Collaborative research involving scientists from The Pirbright Institute has shown that a new vaccine, ChAdOx1 RVF, is effective at protecting pregnant sheep and goats from Rift Valley fever (RVF), a debilitating disease that can also be transmitted to humans. This work will also help progress the development of the vaccine, which could be the first to be used against both a human and animal disease.

RVF is spread across Africa and the Arabian Peninsula and is caused by a virus that infects livestock such as sheep, goats, cattle and camels. Infection of animals with Rift Valley fever virus (RVFV) results in high mortality and poor outcomes during pregnancy, including stillbirths, foetal malformations and abortions. It also poses a severe threat to human health but there is currently no licenced human vaccine available. People can contract the disease through contact with contaminated tissues and fluids of livestock, as well as being bitten by infected mosquitoes.

ChAdOx1 RVF was developed by The Jenner Institute at the University of Oxford and was previously shown to be safe and effective at protecting animals. The vaccine has since been scheduled for human trials, but its effects on pregnant animals still required examination. Pirbright scientists worked with The Jenner Institute, Wageningen University Research in the Netherlands, BioVacc Consulting Ltd and the KEMRI-Wellcome Trust Research Programme in Kenya to demonstrate the vaccine’s safety in pregnant goats and sheep at the Institute’s specialist high containment facilities.

The study, published in npj Vaccines, has shown that animals immunised with a single dose of ChAdOx1 RVF remain healthy and suffer no pregnancy losses after challenge with a virulent strain of RVF virus. The protection was more robust in sheep than goats, despite the similar levels of immune response induced, which suggests that protection mechanisms against RVF could differ between livestock species.

The research demonstrates that ChAdOx1 RVF overcomes drawbacks that current veterinary RVF vaccines experience, such as causing pregnancy complications or requiring multiple booster vaccinations. ChAdOx1 RVF also generates a rapid immune response and allows diagnostic tests to differentiate between infected and vaccinated animals (DIVA). These properties make this vaccine well suited for tackling outbreak situations and could limit the circulation of RVF amongst animals and people.

“This research will aid the development of ChAdOx1 RVF for human use, and for the first time we may see a vaccine that can be deployed against the same virus in both animals and humans”, said Professor Bryan Charleston, Director of The Pirbright Institute. The new vaccine is an excellent example of the One Health approach, where multiple research disciplines work together to provide solutions that simultaneously benefit animals, humans and ecosystems.

 

This research was funded by the Department of Health and Social Care as part of the UK Vaccine Network (UKVN), a UK Aid programme to develop vaccines for diseases with epidemic potential in low and middle-income countries (LMICs).