Nature Communications (Apr 2023)

Large-scale phage-based screening reveals extensive pan-viral mimicry of host short linear motifs

  • Filip Mihalič,
  • Leandro Simonetti,
  • Girolamo Giudice,
  • Marie Rubin Sander,
  • Richard Lindqvist,
  • Marie Berit Akpiroro Peters,
  • Caroline Benz,
  • Eszter Kassa,
  • Dilip Badgujar,
  • Raviteja Inturi,
  • Muhammad Ali,
  • Izabella Krystkowiak,
  • Ahmed Sayadi,
  • Eva Andersson,
  • Hanna Aronsson,
  • Ola Söderberg,
  • Doreen Dobritzsch,
  • Evangelia Petsalaki,
  • Anna K. Överby,
  • Per Jemth,
  • Norman E. Davey,
  • Ylva Ivarsson

DOI
https://doi.org/10.1038/s41467-023-38015-5
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 20

Abstract

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Abstract Viruses mimic host short linear motifs (SLiMs) to hijack and deregulate cellular functions. Studies of motif-mediated interactions therefore provide insight into virus-host dependencies, and reveal targets for therapeutic intervention. Here, we describe the pan-viral discovery of 1712 SLiM-based virus-host interactions using a phage peptidome tiling the intrinsically disordered protein regions of 229 RNA viruses. We find mimicry of host SLiMs to be a ubiquitous viral strategy, reveal novel host proteins hijacked by viruses, and identify cellular pathways frequently deregulated by viral motif mimicry. Using structural and biophysical analyses, we show that viral mimicry-based interactions have similar binding strength and bound conformations as endogenous interactions. Finally, we establish polyadenylate-binding protein 1 as a potential target for broad-spectrum antiviral agent development. Our platform enables rapid discovery of mechanisms of viral interference and the identification of potential therapeutic targets which can aid in combating future epidemics and pandemics.