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

Authors :
Mihalic, Filip
Simonetti, Leandro
Giudice, Girolamo
Sander, Marie Rubin
Lindqvist, Richard
Akprioro Peters, Marie Berit
Benz, Caroline
Kassa, Eszter
Badgujar, Dilip
Inturi, Raviteja
Ali, Muhammad
Krystkowiak, Izabella
Sayadi, Ahmed
Andersson, Eva
Aronsson, Hanna
Söderberg, Ola
Dobritzsch, Doreen
Petsalaki, Evangelia
Överby, Anna K
Jemth, Per
Davey, Norman E.
Ivarsson, Ylva
Mihalic, Filip
Simonetti, Leandro
Giudice, Girolamo
Sander, Marie Rubin
Lindqvist, Richard
Akprioro Peters, Marie Berit
Benz, Caroline
Kassa, Eszter
Badgujar, Dilip
Inturi, Raviteja
Ali, Muhammad
Krystkowiak, Izabella
Sayadi, Ahmed
Andersson, Eva
Aronsson, Hanna
Söderberg, Ola
Dobritzsch, Doreen
Petsalaki, Evangelia
Överby, Anna K
Jemth, Per
Davey, Norman E.
Ivarsson, Ylva
Publication Year :
2022

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 1,712 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.

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1349083870
Document Type :
Electronic Resource
Full Text :
https://doi.org/10.1101.2022.06.19.496705