was performed 26 days after IR treatment, not only the atherosclerotic plaque formation but also the necrotic core formation was significantly enhanced. Lastly, we found a significant increase in p90RSK phosphorylation in the plaques from the IR-treated group compared to those from the non-IR treated group. CONCLUSIONS: Our results demonstrate that IR not only increases atherosclerotic events but also vulnerable plaque formation. These increases were a somewhat delayed effect of IR as they were observed in mice with PCL surgery performed 26 days, but not 10 days, after IR exposure. A proper animal model must be developed to study how to minimize the cardiovascular toxicity due to cancer treatment.
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spelling pubmed-58963042018-04-19 Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors Ko, Kyung Ae Wang, Yin Kotla, Sivareddy Fujii, Yuka Vu, Hang Thi Venkatesulu, Bhanu P. Thomas, Tamlyn N. Medina, Jan L. Gi, Young Jin Hada, Megumi Grande-Allen, Jane Patel, Zarana S. Milgrom, Sarah A. Krishnan, Sunil Fujiwara, Keigi Abe, Jun-Ichi Front Cardiovasc Med Cardiovascular Medicine BACKGROUND: The high incidence of cardiovascular events in cancer survivors has long been noted, but the mechanistic insights of cardiovascular toxicity of cancer treatments, especially for vessel diseases, remain unclear. It is well known that atherosclerotic plaque formation begins in the area exposed to disturbed blood flow, but the relationship between cancer therapy and disturbed flow in regulating plaque formation has not been well studied. Therefore, we had two goals for this study; (1) Generate an affordable, reliable, and reproducible mouse model to recapitulate the cancer therapy-induced cardiovascular events in cancer survivors, and (2) Establish a mouse model to investigate the interplay between disturbed flow and various cancer therapies in the process of atherosclerotic plaque formation. METHODS AND RESULTS: We examined the effects of two cancer drugs and ionizing radiation (IR) on disturbed blood flow-induced plaque formation using a mouse carotid artery partial ligation (PCL) model of atherosclerosis. We found that doxorubicin and cisplatin, which are commonly used anti-cancer drugs, had no effect on plaque formation in partially ligated carotid arteries. Similarly, PCL-induced plaque formation was not affected in mice that received IR (2 Gy) and PCL surgery performed one week later. In contrast, when PCL surgery was performed 26 days after IR treatment, not only the atherosclerotic plaque formation but also the necrotic core formation was significantly enhanced. Lastly, we found a significant increase in p90RSK phosphorylation in the plaques from the IR-treated group compared to those from the non-IR treated group. CONCLUSIONS: Our results demonstrate that IR not only increases atherosclerotic events but also vulnerable plaque formation. These increases were a somewhat delayed effect of IR as they were observed in mice with PCL surgery performed 26 days, but not 10 days, after IR exposure. A proper animal model must be developed to study how to minimize the cardiovascular toxicity due to cancer treatment. Frontiers Media S.A. 2018-04-05 /pmc/articles/PMC5896304/ /pubmed/29675417 http://dx.doi.org/10.3389/fcvm.2018.00026 Text en Copyright © 2018 Ko, Wang, Kotla, Fujii, Vu, Venkatesulu, Thomas, Medina, Gi, Hada, Grande-Allen, Patel, Milgrom, Krishnan, Fujiwara and Abe http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cardiovascular Medicine
Ko, Kyung Ae
Wang, Yin
Kotla, Sivareddy
Fujii, Yuka
Vu, Hang Thi
Venkatesulu, Bhanu P.
Thomas, Tamlyn N.
Medina, Jan L.
Gi, Young Jin
Hada, Megumi
Grande-Allen, Jane
Patel, Zarana S.
Milgrom, Sarah A.
Krishnan, Sunil
Fujiwara, Keigi
Abe, Jun-Ichi
Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors
title Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors
title_full Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors
title_fullStr Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors
title_full_unstemmed Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors
title_short Developing a Reliable Mouse Model for Cancer Therapy-Induced Cardiovascular Toxicity in Cancer Patients and Survivors
title_sort developing a reliable mouse model for cancer therapy-induced cardiovascular toxicity in cancer patients and survivors
topic Cardiovascular Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5896304/
https://www.ncbi.nlm.nih.gov/pubmed/29675417
http://dx.doi.org/10.3389/fcvm.2018.00026
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