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A stress response pathway regulates DNA damage through β2-adrenoreceptors and β-arrestin-1.

Publication ,  Journal Article
Hara, MR; Kovacs, JJ; Whalen, EJ; Rajagopal, S; Strachan, RT; Grant, W; Towers, AJ; Williams, B; Lam, CM; Xiao, K; Shenoy, SK; Gregory, SG ...
Published in: Nature
August 21, 2011

The human mind and body respond to stress, a state of perceived threat to homeostasis, by activating the sympathetic nervous system and secreting the catecholamines adrenaline and noradrenaline in the 'fight-or-flight' response. The stress response is generally transient because its accompanying effects (for example, immunosuppression, growth inhibition and enhanced catabolism) can be harmful in the long term. When chronic, the stress response can be associated with disease symptoms such as peptic ulcers or cardiovascular disorders, and epidemiological studies strongly indicate that chronic stress leads to DNA damage. This stress-induced DNA damage may promote ageing, tumorigenesis, neuropsychiatric conditions and miscarriages. However, the mechanisms by which these DNA-damage events occur in response to stress are unknown. The stress hormone adrenaline stimulates β(2)-adrenoreceptors that are expressed throughout the body, including in germline cells and zygotic embryos. Activated β(2)-adrenoreceptors promote Gs-protein-dependent activation of protein kinase A (PKA), followed by the recruitment of β-arrestins, which desensitize G-protein signalling and function as signal transducers in their own right. Here we elucidate a molecular mechanism by which β-adrenergic catecholamines, acting through both Gs-PKA and β-arrestin-mediated signalling pathways, trigger DNA damage and suppress p53 levels respectively, thus synergistically leading to the accumulation of DNA damage. In mice and in human cell lines, β-arrestin-1 (ARRB1), activated via β(2)-adrenoreceptors, facilitates AKT-mediated activation of MDM2 and also promotes MDM2 binding to, and degradation of, p53, by acting as a molecular scaffold. Catecholamine-induced DNA damage is abrogated in Arrb1-knockout (Arrb1(-/-)) mice, which show preserved p53 levels in both the thymus, an organ that responds prominently to acute or chronic stress, and in the testes, in which paternal stress may affect the offspring's genome. Our results highlight the emerging role of ARRB1 as an E3-ligase adaptor in the nucleus, and reveal how DNA damage may accumulate in response to chronic stress.

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Published In

Nature

DOI

EISSN

1476-4687

Publication Date

August 21, 2011

Volume

477

Issue

7364

Start / End Page

349 / 353

Location

England

Related Subject Headings

  • beta-Arrestins
  • beta-Arrestin 1
  • Tumor Suppressor Protein p53
  • Thymus Gland
  • Testis
  • Stress, Physiological
  • Signal Transduction
  • Receptors, Adrenergic, beta-2
  • Proto-Oncogene Proteins c-mdm2
  • Proto-Oncogene Proteins c-akt
 

Citation

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Hara, M. R., Kovacs, J. J., Whalen, E. J., Rajagopal, S., Strachan, R. T., Grant, W., … Lefkowitz, R. J. (2011). A stress response pathway regulates DNA damage through β2-adrenoreceptors and β-arrestin-1. Nature, 477(7364), 349–353. https://doi.org/10.1038/nature10368
Hara, Makoto R., Jeffrey J. Kovacs, Erin J. Whalen, Sudarshan Rajagopal, Ryan T. Strachan, Wayne Grant, Aaron J. Towers, et al. “A stress response pathway regulates DNA damage through β2-adrenoreceptors and β-arrestin-1.Nature 477, no. 7364 (August 21, 2011): 349–53. https://doi.org/10.1038/nature10368.
Hara MR, Kovacs JJ, Whalen EJ, Rajagopal S, Strachan RT, Grant W, et al. A stress response pathway regulates DNA damage through β2-adrenoreceptors and β-arrestin-1. Nature. 2011 Aug 21;477(7364):349–53.
Hara, Makoto R., et al. “A stress response pathway regulates DNA damage through β2-adrenoreceptors and β-arrestin-1.Nature, vol. 477, no. 7364, Aug. 2011, pp. 349–53. Pubmed, doi:10.1038/nature10368.
Hara MR, Kovacs JJ, Whalen EJ, Rajagopal S, Strachan RT, Grant W, Towers AJ, Williams B, Lam CM, Xiao K, Shenoy SK, Gregory SG, Ahn S, Duckett DR, Lefkowitz RJ. A stress response pathway regulates DNA damage through β2-adrenoreceptors and β-arrestin-1. Nature. 2011 Aug 21;477(7364):349–353.
Journal cover image

Published In

Nature

DOI

EISSN

1476-4687

Publication Date

August 21, 2011

Volume

477

Issue

7364

Start / End Page

349 / 353

Location

England

Related Subject Headings

  • beta-Arrestins
  • beta-Arrestin 1
  • Tumor Suppressor Protein p53
  • Thymus Gland
  • Testis
  • Stress, Physiological
  • Signal Transduction
  • Receptors, Adrenergic, beta-2
  • Proto-Oncogene Proteins c-mdm2
  • Proto-Oncogene Proteins c-akt