Replication-Deficient Particles: New Insights into the Next Generation of Bluetongue Virus Vaccines

Author:

Celma Cristina C.1,Stewart Meredith1,Wernike Kerstin2,Eschbaumer Michael2,Gonzalez-Molleda Lorenzo1,Breard Emmanuel3,Schulz Claudia2,Hoffmann Bernd2,Haegeman Andy4,De Clercq Kris4,Zientara Stephan3,van Rijn Piet A.56,Beer Martin2,Roy Polly1

Affiliation:

1. Department of Pathogen Molecular Biology, London School of Hygiene and Tropical Medicine, London, United Kingdom

2. Institute of Diagnostic Virology, Friedrich-Loeffler-Institut, Greifswald, Insel Riems, Germany

3. Université Paris-Est ANSES Alfort, UMR 1161 ANSES/INRA/ENVA, Maisons-Alfort, France

4. Unit Vesicular and Exotic Diseases, CODA-CERVA, Uccle, Belgium

5. Central Veterinary Institute of Wageningen University, Wageningen, The Netherlands

6. Department of Biochemistry, North-West University, Potchefstroom, South Africa

Abstract

ABSTRACT Bluetongue virus (BTV) is endemic in many parts of the world, often causing severe hemorrhagic disease in livestock. To date, at least 27 different serotypes have been recognized. Vaccination against all serotypes is necessary to protect susceptible animals and to prevent onward spread of the virus by insect vectors. In our previous studies, we generated replication-deficient (disabled infectious single-cycle [DISC]) virus strains for a number of serotypes and reported preliminary data on their protective efficacy in animals. In this report, to advance the DISC vaccines to the marketplace, we investigated different parameters of these DISC vaccines. First, we demonstrated the genetic stabilities of these vaccine strains and also the complementing cell line. Subsequently, the optimal storage conditions of vaccines, including additives, temperature, and desiccation, were determined and their protective efficacies in animals confirmed. Furthermore, to test if mixtures of different vaccine strains could be tolerated, we tested cocktails of DISC vaccines in combinations of three or six different serotypes in sheep and cattle, the two natural hosts of BTV. Groups of sheep vaccinated with a cocktail of six different vaccines were completely protected from challenge with individual virulent serotypes, both in early challenge and after 5 months of challenge without any clinical disease. There was no interference in protection between the different vaccines. Protection was also achieved in cattle with a mixture of three vaccine strains, albeit at a lesser level than in sheep. Our data support and validate the suitability of these virus strains as the next-generation vaccines for BTV. IMPORTANCE Bluetongue (BT) is a debilitating and in many cases lethal disease that affects ruminants of economic importance. Classical vaccines that afford protection against bluetongue virus, the etiological agent, are not free from secondary and undesirable effects. A surge in new approaches to produce highly attenuated, safer vaccines was evident after the development of the BTV reverse-genetics system that allows the introduction of targeted mutations in the virus genome. We targeted an essential gene to develop disabled virus strains as vaccine candidates. The results presented in this report further substantiate our previous evidence and support the suitability of these virus strains as the next-generation BTV vaccines.

Funder

Duth Ministry of Economic Affairs

European Commission

Biotechnology and Biological Sciences Research Council

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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