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      BK Polyomavirus MicroRNA Levels in Exosomes Are Modulated by Non-Coding Control Region Activity and Down-Regulate Viral Replication When Delivered to Non-Infected Cells Prior to Infection

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          Abstract

          In immunosuppressed patients, BKPyV-variants emerge carrying rearranged non-coding control-regions ( rr-NCCRs) that increase early viral gene region (EVGR) expression and replication capacity. BKPyV also encodes microRNAs, which have been reported to downregulate EVGR-encoded large T-antigen transcripts, to decrease viral replication in infected cells and to be secreted in exosomes. To investigate the interplay of NCCR and microRNAs, we compared archetype- and rr-NCCR-BKPyV infection in cell culture. We found that laboratory and clinical rr-NCCR-BKPyV-strains show higher replication rates but significantly lower microRNA levels than archetype virus intracellularly and in exosomes. To investigate whether rr-NCCR or increased EVGR activity modulated microRNA levels, we examined the ( sp1-4) NCCR-BKPyV, which has an archetype NCCR-architecture but shows increased EVGR expression due to point mutations inactivating one Sp1 binding site. We found that microRNA levels following ( sp1-4) NCCR-BKPyV infection were as low as in rr-NCCR-variants. Thus, NCCR rearrangements are not required for lower miRNA levels. Accordingly, Sp1 siRNA knock-down decreased microRNA levels in archetype BKPyV infection but had no effect on ( sp1-4)- or rr-NCCR-BKPyV. However, rr-NCCR-BKPyV replication was downregulated by exosome preparations carrying BKPyV-microRNA prior to infection. To explore the potential relevance in humans, urine samples from 12 natalizumab-treated multiple sclerosis patients were analysed. In 7 patients, rr-NCCR-BKPyV were detected showing high urine BKPyV loads but low microRNAs levels, whereas the opposite was seen in 5 patients with archetype BKPyV. We discuss the results in a dynamic model of BKPyV replication according to NCCR activity and exosome regulation, which integrates immune selection pressure, spread to new host cells and rr-NCCR emergence.

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          SV40-encoded microRNAs regulate viral gene expression and reduce susceptibility to cytotoxic T cells.

          Christopher S Sullivan, Adam Grundhoff, Satvir Tevethia (2005)
          MicroRNAs (miRNAs) are small (approximately 22-nucleotide) RNAs that in lower organisms serve important regulatory roles in development and gene expression, typically by forming imperfect duplexes with target messenger RNAs. miRNAs have also been described in mammalian cells and in infections with Epstein-Barr virus (EBV), but the function of most of them is unknown. Although one EBV miRNA probably altered the processing of a viral mRNA, the regulatory significance of this event is uncertain, because other transcripts exist that can supply the targeted function. Here we report the identification of miRNAs encoded by simian virus 40 (SV40) and define their functional significance for viral infection. SVmiRNAs accumulate at late times in infection, are perfectly complementary to early viral mRNAs, and target those mRNAs for cleavage. This reduces the expression of viral T antigens but does not reduce the yield of infectious virus relative to that generated by a mutant lacking SVmiRNAs. However, wild-type SV40-infected cells are less sensitive than the mutant to lysis by cytotoxic T cells, and trigger less cytokine production by such cells. Thus, viral evolution has taken advantage of the miRNA pathway to generate effectors that enhance the probability of successful infection.
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            Viruses and microRNAs.

            Bryan R. Cullen (2006)
            The discovery of RNA interference and cellular microRNAs (miRNAs) has not only affected how biological research is conducted but also revealed an entirely new level of post-transcriptional gene regulation. Here, I discuss the potential functions of the virally encoded miRNAs recently identified in several pathogenic human viruses and propose that cellular miRNAs may have had a substantial effect on viral evolution and may continue to influence the in vivo tissue tropism of viruses. Our increasing knowledge of the role and importance of virally encoded miRNAs will probably offer new insights into how viruses that establish latent infections, such as herpesviruses, avoid elimination by the host innate or adaptive immune system. Research into viral miRNA function might also suggest new approaches for treating some virally induced diseases.
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              SV40-transformed simian cells support the replication of early SV40 mutants.

              Y. Gluzman (1980)
              CV-1, an established line of simian cells permissive for lytic growth of SV40, were transformed by an origin-defective mutant of SV40 which codes for wild-type T antigen. Three transformed lines (COS-1, -3, -7) were established and found to contain T antigen; retain complete permissiveness for lytic growth of SV40; support the replication of tsA209 virus at 40 degrees C; and support the replication of pure populations of SV40 mutants with deletions in the early region. One of the lines (COS-1) contains a single integrated copy of the complete early region of SV40 DNA. These cells are possible hosts for the propagation of pure populations of recombinant SV40 viruses.
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                Author and article information

                Journal
                Journal ID (nlm-ta): Viruses
                Journal ID (iso-abbrev): Viruses
                Journal ID (publisher-id): viruses
                Title: Viruses
                Publisher: MDPI
                ISSN (Electronic): 1999-4915
                Publication date (Electronic): 30 August 2018
                Publication date Collection: September 2018
                Volume: 10
                Issue: 9
                Electronic Location Identifier: 466
                Affiliations
                [1 ]Department of Experimental and Clinical Medicine, University of Florence, I-50134 Florence, Italy; martelli.francesco85@ 123456gmail.com (F.M.); maria.chiara2591@ 123456gmail.com (M.C.G.)
                [2 ]Transplantation & Clinical Virology, Department Biomedicine (Haus Petersplatz), University of Basel, CH-4003 Basel, Switzerland; zongsong.wu@ 123456unibas.ch (Z.W.); fabian.weissbach@ 123456unibas.ch (F.H.W.)
                [3 ]Department of Biomedical, Surgical and Dental Sciences, University of Milan, I-20100 Milano, Italy; serena.delbue@ 123456unimi.it (S.D.); pasquale.ferrante@ 123456unimi.it (P.F.)
                [4 ]Infectious Diseases & Hospital Epidemiology, University Hospital Basel, CH-4003 Basel, Switzerland
                Author notes
                [†]

                Both authors contributed equally to this study.

                Author information
                https://orcid.org/0000-0001-9647-6115
                https://orcid.org/0000-0003-0969-8153
                https://orcid.org/0000-0003-3374-7621
                Article
                Publisher ID: viruses-10-00466
                DOI: 10.3390/v10090466
                PMC ID: 6164188
                PubMed ID: 30200237
                SO-VID: f3baedb1-abfa-46b0-b784-0ea734d72a03
                Copyright © © 2018 by the authors.
                License:

                Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license ( http://creativecommons.org/licenses/by/4.0/).

                History
                Date received : 30 May 2018
                Date accepted : 29 August 2018
                Categories
                Subject: Article

                ScienceOpen disciplines: Microbiology & Virology
                Keywords: polyomavirus,non-coding control region,microrna,exosomes,persistence,immunosuppression,bk virus
                Data availability:
                ScienceOpen disciplines: Microbiology & Virology
                Keywords: polyomavirus, non-coding control region, microrna, exosomes, persistence, immunosuppression, bk virus

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