Pathogenicity and immunogenicity of recombinant rabies viruses expressing the Lagos bat virus matrix and glycoprotein : perspectives for a pan-lyssavirus vaccine

dc.contributor.authorKgaladi, Joe
dc.contributor.authorFaber, Milosz
dc.contributor.authorDietzschold, Bernhard
dc.contributor.authorNel, Louis Hendrik
dc.contributor.authorMarkotter, Wanda
dc.contributor.emailwanda.markotter@up.ac.zaen_ZA
dc.date.accessioned2018-05-14T08:58:18Z
dc.date.available2018-05-14T08:58:18Z
dc.date.issued2017-08-09
dc.description.abstractLagos bat virus (LBV) is a phylogroup II lyssavirus exclusively found in Africa. Previous studies indicated that this virus is lethal to mice after intracranial and intramuscular inoculation. The antigenic composition of LBV differs substantially from that of rabies virus (RABV) and current rabies vaccines do not provide cross protection against phylogroup II lyssaviruses. To investigate the potential role of the LBV matrix protein (M) and glycoprotein (G) in pathogenesis, reverse genetics technology was used to construct recombinant viruses. The genes encoding the glycoprotein, or the matrix and glycoprotein of the attenuated RABV strain SPBN, were replaced with those of LBV resulting in SPBN-LBVG and SPBN-LBVM-LBVG, respectively. To evaluate the immunogenicity of the LBV G, the recombinant RABV SPBNGAS-LBVG-GAS was constructed with the LBV G inserted between two mutated RABV G genes (termed GAS). All the recombinant viruses were lethal to mice after intracranial (i.c.) inoculation although the pathogenicity of SPBNGAS-LBVG-GAS was lower compared to the other recombinant viruses. Following intramuscular (i.m.) inoculation, only SPBN-LBVM-LBVG was lethal to mice, indicating that both the M and G of LBV play a role in the pathogenesis. Most interestingly, serum collected from mice that were inoculated i.m. with SPBNGAS-LBVG-GAS neutralized phylogroup I and II lyssaviruses including RABV, Duvenhage virus (DUVV), LBV, and Mokola virus (MOKV), indicating that this recombinant virus has potential to be developed as a pan-lyssavirus vaccine.en_ZA
dc.description.departmentMedical Virologyen_ZA
dc.description.departmentMicrobiology and Plant Pathologyen_ZA
dc.description.librarianam2018en_ZA
dc.description.sponsorshipThe National Institutes of Health grant ROIAI093666 (to M.F.), National Research Foundation, South Africa (UID 85786) and International Foundation for Science. J. Kgaladi’s PhD studies were supported by a freestanding bursary from the National Research Foundation, South Africa, the Poliomyelitis Research Foundation and the University of Pretoria study abroad bursary program.en_ZA
dc.description.urihttp://www.mdpi.com/journal/tropicalmeden_ZA
dc.identifier.citationKgaladi, J., Faber, M., Dietzschold, B. et al. 2017, 'Pathogenicity and immunogenicity of recombinant rabies viruses expressing the Lagos bat virus matrix and glycoprotein : perspectives for a pan-lyssavirus vaccine', Tropical Medicine and Infectious Disease, vol. 2, no. 37, pp. 1-5.en_ZA
dc.identifier.issn2414-6366 (online)
dc.identifier.other10.3390/tropicalmed2030037
dc.identifier.urihttp://hdl.handle.net/2263/64936
dc.language.isoenen_ZA
dc.publisherMDPI Publishingen_ZA
dc.rights© 2017 by the authors; licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/4.0/).en_ZA
dc.subjectVaccinesen_ZA
dc.subjectAfricaen_ZA
dc.subjectLyssavirusen_ZA
dc.subjectPathogenesisen_ZA
dc.subjectRecombinant virusesen_ZA
dc.subjectLagos bat virus (LBV)en_ZA
dc.subjectRabies virus (RABV)en_ZA
dc.titlePathogenicity and immunogenicity of recombinant rabies viruses expressing the Lagos bat virus matrix and glycoprotein : perspectives for a pan-lyssavirus vaccineen_ZA
dc.typeArticleen_ZA

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