Molecular dissection of human interleukin-31-mediated signal transduction through site-directed mutagenesis

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Abstract

Interleukin (IL)-31 is a recently described cytokine, preferentially produced by T helper 2 lymphocytes and associated with skin diseases, such as atopic dermatitis. IL-31 is a member of the four α-helix bundle cytokine family and is related to the IL-6 subgroup. Its heterodimeric membrane receptor is composed of the gp130-like receptor (GPL) subunit associated to the oncostatin M receptor subunit. We identified critical amino acids implicated in the ligand receptor interaction by computational analysis combined with site-directed mutagenesis. Six IL-31 residues selected for their putative involvement in cytokine receptor contact sites were alanine-substituted, and the corresponding proteins were expressed in mammalian and bacterial systems. Biochemical, membrane binding, cell signaling, and cell proliferation analyses showed that mutation E44A, E106A, or H110A abolished IL-31 binding to GPL and the subsequent signaling events. A second ligand receptor-binding site involved Lys134, with alanine substitution leading to a protein that still binds GPL, but is unable to recruit the second receptor subunit and the subsequent signaling pathways. The results indicate that IL-31 recognizes its receptor complex through two different binding sites, and we propose a three-dimensional model for IL-31. © 2010 by The American Society for Biochemistry and Molecular Biology, Inc.

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APA

Le Saux, S., Rousseau, F., Barbier, F., Ravon, E., Grimaud, L., Danger, Y., … Gascan, H. (2010). Molecular dissection of human interleukin-31-mediated signal transduction through site-directed mutagenesis. Journal of Biological Chemistry, 285(5), 3470–3477. https://doi.org/10.1074/jbc.M109.049189

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