Nature Communications (Jan 2025)

The Psu protein of phage satellite P4 inhibits transcription termination factor ρ by forced hyper-oligomerization

  • Daniela Gjorgjevikj,
  • Naveen Kumar,
  • Bing Wang,
  • Tarek Hilal,
  • Nelly Said,
  • Bernhard Loll,
  • Irina Artsimovitch,
  • Ranjan Sen,
  • Markus C. Wahl

DOI
https://doi.org/10.1038/s41467-025-55897-9
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 20

Abstract

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Abstract Many bacteriophages modulate host transcription to favor expression of their own genomes. Phage satellite P4 polarity suppression protein, Psu, a building block of the viral capsid, inhibits hexameric transcription termination factor, ρ, by presently unknown mechanisms. Our cryogenic electron microscopy structures of ρ-Psu complexes show that Psu dimers clamp two inactive, open ρ rings and promote their expansion to higher-oligomeric states. ATPase, nucleotide binding and nucleic acid binding studies revealed that Psu hinders ρ ring closure and traps nucleotides in their binding pockets on ρ. Structure-guided mutagenesis in combination with growth, pull-down, and termination assays further delineated the functional ρ-Psu interfaces in vivo. Bioinformatic analyses revealed that Psu is associated with a wide variety of phage defense systems across Enterobacteriaceae, suggesting that Psu may regulate expression of anti-phage genes. Our findings show that modulation of the ρ oligomeric state via diverse strategies is a pervasive gene regulatory principle in bacteria.