SirT7 auto-ADP-ribosylation regulates glucose starvation response through mH2A1

Abstract
Sirtuins are key players of metabolic stress response. Originally described as deacetylases, some sirtuins also exhibit poorly understood mono–adenosine 5′-diphosphate (ADP)–ribosyltransferase (mADPRT) activity. We report that the deacetylase SirT7 is a dual sirtuin, as it also features auto-mADPRT activity. SirT7 mADPRT occurs at a previously undefined active site, and its abrogation alters SirT7 chromatin distribution. We identify an epigenetic pathway by which ADP-ribosyl-SirT7 is recognized by the ADP-ribose reader mH2A1.1 under glucose starvation, inducing SirT7 relocalization to intergenic regions. SirT7 promotes mH2A1 enrichment in a subset of nearby genes, many of them involved in second messenger signaling, resulting in their specific up- or down-regulation. The expression profile of these genes under calorie restriction is consistently abrogated in SirT7-deficient mice, resulting in impaired activation of autophagy. Our work provides a novel perspective on sirtuin duality and suggests a role for SirT7/mH2A1.1 axis in glucose homeostasis and aging.
Funding Information
  • Catalan Government Agency AGAUR (2014-SGR400)
  • Catalan Government Agency AGAUR (2017-SGR148)
  • Catalan Government Agency AGAUR (2017-SGR595)
  • Spanish Ministry of Economy and Competitiveness -MINECO (SAF2011-25860)
  • Spanish Ministry of Economy and Competitiveness -MINECO (SAF2014-55964R)
  • Spanish Ministry of Economy and Competitiveness -MINECO (SAF2017-88975R)
  • Spanish Ministry of Economy and Competitiveness -MINECO (CTQ2016-80364-P)
  • Rutgers Human Genetics Institute of New Jersey (-)
  • ISCIII and ERDF (PT17/0019 from the PE I+D+i 2013-2016)
  • Spanish Ministry of Economy and Competitiveness -MINECO (SAF2016-77830R)
  • German Center for Cardiovascular Research (DZHK) and the Deutsche Forschungsgemeinschaft (DFG SFB TRR81 A02)
  • German Center for Cardiovascular Research (DZHK) and the Deutsche Forschungsgemeinschaft (SFB 1213 TP B02)

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