Expression of VP7, a Bluetongue Virus Group Specific Antigen by Viral Vectors: Analysis of the Induced Immune Responses and Evaluation of Protective Potential in Sheep

Bouet-Cararo, Coraline; Contreras, Vanessa; Caruso, A.; Top, Sokunthea; Szelechowski, Marion; Bergeron, Corinne; Viarouge, Cyril; Desprat, Alexandra; Relmy, Anthony; Guibert, Jean-Michel; Dubois, Éric; Thiéry, Richard; Bréard, Emmanuel; Bertagnoli, Stéphane; Richardson, Jennifer; Foucras, Gilles; Meyer, Gilles; Schwartz-Cornil, Isabelle; Zientara, Stéphan; Klonjkowski, Bernard

doi:10.1371/journal.pone.0111605

Cited by 17 publications

(17 citation statements)

References 38 publications

(57 reference statements)

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“…Investigations into BTV VP7 have shown that VP7 has regions that are exposed on the virion surface and are able to act as epitopes, 65 and vectors presenting VP7 are capable to produce an immune response that is at least partially protective. 76 , 77 This, along with evidence that VP6, the middle layer protein in Rotavirus, which is also a member of the Reoviridae family, has shown to be involved in B-cell immunity which suggests that VP7 of the orbiviruses is a good candidate for B-cell activation as numerous papers point out the similarity of BTV VP7 and Rotavirus VP6. 78 , 79 , 80 In addition to this, in BTV, VP7 is seen to be a major group reactive antigen that has been seen to contain CD8 + and CD4 + T-cell epitopes that are conserved among different serotypes.…”

Section: Discussionmentioning

confidence: 99%

Analysis of Conserved, Computationally Predicted Epitope Regions for VP5 and VP7 Across three Orbiviruses

Russell

Parbhoo

Gildenhuys

2018

Bioinform Biol Insights

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Orbiviruses are double-stranded RNA viruses that have profound economic and veterinary significance, 3 of the most important being African horse sickness virus (AHSV), bluetongue virus (BTV), and epizootic hemorrhagic disease virus (EHDV). Currently, vaccination and vector control are used as preventative measures; however, there are several problems with the current vaccines. Comparing viral amino acid sequences, we obtained an AHSV-BTV-EHDV consensus sequence for VP5 (viral protein 5) and for VP7 (viral protein 7) and generated homology models for these proteins. The structures and sequences were analyzed for amino acid sequence conservation, entropy, surface accessibility, and epitope propensity, to computationally determine whether consensus sequences still possess potential epitope regions. In total, 5 potential linear epitope regions on VP5 and 11 on VP7, as well as potential discontinuous B-cell epitopes, were identified and mapped onto the homology models created. Regions identified for VP5 and VP7 could be important in vaccine design against orbiviruses.

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Section: Discussionmentioning

confidence: 99%

Analysis of Conserved, Computationally Predicted Epitope Regions for VP5 and VP7 Across three Orbiviruses

Russell

Parbhoo

Gildenhuys

2018

Bioinform Biol Insights

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“…Among BTV proteins, VP7 is a major BTV group reactive antigen that contains CD8 + and CD4 + T cell epitopes [ 27 , 28 ] that are conserved among different serotypes. Vaccination with recombinant capripox virus encoding VP7 [ 27 ] and recombinant canine adenovirus type 2 expressing VP7 [ 29 ] showed clinical protection against heterologous challenge, although the virus still replicated. In general, BTV NS proteins have mostly been associated with cellular immune responses [ 15 , 16 , 30 ].…”

Section: Introductionmentioning

confidence: 99%

Protective Efficacy in Sheep of Adenovirus-Vectored Vaccines against Bluetongue Virus Is Associated with Specific T Cell Responses

et al. 2015

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Bluetongue virus (BTV) is an economically important Orbivirus of the Reoviridae family that causes a hemorrhagic disease in ruminants. Its control has been achieved by inactivated-vaccines that have proven to protect against homologous BTV challenge although unable to induce long-term immunity. Therefore, a more efficient control strategy needs to be developed. Recombinant adenovirus vectors are lead vaccine candidates for protection of several diseases, mainly because of their potency to induce potent T cell immunity. Here we report the induction of humoral and T-cell mediated responses able to protect animals against BTV challenge by recombinant replication-defective human adenovirus serotype 5 (Ad5) expressing either VP7, VP2 or NS3 BTV proteins. First we used the IFNAR(-/-) mouse model system to establish a proof of principle, and afterwards we assayed the protective efficacy in sheep, the natural host of BTV. Mice were completely protected against BTV challenge, developing humoral and BTV-specific CD8+- and CD4+-T cell responses by vaccination with the different rAd5. Sheep vaccinated with Ad5-BTV-VP2 and Ad5-BTV-VP7 or only with Ad5-BTV-VP7 and challenged with BTV showed mild disease symptoms and reduced viremia. This partial protection was achieved in the absence of neutralizing antibodies but strong BTV-specific CD8+ T cell responses in those sheep vaccinated with Ad5-BTV-VP7. These data indicate that rAd5 is a suitable vaccine vector to induce T cell immunity during BTV vaccination and provide new data regarding the relevance of T cell responses in protection during BTV infection.

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“…Sheep vaccinated with Ad5-BTV-VP7 elicited sufficient BTV-specific CD8+ T cell response but no neutralizing antibodies response. In other study, the VP7 core protein of BTV2 was expressed either in a non-replicative canine adenovirus type 2 (Cav-VP7 R 0 ) or a leporipoxvirus (SG33-VP7) to elicit immune response in sheep (Bouet-Cararo et al, 2014). Both of the recombinant antigens elicited the humoral immune response in sheep.…”

Section: Adenovirusmentioning

confidence: 99%

“…Later on, Cav-VP7 R 0 vaccine-immunized sheep were challenged with either homologous serotype BTV2 or the heterologous BTV8. The viremia estimation by real-time PCR in plasma showed that the immune response triggered by Cav-VP7 R 0 was insufficient to provide protective immunity against BTV (Bouet-Cararo et al, 2014). It only generated partial protection against homologous serotype.…”

Section: Adenovirusmentioning

confidence: 99%

Bluetongue virus vaccine: conventional to modern approach

Ranjan¹,

Prasad²,

Brar³

et al. 2019

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Bluetongue (BT) is an economically important, infectious and non-contagious disease of ruminant animals. BT disease is caused by bluetongue virus (BTV) of the genus Orbivirus (the family Reoviridae). BTV is transmitted by certain species of biting midges of the genus Culicoides. Although originally BT was restricted to African continent, now it is present in all the continents except Antarctica. Conventional BT vaccines such as live attenuated and inactivated vaccines showed different degree of success in BT control. However, conventional vaccines have certain disadvantages of reversion to virulent strain and frequent booster dose requirement. Several BT outbreaks in India and the rest of the world open a new insight for development of better vaccines. The development in molecular biology techniques allowed the development and validation of several modern vaccines such as subunit vaccine, recombinant vector vaccine, disabled infections single cycle (DISC) vaccine, differentiating infected from vaccinated animals (DIVA) approach etc. Most of these vaccines are considered as safer, having better protective immune response and provided cross-protective immunization against more than one serotype.

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Expression of VP7, a Bluetongue Virus Group Specific Antigen by Viral Vectors: Analysis of the Induced Immune Responses and Evaluation of Protective Potential in Sheep

Cited by 17 publications

References 38 publications

Analysis of Conserved, Computationally Predicted Epitope Regions for VP5 and VP7 Across three Orbiviruses

Analysis of Conserved, Computationally Predicted Epitope Regions for VP5 and VP7 Across three Orbiviruses

Protective Efficacy in Sheep of Adenovirus-Vectored Vaccines against Bluetongue Virus Is Associated with Specific T Cell Responses

Bluetongue virus vaccine: conventional to modern approach

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