4.7 Article

Protein Carbonylation and Heat Shock Proteins in Human Skeletal Muscle: Relationships to Age and Sarcopenia

出版社

OXFORD UNIV PRESS INC
DOI: 10.1093/gerona/glu007

关键词

Sarcopenia; Mitochondria; Carbonylation; Heat shock protein

资金

  1. Biotechnology and Biological Sciences Research Council [BB/X510697/1338, BB/C516779/1]
  2. Biotechnology and Biological Sciences Research Council [BB/C516779/1] Funding Source: researchfish
  3. Medical Research Council [MR/K00414X/1] Funding Source: researchfish
  4. MRC [MR/K00414X/1] Funding Source: UKRI

向作者/读者索取更多资源

Aging is associated with a gradual loss of muscle mass termed sarcopenia, which has significant impact on quality-of-life. Because oxidative stress is proposed to negatively impact upon musculoskeletal aging, we investigated links between human aging and markers of oxidative stress, and relationships to muscle mass and strength in young and old nonsarcopenic and sarcopenic adults. Sixteen young and 16 old males (further subdivided into old and old sarcopenic) were studied. The abundance of protein carbonyl adducts within skeletal muscle sarcoplasmic, myofibrillar, and mitochondrial protein subfractions from musculus vastus lateralis biopsies were determined using Oxyblot immunoblotting techniques. In addition, concentrations of recognized cytoprotective proteins (eg, heat shock proteins [HSP], alpha beta-crystallin) were also assayed. Aging was associated with increased mitochondrial (but not myofibrillar or sarcoplasmic) protein carbonyl adducts, independently of (stage-I) sarcopenia. Correlation analyses of all subjects revealed that mitochondrial protein carbonyl abundance negatively correlated with muscle strength ([1-repetition maximum], p=.02, r(2)=-.16), but not muscle mass (p=.13, r(2)=-.08). Abundance of cytoprotective proteins, including various HSPs (HSP 27 and 70), were unaffected by aging/sarcopenia. To conclude, these data reveal that mitochondrial protein carbonylation increases moderately with age, and that this increase may impact upon skeletal muscle function, but is not a hallmark of (stage-I) sarcopenia, per se.

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