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Título
Role of superoxide–nitric oxide interactions in the accelerated age‐related loss of muscle mass in mice lacking Cu,Zn superoxide dismutase
Autor(es)
Palabras clave
accelerated aging
aging
reactive oxygen
species
skeletal muscle
Clasificación UNESCO
2411.10 Fisiología del Músculo
Fecha de publicación
2011
Editor
Wiley
Citación
Sakellariou, G.K., Pye, D., Vasilaki, A., Zibrik, L., Palomero Labajos, J., Kabayo, T., McArdle, F., van Remmen, H., Richardson, A., Tidball, J.G., McArdle, A., Jackson, M.J. (2011). Role of superoxide–nitric oxide interactions in the accelerated age‐related loss of muscle mass in mice lacking Cu,Zn superoxide dismutase. Aging Cell, 10 (5) pp 749-760. https://doi.org/10.1111/j.1474-9726.2011.00709.x
Resumen
[EN] Mice lacking Cu,Zn superoxide dismutase (SOD1) show accelerated, age-related loss of muscle mass. Lack of SOD1 may lead to
increased superoxide, reduced nitric oxide (NO), and increased
peroxynitrite, each of which could initiate muscle fiber loss. Single
muscle fibers from flexor digitorum brevis of wild-type (WT) and
Sod1) ⁄ ) mice were loaded with NO-sensitive (4-amino-5-methylamino-2¢,7¢-difluorofluorescein diacetate, DAF-FM) and superoxide-sensitive (dihydroethidium, DHE) probes. Gastrocnemius
muscles were analyzed for SOD enzymes, nitric oxide synthases
(NOS), and 3-nitrotyrosine (3-NT) content. A lack of SOD1 did not
increase superoxide availability at rest because no increase in ethidium or 2-hydroxyethidium (2-HE) formation from DHE was seen
in fibers from Sod1) ⁄ ) mice compared with those from WT mice.
Fibers from Sod1) ⁄ ) mice had decreased NO availability
(decreased DAF-FM fluorescence), increased 3-NT in muscle proteins indicating increased peroxynitrite formation and increased
content of peroxiredoxin V (a peroxynitrite reductase), compared
with WT mice. Muscle fibers from Sod1) ⁄ ) mice showed substantially reduced generation of superoxide in response to contractions compared with fibers from WT mice. Inhibition of NOS did
not affect DHE oxidation in fibers from WT or Sod1) ⁄ ) mice at rest
or during contractions, but transgenic mice overexpressing nNOS
showed increased DAF-FM fluorescence and reduced DHE oxidation in resting muscle fibers. It is concluded that formation of peroxynitrite in muscle fibers is a major effect of lack of SOD1 in
Sod1) ⁄ ) mice and may contribute to fiber loss in this model, and
that NO regulates superoxide availability and peroxynitrite formation in muscle.
URI
ISSN
1474-9718
DOI
10.1111/J.1474-9726.2011.00709.X
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