Mitochondrial DNA mutations induce mitochondrial dysfunction, apoptosis and sarcopenia in skeletal muscle of mitochondrial DNA mutator mice

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Fecha de publicación
2010Autor/a
Hiona, Asimina
Sanz, Alberto
Kujoth, Gregory C.
Seo, Arnold Y.
Hofer, Tim
Someya, Shinichi
Miyakawa, Takuya
Nakayama, Chie
Samhan-Arias, Alejandro K.
Servais, Stephane
Barger, Jamie L.
Tanokura, Masaru
Prolla, Tomas A.
Leeuwenburgh, Christiaan
Cita recomendada
Hiona, Asimina;
Sanz, Alberto;
Kujoth, Gregory C.;
Pamplona Gras, Reinald;
Seo, Arnold Y.;
Hofer, Tim;
...
Leeuwenburgh, Christiaan.
(2010)
.
Mitochondrial DNA mutations induce mitochondrial dysfunction, apoptosis and sarcopenia in skeletal muscle of mitochondrial DNA mutator mice.
PLoS ONE, 2010, vol. 5, núm. 7, e11468.
https://doi.org/10.1371/journal.pone.0011468.
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Background: Aging results in a progressive loss of skeletal muscle, a condition known as sarcopenia. Mitochondrial DNA (mtDNA) mutations accumulate with aging in skeletal muscle and correlate with muscle loss, although no causal relationship has been established.
Methodology/Principal Findings: We investigated the relationship between mtDNA mutations and sarcopenia at the gene
expression and biochemical levels using a mouse model that expresses a proofreading-deficient version (D257A) of the mitochondrial DNA Polymerase c, resulting in increased spontaneous mtDNA mutation rates. Gene expression profiling of D257A mice followed by Parametric Analysis of Gene Set Enrichment (PAGE) indicates that the D257A mutation is associated with a profound downregulation of gene sets associated with mitochondrial function. At the biochemical level, sarcopenia in D257A mice is associated with a marked reduction (35–50%) in the content of electron transport chain (ETC) complexes I, III and IV, all of which are partly encoded by mtDNA. D257A mice display impaired mitochondrial bioenergetics
associated with compromised state-3 respiration, lower ATP content and a resulting decrease in mitochondrial membrane
potential (Dym). Surprisingly, mitochondrial dysfunction was not accompanied by an increase in mitochondrial reactive oxygen species (ROS) production or oxidative damage.
Conclusions/Significance: These findings demonstrate that mutations in mtDNA can be causal in sarcopenia by affecting the assembly of functional ETC complexes, the lack of which provokes a decrease in oxidative phosphorylation, without an
increase in oxidative stress, and ultimately, skeletal muscle apoptosis and sarcopenia.
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PLoS ONE, 2010, vol. 5, núm. 7, e11468Proyectos de investigación europeos
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