Literature DB >> 26658683

In vivo reduction of hepatitis B virus antigenemia and viremia by antisense oligonucleotides.

Gaetan Billioud1, Robert L Kruse2, Melissa Carrillo1, Christina Whitten-Bauer1, Dacao Gao3, Aneeza Kim3, Leon Chen2, Michael L McCaleb3, Jeffrey R Crosby3, Robert Hamatake4, Zhi Hong4, Urtzi Garaigorta1, Eric Swayze5, Karl-Dimiter Bissig6, Stefan Wieland7.   

Abstract

BACKGROUND & AIMS: Current treatment of chronic hepatitis B virus infection (CHB) includes interferon and nucleos(t)ide analogues, which generally do not reduce HBV surface antigen (HBsAg) production, a constellation that is associated with poor prognosis of CHB. Here we evaluated the efficacy of an antisense approach using antisense oligonucleotide (ASO) technology already in clinical use for liver targeted therapy to specifically inhibit HBsAg production and viremia in a preclinical setting.
METHODS: A lead ASO was identified and characterized in vitro and subsequently tested for efficacy in vivo and in vitro using HBV transgenic and hydrodynamic transfection mouse and a cell culture HBV infection model, respectively.
RESULTS: ASO treatment decreased serum HBsAg levels ⩾2 logs in a dose and time-dependent manner; HBsAg decreased 2 logs in a week and returned to baseline 4 weeks after a single ASO injection. ASO treatment effectively reduced HBsAg in combination with entecavir, while the nucleoside analogue alone did not. ASO treatment has pan-genotypic antiviral activity in the hydrodynamic transfection system. Finally, cccDNA-driven HBV gene expression is ASO sensitive in HBV infected cells in vitro.
CONCLUSION: Our results demonstrate in a preclinical setting the efficacy of an antisense approach against HBV by efficiently reducing serum HBsAg (as well as viremia) across different genotypes alone or in combination with standard nucleoside therapy. Since the applied antisense technology is already in clinical use, a lead compound can be rapidly validated in a clinical setting and thus, constitutes a novel therapeutic approach targeting chronic HBV infection.
Copyright © 2015 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

Entities:  

Keywords:  2′MOE antisense molecule; HBV Infection; HBV transgenic mice; Hydrodynamic transfection

Mesh:

Substances:

Year:  2015        PMID: 26658683     DOI: 10.1016/j.jhep.2015.11.032

Source DB:  PubMed          Journal:  J Hepatol        ISSN: 0168-8278            Impact factor:   25.083


  18 in total

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Authors:  Kazuto Tajiri; Yukihiro Shimizu
Journal:  World J Hepatol       Date:  2016-07-28

2.  Activity of nucleic acid polymers in rodent models of HBV infection.

Authors:  Katrin Schöneweis; Neil Motter; Pia L Roppert; Mengji Lu; Baoju Wang; Ingo Roehl; Dieter Glebe; Dongliang Yang; John D Morrey; Michael Roggendorf; Andrew Vaillant
Journal:  Antiviral Res       Date:  2017-11-08       Impact factor: 5.970

3.  HBsAg-redirected T cells exhibit antiviral activity in HBV-infected human liver chimeric mice.

Authors:  Robert L Kruse; Thomas Shum; Haruko Tashiro; Mercedes Barzi; Zhongzhen Yi; Christina Whitten-Bauer; Xavier Legras; Beatrice Bissig-Choisat; Urtzi Garaigorta; Stephen Gottschalk; Karl-Dimiter Bissig
Journal:  Cytotherapy       Date:  2018-04-06       Impact factor: 5.414

4.  Cre/LoxP-HBV plasmids generating recombinant covalently closed circular DNA genome upon transfection.

Authors:  Robert L Kruse; Xavier Legras; Mercedes Barzi
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Review 8.  Antisense antimicrobial therapeutics.

Authors:  Erin K Sully; Bruce L Geller
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Review 9.  New Viral and Immunological Targets for Hepatitis B Treatment and Cure: A Review.

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Journal:  Infect Dis Ther       Date:  2017-10-25

Review 10.  Upcoming pharmacological developments in chronic hepatitis B: can we glimpse a cure on the horizon?

Authors:  Sonia Alonso; Adriana-René Guerra; Lourdes Carreira; Juan-Ángel Ferrer; María-Luisa Gutiérrez; Conrado M Fernandez-Rodriguez
Journal:  BMC Gastroenterol       Date:  2017-12-21       Impact factor: 3.067

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