Agonists and Antagonists of Protease-Activated Receptor 2 Discovered within a DNA-Encoded Chemical Library Using Mutational Stabilization of the Target

被引:40
作者
Brown, Dean G. [1 ]
Brown, Giles A. [2 ]
Centrella, Paolo [3 ]
Certel, Kaan [3 ,5 ]
Cooke, Robert M. [2 ]
Cuozzo, John W. [3 ]
Dekker, Niek [4 ]
Dumelin, Christoph E. [3 ,6 ]
Ferguson, Andrew [1 ,7 ]
Fiez-Vandal, Cedric [2 ]
Geschwindner, Stefan [4 ]
Guie, Marie-Aude [3 ]
Habeshian, Sevan [3 ,8 ]
Keefe, Anthony D. [3 ]
Schlenker, Oliver [2 ]
Sigel, Eric A. [3 ]
Snijder, Arjan [4 ]
Soutter, Holly T. [3 ]
Sundstrom, Linda [4 ]
Troast, Dawn M. [3 ,9 ]
Wiggin, Giselle [2 ]
Zhang, Jing [1 ,10 ]
Zhang, Ying [3 ]
Clark, Matthew A. [3 ]
机构
[1] AstraZeneca R&D, Innovat Med & Early Dev Biotech Unit, Discovery Sci, Waltham, MA USA
[2] Heptares Therapeut Ltd, Welwyn Garden City, Herts, England
[3] X Chem Pharmaceut, 100 Beaver St, Waltham, MA 02453 USA
[4] AstraZeneca R&D, Discovery Sci, Innovat Med & Early Dev Biotech Unit, Molndal, Sweden
[5] Novartis Inst BioMed Res, Cambridge, MA USA
[6] Novartis Inst BioMed Res, Basel, Switzerland
[7] X Chem Inc, Waltham, MA USA
[8] Ecole Polytech Fed Lausanne, Lausanne, Switzerland
[9] Morph Therapeut, Waltham, MA USA
[10] Entasis Therapeut, Waltham, MA USA
来源
SLAS DISCOVERY | 2018年 / 23卷 / 05期
关键词
medicinal; organic; synthetic; combinatorial; G-protein-coupled receptor (GPCR); ligand binding; receptor binding; cell-based assays; SMALL-MOLECULE LIBRARIES; COUPLED RECEPTORS; DRUG DISCOVERY; TECHNOLOGY; SELECTION; FRAGMENT;
D O I
10.1177/2472555217749847
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
The discovery of ligands via affinity-mediated selection of DNA-encoded chemical libraries is driven by the quality and concentration of the protein target. G-protein-coupled receptors (GPCRs) and other membrane-bound targets can be difficult to isolate in their functional state and at high concentrations, and therefore have been challenging for affinity-mediated selection. Here, we report a successful selection campaign against protease-activated receptor 2 (PAR2). Using a thermo-stabilized mutant of PAR2, we conducted affinity selection using our >100-billion-compound DNA-encoded library. We observed a number of putative ligands enriched upon selection, and subsequent cellular profiling revealed these ligands to comprise both agonists and antagonists. The agonist series shared structural similarity with known agonists. The antagonists were shown to bind in a novel allosteric binding site on the PAR2 protein. This report serves to demonstrate that cell-free affinity selection against GPCRs can be achieved with mutant stabilized protein targets.
引用
收藏
页码:429 / 436
页数:8
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