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Pregenomic RNA Launch Hepatitis B Virus Replication System Facilitates the Mechanistic Study of Antiviral Agents and Drug-Resistant Variants on Covalently Closed Circular DNA Synthesis

Qiong Zhao, Jinhong Chang, René Rijnbrand, Angela M. Lam, Michael J. Sofia, Andrea Cuconati, Ju‐Tao Guo

2022Journal of Virology22 citationsDOIOpen Access PDF

Abstract

Hepadnaviral pgRNA not only serves as a template for reverse transcriptional replication of viral DNA but also expresses core protein and DNA polymerase to support viral genome replication and cccDNA synthesis. Not surprisingly, cytoplasmic expression of duck hepatitis B virus pgRNA initiated viral replication leading to infectious virion secretion. However, HBV replication and antiviral mechanism were studied primarily in human hepatoma cells transiently or stably transfected with plasmid-based HBV replicons. The presence of large amounts of transfected HBV DNA or transgenes in cellular chromosomes hampered the robust analyses of HBV replication and cccDNA function. As demonstrated here, the pgRNA launch HBV replication system permits the accurate mapping of antiviral target and investigation of cccDNA biosynthesis and transcription using secreted HBsAg as a convenient quantitative marker. The effect of drug-resistant variants on viral capsid assembly, genome replication, and cccDNA biosynthesis and function can also be assessed using this system.

Topics & Concepts

BiologyCircular DNAVirologyViral replicationDNARNAHepatitis B virusReplication (statistics)Antiviral drugVirusGeneticsGeneGenomeHepatitis B Virus StudiesHepatitis C virus researchBacteriophages and microbial interactions