Cancer cachexia in a mouse model of oxidative stress

BACKGROUND: Cancer is associated with muscle atrophy (cancer cachexia) that is linked to up to 40% of cancer‐related deaths. Oxidative stress is a critical player in the induction and progression of age‐related loss of muscle mass and weakness (sarcopenia); however, the role of oxidative stress in c...

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Autores principales: Brown, Jacob L., Lawrence, Marcus M., Ahn, Bumsoo, Kneis, Parker, Piekarz, Katarzyna M., Qaisar, Rizwan, Ranjit, Rojina, Bian, Jan, Pharaoh, Gavin, Brown, Chase, Peelor, Fredrick F., Kinter, Michael T., Miller, Benjamin F., Richardson, Arlan, Van Remmen, Holly
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7749559/
https://www.ncbi.nlm.nih.gov/pubmed/32918528
http://dx.doi.org/10.1002/jcsm.12615
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author Brown, Jacob L.
Lawrence, Marcus M.
Ahn, Bumsoo
Kneis, Parker
Piekarz, Katarzyna M.
Qaisar, Rizwan
Ranjit, Rojina
Bian, Jan
Pharaoh, Gavin
Brown, Chase
Peelor, Fredrick F.
Kinter, Michael T.
Miller, Benjamin F.
Richardson, Arlan
Van Remmen, Holly
author_facet Brown, Jacob L.
Lawrence, Marcus M.
Ahn, Bumsoo
Kneis, Parker
Piekarz, Katarzyna M.
Qaisar, Rizwan
Ranjit, Rojina
Bian, Jan
Pharaoh, Gavin
Brown, Chase
Peelor, Fredrick F.
Kinter, Michael T.
Miller, Benjamin F.
Richardson, Arlan
Van Remmen, Holly
author_sort Brown, Jacob L.
collection PubMed
description BACKGROUND: Cancer is associated with muscle atrophy (cancer cachexia) that is linked to up to 40% of cancer‐related deaths. Oxidative stress is a critical player in the induction and progression of age‐related loss of muscle mass and weakness (sarcopenia); however, the role of oxidative stress in cancer cachexia has not been defined. The purpose of this study was to examine if elevated oxidative stress exacerbates cancer cachexia. METHODS: Cu/Zn superoxide dismutase knockout (Sod1KO) mice were used as an established mouse model of elevated oxidative stress. Cancer cachexia was induced by injection of one million Lewis lung carcinoma (LLC) cells or phosphate‐buffered saline (saline) into the hind flank of female wild‐type mice or Sod1KO mice at approximately 4 months of age. The tumour developed for 3 weeks. Muscle mass, contractile function, neuromuscular junction (NMJ) fragmentation, metabolic proteins, mitochondrial function, and motor neuron function were measured in wild‐type and Sod1KO saline and tumour‐bearing mice. Data were analysed by two‐way ANOVA with Tukey–Kramer post hoc test when significant F ratios were determined and α was set at 0.05. Unless otherwise noted, results in abstract are mean ±SEM. RESULTS: Muscle mass and cross‐sectional area were significantly reduced, in tumour‐bearing mice. Metabolic enzymes were dysregulated in Sod1KO mice and cancer exacerbated this phenotype. NMJ fragmentation was exacerbated in tumour‐bearing Sod1KO mice. Myofibrillar protein degradation increased in tumour‐bearing wild‐type mice (wild‐type saline, 0.00847 ± 0.00205; wildtype LLC, 0.0211 ± 0.00184) and tumour‐bearing Sod1KO mice (Sod1KO saline, 0.0180 ± 0.00118; Sod1KO LLC, 0.0490 ± 0.00132). Muscle mitochondrial oxygen consumption was reduced in tumour‐bearing mice compared with saline‐injected wild‐type mice. Mitochondrial protein degradation increased in tumour‐bearing wild‐type mice (wild‐type saline, 0.0204 ± 0.00159; wild‐type LLC, 0.167 ± 0.00157) and tumour‐bearing Sod1KO mice (Sod1KO saline, 0.0231 ± 0.00108; Sod1 KO LLC, 0.0645 ± 0.000631). Sciatic nerve conduction velocity was decreased in tumour‐bearing wild‐type mice (wild‐type saline, 38.2 ± 0.861; wild‐type LLC, 28.8 ± 0.772). Three out of eleven of the tumour‐bearing Sod1KO mice did not survive the 3‐week period following tumour implantation. CONCLUSIONS: Oxidative stress does not exacerbate cancer‐induced muscle loss; however, cancer cachexia may accelerate NMJ disruption.
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spelling pubmed-77495592020-12-23 Cancer cachexia in a mouse model of oxidative stress Brown, Jacob L. Lawrence, Marcus M. Ahn, Bumsoo Kneis, Parker Piekarz, Katarzyna M. Qaisar, Rizwan Ranjit, Rojina Bian, Jan Pharaoh, Gavin Brown, Chase Peelor, Fredrick F. Kinter, Michael T. Miller, Benjamin F. Richardson, Arlan Van Remmen, Holly J Cachexia Sarcopenia Muscle Original Articles BACKGROUND: Cancer is associated with muscle atrophy (cancer cachexia) that is linked to up to 40% of cancer‐related deaths. Oxidative stress is a critical player in the induction and progression of age‐related loss of muscle mass and weakness (sarcopenia); however, the role of oxidative stress in cancer cachexia has not been defined. The purpose of this study was to examine if elevated oxidative stress exacerbates cancer cachexia. METHODS: Cu/Zn superoxide dismutase knockout (Sod1KO) mice were used as an established mouse model of elevated oxidative stress. Cancer cachexia was induced by injection of one million Lewis lung carcinoma (LLC) cells or phosphate‐buffered saline (saline) into the hind flank of female wild‐type mice or Sod1KO mice at approximately 4 months of age. The tumour developed for 3 weeks. Muscle mass, contractile function, neuromuscular junction (NMJ) fragmentation, metabolic proteins, mitochondrial function, and motor neuron function were measured in wild‐type and Sod1KO saline and tumour‐bearing mice. Data were analysed by two‐way ANOVA with Tukey–Kramer post hoc test when significant F ratios were determined and α was set at 0.05. Unless otherwise noted, results in abstract are mean ±SEM. RESULTS: Muscle mass and cross‐sectional area were significantly reduced, in tumour‐bearing mice. Metabolic enzymes were dysregulated in Sod1KO mice and cancer exacerbated this phenotype. NMJ fragmentation was exacerbated in tumour‐bearing Sod1KO mice. Myofibrillar protein degradation increased in tumour‐bearing wild‐type mice (wild‐type saline, 0.00847 ± 0.00205; wildtype LLC, 0.0211 ± 0.00184) and tumour‐bearing Sod1KO mice (Sod1KO saline, 0.0180 ± 0.00118; Sod1KO LLC, 0.0490 ± 0.00132). Muscle mitochondrial oxygen consumption was reduced in tumour‐bearing mice compared with saline‐injected wild‐type mice. Mitochondrial protein degradation increased in tumour‐bearing wild‐type mice (wild‐type saline, 0.0204 ± 0.00159; wild‐type LLC, 0.167 ± 0.00157) and tumour‐bearing Sod1KO mice (Sod1KO saline, 0.0231 ± 0.00108; Sod1 KO LLC, 0.0645 ± 0.000631). Sciatic nerve conduction velocity was decreased in tumour‐bearing wild‐type mice (wild‐type saline, 38.2 ± 0.861; wild‐type LLC, 28.8 ± 0.772). Three out of eleven of the tumour‐bearing Sod1KO mice did not survive the 3‐week period following tumour implantation. CONCLUSIONS: Oxidative stress does not exacerbate cancer‐induced muscle loss; however, cancer cachexia may accelerate NMJ disruption. John Wiley and Sons Inc. 2020-09-12 2020-12 /pmc/articles/PMC7749559/ /pubmed/32918528 http://dx.doi.org/10.1002/jcsm.12615 Text en © 2020 The Authors. Journal of Cachexia, Sarcopenia and Muscle published by John Wiley & Sons Ltd on behalf of Society on Sarcopenia, Cachexia and Wasting Disorders This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Brown, Jacob L.
Lawrence, Marcus M.
Ahn, Bumsoo
Kneis, Parker
Piekarz, Katarzyna M.
Qaisar, Rizwan
Ranjit, Rojina
Bian, Jan
Pharaoh, Gavin
Brown, Chase
Peelor, Fredrick F.
Kinter, Michael T.
Miller, Benjamin F.
Richardson, Arlan
Van Remmen, Holly
Cancer cachexia in a mouse model of oxidative stress
title Cancer cachexia in a mouse model of oxidative stress
title_full Cancer cachexia in a mouse model of oxidative stress
title_fullStr Cancer cachexia in a mouse model of oxidative stress
title_full_unstemmed Cancer cachexia in a mouse model of oxidative stress
title_short Cancer cachexia in a mouse model of oxidative stress
title_sort cancer cachexia in a mouse model of oxidative stress
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7749559/
https://www.ncbi.nlm.nih.gov/pubmed/32918528
http://dx.doi.org/10.1002/jcsm.12615
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