Literature DB >> 32295912

Impact of Měnglà Virus Proteins on Human and Bat Innate Immune Pathways.

Caroline G Williams1, Joyce Sweeney Gibbons1,2, Timothy R Keiffer1, Priya Luthra1, Megan R Edwards1, Christopher F Basler3.   

Abstract

Měnglà virus (MLAV), identified in Rousettus bats, is a phylogenetically distinct member of the family Filoviridae Because the filoviruses Ebola virus (EBOV) and Marburg virus (MARV) modulate host innate immunity, MLAV VP35, VP40, and VP24 proteins were compared with their EBOV and MARV homologs for innate immune pathway modulation. In human and Rousettus cells, MLAV VP35 behaved like EBOV and MARV VP35s, inhibiting virus-induced activation of the interferon beta (IFN-β) promoter and interferon regulatory factor 3 (IRF3) phosphorylation. MLAV VP35 also interacted with PACT, a host protein engaged by EBOV VP35 to inhibit RIG-I signaling. MLAV VP35 also inhibits PKR activation. MLAV VP40 was demonstrated to inhibit type I IFN-induced gene expression in human and bat cells. It blocked STAT1 tyrosine phosphorylation induced either by type I IFN or overexpressed Jak1, paralleling MARV VP40. MLAV VP40 also inhibited virus-induced IFN-β promoter activation, a property shared by MARV VP40 and EBOV VP24. A Jak kinase inhibitor did not recapitulate this inhibition in the absence of viral proteins. Therefore, inhibition of Jak-STAT signaling is insufficient to explain inhibition of IFN-β promoter activation. MLAV VP24 did not inhibit IFN-induced gene expression or bind karyopherin α proteins, properties of EBOV VP24. MLAV VP24 differed from MARV VP24 in that it failed to interact with Keap1 or activate an antioxidant response element reporter gene due to the absence of a Keap1-binding motif. These functional observations support a closer relationship of MLAV to MARV than to EBOV but also are consistent with MLAV belonging to a distinct genus.IMPORTANCE EBOV and MARV, members of the family Filoviridae, are highly pathogenic zoonotic viruses that cause severe disease in humans. Both viruses use several mechanisms to modulate the host innate immune response, and these likely contribute to the severity of disease. Here, we demonstrate that MLAV, a filovirus newly discovered in a bat, suppresses antiviral type I interferon responses in both human and bat cells. Inhibitory activities are possessed by MLAV VP35 and VP40, which parallels how MARV blocks IFN responses. However, whereas MARV activates cellular antioxidant responses through an interaction between its VP24 protein and host protein Keap1, MLAV VP24 lacks a Keap1-binding motif and fails to activate this cytoprotective response. These data indicate that MLAV possesses immune-suppressing functions that could facilitate human infection. They also support the placement of MLAV in a different genus than either EBOV or MARV.
Copyright © 2020 American Society for Microbiology.

Entities:  

Keywords:  Ebola virus; Marburg virus; filovirus; interferon

Mesh:

Substances:

Year:  2020        PMID: 32295912      PMCID: PMC7307173          DOI: 10.1128/JVI.00191-20

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


  67 in total

1.  Ebola virus VP40-induced particle formation and association with the lipid bilayer.

Authors:  L D Jasenosky; G Neumann; I Lukashevich; Y Kawaoka
Journal:  J Virol       Date:  2001-06       Impact factor: 5.103

2.  The matrix protein of Marburg virus is transported to the plasma membrane along cellular membranes: exploiting the retrograde late endosomal pathway.

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3.  Mapping of the VP40-binding regions of the nucleoprotein of Ebola virus.

Authors:  Takeshi Noda; Shinji Watanabe; Hiroshi Sagara; Yoshihiro Kawaoka
Journal:  J Virol       Date:  2007-01-17       Impact factor: 5.103

4.  Ebola virus VP35 antagonizes PKR activity through its C-terminal interferon inhibitory domain.

Authors:  Michael Schümann; Thorsten Gantke; Elke Mühlberger
Journal:  J Virol       Date:  2009-06-10       Impact factor: 5.103

Review 5.  Ebola and Marburg haemorrhagic fever.

Authors:  V Rougeron; H Feldmann; G Grard; S Becker; E M Leroy
Journal:  J Clin Virol       Date:  2015-01-23       Impact factor: 3.168

6.  Ebola virus VP24 targets a unique NLS binding site on karyopherin alpha 5 to selectively compete with nuclear import of phosphorylated STAT1.

Authors:  Wei Xu; Megan R Edwards; Dominika M Borek; Alicia R Feagins; Anuradha Mittal; Joshua B Alinger; Kayla N Berry; Benjamin Yen; Jennifer Hamilton; Tom J Brett; Rohit V Pappu; Daisy W Leung; Christopher F Basler; Gaya K Amarasinghe
Journal:  Cell Host Microbe       Date:  2014-08-13       Impact factor: 21.023

7.  Ebola virus VP24 binds karyopherin alpha1 and blocks STAT1 nuclear accumulation.

Authors:  St Patrick Reid; Lawrence W Leung; Amy L Hartman; Osvaldo Martinez; Megan L Shaw; Caroline Carbonnelle; Viktor E Volchkov; Stuart T Nichol; Christopher F Basler
Journal:  J Virol       Date:  2006-06       Impact factor: 5.103

8.  Novel activities by ebolavirus and marburgvirus interferon antagonists revealed using a standardized in vitro reporter system.

Authors:  Jonathan C Guito; César G Albariño; Ayan K Chakrabarti; Jonathan S Towner
Journal:  Virology       Date:  2016-12-06       Impact factor: 3.616

9.  Lloviu virus VP24 and VP35 proteins function as innate immune antagonists in human and bat cells.

Authors:  Alicia R Feagins; Christopher F Basler
Journal:  Virology       Date:  2015-08-06       Impact factor: 3.616

Review 10.  A Positive Feedback Amplifier Circuit That Regulates Interferon (IFN)-Stimulated Gene Expression and Controls Type I and Type II IFN Responses.

Authors:  Agata Michalska; Katarzyna Blaszczyk; Joanna Wesoly; Hans A R Bluyssen
Journal:  Front Immunol       Date:  2018-05-28       Impact factor: 7.561

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Journal:  Cell Mol Neurobiol       Date:  2021-09-25       Impact factor: 4.231

2.  High-Throughput Screening Assay to Identify Small Molecule Inhibitors of Marburg Virus VP40 Protein.

Authors:  Priya Luthra; Manu Anantpadma; Sampriti De; Julien Sourimant; Robert A Davey; Richard K Plemper; Christopher F Basler
Journal:  ACS Infect Dis       Date:  2020-09-16       Impact factor: 5.084

3.  Opposite actions of two dsRNA-binding proteins PACT and TRBP on RIG-I mediated signaling.

Authors:  Lauren S Vaughn; Evelyn Chukwurah; Rekha C Patel
Journal:  Biochem J       Date:  2021-02-12       Impact factor: 3.857

Review 4.  A tale of two proteins: PACT and PKR and their roles in inflammation.

Authors:  Evelyn Chukwurah; Kenneth T Farabaugh; Bo-Jhih Guan; Parameswaran Ramakrishnan; Maria Hatzoglou
Journal:  FEBS J       Date:  2021-01-15       Impact factor: 5.622

5.  Characterization of SARS-CoV-2 N protein reveals multiple functional consequences of the C-terminal domain.

Authors:  Chao Wu; Abraham J Qavi; Asmaa Hachim; Niloufar Kavian; Aidan R Cole; Austin B Moyle; Nicole D Wagner; Joyce Sweeney-Gibbons; Henry W Rohrs; Michael L Gross; J S Malik Peiris; Christopher F Basler; Christopher W Farnsworth; Sophie A Valkenburg; Gaya K Amarasinghe; Daisy W Leung
Journal:  bioRxiv       Date:  2020-11-30

6.  Functional Importance of Hydrophobic Patches on the Ebola Virus VP35 IFN-Inhibitory Domain.

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Journal:  Viruses       Date:  2021-11-20       Impact factor: 5.048

7.  Filovirus VP24 Proteins Differentially Regulate RIG-I and MDA5-Dependent Type I and III Interferon Promoter Activation.

Authors:  Felix B He; Hira Khan; Moona Huttunen; Pekka Kolehmainen; Krister Melén; Sari Maljanen; Mengmeng Qu; Miao Jiang; Laura Kakkola; Ilkka Julkunen
Journal:  Front Immunol       Date:  2022-01-05       Impact factor: 7.561

8.  Comparative analyses of small molecule and antibody inhibition on glycoprotein-mediated entry of Měnglà virus with other filoviruses.

Authors:  Laura Cooper; Jazmin Galvan Achi; Lijun Rong
Journal:  J Med Virol       Date:  2022-04-05       Impact factor: 20.693

  8 in total

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