In Vivo Effects of Chicken Interferon-γ During Infection with Eimeria

Newly hatched chickens are highly susceptible to infection by opportunistic pathogens during the first 1 or 2 weeks of life. The use of cytokines as therapeutic agents has been studied in animal models as well as in immunosuppressed patients. This approach has become more feasible in livestock animals, in particular poultry, with the recent cloning of cytokine genes and the development of new technologies, such as live delivery vectors. We have recently cloned the gene for chicken interferon-γ (Ch-IFN-γ). Poly-HIS-tagged recombinant Ch-IFN-γ was expressed in Escherichia coli, was purified by Ni chromatography, and was found to be stable at 4°C and an ambient temperature for at least several months and several weeks, respectively. Ch-IFN-γ was capable of protecting chick fibroblasts from undergoing virus-mediated lysis, induced nitrite secretion from chicken macrophages in vitro, and enhanced MHC class II expression on macrophages. Administration of recombinant Ch-IFN-γ to chickens resulted in enhanced weight gain over a 12-day period. Furthermore, the therapeutic potential of Ch-IFN-γ was assessed using a coccidial challenge model. Birds were treated with Ch-IFN-γ or a diluent control and then infected with Eimeria acervulina. Infected birds treated with Ch-IFN-γ showed improved weight gain relative to noninfected birds. The ability of Ch-IFN-γ to enhance weight gain in the face of coccidial infection makes it an excellent candidate as a therapeutic agent.