The Pharmacology of TUG-891, a Potent and Selective Agonist of the Free Fatty Acid Receptor 4 (FFA4/GPR120), Demonstrates Both Potential Opportunity and Possible Challenges to Therapeutic Agonism

Hudson, Brian D.; Shimpukade, Bharat; Mackenzie, Amanda E.; Butcher, Adrian J.; Pediani, John D.; Christiansen, Elisabeth; Heathcote, Helen R.; Tobin, Andrew B.; Ulven, Trond; Milligan, Graeme

doi:10.1124/mol.113.087783

Cited by 177 publications

(232 citation statements)

References 42 publications

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“…As demonstrated in Table 1, ZQ-16 did not evoke calcium responses in HEK293 cells expressing other FFARs, including GPR40, GPR41, GPR119, and GPR120, at concentrations up to 100 mM. These receptors were functional, since they could be activated by reported ligands with EC 50 values comparable to published data (Briscoe et al, 2003;Xiong et al, 2004;Overton et al, 2006;Shimpukade et al, 2012;Hudson et al, 2013;Suzuki et al, 2013;Song et al, 2015). These results indicate that ZQ-16 is a selective agonist for GPR84.…”

Section: Resultssupporting

confidence: 70%

Discovery and Characterization of a Novel Small-Molecule Agonist for Medium-Chain Free Fatty Acid Receptor G Protein-Coupled Receptor 84

Zhang

Yang

et al. 2016

Journal of Pharmacology and Experimental Therapeutics

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G protein-coupled receptor 84 (GPR84) is a free fatty acid receptor activated by medium-chain free fatty acids with 9-14 carbons. It is expressed mainly in the immune-related tissues, such as spleen, bone marrow, and peripheral blood leukocytes. GPR84 plays significant roles in inflammatory processes and may represent a novel drug target for the treatment of immune-mediated diseases. However, the lack of potent and specific ligands for GPR84 hindered the study of its functions and the development of potential clinical applications. Here, we report the screen of 160,000 smallmolecule compounds with a calcium mobilization assay using a human embryonic kidney 293 cell line stably expressing GPR84 and Ga16, and the identification of 2-(hexylthio)pyrimidine-4,6-diol (ZQ-16) as a potent and selective agonist of GPR84 with a novel structure. ZQ-16 activates several GPR84-mediated signaling pathways, including calcium mobilization, inhibition of cAMP accumulation, phosphorylation of extracellular signal-regulated protein kinase 1/2, receptor desensitization and internalization, and receptor-b-arrestin interaction. This compound may be a useful tool to study the functions of GPR84 and a potential candidate for further structural optimization.

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Section: Resultssupporting

confidence: 70%

Discovery and Characterization of a Novel Small-Molecule Agonist for Medium-Chain Free Fatty Acid Receptor G Protein-Coupled Receptor 84

Zhang

Yang

et al. 2016

Journal of Pharmacology and Experimental Therapeutics

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“…TUG-891 for effects mediated by human FFA4 (Hudson et al, 2013b). The relative potencies of EPA, DHA, GW9508, and TUG-891 are also consistent with previously published values.…”

Section: Ffa4 Agonists Inhibit Prostate Cancer Cell Proliferationsupporting

confidence: 79%

“…TUG-891, a pharmacologic agent that is not a lipid, is not incorporated into phospholipid and acts reversibly (Hudson et al, 2013b). In Fig.…”

Section: Ffa4 Agonists Inhibit Prostate Cancer Cell Proliferationmentioning

confidence: 99%

“…The relative potencies of EPA, DHA, GW9508, and TUG-891 are also consistent with previously published values. TUG-891 was developed as a selective FFAR inhibitor, and has higher potency than the endogenous n-3 FAs (Hudson et al, 2013b). GW9508, the FFA1-selective agonist, inhibited proliferation with an IC 50 of 950 nM.…”

Section: Ffa4 Agonists Inhibit Prostate Cancer Cell Proliferationmentioning

confidence: 99%

“…Both FFA1 and FFA4 are coupled to G q/11 as well as arrestin-3, but many of their actions appear to be arrestin-mediated (Mancini and Poitout, 2013;Butcher et al, 2014). Selective agonists for FFA1 and FFA4 are rapidly being developed (Sun et al, 2010;Hudson et al, 2013b;Du et al, 2014), making it possible to test whether such agents elicit therapeutic effects of interest.…”

Section: Introductionmentioning

confidence: 99%

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Omega-3 Fatty Acids and Other FFA4 Agonists Inhibit Growth Factor Signaling in Human Prostate Cancer Cells

Liu

Hopkins

Quisenberry

et al. 2014

J Pharmacol Exp Ther

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Omega-3 fatty acids (n-3 FAs) are proposed to have many beneficial effects on human health. However, the mechanisms underlying their potential cancer preventative effects are unclear. G protein-coupled receptors (GPCRs) of the free fatty acid receptor (FFAR) family, FFA1/GPR40 and FFA4/GPR120, specifically bind n-3 FAs as agonist ligands. In this study, we examined the effects of n-3 FAs in human prostate cancer cell lines. Initial studies established that the long-chain n-3 FAs, eicosapentaenoic acid (EPA) and docosahexaenoic acid, inhibit proliferation of DU145 cells in response to lysophosphatidic acid (LPA), a mitogenic lipid mediator. When added alone to serumstarved DU145 cells, EPA transiently activates signaling events, including p70S6K phosphorylation. However, when added 15 minutes prior to LPA, EPA suppresses LPA-induced activating phosphorylations of ERK, FAK, and p70S6K, and expression of the matricellular protein CCN1. The rapid onset of the inhibitory action of EPA suggested involvement of a GPCR. Further studies showed that DU145 and PC-3 cells express mRNA and protein for both -2-yl)methoxy]-benzenepropanoic acid), a selective agonist for FFA4, exerts inhibitory effects on LPAand epidermal growth factor-induced proliferation and migration, similar to EPA, in DU145 and PC-3 cells. The effects of TUG-891 and EPA are readily reversible. The FFA1/FFA4 agonist GW9508 (4-[[(3-phenoxyphenyl)methyl]amino]-benzenepropranoic acid) likewise inhibits proliferation at doses that block FFA4. Knockdown of FFA4 expression prevents EPA-and TUG-891-induced inhibition of growth and migration. Together, these results indicate that activation of FFA4 initiates signaling events that can inhibit growth factor-induced signaling, providing a novel mechanism for suppression of cancer cell proliferation.

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The molecular mechanism of phytosphingosine binding to FFAR4/GPR120 differs from that of other fatty acids

et al. 2021

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Free fatty acid receptor 4 (FFAR4)/GPR120 comprises a receptor for medium-and long-chain fatty acids. We previously identified phytosphingosine (PHS) as a novel ligand of FFAR4. Although many natural FFAR4 ligands have carboxyl groups, PHS does not, thus suggesting that binding to FFAR4 is driven by a completely different mechanism than other natural ligands such as a-linolenic acid (ALA). To test this hypothesis, we performed docking simulation analysis using a FFAR4 homology model based on a protein model derived from the crystal structure of activated turkey beta-1 adrenoceptor. The docking simulation revealed that the probable hydrogen bonds to FFAR4 differ between various ligands. In particular, binding was predicted between R264 of the FFAR4 and the oxygen of the carboxylate group in ALA, as well as between E249 of the FFAR4 and the oxygen of the hydroxy group at the C4-position in PHS. Alanine substitution at E249 (E249A) dramatically reduced PHS-induced FFAR4 activation but demonstrated a weaker effect on ALA-induced FFAR4 activation. Kinetic analysis and K m values clearly demonstrated that the E249A substitution resulted in reduced affinity for PHS but not for ALA. Additionally, we observed that sphingosine, lacking a hydroxyl group at C4-position, could not activate FFAR4. Our data show that E249 of the FFAR4 receptor is crucial for binding to the hydroxy group at the C4position in PHS, and this is a completely different molecular mechanism of binding from ALA. Because GPR120 agonists have attracted attention as treatments for type 2 diabetes, our findings may provide new insights into their development.Free fatty acid receptor 4 (FFAR4)/GPR120 comprises a receptor for medium-and long-chain fatty acids that is expressed in small intestinal endocrine cells, L cells and adipose tissue. Activation of FFAR4 promotes the secretion of glucagon-like peptide-1 (GLP-1) [1], which is known as an intestinal hormone incretin. GLP-1 was reported to suppress appetite and increase insulin secretion, exhibiting anti-diabetic effects [2][3][4]. Dipeptidyl peptidase-4, which degrades GLP-1, is known to extend the half-life of GLP-1 in

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The Pharmacology of TUG-891, a Potent and Selective Agonist of the Free Fatty Acid Receptor 4 (FFA4/GPR120), Demonstrates Both Potential Opportunity and Possible Challenges to Therapeutic Agonism

Cited by 177 publications

References 42 publications

Discovery and Characterization of a Novel Small-Molecule Agonist for Medium-Chain Free Fatty Acid Receptor G Protein-Coupled Receptor 84

Discovery and Characterization of a Novel Small-Molecule Agonist for Medium-Chain Free Fatty Acid Receptor G Protein-Coupled Receptor 84

Omega-3 Fatty Acids and Other FFA4 Agonists Inhibit Growth Factor Signaling in Human Prostate Cancer Cells

The molecular mechanism of phytosphingosine binding to FFAR4/GPR120 differs from that of other fatty acids

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