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Título :	SARS-CoV-2 Nsp1 N-terminal and linker regions as a platform for host translational shutoff
Autor:	Andrea Graziadei Fabian Schildhauer Christian Spahn Matthew Kraushar Juri Rappsilber
Nivel de acceso:	Acceso Abierto
Licencia:	Atribución-NoComercial-SinDerivadas
Identificador alternativo:	https://doi.org/10.1101/2022.02.10.479924
Referencia de publicación :	https://www.biorxiv.org/content/10.1101/2022.02.10.479924v1
Resumen o descripción:	In the early stages of SARS-CoV-2 infection, non-structural protein 1 (Nsp1) inhibits the innate immune response by inserting its C-terminal helices into the mRNA entry channel of the ribosome and promoting mRNA degradation. Nevertheless, the mechanism by which Nsp1 achieves host translational shutoff while allowing for viral protein synthesis remains elusive. We set out to characterize the interactome of full-length Nsp1 and its topology by crosslinking mass spectrometry in order to investigate the role of the N-terminal domain and linker regions in host translational shutoff. We find that these regions are in contact with 40S proteins lining the mRNA entry channel and detect a novel interaction with the G subunit of the eIF3 complex. The crosslink-derived distance restraints allowed us to derive an integrative model of full-length Nsp1 on the 40S subunit, reporting on the dynamic interface between Nsp1, the ribosome and the eIF3 complex. The significance of the Nsp1-eIF3G interaction is supported by further evidence that Nsp1 predominantly binds to 40-43S complexes. Our results point towards a mechanism by which Nsp1 is preferentially recruited to canonical initiation complexes, leading to selective inhibition of host-translating ribosomes and subsequent mRNA degradation.
Editor:	medRxiv and bioRxiv
Fecha de publicación :	10-02-2022
Tipo de publicación :	Preimpreso
Fuente:	https://www.biorxiv.org/
Idioma:	Inglés
Cobertura:	Epidemia COVID-19
Audiencia:	Público en general
Área de conocimiento:	VIRUS RESPIRATORIOS
Versión de la publicación:	Versión publicada
Versión de la publicación:	publishedVersion - Versión publicada
Aparece en las colecciones:	Artículos científicos

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