Literature DB >> 24043818

Bats carry pathogenic hepadnaviruses antigenically related to hepatitis B virus and capable of infecting human hepatocytes.

Jan Felix Drexler1, Andreas Geipel, Alexander König, Victor M Corman, Debby van Riel, Lonneke M Leijten, Corinna M Bremer, Andrea Rasche, Veronika M Cottontail, Gael D Maganga, Mathias Schlegel, Marcel A Müller, Alexander Adam, Stefan M Klose, Aroldo José Borges Carneiro, Andreas Stöcker, Carlos Roberto Franke, Florian Gloza-Rausch, Joachim Geyer, Augustina Annan, Yaw Adu-Sarkodie, Samuel Oppong, Tabea Binger, Peter Vallo, Marco Tschapka, Rainer G Ulrich, Wolfram H Gerlich, Eric Leroy, Thijs Kuiken, Dieter Glebe, Christian Drosten.   

Abstract

The hepatitis B virus (HBV), family Hepadnaviridae, is one of most relevant human pathogens. HBV origins are enigmatic, and no zoonotic reservoirs are known. Here, we screened 3,080 specimens from 54 bat species representing 11 bat families for hepadnaviral DNA. Ten specimens (0.3%) from Panama and Gabon yielded unique hepadnaviruses in coancestral relation to HBV. Full genome sequencing allowed classification as three putative orthohepadnavirus species based on genome lengths (3,149-3,377 nt), presence of middle HBV surface and X-protein genes, and sequence distance criteria. Hepatic tropism in bats was shown by quantitative PCR and in situ hybridization. Infected livers showed histopathologic changes compatible with hepatitis. Human hepatocytes transfected with all three bat viruses cross-reacted with sera against the HBV core protein, concordant with the phylogenetic relatedness of these hepadnaviruses and HBV. One virus from Uroderma bilobatum, the tent-making bat, cross-reacted with monoclonal antibodies against the HBV antigenicity determining S domain. Up to 18.4% of bat sera contained antibodies against bat hepadnaviruses. Infectious clones were generated to study all three viruses in detail. Hepatitis D virus particles pseudotyped with surface proteins of U. bilobatum HBV, but neither of the other two viruses could infect primary human and Tupaia belangeri hepatocytes. Hepatocyte infection occurred through the human HBV receptor sodium taurocholate cotransporting polypeptide but could not be neutralized by sera from vaccinated humans. Antihepadnaviral treatment using an approved reverse transcriptase inhibitor blocked replication of all bat hepadnaviruses. Our data suggest that bats may have been ancestral sources of primate hepadnaviruses. The observed zoonotic potential might affect concepts aimed at eradicating HBV.

Entities:  

Keywords:  evolution; metagenomics; reverse genetics; virome; zoonosis

Mesh:

Year:  2013        PMID: 24043818      PMCID: PMC3791787          DOI: 10.1073/pnas.1308049110

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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