Mitochondrionopathy phenotype in doxorubicin-treated Wistar rats depends on treatment protocol and is cardiac-specific

Although doxorubicin (DOX) is a very effective antineoplastic agent, its clinical use is limited by a dose-dependent, persistent and cumulative cardiotoxicity, whose mechanism remains to be elucidated. Previous works in animal models have failed to use a multi-organ approach to demonstrate that DOX-...

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Published in:	PloS one Vol. 7; no. 6; p. e38867
Main Authors:	Pereira, Gonçalo C, Pereira, Susana P, Pereira, Claudia V, Lumini, José A, Magalhães, José, Ascensão, António, Santos, Maria S, Moreno, António J, Oliveira, Paulo J
Format:	Journal Article
Language:	English
Published:	United States Public Library of Science 22-06-2012 Public Library of Science (PLoS)
Subjects:	Animal models Animal tissues Animals Anthracyclines Antibiotics Antibiotics, Antineoplastic - adverse effects Aqueous solutions Biocompatibility Bioenergetics Biology Cancer therapies Cardiotoxicity Doxorubicin Doxorubicin - adverse effects Drug dosages Electron transport Exercise Heart Heart - drug effects Heart diseases Hypotheses In vivo methods and tests Kidney - drug effects Kidney - metabolism Kidneys Laboratory animals Life sciences Liver Liver - drug effects Liver - metabolism Male Medicine Mitochondria Mitochondria, Heart - drug effects Mitochondrial DNA Myocardium - metabolism Neurosciences Oxidation Oxidative stress Permeability Physical fitness Rats Rats, Wistar Respiration Rodents Studies Toxicity Portugal
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Abstract	Although doxorubicin (DOX) is a very effective antineoplastic agent, its clinical use is limited by a dose-dependent, persistent and cumulative cardiotoxicity, whose mechanism remains to be elucidated. Previous works in animal models have failed to use a multi-organ approach to demonstrate that DOX-associated toxicity is selective to the cardiac tissue. In this context, the present work aims to investigate in vivo DOX cardiac, hepatic and renal toxicity in the same animal model, with special relevance on alterations of mitochondrial bioenergetics. To this end, male Wistar rats were sub-chronically (7 wks, 2 mg/Kg) or acutely (20 mg/Kg) treated with DOX and sacrificed one week or 24 hours after the last injection, respectively. Alterations of mitochondrial bioenergetics showed treatment-dependent differences between tissues. No alterations were observed for cardiac mitochondria in the acute model but decreased ADP-stimulated respiration was detected in the sub-chronic treatment. In the acute treatment model, ADP-stimulated respiration was increased in liver and decreased in kidney mitochondria. Aconitase activity, a marker of oxidative stress, was decreased in renal mitochondria in the acute and in heart in the sub-chronic model. Interestingly, alterations of cardiac mitochondrial bioenergetics co-existed with an absence of echocardiograph, histopathological or ultra-structural alterations. Besides, no plasma markers of cardiac injury were found in any of the time points studied. The results confirm that alterations of mitochondrial function, which are more evident in the heart, are an early marker of DOX-induced toxicity, existing even in the absence of cardiac functional alterations.
AbstractList	Although doxorubicin (DOX) is a very effective antineoplastic agent, its clinical use is limited by a dose-dependent, persistent and cumulative cardiotoxicity, whose mechanism remains to be elucidated. Previous works in animal models have failed to use a multi-organ approach to demonstrate that DOX-associated toxicity is selective to the cardiac tissue. In this context, the present work aims to investigate in vivo DOX cardiac, hepatic and renal toxicity in the same animal model, with special relevance on alterations of mitochondrial bioenergetics. To this end, male Wistar rats were sub-chronically (7 wks, 2 mg/Kg) or acutely (20 mg/Kg) treated with DOX and sacrificed one week or 24 hours after the last injection, respectively. Alterations of mitochondrial bioenergetics showed treatment-dependent differences between tissues. No alterations were observed for cardiac mitochondria in the acute model but decreased ADP-stimulated respiration was detected in the sub-chronic treatment. In the acute treatment model, ADP-stimulated respiration was increased in liver and decreased in kidney mitochondria. Aconitase activity, a marker of oxidative stress, was decreased in renal mitochondria in the acute and in heart in the sub-chronic model. Interestingly, alterations of cardiac mitochondrial bioenergetics co-existed with an absence of echocardiograph, histopathological or ultra-structural alterations. Besides, no plasma markers of cardiac injury were found in any of the time points studied. The results confirm that alterations of mitochondrial function, which are more evident in the heart, are an early marker of DOX-induced toxicity, existing even in the absence of cardiac functional alterations. Although doxorubicin (DOX) is a very effective antineoplastic agent, its clinical use is limited by a dose-dependent, persistent and cumulative cardiotoxicity, whose mechanism remains to be elucidated. Previous works in animal models have failed to use a multi-organ approach to demonstrate that DOX-associated toxicity is selective to the cardiac tissue. In this context, the present work aims to investigate in vivo DOX cardiac, hepatic and renal toxicity in the same animal model, with special relevance on alterations of mitochondrial bioenergetics. To this end, male Wistar rats were sub-chronically (7 wks, 2 mg/Kg) or acutely (20 mg/Kg) treated with DOX and sacrificed one week or 24 hours after the last injection, respectively. Alterations of mitochondrial bioenergetics showed treatment-dependent differences between tissues. No alterations were observed for cardiac mitochondria in the acute model but decreased ADP-stimulated respiration was detected in the sub-chronic treatment. In the acute treatment model, ADP-stimulated respiration was increased in liver and decreased in kidney mitochondria. Aconitase activity, a marker of oxidative stress, was decreased in renal mitochondria in the acute and in heart in the sub-chronic model. Interestingly, alterations of cardiac mitochondrial bioenergetics co-existed with an absence of echocardiograph, histopathological or ultra-structural alterations. Besides, no plasma markers of cardiac injury were found in any of the time points studied. The results confirm that alterations of mitochondrial function, which are more evident in the heart, are an early marker of DOX-induced toxicity, existing even in the absence of cardiac functional alterations.
Audience	Academic
Author	Lumini, José A Moreno, António J Pereira, Gonçalo C Magalhães, José Pereira, Claudia V Ascensão, António Santos, Maria S Oliveira, Paulo J Pereira, Susana P
AuthorAffiliation	4 Department of Life Sciences, Institute for Marine Research, University of Coimbra, Coimbra, Portugal Université Joseph Fourier, France 2 Faculty of Sport Sciences, Research Centre in Physical Activity, Health and Leisure, University of Porto, Porto, Portugal 3 Faculty of Health Sciences, University of Fernando Pessoa, Porto, Portugal 1 Department of Life Sciences, Center for Neuroscience and Cell Biology (CNC), University of Coimbra, Coimbra, Portugal
AuthorAffiliation_xml	– name: 1 Department of Life Sciences, Center for Neuroscience and Cell Biology (CNC), University of Coimbra, Coimbra, Portugal – name: 2 Faculty of Sport Sciences, Research Centre in Physical Activity, Health and Leisure, University of Porto, Porto, Portugal – name: 4 Department of Life Sciences, Institute for Marine Research, University of Coimbra, Coimbra, Portugal – name: 3 Faculty of Health Sciences, University of Fernando Pessoa, Porto, Portugal – name: Université Joseph Fourier, France
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Copyright	COPYRIGHT 2012 Public Library of Science 2012 Pereira et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: https://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License. Pereira et al. 2012
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Notes	Conceived and designed the experiments: GCP PJO AJM MSS. Performed the experiments: GCP SPP CVP JAL JM AA. Analyzed the data: GCP SPP AJM PJO JM AA JAL. Contributed reagents/materials/analysis tools: MSS AJM. Wrote the paper: GCP PJO.
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Snippet	Although doxorubicin (DOX) is a very effective antineoplastic agent, its clinical use is limited by a dose-dependent, persistent and cumulative cardiotoxicity,...
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SubjectTerms	Animal models Animal tissues Animals Anthracyclines Antibiotics Antibiotics, Antineoplastic - adverse effects Aqueous solutions Biocompatibility Bioenergetics Biology Cancer therapies Cardiotoxicity Doxorubicin Doxorubicin - adverse effects Drug dosages Electron transport Exercise Heart Heart - drug effects Heart diseases Hypotheses In vivo methods and tests Kidney - drug effects Kidney - metabolism Kidneys Laboratory animals Life sciences Liver Liver - drug effects Liver - metabolism Male Medicine Mitochondria Mitochondria, Heart - drug effects Mitochondrial DNA Myocardium - metabolism Neurosciences Oxidation Oxidative stress Permeability Physical fitness Rats Rats, Wistar Respiration Rodents Studies Toxicity
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Title	Mitochondrionopathy phenotype in doxorubicin-treated Wistar rats depends on treatment protocol and is cardiac-specific
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