Nature Communications (Mar 2024)

Structural basis for phage-mediated activation and repression of bacterial DSR2 anti-phage defense system

  • Jun-Tao Zhang,
  • Xiao-Yu Liu,
  • Zhuolin Li,
  • Xin-Yang Wei,
  • Xin-Yi Song,
  • Ning Cui,
  • Jirui Zhong,
  • Hongchun Li,
  • Ning Jia

DOI
https://doi.org/10.1038/s41467-024-47177-9
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 14

Abstract

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Abstract Silent information regulator 2 (Sir2) proteins typically catalyze NAD+-dependent protein deacetylation. The recently identified bacterial Sir2 domain-containing protein, defense-associated sirtuin 2 (DSR2), recognizes the phage tail tube and depletes NAD+ to abort phage propagation, which is counteracted by the phage-encoded DSR anti-defense 1 (DSAD1), but their molecular mechanisms remain unclear. Here, we determine cryo-EM structures of inactive DSR2 in its apo form, DSR2–DSAD1 and DSR2–DSAD1–NAD+, as well as active DSR2–tube and DSR2–tube–NAD+ complexes. DSR2 forms a tetramer with its C-terminal sensor domains (CTDs) in two distinct conformations: CTDclosed or CTDopen. Monomeric, rather than oligomeric, tail tube proteins preferentially bind to CTDclosed and activate Sir2 for NAD+ hydrolysis. DSAD1 binding to CTDopen allosterically inhibits tube binding and tube-mediated DSR2 activation. Our findings provide mechanistic insight into DSR2 assembly, tube-mediated DSR2 activation, and DSAD1-mediated inhibition and NAD+ substrate catalysis in bacterial DSR2 anti-phage defense systems.