Molecular characteristics of hepatitis B virus among students and pregnant women in Chad
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BMC Infectious Diseases
Abstract
Background Hepatitis B virus (HBV) infection remains a global public health problem claiming about 1, 1 million
lives among the several hundred million people infected with the virus globally. However, low- and middle-income
countries including those in sub-Saharan Africa carry the highest burden but limited knowledge of the pathogen.
This calls for studies to characterise the circulating genotypes of the virus in Sub-Saharan Africa. This study, sought
to determine the molecular characteristics of HBV circulating among pregnant women and students in Chad.
Methods Venous blood samples were collected from pregnant women and students in the capital of Chad between April
and August 2021. Whole blood samples were spun at 2500xg at 4 °C for 10 min to separate the cellular parts from the sera.
The resulting sera were tested for Hepatitis B surface antigen (HBsAg) using enzyme-linked immunosorbent assay (ELISA).
HBsAg positivity was confrmed using the Abbott Architect i1000SR analyser. HBV-DNA viral load detection was performed
for HBsAg positive sera. HBV-DNA viral load was determined in HBsAg positive sera samples. The S gene was amplifed
by nested PCR followed by visualisation of the resulting amplicons under UV transillumination after gel electrophoresis. The
amplicons were sequenced using the Sanger technique and subjected to phylogenetic and mutational analyses.
Results A total of 101 HBsAg-positive participants (recruited among students and pregnant women) were included
in the study. The mean age was 25 years and 51.49% were males. Viral load was measured in 53 participants,
among whom 27 (50.94%) had a viremia higher than 2000 IU/ml. The constructed phylogeny using 31 samples based
of the HBV S gene showed that all strains belonged to the E genotype and evolutionary related to HBV from Cam eroon, Central African Republic, Burkina Faso, Sudan and Ghana. The comparative mutational analysis identifed low
intragroup genetic diversity (0.004%) between Chadian strains with only two loci (codon positions 126 and 141) hav ing nonsynonymous mutations including (Y126H, Y126N, Y126C, L140I, Y141S, Y141R, Y141H, Y141F).
Conclusions The study shows the presence and circulation of HBV genotype E in Chad. The Chadian strains, compared
to other genotype E strains from surrounding countries have very low genetic variability. The presence of immune escape
mutations in the HBV S gene could be responsible for escape vaccine strains and thus reduce the efcacy of vaccination.
Additionally, the presence of the transmembrane domain in the HBV S gene could alter the antigenicity of HBsAg, con tributing to screening failure by standard tests (HBsAg negative despite active infection) or reduce the efcacy of drugs
that target HBsAg. These results highlight the need to evaluate hepatitis B vaccination coverage and efciency in Chad.
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Research Article
