Targeting eEF1A reprograms translation and uncovers broad-spectrum antivirals against cap or m6A protein synthesis routes

Molina Molina, Elisa; Bech-Serra, Joan Josep; Franco-Trepat, Eloi; Jarne, Ignasi; Perez-Zsolt, Daniel; Badia, Roger; Riveira-Muñoz, Eva; Garcia-Vidal, Edurne; Revilla, Lluís; Franco, Sandra; Tarrés Freixas, Ferran; Roca, Núria; Ceada, Gerardo; Kochanowski, Karl; Raïch-Regué, Dàlia; Erkizia, Itziar; Boreika, Rytis; Bordoy, Antoni E.; Soler, Laia; Guil, Sonia; Carrillo, Jorge; Blanco, Julià; Martínez, Miguel Ángel; Paredes, Roger; Losada, Alejandro; Aviles, Pablo; Cuevas, Carmen; Vergara-Alert, Júlia; Segalés, Joaquim; Clotet, Bonaventura; Ballana, Ester; de la Torre, Carolina; Izquierdo-Useros, Nuria

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Data de publicació

2025-02-07

URI http://hdl.handle.net/20.500.12327/3715

DOI

https://doi.org/10.1038/s41467-025-56151-y

ISSN

2041-1723

Resum

Plitidepsin is an antitumoral compound safe for treating COVID-19 that targets the translation elongation factor eEF1A. Here we detect that plitidepsin decreases de novo cap-dependent translation of SARS-CoV-2 and non-viral RNAs but affects less than 13% of the host proteome, thus preserving cellular viability. In response to plitidepsin, cells upregulate EIF2AK3 and proteins that reduce translation, but also proteins that support proteostasis via ribosome synthesis and cap-independent translation by eIF4G2 and IGF2BP2. While plitidepsin inhibits cap- or internal ribosome entry sites (IRES)-mediated translation, its impact on N6-methyladenosine (m6A) translation is limited. In agreement, plitidepsin blocks members of Coronaviridae, Flaviviridae, Pneumoviridae and Herpesviridae families. Yet, it fails to inhibit retroviruses that exploit m6A synthesis routes and are blocked by drugs targeting IGF2BP2 m6A reader. By deciphering the molecular fingerprint of cells treated with therapies targeting translation we identify a rational approach to select broad-spectrum antivirals with potential to counteract future pandemic viruses.

Tipus de document

Article

Versió del document

Versió publicada

Llengua

Anglès

Matèries (CDU)

619 - Veterinària

Pàgines

Publicat per

Nature Research

Publicat a

Nature Communications

Citació recomanada

Molina, Elisa Molina, Joan Josep Bech-Serra, Eloi Franco-Trepat, Ignasi Jarne, Daniel Perez-Zsolt, Roger Badia, Eva Riveira-Muñoz, Ferran Tarrés-Freixas, et al. 2025. “Targeting eEF1A Reprograms Translation and Uncovers Broad-spectrum Antivirals Against Cap or m6A Protein Synthesis Routes.” Nature Communications 16 (1): 1087. https://doi.org/10.1038/s41467-025-56151-y.

Número de l'acord de la subvenció

MICINN/Programa Estatal de I+D+I orientada a los retos de la sociedad/PID2020-117145RB-I00/ES/NUEVAS TERAPIAS ANTIVIRALES E INMUNOMODULADORAS FRENTE AL SARS-COV-2/

MICINN/Programa Estatal para impulsar la Investigación Científico-Técnica y su Transferencia/PID2023-147498OB-I00/ES/NUEVAS TERAPIAS ANTIVIRALES E INMUNOMODULADORAS DE AMPLIO ESPECTRO FRENTE A FACTORES CELULARES DEL HUESPED/

EU/H2020/101046118/EC/RBD Dimer recombinant protein vaccine against SARSCoV2/RBDCOV

MICINN/ /JDC2023-050389-I/ES/ /

MICINN/Programa Estatal para Desarrollar, Atraer y Retener Talento/RYC2021-033035-I/ES/ /

MICINN/ /PLEC2022-009171/ES/Granja in vitro: desarrollo del primer biobanco de organoides de animales de granja como alternativa a los experimentos con animales en la investigación de enfermedades infecciosas/FARMBANK

Programa

Sanitat Animal

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