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Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model

Marfan syndrome (MFS) cardiovascular manifestations such as aortic aneurysms and cardiomyopathy carry substantial morbidity/mortality. We investigated the effects of lipoic acid, an antioxidant, on ROS production and aortic remodeling in a MFS mgΔ(loxPneo) mouse model. MFS and WT (wild-type) 1-month...

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Autores principales: Guido, Maria C., Debbas, Victor, Salemi, Vera M., Tavares, Elaine R., Meirelles, Thayna, Araujo, Thaís L. S., Nolasco, Patricia, Ferreira-Filho, Julio C. A., Takimura, Celso K., Pereira, Lygia V., Laurindo, Francisco R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5889865/
https://www.ncbi.nlm.nih.gov/pubmed/29765495
http://dx.doi.org/10.1155/2018/3967213
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author Guido, Maria C.
Debbas, Victor
Salemi, Vera M.
Tavares, Elaine R.
Meirelles, Thayna
Araujo, Thaís L. S.
Nolasco, Patricia
Ferreira-Filho, Julio C. A.
Takimura, Celso K.
Pereira, Lygia V.
Laurindo, Francisco R.
author_facet Guido, Maria C.
Debbas, Victor
Salemi, Vera M.
Tavares, Elaine R.
Meirelles, Thayna
Araujo, Thaís L. S.
Nolasco, Patricia
Ferreira-Filho, Julio C. A.
Takimura, Celso K.
Pereira, Lygia V.
Laurindo, Francisco R.
author_sort Guido, Maria C.
collection PubMed
description Marfan syndrome (MFS) cardiovascular manifestations such as aortic aneurysms and cardiomyopathy carry substantial morbidity/mortality. We investigated the effects of lipoic acid, an antioxidant, on ROS production and aortic remodeling in a MFS mgΔ(loxPneo) mouse model. MFS and WT (wild-type) 1-month-old mice were allocated to 3 groups: untreated, treated with losartan, and treated with lipoic acid. At 6 months old, echocardiography, ROS production, and morphological analysis of aortas were performed. Aortic ROS generation in 6-month-old MFS animals was higher at advanced stages of disease in MFS. An unprecedented finding in MFS mice analyzed by OCT was the occurrence of focal inhomogeneous regions in the aortic arch, either collagen-rich extremely thickened or collagen-poor hypotrophic regions. MFS animals treated with lipoic acid showed markedly reduced ROS production and lower ERK1/2 phosphorylation; meanwhile, aortic dilation and elastic fiber breakdown were unaltered. Of note, lipoic acid treatment associated with the absence of focal inhomogeneous regions in MFS animals. Losartan reduced aortic dilation and elastic fiber breakdown despite no change in ROS generation. In conclusion, oxidant generation by itself seems neutral with respect to aneurysm progression in MFS; however, lipoic acid-mediated reduction of inhomogeneous regions may potentially associate with less anisotropy and reduced chance of dissection/rupture.
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spelling pubmed-58898652018-05-14 Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model Guido, Maria C. Debbas, Victor Salemi, Vera M. Tavares, Elaine R. Meirelles, Thayna Araujo, Thaís L. S. Nolasco, Patricia Ferreira-Filho, Julio C. A. Takimura, Celso K. Pereira, Lygia V. Laurindo, Francisco R. Oxid Med Cell Longev Research Article Marfan syndrome (MFS) cardiovascular manifestations such as aortic aneurysms and cardiomyopathy carry substantial morbidity/mortality. We investigated the effects of lipoic acid, an antioxidant, on ROS production and aortic remodeling in a MFS mgΔ(loxPneo) mouse model. MFS and WT (wild-type) 1-month-old mice were allocated to 3 groups: untreated, treated with losartan, and treated with lipoic acid. At 6 months old, echocardiography, ROS production, and morphological analysis of aortas were performed. Aortic ROS generation in 6-month-old MFS animals was higher at advanced stages of disease in MFS. An unprecedented finding in MFS mice analyzed by OCT was the occurrence of focal inhomogeneous regions in the aortic arch, either collagen-rich extremely thickened or collagen-poor hypotrophic regions. MFS animals treated with lipoic acid showed markedly reduced ROS production and lower ERK1/2 phosphorylation; meanwhile, aortic dilation and elastic fiber breakdown were unaltered. Of note, lipoic acid treatment associated with the absence of focal inhomogeneous regions in MFS animals. Losartan reduced aortic dilation and elastic fiber breakdown despite no change in ROS generation. In conclusion, oxidant generation by itself seems neutral with respect to aneurysm progression in MFS; however, lipoic acid-mediated reduction of inhomogeneous regions may potentially associate with less anisotropy and reduced chance of dissection/rupture. Hindawi 2018-03-25 /pmc/articles/PMC5889865/ /pubmed/29765495 http://dx.doi.org/10.1155/2018/3967213 Text en Copyright © 2018 Maria C. Guido et al. http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Guido, Maria C.
Debbas, Victor
Salemi, Vera M.
Tavares, Elaine R.
Meirelles, Thayna
Araujo, Thaís L. S.
Nolasco, Patricia
Ferreira-Filho, Julio C. A.
Takimura, Celso K.
Pereira, Lygia V.
Laurindo, Francisco R.
Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model
title Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model
title_full Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model
title_fullStr Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model
title_full_unstemmed Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model
title_short Effect of the Antioxidant Lipoic Acid in Aortic Phenotype in a Marfan Syndrome Mouse Model
title_sort effect of the antioxidant lipoic acid in aortic phenotype in a marfan syndrome mouse model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5889865/
https://www.ncbi.nlm.nih.gov/pubmed/29765495
http://dx.doi.org/10.1155/2018/3967213
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