| Literature DB >> 30304672 |
Nadine Krüger1, Christian Sauder2, Sarah Hüttl3, Jan Papies4, Kathleen Voigt3, Georg Herrler5, Kornelia Hardes6, Torsten Steinmetzer6, Claes Örvell7, Jan Felix Drexler4, Christian Drosten4, Steven Rubin2, Marcel Alexander Müller4, Markus Hoffmann8.
Abstract
Bats harbor a plethora of viruses with an unknown zoonotic potential. In-depth functional characterization of such viruses is often hampered by a lack of virus isolates. The genome of a virus closely related to human mumps viruses (hMuV) was detected in African fruit bats, batMuV. Efforts to characterize batMuV were based on directed expression of the batMuV glycoproteins or use of recombinant chimeric hMuVs harboring batMuV glycoprotein. Although these studies provided initial insights into the functionality of batMuV glycoproteins, the host range, replication competence, immunomodulatory functions, virulence, and zoonotic potential of batMuV remained elusive. Here, we report the successful rescue of recombinant batMuV. BatMuV infects human cells, is largely resistant to the host interferon response, blocks interferon induction and TNF-α activation, and is neurotoxic in rats. Anti-hMuV antibodies efficiently neutralize batMuV. The striking similarities between hMuV and batMuV point at the putative zoonotic potential of batMuV.Entities:
Keywords: bat-derived viruses; immune evasion; mumps virus; reverse genetics; viral entry; zoonosis
Year: 2018 PMID: 30304672 DOI: 10.1016/j.celrep.2018.09.018
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423