The Genome of Human Parvovirus B19 Can Replicate in Nonpermissive Cells with the Help of Adenovirus Genes and Produces Infectious Virus

Guan, Wuxiang; Wong, Susan; Zhi, Ning; Qiu, Jianming

doi:10.1128/jvi.00702-09

Cited by 75 publications

(124 citation statements)

References 53 publications

(65 reference statements)

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“…In agreement with these results, adenovirus 2 facilitated DNA replication of the closely related parvovirus MVM, 27 whereas pXX6 adenoviral vector, enabled the erythrovirus B19 to replicate its DNA and produce infectious progeny particles in non-permissive HEK 293 cells. 25 This led us to speculate that one or several gene products of pXX6 may directly modulate parvoviral DNA replication or set up favorable cellular conditions for that. In support of an active role of adenovirus genes in parvoviral DNA replication, it has been shown that E4(orf6) participates in the conversion of the singlestranded AAV-2 viral genome into the double-stranded replicative forms.…”

Section: Discussionmentioning

confidence: 99%

“…The adenovirus genes E2a, E4(orf6) and VA RNA were found to boost human erythrovirus B19 replication and production in HEK 293 cells, an otherwise non-permissive cell line for B19 production. 25 Furthermore, parvovirus H-1PV failed to initiate replication in secondary cultures of normal human embryonic lung cells, unless these cells are co-infected with adenovirus serotype 12. 26 In addition, adenovirus serotype 2 induced an increase in parvovirus MVMp DNA replication in HeLa cells, associated with re-localization of MVMp DNA from host nucleoli to adenovirus replication factories.…”

Section: Introductionmentioning

confidence: 99%

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Novel adenovirus-based helper system to support production of recombinant parvovirus

et al. 2010

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Preclinical studies using various cell culture and animal systems highlight the potential of recombinant rodent parvoviruses (recPVs) for cancer therapy. Production of these viruses is, however, not efficient and this hampers the clinical applications of these agents. In this study, we show that the adenovirus genes E2a, E4(orf6) and VA RNA increase the production of recPVs by more than 10-fold and reduce the time of production from 3 to 2 days in HEK293T cells. The helper effects of these genes can be observed with different recPVs, regardless of the nature and size of the inserted transgene. Furthermore, we generated a recombinant Adenovirus 5 carrying the parvovirus VP transcription unit. This helper, named Ad-VP, allows recPVs to be efficiently produced through a protocol based only on cell infection, making possible to use cell lines, such as NB324K, which are good producers of parvoviruses but are hardly transfectable. Hence, we could further improve viral titers and reduce time and costs of production. This Ad-VP helper-based protocol could be scaled up to a bioreactor format for the generation of the large amounts of recPVs needed for future clinical applications.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Novel adenovirus-based helper system to support production of recombinant parvovirus

et al. 2010

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“…AY386330) (19). The parent plasmid C1NS1(Ϫ), which contains the SV40 replication origin and produces a prematurely terminated NS1 gene has been described previously (14,17,20). The parent plasmid pB19-N8 was described previously (19 -21).…”

Section: Methodsmentioning

confidence: 99%

“…Cells were transfected with 2 g of DNA per 60-mm plate using Lipofectamine TM and PLUS TM reagent (Invitrogen) according to the manufacturer's instructions. UT7/Epo-S1 cells, which are permissive to B19V infection (20,25,26), were cultured in DMEM with 10% FCS and 2 units/ml of Epo (Epogen; Amgen, Thousand Oaks, CA) at 37°C in 5% CO 2 . Plasmids B19-N8, B19-N8A2-1U2AF, and B19-N8A2-1/ 2KO were digested with XhoI/EcoRI to recover the excised B19V DNA fragments that were used for electroporation.…”

Section: Cells Transfection and Virus Infection-cos-7 Cellsmentioning

confidence: 99%

“…Plasmids B19-N8, B19-N8A2-1U2AF, and B19-N8A2-1/ 2KO were digested with XhoI/EcoRI to recover the excised B19V DNA fragments that were used for electroporation. UT7/ Epo-S1 cells were electroporated with 2 g of linearized B19V DNA per 2 ϫ 10 6 cells with an Amaxa Nucleofector device (Lonza) as described previously (20). Primary human erythroid progenitor cells (CD36 ϩ EPCs) were generated; large numbers of CD36…”

Section: Cells Transfection and Virus Infection-cos-7 Cellsmentioning

confidence: 99%

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Internal Polyadenylation of the Parvovirus B19 Precursor mRNA Is Regulated by Alternative Splicing

Guan

Huang

Cheng

et al. 2011

Journal of Biological Chemistry

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Alternative processing of parvovirus B19 (B19V) pre-mRNA is critical to generating appropriate levels of B19V mRNA transcripts encoding capsid proteins and small nonstructural proteins. Polyadenylation of the B19V pre-mRNA at the proximal polyadenylation site ((pA)p), which prevents generation of fulllength capsid proteins encoding mRNA transcripts, has been suggested as a step that blocks B19V permissiveness. We report here that efficient splicing of the B19V pre-mRNA within the first intron (upstream of the (pA)p site) stimulated the polyadenylation; in contrast, splicing of the B19V pre-mRNA within the second intron (in which the (pA)p site resides) interfered with the polyadenylation, leading to the generation of a sufficient number of B19V mRNA transcripts polyadenylated at the distal polyadenylation site ((pA)d). We also found that splicing within the second intron and polyadenylation at the (pA)p site compete during processing of the B19V pre-mRNA. Furthermore, we discovered that the U1 RNA that binds to the 5 splice donor site of the second intron is fully responsible for inhibiting polyadenylation at the (pA)p site, whereas actual splicing, and perhaps assembly of the functional spliceosome, is not required. Finally, we demonstrated that inhibition of B19V pre-mRNA splicing within the second intron by targeting an intronic splicing enhancer using a Morpholino antisense oligonucleotide prevented B19V mRNA transcripts polyadenylated at the (pA)d site during B19V infection of human erythroid progenitors. Thus, our study reveals the mechanism by which alternative splicing coordinates alternative polyadenylation to generate full-length B19V mRNA transcripts at levels sufficient to support productive B19V infection. Human parvovirus B19 (B19V)2 is a member of the genus Erythrovirus of the family Parvoviridae. B19V causes several diseases in humans (1), the most common of which is erythema infectiosum or Fifth disease. Other diseases include acute and chronic arthropathy, transient aplastic crisis (infection of patients with a high rate of red blood cell turnover), pure red cell aplasia (infection of immunocompromised patients), and hydrops fetalis (infection of pregnant women). Like other parvoviruses, B19V contains a linear single-stranded DNA genome of approximately (ϳ)5.6 kb, which is encapsidated by an icosahedrally symmetric capsid without an envelope (2, 3). In addition to infecting only humans, B19V infection shows a remarkable tropism for human erythroid progenitor cells (4 -7).Like members in the genus Bocavirus (8, 9) and Aleutian mink disease virus (10), also of the Parvoviridae family, the transcription profile of B19V is unusual for a DNA virus in that all of the mRNA transcripts are generated from a single precursor mRNA (pre-mRNA) transcribed from a single promoter at map unit 6 (P6) and feature alternative polyadenylation and splicing (see Fig. 1A) (11, 12). The only unspliced mRNA encoding the large nonstructural protein (NS1) is polyadenylated at the proximal poly(A) site ((pA)p) and retains...

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Telbivudine in chronic lymphocytic myocarditis and human parvovirus B19 transcriptional activity

et al. 2018

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AimsMyocarditis is often associated with parvovirus B19 (B19V) persistence, which can induce vascular damage. Based on the antiviral and anti‐inflammatory properties of telbivudine, we aimed to evaluate its efficacy to protect B19V‐infected endothelial cells in vitro and to treat chronic lymphocytic myocarditis patients with B19V transcriptional activity.Methods and resultsWe evaluated the endothelial‐protective potential of telbivudine in human microvascular endothelial cells‐1, which were infected with B19V. Treatment with 10 ng/mL of telbivudine decreased the B19V‐induced endothelial cell apoptosis and endothelial‐to‐mesenchymal transition. Along with this finding, telbivudine reduced the expression of transforming growth factor‐β1 and of tenascin‐C. The endothelial‐protective properties of telbivudine were also found in tumour necrosis factor‐α‐stressed human microvascular endothelial cells‐1. In addition, oxidative stress in angiotensin II‐stressed and transforming growth factor‐β1‐stressed HL‐1 cardiomyocytes and fibroblasts, respectively, was reduced upon telbivudine treatment, illustrating that telbivudine exerts multimodal protective effects. Based on these in vitro findings, four patients severely suffering from an endomyocardial biopsy‐proven myocarditis associated with B19V transcriptional activity (VP1/VP2‐mRNA positive) were treated with telbivudine (600 mg/dL) for 6 months in a single‐patient‐use approach. Follow‐up biopsies 6 months after treatment showed that VP1/VP2‐mRNA levels and CD3 cells decreased in all patients and were associated with an improvement in ejection fraction and New York Heart Association class. These findings were paralleled by a drop in tenascin‐C expression as shown via matrix‐assisted laser desorption ionization–imaging mass spectrometry.ConclusionsTelbivudine exerts endothelial‐protective effects in B19V‐infected endothelial cells and improves chronic myocarditis associated with B19V transcriptional activity. These findings will be further evaluated in the clinical exploratory trial: the PreTopic study.

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The Genome of Human Parvovirus B19 Can Replicate in Nonpermissive Cells with the Help of Adenovirus Genes and Produces Infectious Virus

Cited by 75 publications

References 53 publications

Novel adenovirus-based helper system to support production of recombinant parvovirus

Novel adenovirus-based helper system to support production of recombinant parvovirus

Internal Polyadenylation of the Parvovirus B19 Precursor mRNA Is Regulated by Alternative Splicing

Telbivudine in chronic lymphocytic myocarditis and human parvovirus B19 transcriptional activity

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