Artículo de revista
Replication of a chronic hepatitis B virus genotype F1b construct
Fecha
2016Registro en:
Arch Virol (2016) 161:583–594
DOI 10.1007/s00705-015-2702-x
Autor
Hernández, Sergio
Jiménez, Gustavo
Alarcón, Valentina
Prieto, Cristian
Muñoz, Francisca
Riquelme, Constanza
Venegas Santos, Mauricio
Brahm Barril, Javier
Loyola, Alejandra
Villanueva, Rodrigo A.
Institución
Resumen
Genotype F is one of the less-studied genotypes
of human hepatitis B virus, although it is widely distributed
in regions of Central and South American. Our previous
studies have shown that HBV genotype F is prevalent in
Chile, and phylogenetic analysis of its full-length sequence
amplified from the sera of chronically infected patients
identified it as HBV subgenotype F1b. We have previously
reported the full-length sequence of a HBV molecular
clone obtained from a patient chronically infected with
genotype F1b. In this report, we established a system to
study HBV replication based on hepatoma cell lines
transfected with full-length monomers of the HBV genome.
Culture supernatants were analyzed after transfection
and found to contain both HBsAg and HBeAg viral antigens.
Consistently, fractionated cell extracts revealed the
presence of viral replication, with both cytoplasmic and
nuclear DNA intermediates. Analysis of HBV-transfected
cells by indirect immunofluorescence or immunoelectron
microscopy revealed the expression of viral antigens and
cytoplasmic viral particles, respectively. To test the functionality
of the ongoing viral replication further at the level
of chromatinized cccDNA, transfected cells were treated
with a histone deacetylase inhibitor, and this resulted in
increased viral replication. This correlated with changes
posttranslational modifications of histones at viral promoters.
Thus, the development of this viral replication
system for HBV genotype F will facilitate studies on the
regulation of viral replication and the identification of new
antiviral drugs.