Bimodal distribution and set point HBV DNA viral loads in chronic infection: retrospective analysis of cohorts from the UK and South Africa

Author:

Downs Louise O.ORCID,Vawda Sabeehah,Bester Phillip Armand,Lythgoe Katrina A.,Wang TingyanORCID,McNaughton Anna L.ORCID,Smith David A.,Maponga Tongai,Freeman Oliver,Várnai Kinga A.ORCID,Davies Jim,Woods KerrieORCID,Fraser Christophe,Barnes Eleanor,Goedhals Dominique,Matthews Philippa C.ORCID

Abstract

Hepatitis B virus (HBV) viral load (VL) is used as a biomarker to assess risk of disease progression, and to determine eligibility for treatment. While there is a well recognised association between VL and the expression of the viral e-antigen protein, the distributions of VL at a population level are not well described. We here present cross-sectional, observational HBV VL data from two large population cohorts in the UK and in South Africa, demonstrating a consistent bimodal distribution. The right skewed distribution and low median viral loads are different from the left-skew and higher viraemia in seen in HIV and hepatitis C virus (HCV) cohorts in the same settings. Using longitudinal data, we present evidence for a stable ‘set-point’ VL in peripheral blood during chronic HBV infection. These results are important to underpin improved understanding of HBV biology, to inform approaches to viral sequencing, and to plan public health interventions.

Funder

Royal Society

National Institute for Health Research

Wellcome Trust

Publisher

F1000 Research Ltd

Subject

General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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