NF-κB inhibition delays DNA damage-induced senescence and aging in mice.

نویسندگان

  • Jeremy S Tilstra
  • Andria R Robinson
  • Jin Wang
  • Siobhán Q Gregg
  • Cheryl L Clauson
  • Daniel P Reay
  • Luigi A Nasto
  • Claudette M St Croix
  • Arvydas Usas
  • Nam Vo
  • Johnny Huard
  • Paula R Clemens
  • Donna B Stolz
  • Denis C Guttridge
  • Simon C Watkins
  • George A Garinis
  • Yinsheng Wang
  • Laura J Niedernhofer
  • Paul D Robbins
چکیده

The accumulation of cellular damage, including DNA damage, is thought to contribute to aging-related degenerative changes, but how damage drives aging is unknown. XFE progeroid syndrome is a disease of accelerated aging caused by a defect in DNA repair. NF-κB, a transcription factor activated by cellular damage and stress, has increased activity with aging and aging-related chronic diseases. To determine whether NF-κB drives aging in response to the accumulation of spontaneous, endogenous DNA damage, we measured the activation of NF-κB in WT and progeroid model mice. As both WT and progeroid mice aged, NF-κB was activated stochastically in a variety of cell types. Genetic depletion of one allele of the p65 subunit of NF-κB or treatment with a pharmacological inhibitor of the NF-κB-activating kinase, IKK, delayed the age-related symptoms and pathologies of progeroid mice. Additionally, inhibition of NF-κB reduced oxidative DNA damage and stress and delayed cellular senescence. These results indicate that the mechanism by which DNA damage drives aging is due in part to NF-κB activation. IKK/NF-κB inhibitors are sufficient to attenuate this damage and could provide clinical benefit for degenerative changes associated with accelerated aging disorders and normal aging.

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عنوان ژورنال:
  • The Journal of clinical investigation

دوره 122 7  شماره 

صفحات  -

تاریخ انتشار 2012