Identification of a gp130 Cytokine Receptor Critical Site Involved in Oncostatin M Response

Abstract Gp130 cytokine receptor is involved in the formation of multimeric functional receptors for interleukin-6 (IL-6), IL-11, leukemia inhibitory factor (LIF), oncostatin M (OSM), ciliary neurotrophic factor, and cardiotrophin-1. Cloning of the epitope recognized by an OSM-neutralizing anti-gp130 monoclonal antibody identified a portion of gp130 receptor localized in the EF loop of the cytokine binding domain. Site-directed mutagenesis of the corresponding region was carried out by alanine substitution of residues 186–198. To generate type 1 or type 2 OSM receptors, gp130 mutants were expressed together with either LIF receptor β or OSM receptor β. When positions Val-189/Tyr-190 and Phe-191/Val-192 were alanine-substituted, Scatchard analyses indicated a complete abrogation of OSM binding to both type receptors. Interestingly, binding of LIF to type 1 receptor was not affected, corroborating the notion that in this case gp130 mostly behaves as a converter protein rather than a binding receptor. The present study demonstrates that positions 189–192 of gp130 cytokine binding domain are essential for OSM binding to both gp130/LIF receptor β and gp130/OSM receptor β heterocomplexes.