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Small molecule inhibitors reveal an indispensable scaffolding role of <scp>RIPK</scp> 2 in <scp>NOD</scp> 2 signaling

Authors :
Sarah Picaud
Sameer Nikhar
Gregory D. Cuny
Chalada Suebsuwong
Panagis Filippakopoulos
Mads Gyrd-Hansen
Alexei Degterev
Daniel M. Pinkas
Lisa Schlicher
Alex N. Bullock
Joshua C. Bufton
Bing Dai
Kilian Huber
Jennifer A. Ward
Catherine Rogers
Matous Hrdinka
Source :
Hrdinka, M, Schlicher, L, Dai, B, Pinkas, D M, Bufton, J C, Picaud, S, Ward, J A, Rogers, C, Suebsuwong, C, Nikhar, S, Cuny, G D, Huber, K V M, Filippakopoulos, P, Bullock, A N, Degterev, A & Gyrd-Hansen, M 2018, ' Small molecule inhibitors reveal an indispensable scaffolding role of RIPK2 in NOD2 signaling ', EMBO Journal, vol. 37, no. 17, e99372 . https://doi.org/10.15252/embj.201899372, The EMBO Journal
Publication Year :
2018
Publisher :
EMBO, 2018.

Abstract

RIPK2 mediates inflammatory signaling by the bacteria‐sensing receptors NOD1 and NOD2. Kinase inhibitors targeting RIPK2 are a proposed strategy to ameliorate NOD‐mediated pathologies. Here, we reveal that RIPK2 kinase activity is dispensable for NOD2 inflammatory signaling and show that RIPK2 inhibitors function instead by antagonizing XIAP‐binding and XIAP‐mediated ubiquitination of RIPK2. We map the XIAP binding site on RIPK2 to the loop between β2 and β3 of the N‐lobe of the kinase, which is in close proximity to the ATP‐binding pocket. Through characterization of a new series of ATP pocket‐binding RIPK2 inhibitors, we identify the molecular features that determine their inhibition of both the RIPK2‐XIAP interaction, and of cellular and in vivo NOD2 signaling. Our study exemplifies how targeting of the ATP‐binding pocket in RIPK2 can be exploited to interfere with the RIPK2‐XIAP interaction for modulation of NOD signaling.

Details

ISSN :
14602075 and 02614189
Volume :
37
Database :
OpenAIRE
Journal :
The EMBO Journal
Accession number :
edsair.doi.dedup.....d525dbc840945c9e13b0f0df01042759
Full Text :
https://doi.org/10.15252/embj.201899372