Abstract
Two mouse IFN-gamma receptor (MoIFN gamma R)-Ig fusion proteins, which were constructed for the purpose of creating new efficient mouse IFN-gamma (MoIFN-gamma) inhibitor molecules, were studied in vivo to determine their plasma half-life and immunogenicity, and to show their biologic activity. The hybrid proteins show 40-h blood persistency. They do not provoke an antibody response when injected into mice, and they are biologically active in vivo, as demonstrated by the prevention of streptozotocin-induced diabetes. The two fusion proteins are efficient MoIFN-gamma antagonists and can be used in mouse models of human diseases to investigate the role of MoIFN gamma in these pathologic states.
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CITATION STYLE
Kürschner, C., Ozmen, L., Garotta, G., & Dembic, Z. (1992). IFN-gamma receptor-Ig fusion proteins. Half-life, immunogenicity, and in vivo activity. The Journal of Immunology, 149(12), 4096–4100. https://doi.org/10.4049/jimmunol.149.12.4096
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