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Sustainable Livestock Production LINK Programme OVERVIEW Project LK0699/OD0720: Development of rationally attenuated live vaccines for effective control of infectious bronchitis Start Date: 08/10/2009 End Date: 07/10/2013 Background Control of infectious diseases and a reduction in the use of therapeutic antibiotics are two major challenges faced by the UK poultry industry. The avian coronavirus, IBV, is a highly contagious poultry pathogen prevalent in all types of poultry flocks worldwide. IBV is the causal agent of infectious bronchitis (IB) and continues to be responsible for economic loss, welfare problems in chickens and a potential risk to food security. IBV preferentially causes respiratory disease, but can also infect other organs such as the kidneys (resulting in kidney disease) or the reproductive tract (resulting in loss of egg production and/or egg quality). IBV has been reported to be responsible for more economic loss to the UK poultry industry than any other infectious disease. Although live attenuated vaccines and inactivated vaccines are universally used in the control of IBV, the protection gained by use of vaccination can be lost either due to vaccine breakdown or the introduction of a new IBV serotype that is not related to the vaccine used, posing a risk to the poultry industry. It is important that new and safer vaccines are developed for the control of IBV. Relaxation of IBV vaccination strategies or the breakdown of vaccination, due to new IBV strains, would have a profound and devastating effect on the UK poultry industry in terms of bird welfare and production costs, with associated risks to food security. Objective The overall aim of this project is to attenuate the pathogenicity of infectious bronchitis virus (IBV) of poultry in a non-reversible way, whilst maintaining immunogenicity for both vaccination of chickens and for in ovo application. The work seeks to develop an infectious clone system for the generation of rationally attenuated IBV vaccines, identifying two spatially distant regions of the genome that can be modified for attenuation. The project is divided into four sub-objectives:1. To produce an IBV reverse genetics system based on the pathogenic M41 strain of IBV. 2. To remove the M41 accessory non-structural genes to identify whether they play a role in pathogenicity. 3. To study the role of the M41 essential (replicase) non-structural protein genes in pathogenicity. 4. To investigate the attenuation of IBV for in ovo vaccination. This work will pave the way for new rationally modified and safer vaccines, as they will be less likely to revert. A further expected benefit from the development of safer vaccines, is a reduction in the amount of antibiotics used to counteract secondary bacterial infections associated with IB. CONTACT Dr Paul Britton Institute for Animal Health Compton Laboratory Compton, Newbury Berkshire, RG20 7NN [email protected] PARTNERS Pfizer Animal Health British Poultry Council British Egg Industry Council. GOVERNMENT SPONSORS Defra/BBSRC