G-Protein-Coupled Receptor 35 Is a Target of the Asthma Drugs Cromolyn Disodium and Nedocromil Sodium

Yang, Yuhua; Lu, Jenny Ying-Lin; Wu, Xingkun; Summer, Shamin; Whoriskey, John; Saris, Christiaan J. M.; Reagan, Jeff D.

doi:10.1159/000314164

Cited by 121 publications

(133 citation statements)

References 27 publications

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“…Previous studies showed that the antiasthma and antiallergic agents cromolyn disodium (Jenkins et al, 2010;Yang et al, 2010) and nedocromil sodium (Yang et al, 2010) are modestly potent agonists of GPR35. This was confirmed in Mast Cell Stabilizers and GPR35 a PathHunter human GPR35a-b-arrestin-2 interaction and complementation assay (Table 1), with nedocromil sodium (EC 50 5 0.97 6 0.09 mM) being approximately 3-fold more potent than cromolyn disodium (EC 50 5 2.98 6 1.27 mM).…”

Section: Resultsmentioning

confidence: 99%

“…This was confirmed in Mast Cell Stabilizers and GPR35 a PathHunter human GPR35a-b-arrestin-2 interaction and complementation assay (Table 1), with nedocromil sodium (EC 50 5 0.97 6 0.09 mM) being approximately 3-fold more potent than cromolyn disodium (EC 50 5 2.98 6 1.27 mM). Because GPR35 is expressed by human mast cells and levels are reportedly upregulated by exposure to the allergic stimulus IgE (Yang et al, 2010), we set out to investigate whether other antiallergic ligands and mast cell stabilizers might also act as agonists at GPR35 and, if so, potentially provide a common mode of action. Bufrolin (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Glu6.58Arg, Ser7.32Arg pEC antiallergenic drugs cromolyn disodium (Jenkins et al, 2010;Yang et al, 2010) and nedocromil sodium (Yang et al, 2010) have been shown to have agonist activity at GPR35. Although these drugs have modest potency, this encouraged us to explore the possibility that other drugs with similar functional pharmacology might also be GPR35 agonists.…”

Section: Discussionmentioning

confidence: 99%

“…The antiasthma and antiallergic agents cromolyn disodium (Jenkins et al, 2010;Yang et al, 2010) and nedocromil sodium (Yang et al, 2010) were recently shown to act as moderately potent agonists of GPR35. These ligands are both di-acids with marked mirror image symmetry (Fig.…”

Section: Introductionmentioning

confidence: 99%

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The Antiallergic Mast Cell Stabilizers Lodoxamide and Bufrolin as the First High and Equipotent Agonists of Human and Rat GPR35

Mackenzie¹,

Caltabiano

Kent

et al. 2013

Mol Pharmacol

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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.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The Antiallergic Mast Cell Stabilizers Lodoxamide and Bufrolin as the First High and Equipotent Agonists of Human and Rat GPR35

Mackenzie¹,

Caltabiano

Kent

et al. 2013

Mol Pharmacol

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show abstract

“…The antiasthma medicine and histamine sensitizer cromolyn disodium ( Fig. 1) (Jenkins et al, 2010;Yang et al, 2010) also acted as an agonist with efficacy equal to that of zaprinast at all three species orthologs. In this case ligand potency was lower, but was relatively similar between the human and rat orthologs with pEC 50 ϭ 4.78 Ϯ 0.10 (mean Ϯ S.E.M.…”

Section: Pamoate Is a Highly Selective But Partial Agonist Formentioning

confidence: 99%

Antagonists of GPR35 Display High Species Ortholog Selectivity and Varying Modes of Action

Jenkins

Harries

Lappin

et al. 2012

J Pharmacol Exp Ther

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Variation in pharmacology and function of ligands at species orthologs can be a confounding feature in understanding the biology and role of poorly characterized receptors. Substantial selectivity in potency of a number of GPR35 agonists has previously been demonstrated between human and rat orthologs of this G protein-coupled receptor. Via a bioluminescence resonance energy transfer-based assay of induced interactions between GPR35 and ␤-arrestin-2, addition of the mouse ortholog to such studies indicated that, as for the rat ortholog, murine GPR35 displayed very low potency for pamoate, whereas potency for the reference GPR35 agonist zaprinast was intermediate between the rat and human orthologs. This pattern was replicated in receptor internalization and G protein activation assays. The effectiveness and mode of action of two recently reported GPR35 antagonists, methyl-5-[(tert-butylcarbamothioylhydrazinylidene)methyl]-1-(2,4-difluorophenyl)pyrazole-4-carboxylate (CID-2745687) and 2-hydroxy-4-[4-(5Z)-5-[(E)-2-methyl-3-phenylprop-2-enylidene]-4-oxo-2-sulfanylidene-1,3-thiazolidin-3-yl]butanoylamino)benzoic acid (ML-145), were investigated. Both CID-2745687 and ML-145 competitively inhibited the effects at human GPR35 of cromolyn disodium and zaprinast, two agonists that share an overlapping binding site. By contrast, although ML-145 also competitively antagonized the effects of pamoate, CID-2745687 acted in a noncompetitive fashion. Neither ML-145 nor CID-2745687 was able to effectively antagonize the agonist effects of either zaprinast or cromolyn disodium at either rodent ortholog of GPR35. These studies demonstrate that marked species selectivity of ligands at GPR35 is not restricted to agonists and considerable care is required to select appropriate ligands to explore the function of GPR35 in nonhuman cells and tissues.

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Synthesis of Flavones and γ‐Benzopyranones Using Mild Sonogashira Coupling and 18‐Crown‐6 Ether Mediated 6‐endo Cyclization

Chuang¹,

El-Shazly²,

Balaji³

et al. 2012

Eur J Org Chem

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An efficient method for the synthesis of flavones and γbenzopyranones has been developed utilizing a mild Sonogashira coupling and 18-crown-6 ether mediated 6-endo cyclization of o-alkynoylphenyl acetates. By using this strategy,[a] Graduate 4533 flavones and γ-benzopyranones bearing electron-donating groups, halogens, and simple alkyl substituents were synthesized in satisfactory yields.www.eurjoc.org

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G-Protein-Coupled Receptor 35 Is a Target of the Asthma Drugs Cromolyn Disodium and Nedocromil Sodium

Cited by 121 publications

References 27 publications

The Antiallergic Mast Cell Stabilizers Lodoxamide and Bufrolin as the First High and Equipotent Agonists of Human and Rat GPR35

The Antiallergic Mast Cell Stabilizers Lodoxamide and Bufrolin as the First High and Equipotent Agonists of Human and Rat GPR35

Antagonists of GPR35 Display High Species Ortholog Selectivity and Varying Modes of Action

Synthesis of Flavones and γ‐Benzopyranones Using Mild Sonogashira Coupling and 18‐Crown‐6 Ether Mediated 6‐endo Cyclization

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