The Development of Dual Vaccines against Lumpy Skin Disease (LSD) and Bovine Ephemeral Fever (BEF)

Douglass, Nicola; Omar, Ruzaiq; Munyanduki, Henry; Suzuki, Akiko; Moor, Warren de; Mutowembwa, Paidamwoyo; Pretorius, Ashley; Nefefe, Tshifhiwa; Schalkwyk, Antoinette van; Kara, Pravesh; Heath, Livio; Williamson, Anna‐Lise

doi:10.3390/vaccines9111215

Cited by 10 publications

(16 citation statements)

References 51 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The recombinant LSDV (LSDVGC5) was constructed using nLSDVSODis-UCT as a vector backbone [44]. For the construction of LSDVGC5, the green fluorescing LSDV(SODis)BEFV-Gb [48] was used as a parent virus so that the gene cassette between ORFs 49 and 50 could be replaced with a gene cassette, including the mCherry gene, which encodes a red fluorescing protein. A transfer vector was constructed in which the gene cassette-containing TPA-gp150-FL-IP under the control of the VACV mH5 promoter, gag M under the control of the pLEO promoter, and the fluorescent marker mCherry under the control of the modified fowl poxvirus promoter [49]-was placed in between flanking sequences from the LSDV 49-50 locus (Figure 1b) [50].…”

Section: Design and Construction Of Dna Mva And Lsdv Vaccines Expressing Env And Gagmentioning

confidence: 99%

Assessment of an LSDV-Vectored Vaccine for Heterologous Prime-Boost Immunizations against HIV

et al. 2021

Self Cite

View full text Add to dashboard Cite

The modest protective effects of the RV144 HIV-1 vaccine trial have prompted the further exploration of improved poxvirus vector systems that can yield better immune responses and protection. In this study, a recombinant lumpy skin disease virus (LSDV) expressing HIV-1 CAP256.SU gp150 (Env) and a subtype C mosaic Gag was constructed (LSDVGC5) and compared to the equivalent recombinant modified vaccinia Ankara (MVAGC5). In vitro characterization confirmed that cells infected with recombinant LSDV produced Gag virus-like particles containing Env, and that Env expressed on the surface of the cells infected with LSDV was in a native-like conformation. This candidate HIV-1 vaccine (L) was tested in a rabbit model using different heterologous vaccination regimens, in combination with DNA (D) and MVA (M) vectors expressing the equivalent HIV-1 antigens. The four different vaccination regimens (DDMMLL, DDMLML, DDLMLM, and DDLLMM) all elicited high titers of binding and Tier 1A neutralizing antibodies (NAbs), and some regimens induced Tier 1B NAbs. Furthermore, two rabbits in the DDLMLM group developed low levels of autologous Tier 2 NAbs. The humoral immune responses elicited against HIV-1 Env by the recombinant LSDVGC5 were comparable to those induced by MVAGC5.

show abstract

Section: Design and Construction Of Dna Mva And Lsdv Vaccines Expressing Env And Gagmentioning

confidence: 99%

Assessment of an LSDV-Vectored Vaccine for Heterologous Prime-Boost Immunizations against HIV

et al. 2021

Self Cite

View full text Add to dashboard Cite

show abstract

“…A putative non-essential gene encoding a G-protein-coupled chemokine receptor subfamily homologue has been tested as a site for homologous recombination [ 103 ]. The region between the convergent LSDV open reading frames (ORFs) 49 and 50 have also been used without gene disruption [ 20 , 104 , 105 ].…”

Section: Introductionmentioning

confidence: 99%

“…LSDV expressing bovine ephemeral fever virus (BEFV) proteins induced good BEFV and LSDV neutralising antibody responses in rabbits and cattle. The cattle were protected from LSDV challenge [ 104 ]. Despite the success of recombinant LSDV vaccines, there are still none that have been commercialized.…”

Section: Introductionmentioning

confidence: 99%

Lumpy Skin Disease—An Emerging Cattle Disease in Europe and Asia

2023

Self Cite

View full text Add to dashboard Cite

Lumpy skin disease virus (LSDV) is a member of the Capripoxvirus genus, mainly infecting cattle and buffalo, which until relatively recently was only endemic in parts of Africa and then spread to the Middle East and lately Europe and Asia. Lumpy skin disease (LSD) is a notifiable disease with a serious impact on the beef industry as it causes mortality of up to 10% and has impacts on milk and meat production, as well as fertility. The close serological relationship between LSDV, goat poxvirus (GTPV) and sheep poxvirus (SPPV) has led to live attenuated GTPV and SPPV vaccines being used to protect against LSD in some countries. There is evidence that the SPPV vaccine does not protect from LSD as well as the GTPV and LSDV vaccines. One of the LSD vaccines used in Eastern Europe was found to be a combination of different Capripoxviruses, and a series of recombination events in the manufacturing process resulted in cattle being vaccinated with a range of recombinant LSDVs resulting in virulent LSDV which spread throughout Asia. It is likely that LSD will become endemic throughout Asia as it will be very challenging to control the spread of the virus without widespread vaccination.

show abstract

“…However, understanding this requires an understanding of how superinfection is governed. In laboratory experiments, homologous recombination has been widely used to disrupt and/or insert genes of interest, to study the functions of specific genes, and to generate recombinant viral vectored vaccine candidates ( Wallace et al, 2020 ; Douglass et al, 2021 ). Poxviruses are suitable vaccine vectors due to their conserved large genomes, relative safety, and capacity to elicit an adequate immune response ( Pastoret and Vanderplasschen, 2003 ).…”

Section: Requirements For the Generation Of Recombinant Poxvirusesmentioning

confidence: 99%

“…Poxviruses are suitable vaccine vectors due to their conserved large genomes, relative safety, and capacity to elicit an adequate immune response ( Pastoret and Vanderplasschen, 2003 ). Examples of recombinant vaccines include the vaccinia rabies vaccine ( Pastoret and Brochier, 1996 ), LSDV based Rift Valley fever virus (RVFV) ( Wallace et al, 2020 ), bovine ephemeral fever (BEFV) ( Douglass et al, 2021 ) and even human immunodeficiency virus (HIV) ( Shen et al, 2011 ; Chapman et al, 2021 ). The procedures developed for the construction of recombinant vaccinia viruses have been applied to members of other poxvirus genera including avian poxviruses ( Boyle and Coupar, 1988 ) and capripoxviruses ( Romero et al, 1993 ).…”

Section: Requirements For the Generation Of Recombinant Poxvirusesmentioning

confidence: 99%

Capripoxviruses, leporipoxviruses, and orthopoxviruses: Occurrences of recombination

et al. 2022

View full text Add to dashboard Cite

Poxviruses are double-stranded DNA viruses with several members displaying restricted host ranges. They are genetically stable with low nucleotide mutation rates compared to other viruses, due to the poxviral high-fidelity DNA polymerase. Despite the low accumulation of mutations per replication cycle, poxvirus genomes can recombine with each other to generate genetically rearranged viruses through recombination, a process directly associated with replication and the aforementioned DNA polymerase. Orthopoxvirus replication is intimately tethered to high frequencies of homologous recombination between co-infecting viruses, duplicated sequences of the same virus, and plasmid DNA transfected into poxvirus-infected cells. Unfortunately, the effect of these genomic alterations on the cellular context for all poxviruses across the family Poxviridae remains elusive. However, emerging sequence data on currently circulating and archived poxviruses, such as the genera orthopoxviruses and capripoxviruses, display a wide degree of divergence. This genetic variability cannot be explained by clonality or genetic drift alone, but are probably a result of significant genomic alterations, such as homologous recombination, gene loss and gain, or gene duplications as the major selection forces acting on viral progeny. The objective of this review is to cross-sectionally overview the currently available findings on natural and laboratory observations of recombination in orthopoxviruses, capripoxviruses, and leporipoxviruses, as well as the possible mechanisms involved. Overall, the reviewed available evidence allows us to conclude that the current state of knowledge is limited in terms of the relevance of genetic variations across even a genus of poxviruses as well as fundamental features governing and precipitating intrinsic gene flow and recombination events.

show abstract

The Development of Dual Vaccines against Lumpy Skin Disease (LSD) and Bovine Ephemeral Fever (BEF)

Cited by 10 publications

References 51 publications

Assessment of an LSDV-Vectored Vaccine for Heterologous Prime-Boost Immunizations against HIV

Assessment of an LSDV-Vectored Vaccine for Heterologous Prime-Boost Immunizations against HIV

Lumpy Skin Disease—An Emerging Cattle Disease in Europe and Asia

Capripoxviruses, leporipoxviruses, and orthopoxviruses: Occurrences of recombination

Contact Info

Product

Resources

About