Impact of Genetic Heterogeneity in Polymerase of Hepatitis B Virus on Dynamics of Viral Load and Hepatitis B Progression
Journal
PLoS ONE
Journal Volume
8
Journal Issue
7
Pages
e70169
Date Issued
2013
Author(s)
Abstract
Objective:The hepatitis B virus (HBV)-polymerase region overlaps pre-S/S genes with high epitope density and plays an essential role in viral replication. We investigated whether genetic variation in the polymerase region determined long-term dynamics of viral load and the risk of hepatitis B progression in a population-based cohort study.Methods:We sequenced the HBV-polymerase region using baseline plasma from treatment-na?ve individuals with HBV-DNA levels?1000 copies/mL in a longitudinal viral-load study of participants with chronic HBV infection followed-up for 17 years, and obtained sequences from 575 participants (80% with HBV genotype Ba and 17% with Ce).Results:Patterns of viral sequence diversity across phases (i.e., immune-tolerant, immune-clearance, non/low replicative, and hepatitis B e antigen (HBeAg)-negative hepatitis phases) of HBV-infection, which were associated with viral and clinical features at baseline and during follow-up, were similar between HBV genotypes, despite greater diversity for genotype Ce vs. Ba. Irrespective of genotypes, however, HBeAg-negative participants had 1.5-to-2-fold higher levels of sequence diversity than HBeAg-positive participants (P<0.0001). Furthermore, levels of viral genetic divergence from the population consensus sequence, estimated by numbers of nucleotide substitutions, were inversely associated with long-term viral load even in HBeAg-negative participants. A mixed model developed through analysis of the entire HBV-polymerase region identified 153 viral load-associated single nucleotide polymorphisms in overall and 136 in HBeAg-negative participants, with distinct profiles between HBV genotypes. These polymorphisms were most evident at sites within or flanking T-cell epitopes. Seven polymorphisms revealed associations with both enhanced viral load and a more than 4-fold increased risk of hepatocellular carcinoma and/or liver cirrhosis.Conclusions:The data highlight a role of viral genetic divergence in the natural course of HBV-infection. Interindividual differences in the long-term dynamics of viral load is not only associated with accumulation of mutations in HBV-polymerase region, but differences in specific viral polymorphisms which differ between genotypes. ? 2013 Huang et al.
SDGs
Other Subjects
epitope; hepatitis B virus polymerase; hepatitis B(e) antigen; unclassified drug; virus DNA; virus enzyme; adult; aged; article; cancer risk; clinical feature; cohort analysis; disease association; disease course; follow up; gene sequence; genetic association; genetic polymorphism; genetic risk; genetic variability; genotype; hepatitis B; Hepatitis B virus; human; immunological tolerance; liver cell carcinoma; liver cirrhosis; major clinical study; nucleic acid base substitution; nucleotide sequence; population research; single nucleotide polymorphism; T lymphocyte; unindexed sequence; viral clearance; virus genome; virus load; virus mutation; virus replication; Adult; Carcinoma, Hepatocellular; Disease Progression; Genes, Viral; Genetic Heterogeneity; Genotype; Hepatitis B virus; Hepatitis B, Chronic; Humans; Liver Cirrhosis; Middle Aged; Mutation; Polymorphism, Single Nucleotide; Viral Load; Virulence
Type
journal article