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  • Faculty of Science / Naturvetenskapliga fakulteten
  • Department of Chemistry and Molecular Biology / Institutionen för kemi och molekylärbiologi (2012-)
  • Doctoral Theses / Doktorsavhandlingar Institutionen för kemi och molekylärbiologi
  • Redigera dokument
  •   Startsida
  • Faculty of Science / Naturvetenskapliga fakulteten
  • Department of Chemistry and Molecular Biology / Institutionen för kemi och molekylärbiologi (2012-)
  • Doctoral Theses / Doktorsavhandlingar Institutionen för kemi och molekylärbiologi
  • Redigera dokument
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Peroxiredoxins in Redox Signaling and Aging

Sammanfattning
Peroxiredoxins have emerged as conserved modulators of the rate of aging in yeast and multicellular organisms and play a role in lifespan extension through the anti-aging intervention caloric restriction. Yet, it is not clear through what mechanism peroxiredoxins extend lifespan. First discovered as hydrogen peroxide scavengers, peroxiredoxins have been shown to have a genome protective function, to act as chaperones, to play a role in circadian rhythms and to be involved in redox signaling. In this thesis, I tried to identify the underlying mechanisms for peroxiredoxin mediated lifespan extension and its role in redox signaling. Using the yeast Saccharomyces cerevisiae as a model organism, we could show that the lifespan extension by the peroxiredoxin Tsa1 is not linked to increased genome stability. Our data indicates that Tsa1 recruits molecular chaperones to protein aggregates formed during oxidative stress and reduces the number of protein aggregates that accumulate during aging. Surprisingly, this contributes just to a limited extend to lifespan extension, as a mutant not able to form a chaperone still has a normal lifespan. Instead, redox-signaling that reduces protein kinase A (PKA) activity through Tsa1 mediated oxidation seems to be preeminently responsible for lifespan extension. Interestingly, the same signaling pathway is used in yeast to react to light stress. Hydrogen peroxide formed upon illumination by a conserved peroxisomal oxidase leads to increased redox cycling of Tsa1. Tsa1 then reduces PKA activity allowing the subsequent nuclear localization of the transcription factors Msn2 and Msn4 that induce transcription of stress related genes. Our data thus clarify an important aspect of the role of peroxiredoxins in circadian rhythms, namely they mediate an organismal light response.
Delarbeten
Bodvard, K., Peeters, K., Roger, F., Romanov, N., Igbaria, A., Welkenhuysen, N., ... & Molin, M. (2017). Light-sensing via hydrogen peroxide and a peroxiredoxin. Nature Communications, 8, 14791. ::doi::10.1038/ncomms14791
 
Hanzén, S., Vielfort, K., Yang, J., Roger, F., Andersson, V., Zamarbide-Forés, S., ... & Liu, B. (2016). Lifespan control by redox-dependent recruitment of chaperones to misfolded proteins. Cell, 166(1), 140-151. ::doi::10.1016/j.cell.2016.05.006
 
Roger, F., Asami, C., Hanzén, S., Lagniel, G., Labarre, J., Nyström, T., and Molin, M. (2017) Redox signaling via the yeast peroxiredoxin Tsa1 promotes longevity by inhibiting nutrient signaling Manuscript
 
Examinationsnivå
Doctor of Philosophy
Universitet
University of Gothenburg. Faculty of Science
Institution
Department of Chemistry and Molecular Biology ; Institutionen för kemi och molekylärbiologi
Disputation
Fredagen den 3. november 2017, kl. 10:00 i föreläsningssal Ragnar Sandberg, Medicinaregatan 7
Datum för disputation
2017-11-03
E-post
friederikeroger@gmail.com
URL:
http://hdl.handle.net/2077/54120
Samlingar
  • Doctoral Theses / Doktorsavhandlingar Institutionen för kemi och molekylärbiologi
  • Doctoral Theses from University of Gothenburg / Doktorsavhandlingar från Göteborgs universitet
Fil(er)
Thesis frame (3.570Mb)
Abstract/Spikblad (128.5Kb)
Datum
2017-10-23
Författare
Roger, Friederike
Nyckelord
Aging
Peroxiredoxin
Redox Signaling
Caloric restriction
light sensing
Publikationstyp
Doctoral thesis
ISBN
978-91-629-0329-9
Språk
eng
Metadata
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