Coronaviruses Hijack the LC3-I-positive EDEMosomes, ER-derived vesicles exporting short-lived ERAD regulators, for replication

Coronaviruses (CoV), including SARS and mouse hepatitis virus (MHV), are enveloped RNA viruses that induce formation of double-membrane vesicles (DMVs) and target their replication and transcription complexes (RTCs) on the DMV-limiting membranes. The DMV biogenesis has been connected with the early...

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Bibliographic Details
Published in:Cell host & microbe 2010-06, Vol.7 (6), p.500-508
Main Authors: Reggiori, Fulvio, Monastyrska, Iryna, Verheije, Monique H, Calì, Tito, Ulasli, Mustafa, Bianchi, Siro, Bernasconi, Riccardo, de Haan, Cornelis A M, Molinari, Maurizio
Format: Article
Language:English
Subjects:
Animals
Cells, Cultured
Cytoplasmic Vesicles - chemistry
Cytoplasmic Vesicles - virology
Endoplasmic Reticulum - virology
Membrane Proteins - metabolism
Microscopy, Confocal
Microscopy, Electron, Transmission
Microscopy, Fluorescence
Microtubule-Associated Proteins - analysis
Murine hepatitis virus - physiology
Ubiquitins - analysis
Virus Replication
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Summary:Coronaviruses (CoV), including SARS and mouse hepatitis virus (MHV), are enveloped RNA viruses that induce formation of double-membrane vesicles (DMVs) and target their replication and transcription complexes (RTCs) on the DMV-limiting membranes. The DMV biogenesis has been connected with the early secretory pathway. CoV-induced DMVs, however, lack conventional endoplasmic reticulum (ER) or Golgi protein markers, leaving their membrane origins in question. We show that MHV co-opts the host cell machinery for COPII-independent vesicular ER export of a short-living regulator of ER-associated degradation (ERAD), EDEM1, to derive cellular membranes for replication. MHV infection causes accumulation of EDEM1 and OS-9, another short-living ER chaperone, in the DMVs. DMVs are coated with the nonlipidated LC3/Atg8 autophagy marker. Downregulation of LC3, but not inactivation of host cell autophagy, protects cells from CoV infection. Our study identifies the host cellular pathway hijacked for supplying CoV replication membranes and describes an autophagy-independent role for nonlipidated LC3-I.
ISSN:1931-3128
1934-6069
DOI:10.1016/j.chom.2010.05.013