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Literature DB >> 29212929

Nucleic Acid Polymers Are Active against Hepatitis Delta Virus Infection In Vitro.

Frauke Beilstein¹, Matthieu Blanchet², Andrew Vaillant³, Camille Sureau⁴.

Abstract

In this study, an in vitro infection model for the hepatitis delta virus (HDV) was used to evaluate the antiviral effects of phosphorothioate nucleic acid polymers (NAPs) and investigate their mechanism of action. The results show that NAPs inhibit HDV infection at concentrations less than 4 μM in cultures of differentiated human hepatoma cells. NAPs were shown to be active at viral entry but inactive postentry on HDV RNA replication. Inhibition was independent of the NAP nucleotide sequence but dependent on both size and amphipathicity of the polymer. NAP antiviral activity was effective against HDV virions bearing the main hepatitis B virus (HBV) immune escape substitutions (D144A and G145R) and was pangenomic with regard to HBV envelope proteins. Furthermore, similar to immobilized heparin, immobilized NAPs could bind HDV particles, suggesting that entry inhibition was due, at least in part, to preventing attachment of the virus to cell surface glycosaminoglycans. The results document NAPs as a novel class of antiviral compounds that can prevent HDV propagation.IMPORTANCE HDV infection causes the most severe form of viral hepatitis in humans and one of the most difficult to cure. Currently, treatments are limited to long-term administration of interferon at high doses, which provide only partial efficacy. There is thus an urgent need for innovative approaches to identify new antiviral against HDV. The significance of our study is in demonstrating that nucleic acid polymers (NAPs) are active against HDV by targeting the envelope of HDV virions. In an in vitro infection assay, NAP activity was recorded at concentrations less than 4 μM in the absence of cell toxicity. Furthermore, the fact that NAPs could block HDV at viral entry suggests their potential to control the spread of HDV in a chronically HBV-infected liver. In addition, NAP anti-HDV activity was pangenomic with regard to HBV envelope proteins and not circumvented by HBsAg substitutions associated with HBV immune escape.

Entities: Chemical Disease Gene Mutation Species

Keywords: HDV; NAPs; hepatitis D virus; nucleic acid polymers

Mesh：

Substances：

Year: 2018 PMID： 29212929 PMCID： PMC5790928 DOI： 10.1128/JVI.01416-17

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

34 in total

1. Analytical study of phosphorothioate analogues of oligodeoxynucleotides using high-performance liquid chromatography.

Authors: S Agrawal; J Y Tang; D M Brown
Journal: J Chromatogr Date: 1990-06-22

Review 2. Nucleic acid polymers: Broad spectrum antiviral activity, antiviral mechanisms and optimization for the treatment of hepatitis B and hepatitis D infection.

Authors: Andrew Vaillant
Journal: Antiviral Res Date: 2016-07-09 Impact factor: 5.970

3. Phosphorothioate oligonucleotides inhibit human immunodeficiency virus type 1 fusion by blocking gp41 core formation.

Authors: Andrew Vaillant; Jean-Marc Juteau; Hong Lu; Shuwen Liu; Carol Lackman-Smith; Roger Ptak; Shibo Jiang
Journal: Antimicrob Agents Chemother Date: 2006-04 Impact factor: 5.191

4. Persistent hepatitis D virus mono-infection in humanized mice is efficiently converted by hepatitis B virus to a productive co-infection.

Authors: Katja Giersch; Martina Helbig; Tassilo Volz; Lena Allweiss; Lida V Mancke; Ansgar W Lohse; Susanne Polywka; Jörg M Pollok; Jörg Petersen; John Taylor; Maura Dandri; Marc Lütgehetmann
Journal: J Hepatol Date: 2013-11-23 Impact factor: 25.083

5. Pharmacokinetics, biodistribution, and stability of oligodeoxynucleotide phosphorothioates in mice.

Authors: S Agrawal; J Temsamani; J Y Tang
Journal: Proc Natl Acad Sci U S A Date: 1991-09-01 Impact factor: 11.205

6. Entry of hepatitis delta virus requires the conserved cysteine residues of the hepatitis B virus envelope protein antigenic loop and is blocked by inhibitors of thiol-disulfide exchange.

Authors: Georges Abou-Jaoudé; Camille Sureau
Journal: J Virol Date: 2007-09-26 Impact factor: 5.103

7. Amphipathic DNA polymers are candidate vaginal microbicides and block herpes simplex virus binding, entry and viral gene expression.

Authors: Esmeralda M Guzman; Natalia Cheshenko; Vikas Shende; Marla J Keller; Nathalie Goyette; Jean-Marc Juteau; Guy Boivin; Andrew Vaillant; Betsy C Herold
Journal: Antivir Ther Date: 2007

8. Role of glycosaminoglycans for binding and infection of hepatitis B virus.

Authors: Corinna M Leistner; Stefanie Gruen-Bernhard; Dieter Glebe
Journal: Cell Microbiol Date: 2008-01 Impact factor: 3.715

9. Proteoglycans act as cellular hepatitis delta virus attachment receptors.

Authors: Oscar Lamas Longarela; Tobias T Schmidt; Katrin Schöneweis; Raffaella Romeo; Heiner Wedemeyer; Stephan Urban; Andreas Schulze
Journal: PLoS One Date: 2013-03-07 Impact factor: 3.240

10. Therapeutic Antiviral Effect of the Nucleic Acid Polymer REP 2055 against Persistent Duck Hepatitis B Virus Infection.

Authors: Faseeha Noordeen; Catherine A Scougall; Arend Grosse; Qiao Qiao; Behzad B Ajilian; Georget Reaiche-Miller; John Finnie; Melanie Werner; Ruth Broering; Joerg F Schlaak; Andrew Vaillant; Allison R Jilbert
Journal: PLoS One Date: 2015-11-11 Impact factor: 3.240

11 in total

Review 10. Hepatitis D virus in 2021: virology, immunology and new treatment approaches for a difficult-to-treat disease.

Authors: Stephan Urban; Christoph Neumann-Haefelin; Pietro Lampertico
Journal: Gut Date: 2021-06-08 Impact factor: 23.059

Nucleic Acid Polymers Are Active against Hepatitis Delta Virus Infection In Vitro.

1. Analytical study of phosphorothioate analogues of oligodeoxynucleotides using high-performance liquid chromatography.

Review 2. Nucleic acid polymers: Broad spectrum antiviral activity, antiviral mechanisms and optimization for the treatment of hepatitis B and hepatitis D infection.

3. Phosphorothioate oligonucleotides inhibit human immunodeficiency virus type 1 fusion by blocking gp41 core formation.

4. Persistent hepatitis D virus mono-infection in humanized mice is efficiently converted by hepatitis B virus to a productive co-infection.

5. Pharmacokinetics, biodistribution, and stability of oligodeoxynucleotide phosphorothioates in mice.

6. Entry of hepatitis delta virus requires the conserved cysteine residues of the hepatitis B virus envelope protein antigenic loop and is blocked by inhibitors of thiol-disulfide exchange.

7. Amphipathic DNA polymers are candidate vaginal microbicides and block herpes simplex virus binding, entry and viral gene expression.

8. Role of glycosaminoglycans for binding and infection of hepatitis B virus.

9. Proteoglycans act as cellular hepatitis delta virus attachment receptors.

10. Therapeutic Antiviral Effect of the Nucleic Acid Polymer REP 2055 against Persistent Duck Hepatitis B Virus Infection.

Review 1. HBV/HDV Coinfection: A Challenge for Therapeutics.

Review 2. Hepatitis B Virus: Advances in Prevention, Diagnosis, and Therapy.

3. Hepatitis Delta Virus Alters the Autophagy Process To Promote Its Genome Replication.

4. Hepatitis D infection: from initial discovery to current investigational therapies.

Review 5. Novel Pegylated Interferon for the Treatment of Chronic Viral Hepatitis.

6. HDVdb: A Comprehensive Hepatitis D Virus Database.

7. Mechanism of action of hepatitis B virus S antigen transport-inhibiting oligonucleotide polymer, STOPS, molecules.

8. Editorial: In vitro mechanistic evaluation of nucleic acid polymers: A cautionary tale.

Review 9. Targeting the Host for New Therapeutic Perspectives in Hepatitis D.

Review 10. Hepatitis D virus in 2021: virology, immunology and new treatment approaches for a difficult-to-treat disease.