Selected article for: "adp ribose and macrodomain family"

Author: Jankevicius, Gytis; Hassler, Markus; Golia, Barbara; Rybin, Vladimir; Zacharias, Martin; Timinszky, Gyula; Ladurner, Andreas G
Title: A family of macrodomain proteins reverses cellular mono-ADP-ribosylation
  • Cord-id: fv0ag2be
  • Document date: 2013_3_10
  • ID: fv0ag2be
    Snippet: ADP-ribosylation is a reversible post-translational modification with wide-ranging biological functions in all kingdoms of life. A variety of enzymes use NAD(+) to transfer either single or multiple ADP-ribose (ADPr) moieties onto distinct amino acid substrates, often in response to DNA damage or other stresses. Poly-ADPr-glycohydrolase readily reverses poly-ADP-ribosylation induced by the DNA-damage sensor PARP1 and other enzymes, but it does not remove the most proximal ADPr linked to the targ
    Document: ADP-ribosylation is a reversible post-translational modification with wide-ranging biological functions in all kingdoms of life. A variety of enzymes use NAD(+) to transfer either single or multiple ADP-ribose (ADPr) moieties onto distinct amino acid substrates, often in response to DNA damage or other stresses. Poly-ADPr-glycohydrolase readily reverses poly-ADP-ribosylation induced by the DNA-damage sensor PARP1 and other enzymes, but it does not remove the most proximal ADPr linked to the target amino acid. Searches for enzymes capable of fully reversing cellular mono-ADP-ribosylation back to the unmodified state have proved elusive, which leaves a gap in the understanding of this modification. Here, we identify a family of macrodomain enzymes present in viruses, yeast and animals that reverse cellular ADP-ribosylation by acting on mono-ADP-ribosylated substrates. Our discoveries establish the complete reversibility of PARP-catalyzed cellular ADP-ribosylation as a regulatory modification. SUPPLEMENTARY INFORMATION: The online version of this article (doi:10.1038/nsmb.2523) contains supplementary material, which is available to authorized users.

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