Synthetic RNAi triggers and their use in chronic hepatitis B therapies with curative intent

Robert G Gish; Man-Fung Yuen; Henry Lik Yuen Chan; Bruce D Given; Ching-Lung Lai; Stephen A Locarnini; Johnson Y N Lau; Christine I Wooddell; Thomas Schluep; David L Lewis

doi:10.1016/j.antiviral.2015.06.019

Synthetic RNAi triggers and their use in chronic hepatitis B therapies with curative intent

Antiviral Res. 2015 Sep:121:97-108. doi: 10.1016/j.antiviral.2015.06.019. Epub 2015 Jun 27.

Authors

Affiliations

¹ Department of Medicine, Division of Gastroenterology and Hepatology, Stanford University, Stanford, CA, USA; Hepatitis B Foundation, Doylestown, PA, USA. Electronic address: rgish@robertgish.com.
² The University of Hong Kong, Hong Kong, China.
³ The Chinese University of Hong Kong, Hong Kong, China.
⁴ Arrowhead Research Corporation, Pasadena, CA, USA.
⁵ Victorian Infectious Diseases Reference Laboratory, Victoria, Australia.
⁶ Hong Kong Polytechnic University, Hong Kong, China.

PMID: 26129970
DOI: 10.1016/j.antiviral.2015.06.019

Abstract

Current therapies for chronic hepatitis B virus infection (CHB) - nucleos(t)ide analogue reverse transcriptase inhibitors and interferons - result in low rates of functional cure defined as sustained off-therapy seroclearance of hepatitis B surface antigen (HBsAg). One likely reason is the inability of these therapies to consistently and substantially reduce the levels of viral antigen production. Accumulated evidence suggests that high serum levels of HBsAg result in exhaustion of the host immune system, rendering it unable to mount the effective antiviral response required for HBsAg clearance. New mechanistic approaches are required to produce high rates of HBsAg seroclearance in order to greatly reduce off-treatment disease progression. Already shown to be a clinically viable means of reducing gene expression in a number of other diseases, therapies based on RNA interference (RNAi) can directly target hepatitis B virus transcripts with high specificity, profoundly reducing the production of viral proteins. The fact that the viral RNA transcripts contain overlapping sequences means that a single RNAi trigger can result in the degradation of all viral transcripts, including all messenger RNAs and pregenomic RNA. Advances in the design of RNAi triggers have increased resistance to degradation and reduced nonspecific innate immune stimulation. Additionally, new methods to effectively deliver the trigger to liver hepatocytes, and specifically to the cytoplasmic compartment, have resulted in increased efficacy and tolerability. An RNAi-based drug currently in clinical trials is ARC-520, a dynamic polyconjugate in which the RNAi trigger is conjugated to cholesterol, which is coinjected with a hepatocyte-targeted, membrane-active peptide. Phase 2a clinical trial results indicate that ARC-520 was well tolerated and resulted in significant, dose-dependent reduction in HBsAg for up to 57days in CHB patients. RNAi-based therapies may play an important role in future therapeutic regimes aimed at improving HBsAg seroclearance and eliminating the need for lifelong therapy. This paper forms part of a symposium in Antiviral Research on "An unfinished story: from the discovery of the Australia antigen to the development of new curative therapies for hepatitis B."

Keywords: Antigenemia; Antiviral therapy; Hepatitis B virus; RNAi; T-cell exhaustion.

Publication types

Review

MeSH terms

Biological Products / adverse effects
Biological Products / therapeutic use*
Biological Therapy / methods*
Clinical Trials, Phase II as Topic
Hepatitis B, Chronic / drug therapy*
Humans
RNA Interference*
RNA, Small Interfering / adverse effects
RNA, Small Interfering / therapeutic use*
Treatment Outcome

Substances

Biological Products
RNA, Small Interfering