Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice

Aging is associated with reduced muscle mass (sarcopenia) and poor bone quality (osteoporosis), which together increase the incidence of falls and bone fractures. It is widely appreciated that aging triggers systemic oxidative stress, which can impair myoblast cell survival and differentiation. We p...

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Autores principales: Pandya, Chirayu D., Lee, Byung, Toque, Haroldo A., Mendhe, Bharati, Bragg, Robert T., Pandya, Bhaumik, Atawia, Reem T., Isales, Carlos, Hamrick, Mark, Caldwell, R. William, Fulzele, Sadanand
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6530149/
https://www.ncbi.nlm.nih.gov/pubmed/31205583
http://dx.doi.org/10.1155/2019/1704650
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author Pandya, Chirayu D.
Lee, Byung
Toque, Haroldo A.
Mendhe, Bharati
Bragg, Robert T.
Pandya, Bhaumik
Atawia, Reem T.
Isales, Carlos
Hamrick, Mark
Caldwell, R. William
Fulzele, Sadanand
author_facet Pandya, Chirayu D.
Lee, Byung
Toque, Haroldo A.
Mendhe, Bharati
Bragg, Robert T.
Pandya, Bhaumik
Atawia, Reem T.
Isales, Carlos
Hamrick, Mark
Caldwell, R. William
Fulzele, Sadanand
author_sort Pandya, Chirayu D.
collection PubMed
description Aging is associated with reduced muscle mass (sarcopenia) and poor bone quality (osteoporosis), which together increase the incidence of falls and bone fractures. It is widely appreciated that aging triggers systemic oxidative stress, which can impair myoblast cell survival and differentiation. We previously reported that arginase plays an important role in oxidative stress-dependent bone loss. We hypothesized that arginase activity is dysregulated with aging in muscles and may be involved in muscle pathophysiology. To investigate this, we analyzed arginase activity and its expression in skeletal muscles of young and aged mice. We found that arginase activity and arginase 1 expression were significantly elevated in aged muscles. We also demonstrated that SOD2, GPx1, and NOX2 increased with age in skeletal muscle. Most importantly, we also demonstrated elevated levels of peroxynitrite formation and uncoupling of eNOS in aged muscles. Our in vitro studies using C2C12 myoblasts showed that the oxidative stress treatment increased arginase activity, decreased cell survival, and increased apoptotic markers. These effects were reversed by treatment with an arginase inhibitor, 2(S)-amino-6-boronohexanoic acid (ABH). Our study provides strong evidence that L-arginine metabolism is altered in aged muscle and that arginase inhibition could be used as a novel therapeutic target for age-related muscle complications.
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spelling pubmed-65301492019-06-16 Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice Pandya, Chirayu D. Lee, Byung Toque, Haroldo A. Mendhe, Bharati Bragg, Robert T. Pandya, Bhaumik Atawia, Reem T. Isales, Carlos Hamrick, Mark Caldwell, R. William Fulzele, Sadanand Oxid Med Cell Longev Research Article Aging is associated with reduced muscle mass (sarcopenia) and poor bone quality (osteoporosis), which together increase the incidence of falls and bone fractures. It is widely appreciated that aging triggers systemic oxidative stress, which can impair myoblast cell survival and differentiation. We previously reported that arginase plays an important role in oxidative stress-dependent bone loss. We hypothesized that arginase activity is dysregulated with aging in muscles and may be involved in muscle pathophysiology. To investigate this, we analyzed arginase activity and its expression in skeletal muscles of young and aged mice. We found that arginase activity and arginase 1 expression were significantly elevated in aged muscles. We also demonstrated that SOD2, GPx1, and NOX2 increased with age in skeletal muscle. Most importantly, we also demonstrated elevated levels of peroxynitrite formation and uncoupling of eNOS in aged muscles. Our in vitro studies using C2C12 myoblasts showed that the oxidative stress treatment increased arginase activity, decreased cell survival, and increased apoptotic markers. These effects were reversed by treatment with an arginase inhibitor, 2(S)-amino-6-boronohexanoic acid (ABH). Our study provides strong evidence that L-arginine metabolism is altered in aged muscle and that arginase inhibition could be used as a novel therapeutic target for age-related muscle complications. Hindawi 2019-05-08 /pmc/articles/PMC6530149/ /pubmed/31205583 http://dx.doi.org/10.1155/2019/1704650 Text en Copyright © 2019 Chirayu D. Pandya 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
Pandya, Chirayu D.
Lee, Byung
Toque, Haroldo A.
Mendhe, Bharati
Bragg, Robert T.
Pandya, Bhaumik
Atawia, Reem T.
Isales, Carlos
Hamrick, Mark
Caldwell, R. William
Fulzele, Sadanand
Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice
title Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice
title_full Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice
title_fullStr Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice
title_full_unstemmed Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice
title_short Age-Dependent Oxidative Stress Elevates Arginase 1 and Uncoupled Nitric Oxide Synthesis in Skeletal Muscle of Aged Mice
title_sort age-dependent oxidative stress elevates arginase 1 and uncoupled nitric oxide synthesis in skeletal muscle of aged mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6530149/
https://www.ncbi.nlm.nih.gov/pubmed/31205583
http://dx.doi.org/10.1155/2019/1704650
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