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      A SAP30 Complex Inhibits IFN-β Expression in Rift Valley Fever Virus Infected Cells

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          Abstract

          Rift Valley fever virus (RVFV) nonstructural protein NSs acts as the major determinant of virulence by antagonizing interferon β (IFN-β) gene expression. We demonstrate here that NSs interacts with the host protein SAP30, which belongs to Sin3A/NCoR/HDACs repressor complexes and interacts with the transcription factor YY1 that regulates IFN-β gene expression. Using confocal microscopy and chromatin immunoprecipitation, we show that SAP30, YY1, and Sin3A-associated corepressor factors strongly colocalize with nuclear NSs filaments and that NSs, SAP30 and Sin3A-associated factors are recruited on the IFN-β promoter through YY1, inhibiting CBP recruitment, histone acetylation, and transcriptional activation. To ascertain the role of SAP30, we produced, by reverse genetics, a recombinant RVFV in which the interacting domain in NSs was deleted. The virus was unable to inhibit the IFN response and was avirulent for mice. We discuss here the strategy developed by the highly pathogenic RVFV to evade the host antiviral response, affecting nuclear organization and IFN-β promoter chromatin structure.

          Author Summary

          Rift Valley fever is a viral mosquito-borne disease affecting ruminants and humans. The disease occurs in Africa and recently it spread to the Arabian Peninsula. In humans, infection can progress to fatal hemorrhagic fever and in ruminants it leads to hepatitis, abortions, or deaths of young lambs. It has been previously shown that the RVFV protein NSs is the major factor of virulence and that pathogenicity is associated with the lack of interferon production. In this study, we analyzed the interaction of NSs with SAP30, a subunit of complexes intervening in gene transcription regulation. We show that SAP30 through its binding to NSs on one hand and to YY1 (the activator/repressor of interferon transcription) on the other hand, forms a multiprotein repression complex on the interferon β promoter. As a consequence, interferon expression is blocked, allowing virus to invade the whole organism. The relevance of the NSs–SAP30 interaction was ascertained by constructing a recombinant virus in which the interacting domain is disrupted. This virus is able to induce interferon expression and when inoculated to the mouse model it was found nonpathogenic.

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          The interferon response circuit: Induction and suppression by pathogenic viruses

          Otto Haller, Georg Kochs, Friedemann Weber (2005)
          Type I interferons (IFN-α/β) are potent antiviral cytokines and modulators of the adaptive immune system. They are induced by viral infection or by double-stranded RNA (dsRNA), a by-product of viral replication, and lead to the production of a broad range of antiviral proteins and immunoactive cytokines. Viruses, in turn, have evolved multiple strategies to counter the IFN system which would otherwise stop virus growth early in infection. Here we discuss the current view on the balancing act between virus-induced IFN responses and the viral counterplayers.
          Article 0 comments Cited 194 times – based on 0 reviews     Review now
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            Alteration of nucleosome structure as a mechanism of transcriptional regulation.

            Elena R. Kingston, Jason Workman (1997)
            The nucleosome, which is the primary building block of chromatin, is not a static structure: It can adopt alternative conformations. Changes in solution conditions or changes in histone acetylation state cause nucleosomes and nucleosomal arrays to behave with altered biophysical properties. Distinct subpopulations of nucleosomes isolated from cells have chromatographic properties and nuclease sensitivity different from those of bulk nucleosomes. Recently, proteins that were initially identified as necessary for transcriptional regulation have been shown to alter nucleosomal structure. These proteins are found in three types of multiprotein complexes that can acetylate nucleosomes, deacetylate nucleosomes, or alter nucleosome structure in an ATP-dependent manner. The direct modification of nucleosome structure by these complexes is likely to play a central role in appropriate regulation of eukaryotic genes.
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              Virus infection induces the assembly of coordinately activated transcription factors on the IFN-beta enhancer in vivo.

              Marc G. Wathelet, Charles Lin, Bhavin Parekh (1998)
              We have identified a virus-activated factor (VAF) that binds to a regulatory element shared by different virus-inducible genes. We provide evidence that VAF contains two members of the interferon regulatory factor (IRF) family of transcriptional activator proteins (IRF-3 and IRF-7), as well as the transcriptional coactivator proteins p300 and CBP. Remarkably, VAF, as well as recombinant IRF-3 and IRF-7 proteins, binds very weakly to the interferon-beta (IFN-beta) gene promoter in vitro. However, in virus-infected cells, both proteins are recruited to the endogenous IFN-beta promoter as part of a protein complex that includes ATF-2/c-Jun and NF-kappa B. These observations provide a unique example of the coordinate activation of multiple transcriptional activator proteins and their highly cooperative assembly into a transcriptional enhancer complex in vivo.
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                Author and article information

                Contributors
                : Role: Editor
                Journal
                Journal ID (nlm-ta): PLoS Pathog
                Journal ID (publisher-id): ppat
                Journal ID (publisher-id): plpa
                Journal ID (pmc): plospath
                Title: PLoS Pathogens
                Publisher: Public Library of Science (San Francisco, USA )
                ISSN (Print): 1553-7366
                ISSN (Electronic): 1553-7374
                Publication date (Print): January 2008
                Publication date (Electronic): 25 January 2008
                Volume: 4
                Issue: 1
                Electronic Location Identifier: e13
                Affiliations
                [1 ] Unité de Génétique Moléculaire des Bunyavirus, Institut Pasteur, Paris, France
                [2 ] Régulation de la Transcription et Maladies Génétiques, CNRS UPR2228, UFR Biomédicale, Université Paris Descartes, Paris, France
                [3 ] BioProtection Systems Corporation, Ames, Iowa, United States of America
                [4 ] Unité de Génétique, Papillomavirus et Cancer Humain, Institut Pasteur, Paris, France
                Mount Sinai School of Medicine, United States of America
                Author notes
                * To whom correspondence should be addressed. E-mail: bonnefoy@ 123456biomedicale.univ-paris5.fr (EB); mbouloy@ 123456pasteur.fr (MB)
                Article
                Publisher ID: 07-PLPA-RA-0344R3 Serial Item and Contribution ID: plpa-04-01-12
                DOI: 10.1371/journal.ppat.0040013
                PMC ID: 2323286
                PubMed ID: 18225953
                SO-VID: 8a6adddd-bb2f-4ef5-b756-e61b68690096
                Copyright © Copyright: © 2008 Le May et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
                History
                Date received : 7 June 2007
                Date accepted : 13 December 2007
                Page count
                Pages: 11
                Categories
                Subject: Research Article
                Subject: Cell Biology
                Subject: Infectious Diseases
                Subject: Microbiology
                Subject: Virology
                Subject: Viruses
                Subject: Eukaryotes
                Subject: Mammals
                Custom metadata
                citation Le May N, Mansuroglu Z, Léger P, Josse T, Blot G, et al. (2008) A SAP30 complex inhibits IFN-β expression in Rift Valley Fever Virus infected cells. PLoS Pathog 4(1): e13. doi: 10.1371/journal.ppat.0040013

                ScienceOpen disciplines: Infectious disease & Microbiology
                Data availability:
                ScienceOpen disciplines: Infectious disease & Microbiology

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