Literature DB >> 22915810

Inclusion bodies are a site of ebolavirus replication.

Thomas Hoenen1, Reed S Shabman, Allison Groseth, Astrid Herwig, Michaela Weber, Gordian Schudt, Olga Dolnik, Christopher F Basler, Stephan Becker, Heinz Feldmann.   

Abstract

Inclusion bodies are a characteristic feature of ebolavirus infections in cells. They contain large numbers of preformed nucleocapsids, but their biological significance has been debated, and they have been suggested to be aggregates of viral proteins without any further biological function. However, recent data for other viruses that produce similar structures have suggested that inclusion bodies might be involved in genome replication and transcription. In order to study filovirus inclusion bodies, we fused mCherry to the ebolavirus polymerase L, which is found in inclusion bodies. The resulting L-mCherry fusion protein was functional in minigenome assays and incorporated into virus-like particles. Importantly, L-mCherry fluorescence in transfected cells was readily detectable and distributed in a punctate pattern characteristic for inclusion bodies. A recombinant ebolavirus encoding L-mCherry instead of L was rescued and showed virtually identical growth kinetics and endpoint titers to those for wild-type virus. Using this virus, we showed that the onset of inclusion body formation corresponds to the onset of viral genome replication, but that viral transcription occurs prior to inclusion body formation. Live-cell imaging further showed that inclusion bodies are highly dynamic structures and that they can undergo dramatic reorganization during cell division. Finally, by labeling nascent RNAs using click technology we showed that inclusion bodies are indeed the site of viral RNA synthesis. Based on these data we conclude that, rather than being inert aggregates of nucleocapsids, ebolavirus inclusion bodies are in fact complex and dynamic structures and an important site at which viral RNA replication takes place.

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Year:  2012        PMID: 22915810      PMCID: PMC3486333          DOI: 10.1128/JVI.01525-12

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  40 in total

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2.  Vaccinia virus cores are transported on microtubules.

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3.  Structural dissection of Ebola virus and its assembly determinants using cryo-electron tomography.

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4.  Association of Ebola-related Reston virus particles and antigen with tissue lesions of monkeys imported to the United States.

Authors:  T W Geisbert; P B Jahrling; M A Hanes; P M Zack
Journal:  J Comp Pathol       Date:  1992-02       Impact factor: 1.311

5.  Infection of naive target cells with virus-like particles: implications for the function of ebola virus VP24.

Authors:  Thomas Hoenen; Allison Groseth; Larissa Kolesnikova; Steven Theriault; Hideki Ebihara; Bettina Hartlieb; Sandra Bamberg; Heinz Feldmann; Ute Ströher; Stephan Becker
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6.  A reconstituted replication and transcription system for Ebola virus Reston and comparison with Ebola virus Zaire.

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7.  Ultrastructural pathology of experimental Ebola haemorrhagic fever virus infection.

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Review 8.  Intracellular events and cell fate in filovirus infection.

Authors:  Judith Olejnik; Elena Ryabchikova; Ronald B Corley; Elke Mühlberger
Journal:  Viruses       Date:  2011-08       Impact factor: 5.048

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Authors:  Benjamin G Kopek; Guy Perkins; David J Miller; Mark H Ellisman; Paul Ahlquist
Journal:  PLoS Biol       Date:  2007-09       Impact factor: 8.029

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  89 in total

Review 1.  Conformational plasticity of the Ebola virus matrix protein.

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2.  Live-cell imaging of Marburg virus-infected cells uncovers actin-dependent transport of nucleocapsids over long distances.

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3.  DNA topoisomerase 1 facilitates the transcription and replication of the Ebola virus genome.

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4.  The structure of the C-terminal domain of the nucleoprotein from the Bundibugyo strain of the Ebola virus in complex with a pan-specific synthetic Fab.

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5.  An Improved Reverse Genetics System to Overcome Cell-Type-Dependent Ebola Virus Genome Plasticity.

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6.  Ebola Virus Inclusion Body Formation and RNA Synthesis Are Controlled by a Novel Domain of Nucleoprotein Interacting with VP35.

Authors:  Tsuyoshi Miyake; Charlotte M Farley; Benjamin E Neubauer; Thomas P Beddow; Thomas Hoenen; Daniel A Engel
Journal:  J Virol       Date:  2020-07-30       Impact factor: 5.103

7.  Importin-α7 Is Involved in the Formation of Ebola Virus Inclusion Bodies but Is Not Essential for Pathogenicity in Mice.

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8.  Measles Virus Forms Inclusion Bodies with Properties of Liquid Organelles.

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Review 9.  Development and application of reporter-expressing mononegaviruses: current challenges and perspectives.

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Review 10.  Post-exposure treatments for Ebola and Marburg virus infections.

Authors:  Robert W Cross; Chad E Mire; Heinz Feldmann; Thomas W Geisbert
Journal:  Nat Rev Drug Discov       Date:  2018-01-29       Impact factor: 84.694

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