Nature Communications (Aug 2023)

Next-generation proteomics for quantitative Jumbophage-bacteria interaction mapping

  • Andrea Fossati,
  • Deepto Mozumdar,
  • Claire Kokontis,
  • Melissa Mèndez-Moran,
  • Eliza Nieweglowska,
  • Adrian Pelin,
  • Yuping Li,
  • Baron Guo,
  • Nevan J. Krogan,
  • David A. Agard,
  • Joseph Bondy-Denomy,
  • Danielle L. Swaney

DOI
https://doi.org/10.1038/s41467-023-40724-w
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 16

Abstract

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Abstract Host-pathogen interactions are pivotal in regulating establishment, progression, and outcome of an infection. While affinity-purification mass spectrometry has become instrumental in characterizing such interactions, it suffers from limitations in scalability and biological authenticity. Here we present the use of co-fractionation mass spectrometry for high throughput analysis of host-pathogen interactions from native viral infections of two jumbophages (ϕKZ and ϕPA3) in Pseudomonas aeruginosa. This approach enabled the detection of > 6000 unique host-pathogen interactions for each phage, encompassing > 50% of their respective proteomes. This deep coverage provided evidence for interactions between KZ-like phage proteins and the host ribosome, and revealed protein complexes for previously undescribed phage ORFs, including a ϕPA3 complex showing strong structural and sequence similarity to ϕKZ non-virion RNA polymerase. Interactome-wide comparison across phages showed similar perturbed protein interactions suggesting fundamentally conserved mechanisms of phage predation within the KZ-like phage family. To enable accessibility to this data, we developed PhageMAP, an online resource for network query, visualization, and interaction prediction ( https://phagemap.ucsf.edu/ ). We anticipate this study will lay the foundation for the application of co-fractionation mass spectrometry for the scalable profiling of host-pathogen interactomes and protein complex dynamics upon infection.