Dietary Fatty Acids and Their Potential for Controlling Metabolic Diseases Through Activation of FFA4/GPR120

Ulven, Trond; Christiansen, Elisabeth

doi:10.1146/annurev-nutr-071714-034410

Cited by 95 publications

(95 citation statements)

References 142 publications

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“…The insulin sensitising and anti-inflammatory actions of GPR120, which is a receptor for n-3 polyunsaturated fatty acids [2][3], is unlikely to be modified by IL-33 contrary to what has been projected with IL-1β and TNFα [7]. The intracellular signalling pathways linked to the IL-33 receptor, ST2 (and its co-receptor IL-1 receptor accessory protein) [15], which are expressed in human adipocytes [11], would appear to be implicated in the modulation of the transcription of the GPR84 gene, but not GPR120.…”

Section: Discussionmentioning

confidence: 99%

“…Several G-protein coupled receptors act as sensors/receptors for fatty acids [1][2]. GPR120 (or FFAR4), is a receptor for n-3 polyunsaturated fatty acids, and has been linked to the antiinflammatory action of these lipids [2][3].…”

Section: Introductionmentioning

confidence: 99%

“…GPR120 (or FFAR4), is a receptor for n-3 polyunsaturated fatty acids, and has been linked to the antiinflammatory action of these lipids [2][3]. The primary ligands for GPR41 (FFAR3) and GPR43 (FFAR2) are short chain fatty acids, while GPR40 (FFAR1) is activated by medium and long chain saturated and mono-unsaturated fatty acids [1][2]. GPR84 (EX33), a pro-inflammatory receptor, is also activated by medium chain fatty acids [4][5].…”

Section: Introductionmentioning

confidence: 99%

“…GPR84 (EX33), a pro-inflammatory receptor, is also activated by medium chain fatty acids [4][5]. Each of these GPCRs has a distinct tissue distribution, with GPR120 being strongly expressed in both adipocytes and macrophages (M1 and M2) in white adipose tissue, where it promotes adipogenesis [6] in addition to insulin sensitising and anti-inflammatory actions [2][3]. Adipocytes also express GPR84, and at least in the case of human fat cells GPR40, GPR41 and GPR43, albeit at low levels [7].…”

Section: Introductionmentioning

confidence: 99%

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IL-33 stimulates expression of the GPR84 (EX33) fatty acid receptor gene and of cytokine and chemokine genes in human adipocytes

et al. 2018

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Expression of GPCR fatty acid sensor/receptor genes in adipocytes is modulated by inflammatory mediators, particularly IL-1β. In this study we examined whether the IL-1 gene superfamily member, IL-33, also regulates expression of the fatty acid receptor genes in adipocytes. Human fat cells, differentiated from preadipocytes, were incubated with IL-33 at three different dose levels for 3 or 24 h and mRNA measured by qPCR. Treatment with IL-33 induced a dose-dependent increase in GPR84 mRNA at 3 h, the level with the highest dose being 13.7-fold greater than in controls. Stimulation of GPR84 expression was transitory; the mRNA level was not elevated at 24 h. In contrast to GPR84, IL-33 had no effect on GPR120 expression. IL-33 markedly stimulated expression of the IL1B, CCL2, IL6, CXCL2 and CSF3 genes, but there was no effect on ADIPOQ expression. The largest effect was on CSF3, the mRNA level of which increased 183-fold over controls at 3 h with the highest dose of IL-33;there was a parallel increase in the secretion of G-CSF protein into the medium. It is concluded that in human adipocytes IL-33, which is synthesised in adipose tissue, has a strong stimulatory effect on the expression of cytokine and chemokine genes, particularly CSF3, and on the expression of GPR84, a pro-inflammatory fatty acid receptor.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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IL-33 stimulates expression of the GPR84 (EX33) fatty acid receptor gene and of cytokine and chemokine genes in human adipocytes

et al. 2018

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“…Macrophages directly participate in the process of obesity-induced chronic low-grade inflammation, which is tightly associated with macrophage infiltration into peripheral tissues and the pathogenesis of insulin resistance [32,33] . Recent research has indicated that GPR120 plays an important role in energy homeostasis, chronic inflammation and insulin resistance and represents a promising target for obesity and type 2 diabetes (T2DM) therapy [34] . In the present study, LPS-induced production of NO, TNF-α and IL-6 as well as expression of iNOS and COX-2 tended to be reduced by ALA. Incubation with Rb2 prior to ALA treatment dramatically amplified the inhibitory effect of ALA, leading to statistically significantly lower levels of these cytokines and pro-inflammatory enzymes than with ALA treatment alone.…”

Section: Discussionmentioning

confidence: 99%

Ginsenoside Rb2 enhances the anti-inflammatory effect of ω-3 fatty acid in LPS-stimulated RAW264.7 macrophages by upregulating GPR120 expression

Huang

Wang

2016

Acta Pharmacol Sin

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Recent studies confirm that chronic low-grade inflammation is closely associated with metabolic syndromes, and anti-inflammatory therapy is a potential approach for treating cardiovascular diseases and type 2 diabetes. Accumulating evidence suggests that GPR120 activation is a feasible solution to ameliorating chronic inflammation and improving glucose metabolism. In this study we investigated whether ginsenoside Rb2 (Rb2), which exhibited regulatory activities in glucose and lipid metabolism, affected GPR120 expression in lipopolysaccharide (LPS)-activated mouse macrophage RAW264.7 cells, and examined the contribution of GPR120 activation to reducing the LPS-induced inflammatory response. LPS (100 ng/mL) activated the macrophages, resulting in dramatic increases in TNF-α, IL-6, IL-1β and NO production. Treatment with a ω-3 fatty acid α-linolenic acid (ALA, 50 μmol/L) produced moderate reduction in LPS-stimulated inflammatory cytokines and NO production (TNF-α and IL-6 were decreased by 46% and 42%, respectively). Preincubation with Rb2 (1 or 10 μmol/L) for 12 h before ALA treatment dramatically amplified the inhibitory effects of ALA (TNF-α and IL-6 were decreased by 74% and 86%, respectively). Compared to the treatment with ALA alone, pre-incubation with Rb2 resulted in a more prominent reduction in LPS-stimulated expression of iNOS and COX-2 and LPS-stimulated IKK/NF-κB phosphorylation and MAPK pathway activation. Rb2 (0.1-100 μmol/L) dose-and time-dependently increased both mRNA and protein expression of GPR120 in RAW264.7 cells, but treatment with Rb2 alone did not exert anti-inflammatory effect in LPS-activated RAW264.7 cells. In RAW264.7 cells transfected with GPR120 shRNA, the ameliorating effects of Rb2 on LPS-induced inflammation were abolished. In conclusion, Rb2 exerts anti-inflammatory effect in LPS-stimulated mouse macrophage RAW264.7 cells in vitro by increasing GPR120 expression and subsequently enhancing ω-3 fatty acid-induced GPR120 activation.

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2‐Arachidonoyl glycerol potently induces cholecystokinin secretion in murine enteroendocrine STC‐1 cells via cannabinoid receptor CB1

Ochiai

Hirooka²,

Sakaino³

et al. 2021

Lipids

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Cholecystokinin (CCK) is a peptide hormone secreted from enteroendocrine cells and regulates the exocrine pancreas, gastric motility, and appetite. Dietary triacylglycerols are hydrolyzed to fatty acids (FA) and 2‐monoacylglycerols (2‐MAG) in the small intestine. Although it is well known that FA stimulate CCK secretion, whether 2‐MAG have the CCK‐releasing activity remains unclear. We examined the CCK‐releasing activity of four commercially available 2‐MAG in a murine CCK‐producing cell line, STC‐1, and the molecular mechanism underlying 2‐MAG‐induced CCK secretion. CCK released from the cells was measured using ELISA. Among four 2‐MAG (2‐palmitoyl, 2‐oleoyl, 2‐linoleoyl, and 2‐arachidonoyl monoacylglycerols) examined, 2‐arachidonoyl glycerol (2‐AG) potently stimulated CCK secretion in a dose‐dependent manner. Structurally related compounds, such as 2‐arachidonoyl glycerol ether and 1‐arachidonoyl glycerol, did not stimulate CCK secretion. Both arachidonic acid and 2‐AG stimulated CCK secretion at 100 μM, but only 2‐AG did at 50 μM. 2‐AG‐induced CCK secretion but not arachidonic acid‐induced CCK secretion was attenuated by treatment with a cannabinoid receptor 1 (CB1) antagonist. These results indicate that a specific 2‐MAG, 2‐AG, directly stimulates CCK secretion via CB1.

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Dietary Fatty Acids and Their Potential for Controlling Metabolic Diseases Through Activation of FFA4/GPR120

Cited by 95 publications

References 142 publications

IL-33 stimulates expression of the GPR84 (EX33) fatty acid receptor gene and of cytokine and chemokine genes in human adipocytes

IL-33 stimulates expression of the GPR84 (EX33) fatty acid receptor gene and of cytokine and chemokine genes in human adipocytes

Ginsenoside Rb2 enhances the anti-inflammatory effect of ω-3 fatty acid in LPS-stimulated RAW264.7 macrophages by upregulating GPR120 expression

2‐Arachidonoyl glycerol potently induces cholecystokinin secretion in murine enteroendocrine STC‐1 cells via cannabinoid receptor CB1

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