Abstract
Sudan virus (SUDV) and Ebola viruses (EBOV) are both members of the Ebolavirus genus and have been sources of epidemics and outbreaks for several decades. We present here the generation and characterization of cross-reactive antibodies to both SUDV and EBOV, which were produced in a cell-free system and protective against SUDV in mice. A non-human primate, cynomolgus macaque, was immunized with viral-replicon particles expressing the glycoprotein of SUDV-Boniface (8A). Two separate antibody fragment phage display libraries were constructed after four immunogen injections. Both libraries were screened first against the SUDV and a second library was cross-selected against EBOV-Kikwit. Sequencing of 288 selected clones from the two distinct libraries identified 58 clones with distinct VH and VL sequences. Many of these clones were cross-reactive to EBOV and SUDV and able to neutralize SUDV. Three of these recombinant antibodies (X10B1, X10F3, and X10H2) were produced in the scFv-Fc format utilizing a cell-free production system. Mice that were challenged with SUDV-Boniface receiving 100µg of the X10B1/X10H2 scFv-Fc combination 6 and 48-h post-exposure demonstrated partial protection individually and complete protection as a combination. The data herein suggests these antibodies may be promising candidates for further therapeutic development.
Highlights
Sudan virus (SUDV) along with the other four members of the Ebolavirus genus, with Marburgvirus and Cuevavirus, constitutes the family Filoviridae of the order Mononegavirales
We have recently presented the development of macaque derived antibodies to Marburg virus (MARV) utilizing a similar method [15]
Previous studies studies have have demonstrated demonstrated that that post-exposure post-exposure polyclonal polyclonal antibodies antibodies as as well well as as Previous recombinantmonoclonal monoclonalantibodies antibodiesprovide provideprotection protectionagainst againstfiloviruses filovirusesininNHP
Summary
Sudan virus (SUDV) along with the other four members of the Ebolavirus genus, with Marburgvirus and Cuevavirus, constitutes the family Filoviridae of the order Mononegavirales. SUDV causes severe and highly lethal viral hemorrhagic fevers (VHF) in both non-human primates (NHP) and humans [1]. This class of viruses have the capacity to elicit devastating impact on global health, as was made evident by Ebola virus (EBOV) in the 2014–2016 West Africa outbreak. Viruses 2018, 10, 286 of SUDV is through contact with infected bodily fluids from infected humans or animals. SUDV was first identified in an outbreak in South Sudan in 1976 and continues to cause sporadic outbreaks throughout equatorial Africa [2].
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
