• Title of article

    Protein turnover by the proteasome in aging and disease,

  • Author/Authors

    Reshma Shringarpure، نويسنده , , Kelvin J. A. Davies، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2002
  • Pages
    6
  • From page
    1084
  • To page
    1089
  • Abstract
    A significant body of evidence supports a key role for free radicals in causing cumulative damage to cellular macromolecules, thereby contributing to senescence/aging, and a number of age-related disorders. Proteins are recognized as major targets for oxidative damage (in addition to DNA and lipids) and the accumulation of oxidized proteins has been reported for many experimental aging models, as measured by several markers for protein oxidation. In young and healthy individuals, moderately oxidized soluble cell proteins are selectively and rapidly degraded by the proteasome. However, severely oxidized, cross-linked proteins are poor substrates for degradation and actually inhibit the proteasome. Considerable evidence now indicates that proteasome activity declines during aging, as the protease is progressively inhibited by binding to ever increasing levels of oxidized and cross-linked protein aggregates. Cellular aging probably involves both an increase in the generation of reactive oxygen species and a progressive decline in proteasome activity, resulting in the progressive accumulation of oxidatively damaged protein aggregates that eventually contribute to cellular dysfunction and senescence.
  • Keywords
    Proteolysis , aging , Protein oxidation , free radicals , Proteasome
  • Journal title
    Free Radical Biology and Medicine
  • Serial Year
    2002
  • Journal title
    Free Radical Biology and Medicine
  • Record number

    519154