Literature DB >> 21498659

Extracellular loop 2 of the free fatty acid receptor 2 mediates allosterism of a phenylacetamide ago-allosteric modulator.

Nicola J Smith1, Richard J Ward, Leigh A Stoddart, Brian D Hudson, Evi Kostenis, Trond Ulven, Joanne C Morris, Christian Tränkle, Irina G Tikhonova, David R Adams, Graeme Milligan.   

Abstract

Allosteric agonists are powerful tools for exploring the pharmacology of closely related G protein-coupled receptors that have nonselective endogenous ligands, such as the short chain fatty acids at free fatty acid receptors 2 and 3 (FFA2/GPR43 and FFA3/GPR41, respectively). We explored the molecular mechanisms mediating the activity of 4-chloro-α-(1-methylethyl)-N-2-thiazolylbenzeneacetamide (4-CMTB), a recently described phenylacetamide allosteric agonist and allosteric modulator of endogenous ligand function at human FFA2, by combining our previous knowledge of the orthosteric binding site with targeted examination of 4-CMTB structure-activity relationships and mutagenesis and chimeric receptor generation. Here we show that 4-CMTB is a selective agonist for FFA2 that binds to a site distinct from the orthosteric site of the receptor. Ligand structure-activity relationship studies indicated that the N-thiazolyl amide is likely to provide hydrogen bond donor/acceptor interactions with the receptor. Substitution at Leu(173) or the exchange of the entire extracellular loop 2 of FFA2 with that of FFA3 was sufficient to reduce or ablate, respectively, allosteric communication between the endogenous and allosteric agonists. Thus, we conclude that extracellular loop 2 of human FFA2 is required for transduction of cooperative signaling between the orthosteric and an as-yet-undefined allosteric binding site of the FFA2 receptor that is occupied by 4-CMTB.

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Year:  2011        PMID: 21498659      PMCID: PMC3127537          DOI: 10.1124/mol.110.070789

Source DB:  PubMed          Journal:  Mol Pharmacol        ISSN: 0026-895X            Impact factor:   4.436


  40 in total

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Review 2.  When simple agonism is not enough: emerging modalities of GPCR ligands.

Authors:  Nicola J Smith; Kirstie A Bennett; Graeme Milligan
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Journal:  Trends Pharmacol Sci       Date:  2011-01       Impact factor: 14.819

Review 5.  Allostery at G protein-coupled receptor homo- and heteromers: uncharted pharmacological landscapes.

Authors:  Nicola J Smith; Graeme Milligan
Journal:  Pharmacol Rev       Date:  2010-12       Impact factor: 25.468

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8.  The first synthetic agonists of FFA2: Discovery and SAR of phenylacetamides as allosteric modulators.

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  33 in total

Review 1.  Role of Short Chain Fatty Acid Receptors in Intestinal Physiology and Pathophysiology.

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3.  Allosteric and orthosteric pharmacology of cannabidiol and cannabidiol-dimethylheptyl at the type 1 and type 2 cannabinoid receptors.

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Review 4.  The therapeutic potential of GPR43: a novel role in modulating metabolic health.

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Review 8.  Allosteric Modulation of Class A GPCRs: Targets, Agents, and Emerging Concepts.

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9.  Drug discovery opportunities and challenges at g protein coupled receptors for long chain free Fatty acids.

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10.  Short-chain free fatty acid receptors FFA2/GPR43 and FFA3/GPR41 as new potential therapeutic targets.

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