Current Progress in the Development of Hepatitis B Virus Capsid Assembly Modulators: Chemical Structure, Mode-of-Action and Efficacy.
Hyejin KimChunkyu KoJoo-Youn LeeMeehyein KimPublished in: Molecules (Basel, Switzerland) (2021)
Hepatitis B virus (HBV) is a major causative agent of human hepatitis. Its viral genome comprises partially double-stranded DNA, which is complexed with viral polymerase within an icosahedral capsid consisting of a dimeric core protein. Here, we describe the effects of capsid assembly modulators (CAMs) on the geometric or kinetic disruption of capsid construction and the virus life cycle. We highlight classical, early-generation CAMs such as heteroaryldihydropyrimidines, phenylpropenamides or sulfamoylbenzamides, and focus on the chemical structure and antiviral efficacy of recently identified non-classical CAMs, which consist of carboxamides, aryl ureas, bithiazoles, hydrazones, benzylpyridazinones, pyrimidines, quinolines, dyes, and antimicrobial compounds. We summarize the therapeutic efficacy of four representative classical compounds with data from clinical phase 1 studies in chronic HBV patients. Most of these compounds are in phase 2 trials, either as monotherapy or in combination with approved nucleos(t)ides drugs or other immunostimulatory molecules. As followers of the early CAMs, the therapeutic efficacy of several non-classical CAMs has been evaluated in humanized mouse models of HBV infection. It is expected that these next-generation HBV CAMs will be promising candidates for a series of extended human clinical trials.
Keyphrases
- hepatitis b virus
- endothelial cells
- liver failure
- clinical trial
- life cycle
- end stage renal disease
- small molecule
- sars cov
- newly diagnosed
- ejection fraction
- mouse model
- pluripotent stem cells
- staphylococcus aureus
- chronic kidney disease
- prognostic factors
- single molecule
- randomized controlled trial
- binding protein
- peritoneal dialysis
- cross sectional
- big data
- cell free
- amino acid
- case control
- phase ii
- circulating tumor cells
- drug induced
- data analysis
- monoclonal antibody