Systematic analysis of the IL-17 receptor signalosome reveals a robust regulatory feedback loop.

The EMBO Journal
Helena DraberovaPeter Draber

Abstract

IL-17 mediates immune protection from fungi and bacteria, as well as it promotes autoimmune pathologies. However, the regulation of the signal transduction from the IL-17 receptor (IL-17R) remained elusive. We developed a novel mass spectrometry-based approach to identify components of the IL-17R complex followed by analysis of their roles using reverse genetics. Besides the identification of linear ubiquitin chain assembly complex (LUBAC) as an important signal transducing component of IL-17R, we established that IL-17 signaling is regulated by a robust negative feedback loop mediated by TBK1 and IKKε. These kinases terminate IL-17 signaling by phosphorylating the adaptor ACT1 leading to the release of the essential ubiquitin ligase TRAF6 from the complex. NEMO recruits both kinases to the IL-17R complex, documenting that NEMO has an unprecedented negative function in IL-17 signaling, distinct from its role in NF-κB activation. Our study provides a comprehensive view of the molecular events of the IL-17 signal transduction and its regulation.

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Methods Mentioned

BETA
tandem affinity purification
immunoprecipitation
FACS
PCR
transfection
PCAs
PCA
FCS

Software Mentioned

MaxQuant
IUPred2A
Salmon
SPOT disorder
MFDp2
Prism
Perseus
gplots
GraphPad
tximport

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