Publikation:

SET7/9-dependent methylation of ARTD1 at K508 stimulates poly-ADP-ribose formation after oxidative stress

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2013

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Kassner, Ingrid
Andersson, Anneli
Fey, Monika
Hottiger, Michael

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Open Biology. 2013, 3(10), pp. 120173-120173. eISSN 2046-2441. Available under: doi: 10.1098/rsob.120173

Zusammenfassung

ADP-ribosyltransferase diphtheria toxin-like 1 (ARTD1, formerly PARP1) is localized in the nucleus, where it ADP-ribosylates specific target proteins. The post-translational modification (PTM) with a single ADP-ribose unit or with polymeric ADP-ribose (PAR) chains regulates protein function as well as protein–protein interactions and is implicated in many biological processes and diseases. SET7/9 (Setd7, KMT7) is a protein methyltransferase that catalyses lysine monomethylation of histones, but also methylates many non-histone target proteins such as p53 or DNMT1. Here, we identify ARTD1 as a new SET7/9 target protein that is methylated at K508 in vitro and in vivo. ARTD1 auto-modification inhibits its methylation by SET7/9, while auto-poly-ADP-ribosylation is not impaired by prior methylation of ARTD1. Moreover, ARTD1 methylation by SET7/9 enhances the synthesis of PAR upon oxidative stress in vivo. Furthermore, laser irradiation-induced PAR formation and ARTD1 recruitment to sites of DNA damage in a SET7/9-dependent manner. Together, these results reveal a novel mechanism for the regulation of cellular ARTD1 activity by SET7/9 to assure efficient PAR formation upon cellular stress.

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570 Biowissenschaften, Biologie

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ISO 690KASSNER, Ingrid, Anneli ANDERSSON, Monika FEY, Martin TOMAS, Elisa FERRANDO-MAY, Michael HOTTIGER, 2013. SET7/9-dependent methylation of ARTD1 at K508 stimulates poly-ADP-ribose formation after oxidative stress. In: Open Biology. 2013, 3(10), pp. 120173-120173. eISSN 2046-2441. Available under: doi: 10.1098/rsob.120173
BibTex
@article{Kassner2013-10SET79-25698,
  year={2013},
  doi={10.1098/rsob.120173},
  title={SET7/9-dependent methylation of ARTD1 at K508 stimulates poly-ADP-ribose formation after oxidative stress},
  number={10},
  volume={3},
  journal={Open Biology},
  pages={120173--120173},
  author={Kassner, Ingrid and Andersson, Anneli and Fey, Monika and Tomas, Martin and Ferrando-May, Elisa and Hottiger, Michael}
}
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