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Human Receptor-Interacting Serine/Threonine-Protein Kinase 2 (RIPK2); A Target Enabling Package

Main Authors: Peter Canning, Daniel M. Pinkas, Joshua C. Bufton, Sarah Picaud, Jennifer A. Ward, Catherine Rogers, Benedict-Tilman Berger, Matous Hrdinka, Qui Ruan, Chalada Suebsuwong, Lisa Schlicher, Bing Dai, Jenny L. Maki, Soumya S. Ray, Danish Saleh, Sameer Nikhar, Tobias Schwerd, Holm H. Uhlig, Stefan Knapp, Susanne Muller-Knapp, Paul E. Brennan, Kilian V. M. Huber, Panagis Filippakopoulos, Gregory D. Cuny, Alexei Degterev, Mads Gyrd-Hansen, Alex N. Bullock
Format: info dataset Journal
Terbitan: , 2018
Subjects:
Protein
Target Enabling Package
Disease
Structure
Cancer
Neuropsychiatry
Neuro
Neurological Genetic Disorders
Metabolic Diseases
Oncology
Infectious Disease
Malarai
Structural Genomics
Chemical Biology
Orphan Disease
Drug Target
Probe
Structure Discovery
RIPK2
Online Access: https://zenodo.org/record/1344545
Daftar Isi:
  • RIPK2 inflammatory signalling downstream from the bacteria-sensing receptors NOD1 and NOD2 is associated with auto-immune and inflammatory conditions. RIPK2 inhibition has shown promise in disease models of inflammatory bowel disease and multiple sclerosis. In this TEP, we reveal a lack of correlation between inhibitor efficacy in cells and their potency using in vitro kinase assays. We show that RIPK2 kinase activity is in fact dispensable for NOD2 inflammatory signalling and that RIPK2 inhibitors function instead by antagonizing XIAP-binding and ubiquitination of RIPK2. We characterise the molecular basis for this effect. We also solved the first crystal structure of the RIPK2 kinase domain and applied a range of biochemical and cellular assays to profile type I and type II RIPK2 kinase inhibitors. Overall, our study illustrates how to target the ATP-binding pocket in RIPK2 to interfere with the RIPK2-XIAP interaction for modulation of NOD signalling.

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