Open Access
Skeletal muscle metabolic adaptations to endurance exercise training are attainable in mice with simvastatin treatment
Publication type: Journal Article
Publication date: 2017-02-16
scimago Q1
wos Q2
SJR: 0.803
CiteScore: 5.4
Impact factor: 2.6
ISSN: 19326203
PubMed ID:
28207880
Multidisciplinary
Abstract
We tested the hypothesis that a 6-week regimen of simvastatin would attenuate skeletal muscle adaptation to low-intensity exercise. Male C57BL/6J wildtype mice were subjected to 6-weeks of voluntary wheel running or normal cage activities with or without simvastatin treatment (20 mg/kg/d, n = 7–8 per group). Adaptations in in vivo fatigue resistance were determined by a treadmill running test, and by ankle plantarflexor contractile assessment. The tibialis anterior, gastrocnemius, and plantaris muscles were evaluated for exercised-induced mitochondrial adaptations (i.e., biogenesis, function, autophagy). There was no difference in weekly wheel running distance between control and simvastatin-treated mice (P = 0.51). Trained mice had greater treadmill running distance (296%, P<0.001), and ankle plantarflexor contractile fatigue resistance (9%, P<0.05) compared to sedentary mice, independent of simvastatin treatment. At the cellular level, trained mice had greater mitochondrial biogenesis (e.g., ~2-fold greater PGC1α expression, P<0.05) and mitochondrial content (e.g., 25% greater citrate synthase activity, P<0.05), independent of simvastatin treatment. Mitochondrial autophagy-related protein contents were greater in trained mice (e.g., 40% greater Bnip3, P<0.05), independent of simvastatin treatment. However, Drp1, a marker of mitochondrial fission, was less in simvastatin treated mice, independent of exercise training, and there was a significant interaction between training and statin treatment (P<0.022) for LC3-II protein content, a marker of autophagy flux. These data indicate that whole body and skeletal muscle adaptations to endurance exercise training are attainable with simvastatin treatment, but simvastatin may have side effects on muscle mitochondrial maintenance via autophagy, which could have long-term implications on muscle health.
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33
Total citations:
33
Citations from 2024:
5
(15.63%)
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GOST
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Southern W. M. et al. Skeletal muscle metabolic adaptations to endurance exercise training are attainable in mice with simvastatin treatment // PLoS ONE. 2017. Vol. 12. No. 2. p. e0172551.
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Southern W. M., Nichenko A. S., Shill D. D., Spencer C. C., Jenkins N. T., MCCULLY K. K., CALL J. A. Skeletal muscle metabolic adaptations to endurance exercise training are attainable in mice with simvastatin treatment // PLoS ONE. 2017. Vol. 12. No. 2. p. e0172551.
Cite this
RIS
Copy
TY - JOUR
DO - 10.1371/journal.pone.0172551
UR - https://doi.org/10.1371/journal.pone.0172551
TI - Skeletal muscle metabolic adaptations to endurance exercise training are attainable in mice with simvastatin treatment
T2 - PLoS ONE
AU - Southern, William M.
AU - Nichenko, Anna S.
AU - Shill, Daniel D.
AU - Spencer, Corey C
AU - Jenkins, Nathan T.
AU - MCCULLY, KEVIN K.
AU - CALL, JARROD A.
PY - 2017
DA - 2017/02/16
PB - Public Library of Science (PLoS)
SP - e0172551
IS - 2
VL - 12
PMID - 28207880
SN - 1932-6203
ER -
Cite this
BibTex (up to 50 authors)
Copy
@article{2017_Southern,
author = {William M. Southern and Anna S. Nichenko and Daniel D. Shill and Corey C Spencer and Nathan T. Jenkins and KEVIN K. MCCULLY and JARROD A. CALL},
title = {Skeletal muscle metabolic adaptations to endurance exercise training are attainable in mice with simvastatin treatment},
journal = {PLoS ONE},
year = {2017},
volume = {12},
publisher = {Public Library of Science (PLoS)},
month = {feb},
url = {https://doi.org/10.1371/journal.pone.0172551},
number = {2},
pages = {e0172551},
doi = {10.1371/journal.pone.0172551}
}
Cite this
MLA
Copy
Southern, William M., et al. “Skeletal muscle metabolic adaptations to endurance exercise training are attainable in mice with simvastatin treatment.” PLoS ONE, vol. 12, no. 2, Feb. 2017, p. e0172551. https://doi.org/10.1371/journal.pone.0172551.