Integrated hepatitis B virus DNA maintains surface antigen production during antiviral treatment
Tanner Grudda, Hyon S. Hwang, Maraake Taddese, Jeffrey Quinn, Mark S. Sulkowski, Richard K. Sterling, Ashwin Balagopal, Chloe L. Thio
Tanner Grudda, Hyon S. Hwang, Maraake Taddese, Jeffrey Quinn, Mark S. Sulkowski, Richard K. Sterling, Ashwin Balagopal, Chloe L. Thio
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Research Article Infectious disease Virology

Integrated hepatitis B virus DNA maintains surface antigen production during antiviral treatment

Abstract

The focus of hepatitis B functional cure, defined as sustained loss of hepatitis B virus (HBV) surface antigen (HBsAg) and HBV DNA from blood, is on eliminating or silencing the intranuclear template for HBV replication, covalently closed circular DNA (cccDNA). However, HBsAg also derives from HBV DNA integrated into the host genome (iDNA). Little is known about the contribution of iDNA to circulating HBsAg with current therapeutics. We applied a multiplex droplet digital PCR assay to demonstrate that iDNA is responsible for maintaining HBsAg quantities in some individuals. Using paired bulk liver tissue from 16 HIV/HBV-coinfected persons on nucleos(t)ide analog (NUC) therapy, we demonstrate that people with larger HBsAg declines between biopsies derive HBsAg from cccDNA, whereas people with stable HBsAg levels derive predominantly from iDNA. We applied our assay to individual hepatocytes in paired tissues from 3 people and demonstrated that the individual with significant HBsAg decline had a commensurate loss of infected cells with transcriptionally active cccDNA, while individuals without HBsAg decline had stable or increasing numbers of cells producing HBsAg from iDNA. We demonstrate that while NUC therapy may be effective at controlling cccDNA replication and transcription, innovative treatments are required to address iDNA transcription that sustains HBsAg production.

Authors

Tanner Grudda, Hyon S. Hwang, Maraake Taddese, Jeffrey Quinn, Mark S. Sulkowski, Richard K. Sterling, Ashwin Balagopal, Chloe L. Thio

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Figure 3

HBV transcriptional activity and serum HBsAg levels.

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HBV transcriptional activity and serum HBsAg levels. Total HBV transcrip...
Total HBV transcriptional activity in liver was measured by the mid-HBV assay that targets all HBV transcripts (except low-abundance 0.7 kb transcripts) and is located in the middle of the S ORF. Quantities were adjusted for the number of cells in each sample using ERV-3 quantities. HBV transcriptional activity in liver was correlated with contemporaneous serum HBsAg levels. Each data point represents 1 person at each biopsy (n = 32) and the black trendline was calculated using simple linear regression, while the shaded region depicts the 95% confidence intervals along the trendline. Black symbols depict the 4 individuals with >log10 0.5 IU/mL declines in serum HBsAg at biopsy 1 with lines drawn to biopsy 2 for each person. Spearman’s correlation coefficient is shown with its P value and the shape of symbols (circles or triangles) corresponds to HBeAg status at the time of biopsy, as indicated in the legend.