Destabilization of the human RED–SMU1 splicing complex as a basis for host-directed antiinfluenza strategy

Author:

Ashraf Usama,Tengo Laura,Le Corre Laurent,Fournier Guillaume,Busca Patricia,McCarthy Andrew A.,Rameix-Welti Marie-Anne,Gravier-Pelletier Christine,Ruigrok Rob W. H.,Jacob YvesORCID,Vidalain Pierre-Olivier,Pietrancosta NicolasORCID,Crépin Thibaut,Naffakh Nadia

Abstract

New therapeutic strategies targeting influenza are actively sought due to limitations in current drugs available. Host-directed therapy is an emerging concept to target host functions involved in pathogen life cycles and/or pathogenesis, rather than pathogen components themselves. From this perspective, we focused on an essential host partner of influenza viruses, the RED–SMU1 splicing complex. Here, we identified two synthetic molecules targeting an α-helix/groove interface essential for RED–SMU1 complex assembly. We solved the structure of the SMU1 N-terminal domain in complex with RED or bound to one of the molecules identified to disrupt this complex. We show that these compounds inhibiting RED–SMU1 interaction also decrease endogenous RED-SMU1 levels and inhibit viral mRNA splicing and viral multiplication, while preserving cell viability. Overall, our data demonstrate the potential of RED-SMU1 destabilizing molecules as an antiviral therapy that could be active against a wide range of influenza viruses and be less prone to drug resistance.

Funder

Agence Nationale de la Recherche

Institut Carnot Pasteur Microbes et Santé

EC | Seventh Framework Programme

EC | Horizon 2020

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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