Ligand‐Biased and Probe‐Dependent Modulation of Chemokine Receptor CXCR3 Signaling by Negative Allosteric Modulators |
| |
| Authors: | Dr Viachaslau Bernat Regine Brox Prof?Dr Markus R Heinrich Dr Yves P Auberson Dr Nuska Tschammer |
| |
| Affiliation: | 1. Department of Chemistry and Pharmacy, Medicinal Chemistry, Emil Fischer Center, Friedrich Alexander University, Schuhstra?e 19, 91052 Erlangen (Germany);2. Current affiliation: Department of Chemistry, The Scripps Research Institute, 130 Scripps Way, 3A1, 33458 Jupiter, FL (USA);3. Novartis Institutes for BioMedical Research, Global Discovery Chemistry, WKL‐136.6.82, Klybeckstrasse 141, Basel (Switzerland) |
| |
| Abstract: | Over the last decade, functional selectivity (or ligand bias) has evolved from being a peculiar phenomenon to being recognized as an essential feature of synthetic ligands that target G protein‐coupled receptors (GPCRs). The CXC chemokine receptor 3 (CXCR3) is an outstanding platform to study various aspects of biased signaling, because nature itself uses functional selectivity to manipulate receptor signaling. At the same time, CXCR3 is an attractive therapeutic target in the treatment of autoimmune diseases and cancer. Herein we report the discovery of an 8‐azaquinazolinone derivative (N‐{1‐3‐(4‐ethoxyphenyl)‐4‐oxo‐3,4‐dihydropyrido2,3‐d]pyrimidin‐2‐yl]ethyl}‐4‐(4‐fluorobutoxy)‐N‐(1‐methylpiperidin‐4‐yl)methyl]butanamide, 1 b ) that can inhibit CXC chemokine 11 (CXCL11)‐dependent G protein activation over β‐arrestin recruitment with 187‐fold selectivity. This compound also demonstrates probe‐dependent activity, that is, it inhibits CXCL11‐ over CXCL10‐mediated G protein activation with 12‐fold selectivity. Together with a previously reported biased negative allosteric modulator from our group, the present study provides additional information on the molecular requirements for allosteric modulation of CXCR3. |
| |
| Keywords: | allosteric modulation chemokine receptor CXCR3 ligand‐biased signaling probe dependence |
|
|
