Katarzyna Bulek, Caini Liu, Shadi Swaidani, Liwen Wang, Richard C Page, Muhammet F Gulen, Tomasz Herjan, Amina Abbadi, Wen Qian, Dongxu Sun, Mark Lauer, Vincent Hascall, Saurav Misra, Mark R Chance, Mark Aronica, Thomas Hamilton, Xiaoxia Li
Nature immunology 2011 SepInterleukin 17 (IL-17) is critical in the pathogenesis of inflammatory and autoimmune diseases. Here we report that Act1, the key adaptor for the IL-17 receptor (IL-7R), formed a complex with the inducible kinase IKKi after stimulation with IL-17. Through the use of IKKi-deficient mice, we found that IKKi was required for IL-17-induced expression of genes encoding inflammatory molecules in primary airway epithelial cells, neutrophilia and pulmonary inflammation. IKKi deficiency abolished IL-17-induced formation of the complex of Act1 and the adaptors TRAF2 and TRAF5, activation of mitogen-activated protein kinases (MAPKs) and mRNA stability, whereas the Act1-TRAF6-transcription factor NF-κB axis was retained. IKKi was required for IL-17-induced phosphorylation of Act1 on Ser311, adjacent to a putative TRAF-binding motif. Substitution of the serine at position 311 with alanine impaired the IL-17-mediated Act1-TRAF2-TRAF5 interaction and gene expression. Thus, IKKi is a kinase newly identified as modulating IL-17 signaling through its effect on Act1 phosphorylation and consequent function.
Katarzyna Bulek, Caini Liu, Shadi Swaidani, Liwen Wang, Richard C Page, Muhammet F Gulen, Tomasz Herjan, Amina Abbadi, Wen Qian, Dongxu Sun, Mark Lauer, Vincent Hascall, Saurav Misra, Mark R Chance, Mark Aronica, Thomas Hamilton, Xiaoxia Li. The inducible kinase IKKi is required for IL-17-dependent signaling associated with neutrophilia and pulmonary inflammation. Nature immunology. 2011 Sep;12(9):844-52
PMID: 21822257
View Full Text