A DNA-Modified Live Vaccine Prime–Boost Strategy Broadens the T-Cell Response and Enhances the Antibody Response against the Porcine Reproductive and Respiratory Syndrome Virus

Bernelin-Cottet, Cindy; Urien, Céline; Stubsrud, Elisabeth; Jakob, Virginie; Bouguyon, Edwige; Bordet, Elise; Barc, Céline; Boulesteix, Olivier; Contreras, Vanessa; Barnier-Quer, Christophe; Collin, Nicolas; Trus, Ivan; Nauwynck, Hans; Bertho, Nicolas; Schwartz-Cornil, Isabelle

doi:10.3390/v11060551

Cited by 10 publications

(18 citation statements)

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“…We showed in ref. [9] that an improvement of the T-cell response breadth was achieved by a DNA-MLV prime-boost strategy, versus DNA-only or MLV-only. We selected DNA plasmids from the ones that were used in that study (see Material and Method section).…”

Section: Resultsmentioning

confidence: 99%

“…All sequences were codon-optimized according to the porcine species, synthesized by GenScript (Piscataway, NJ, USA) and cloned in a pUMVC4a vector (Aldevron, Fargo, ND, USA). The four VB plasmids encoding PRRSV AG are pXCL1-N, pXCL1-GP4GP5M, pXCL1-NSP1β1 (AA1 to 202 of NSP1β), and pXCL1-NSP1β2 (AA182 to 383 of NSP1β) and are further described in submitted manuscript 1 [9]. The NSP1β sequence had to be separated into two parts to allow expression of the chimera.…”

Section: Methodsmentioning

confidence: 99%

“…The NSP1β sequence had to be separated into two parts to allow expression of the chimera. Vaccibody constructs encoding for RdRp did not lead to detectable expression upon transfection in HEK293 cells and therefore were not used [9]. Plasmid productions for immunization were prepared using endotoxin-free NucleoBond ® EF kit (Nagel Macherey GmbH, Düren, Germany) according to the manufacturer’s instructions and were stored at −20 °C until use.…”

Section: Methodsmentioning

confidence: 99%

“…Interestingly, T-cell epitopes from different PRRSV ORFs have been described that are conserved through European distant strains [8]. In a parallel study, in order to enhance and broaden the T-cell mediated immunity induced by MLVs, we used a DNA-MLV prime-boost strategy with plasmids encoding PRRSV antigens (PRRSV-AG) including conserved T-cell epitopes (NSP1β, RdRp, M-derived antigens) as well as the B cell immuno-dominant nucleoprotein N from a recent Western European strain [9]. We found that the DNA prime broadened the T-cell response and potently enhanced the anti-N IgG response induced by MLV.…”

Section: Introductionmentioning

confidence: 99%

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A DNA Prime Immuno-Potentiates a Modified Live Vaccine against the Porcine Reproductive and Respiratory Syndrome Virus but Does Not Improve Heterologous Protection

Bernelin-Cottet

Urien

Frétaud

et al. 2019

Viruses

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The porcine reproductive and respiratory syndrome virus (PRRSV), an RNA virus inducing abortion in sows and respiratory disease in young pigs, is a leading infectious cause of economic losses in the swine industry. Modified live vaccines (MLVs) help in controlling the disease, but their efficacy is often compromised by the high genetic diversity of circulating viruses, leading to vaccine escape variants in the field. In this study, we hypothesized that a DNA prime with naked plasmids encoding PRRSV antigens containing conserved T-cell epitopes may improve the protection of MLV against a heterologous challenge. Plasmids were delivered with surface electroporation or needle-free jet injection and European strain-derived PRRSV antigens were targeted or not to the dendritic cell receptor XCR1. Compared to MLV-alone, the DNA-MLV prime- boost regimen slightly improved the IFNγ T-cell response, and substantially increased the antibody response against envelope motives and the nucleoprotein N. The XCR1-targeting of N significantly improved the anti-N specific antibody response. Despite this immuno-potentiation, the DNA-MLV regimen did not further decrease the serum viral load or the nasal viral shedding of the challenge strain over MLV-alone. Finally, the heterologous protection, achieved in absence of detectable effective neutralizing antibodies, was not correlated to the measured antibody or to the IFNγ T-cell response. Therefore, immune correlates of protection remain to be identified and represent an important gap of knowledge in PRRSV vaccinology. This study importantly shows that a naked DNA prime immuno-potentiates an MLV, more on the B than on the IFNγ T-cell response side, and has to be further improved to reach cross-protection.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A DNA Prime Immuno-Potentiates a Modified Live Vaccine against the Porcine Reproductive and Respiratory Syndrome Virus but Does Not Improve Heterologous Protection

Bernelin-Cottet

Urien

Frétaud

et al. 2019

Viruses

Self Cite

View full text Add to dashboard Cite

show abstract

“…Besides the commercially available inactivated vaccines and modified-live virus vaccines (MLV), new techniques for administration have been explored and developed and research on the use of DNA vaccines to further improve efficacy of MLV vaccines has been conducted (7)(8)(9). However, current vaccines fail to provide complete protection against heterologous field strains and commercially available vaccines only partially prevent or mitigate the disease and show limited effectiveness in the field (10)(11)(12)(13).…”

Section: Introductionmentioning

confidence: 99%

Modeling Economic Effects of Vaccination Against Porcine Reproductive and Respiratory Syndrome: Impact of Vaccination Effectiveness, Vaccine Price, and Vaccination Coverage

2020

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Porcine reproductive and respiratory syndrome (PRRS) causes substantial financial losses in pig farms and economic losses to societies worldwide. Vaccination against PRRS virus (PRRSV) is a common intervention in affected farms. The aim of this study was to assess the economic impact and profitability of potential new PRRS vaccines with improved efficacy at animal, herd, and national level. Two vaccination strategies were modeled; (i) mass vaccination of sows only (MS) and (ii) mass vaccination of sows and vaccination of piglets (MSP), comprising different scenarios of vaccine effectiveness, vaccine price, and vaccination coverage. A farrow-to-finish farm with 1,000 working sows from a pig-dense region in Germany served as an example farm. Financial benefits were obtained from gross margin analyses and were defined as difference in gross margin between a PRRSV-infected farm without vaccination (baseline) and with vaccination (intervention). Financial benefits were highest if both sows and piglets (MSP) were vaccinated. In these scenarios, median annual net benefits per working sow ranged from e170 to 340. If sows only were vaccinated (MS), estimated benefits attributable to vaccination were between e148 and 270. Decisive variables for the estimation of national level benefits were the number of farmers switching from existing to a better protecting vaccine, the number of previously non-vaccinating herds adopting the new vaccine, and the effectiveness of the new vaccine relative to those already available. Benefits were greatest when the new vaccine was adopted by previously non-vaccinating herds. The analyses showed that vaccination against PRRS was beneficial for all modeled scenarios. The magnitude of benefits derived from vaccination was more susceptible to changes in vaccination effectiveness than to vaccine price changes. This study provides evidence to support future vaccine development. The estimates indicate that the introduction of more efficient vaccines might lead to substantial financial benefits, is of socioeconomic importance and that new vaccines might significantly contribute to the reduction of disease burden.

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Recent advances in antigen targeting to antigen-presenting cells in veterinary medicine

2023

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Advances in antigen targeting in veterinary medicine have gained traction over the years as an alternative approach for diseases that remain a challenge for traditional vaccines. In addition to the nature of the immunogen, antigen-targeting success relies heavily on the chosen receptor for its direct influence on the elicited response that will ensue after antigen uptake. Different approaches using antibodies, natural or synthetic ligands, fused proteins, and DNA vaccines have been explored in various veterinary species, with pigs, cattle, sheep, and poultry as the most frequent models. Antigen-presenting cells can be targeted using a generic approach, such as broadly expressed receptors such as MHC-II, CD80/86, CD40, CD83, etc., or focused on specific cell populations such as dendritic cells or macrophages (Langerin, DC-SIGN, XCR1, DC peptides, sialoadhesin, mannose receptors, etc.) with contrasting results. Interestingly, DC peptides show high specificity to DCs, boosting activation, stimulating cellular and humoral responses, and a higher rate of clinical protection. Likewise, MHC-II targeting shows consistent results in enhancing both immune responses; an example of this strategy of targeting is the approved vaccine against the bovine viral diarrhea virus in South America. This significant milestone opens the door to continuing efforts toward antigen-targeting vaccines to benefit animal health. This review discusses the recent advances in antigen targeting to antigen-presenting cells in veterinary medicine, with a special interest in pigs, sheep, cattle, poultry, and dogs.

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A DNA-Modified Live Vaccine Prime–Boost Strategy Broadens the T-Cell Response and Enhances the Antibody Response against the Porcine Reproductive and Respiratory Syndrome Virus

Cited by 10 publications

References 59 publications

A DNA Prime Immuno-Potentiates a Modified Live Vaccine against the Porcine Reproductive and Respiratory Syndrome Virus but Does Not Improve Heterologous Protection

A DNA Prime Immuno-Potentiates a Modified Live Vaccine against the Porcine Reproductive and Respiratory Syndrome Virus but Does Not Improve Heterologous Protection

Modeling Economic Effects of Vaccination Against Porcine Reproductive and Respiratory Syndrome: Impact of Vaccination Effectiveness, Vaccine Price, and Vaccination Coverage

Recent advances in antigen targeting to antigen-presenting cells in veterinary medicine

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