Abstract
Lack of high potency agonists has restricted analysis of the G protein–coupled receptor GPR35. Moreover, marked variation in potency and/or affinity of current ligands between human and rodent orthologs of GPR35 has limited their productive use in rodent models of physiology. Based on the reported modest potency of the antiasthma and antiallergic ligands cromolyn disodium and nedocromil sodium, we identified the related compounds lodoxamide and bufrolin as high potency agonists of human GPR35. Unlike previously identified high potency agonists that are highly selective for human GPR35, both lodoxamide and bufrolin displayed equivalent potency at rat GPR35. Further synthetic antiallergic ligands, either sharing features of the standard surrogate agonist zaprinast, or with lodoxamide and bufrolin, were also shown to display agonism at either human or rat GPR35. Because both lodoxamide and bufrolin are symmetric di-acids, their potential mode of binding was explored via mutagenesis based on swapping between the rat and human ortholog nonconserved arginine residues within proximity of a key conserved arginine at position 3.36. Computational modeling and ligand docking predicted the contributions of different arginine residues, other than at 3.36, in human GPR35 for these two ligands and were consistent with selective loss of potency of either bufrolin or lodoxamide at distinct arginine mutants. The computational models also suggested that bufrolin and lodoxamide would display reduced potency at a low-frequency human GPR35 single nucleotide polymorphism. This prediction was confirmed experimentally.
Footnotes
- Received September 9, 2013.
- Accepted October 10, 2013.
This work was supported by the Biotechnology and Biosciences Research Council (BBSRC DTG FO1673511); Medical Research Council Technology [Industrial CASE Studentship to A.E.M.]; the British Heart Foundation (FS/09/052/28032) [Studentship Support to J.E.M.]; and the Spanish Ministry of Education, Culture, and Sport National Program on Mobility of Human Resources of National I+D Plan 2008–2011 [José Castillejo 2012 Fellowship to G.C.].
- Copyright © 2013 by The American Society for Pharmacology and Experimental Therapeutics
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