Targeting the multifunctional HBV core protein as a potential cure for chronic hepatitis B

Usha Viswanathan; Nagraj Mani; Zhanying Hu; Haiqun Ban; Yanming Du; Jin Hu; Jinhong Chang; Ju-Tao Guo

doi:10.1016/j.antiviral.2020.104917

Targeting the multifunctional HBV core protein as a potential cure for chronic hepatitis B

Antiviral Res. 2020 Oct:182:104917. doi: 10.1016/j.antiviral.2020.104917. Epub 2020 Aug 17.

Authors

Usha Viswanathan¹, Nagraj Mani², Zhanying Hu¹, Haiqun Ban¹, Yanming Du¹, Jin Hu¹, Jinhong Chang¹, Ju-Tao Guo³

Affiliations

¹ Baruch S. Blumberg Institute, 3805 Old Easton Road, Doylestown, PA, 18902, USA.
² Arbutus Biopharma Inc., 701 Veterans Circle, Warminster, PA, 18974, USA.
³ Baruch S. Blumberg Institute, 3805 Old Easton Road, Doylestown, PA, 18902, USA. Electronic address: ju-tao.guo@bblumberg.org.

Abstract

The core (capsid) protein of hepatitis B virus (HBV) is the building block of nucleocapsids where viral DNA reverse transcriptional replication takes place and mediates virus-host cell interaction important for the persistence of HBV infection. The pleiotropic role of core protein (Cp) in HBV replication makes it an attractive target for antiviral therapies of chronic hepatitis B, a disease that affects more than 257 million people worldwide without a cure. Recent clinical studies indicate that core protein allosteric modulators (CpAMs) have a great promise as a key component of hepatitis B curative therapies. Particularly, it has been demonstrated that modulation of Cp dimer-dimer interactions by several chemical series of CpAMs not only inhibit nucleocapsid assembly and viral DNA replication, but also induce the disassembly of double-stranded DNA-containing nucleocapsids to prevent the synthesis of cccDNA. Moreover, the different chemotypes of CpAMs modulate Cp assembly by interaction with distinct amino acid residues at the HAP pocket between Cp dimer-dimer interfaces, which results in the assembly of Cp dimers into either non-capsid Cp polymers (type I CpAMs) or empty capsids with distinct physical property (type II CpAMs). The different CpAMs also differentially modulate Cp metabolism and subcellular distribution, which may impact cccDNA metabolism and host antiviral immune responses, the critical factors for the cure of chronic HBV infection. This review article highlights the recent research progress on the structure and function of core protein in HBV replication cycle, the mode of action of CpAMs, as well as the current status and perspectives on the discovery and development of core protein-targeting antivirals. This article forms part of a symposium in Antiviral Research on "Wide-ranging immune and direct-acting antiviral approaches to curing HBV and HDV infections."

Keywords: Capsid; Core protein allosteric modulators; Hepatitis B virus; Nucleocapsid; cccDNA.

Publication types

Research Support, N.I.H., Extramural
Research Support, U.S. Gov't, Non-P.H.S.
Review

MeSH terms

Animals
Antiviral Agents / therapeutic use
DNA Replication / drug effects
DNA, Viral
Hep G2 Cells
Hepatitis B Core Antigens*
Hepatitis B virus / drug effects*
Hepatitis B, Chronic / drug therapy*
Humans
Mice
Nucleocapsid / drug effects
Viral Core Proteins / antagonists & inhibitors*
Virus Replication / drug effects

Substances

Antiviral Agents
DNA, Viral
Hepatitis B Core Antigens
Viral Core Proteins

Grants and funding

R01 AI113267/AI/NIAID NIH HHS/United States