GPR40 is a low-affinity epoxyeicosatrienoic acid receptor in vascular cells

Park, Soo Young; Herrnreiter, Anja; Pfister, Sandra L.; Gauthier, Kathryn M.; Falck, Benjamin; Falck, John R.; Campbell, William B.

doi:10.1074/jbc.ra117.001297

Cited by 51 publications

(39 citation statements)

References 84 publications

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“…However, we were only able to obtain H 3 -9-HODE with a very low specific activity (0.13 Ci/mMol) after HPLC isolation and purification, which impeded accurate assessments of specific binding. Other proposed EET receptors include TRPV/TRPC receptors (41)(42)(43), peroxisome-proliferatoractivated receptors (44), prostaglandin receptors (20,45), and FFAR1 (38,46). FFAR1 had very low expression in our EaHy samples (average FPKM = 0.14).…”

Section: Discussionmentioning

confidence: 84%

“…sEH shows a strong substrate preference for 14,15-EET over 11,, whereas cyclooxygenases were recently shown to metabolize 11,12-EET, but not 14,15-EET (36). 14,15-EET is a stronger inhibitor of a calcium-regulated potassium channel than 11,12-EET (37), and a stronger activator of free fatty acid receptor 1 (FFAR1, also called GPR40) (38). 11,12-EET, but not other regioisomers, caused changes in the electrical potential of rat tracheal epithelial cells (39) and enhanced endothelial cell migration and tube formation (11).…”

Section: Discussionmentioning

confidence: 99%

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Specific oxylipins enhance vertebrate hematopoiesis via the receptor GPR132

Lahvic

Ammerman

et al. 2018

Proc. Natl. Acad. Sci. U.S.A.

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Epoxyeicosatrienoic acids (EETs) are lipid-derived signaling molecules with cardioprotective and vasodilatory actions. We recently showed that 11,12-EET enhances hematopoietic induction and engraftment in mice and zebrafish. EETs are known to signal via G protein-coupled receptors, with evidence supporting the existence of a specific high-affinity receptor. Identification of a hematopoietic-specific EET receptor would enable genetic interrogation of EET signaling pathways, and perhaps clinical use of this molecule. We developed a bioinformatic approach to identify an EET receptor based on the expression of G protein-coupled receptors in cell lines with differential responses to EETs. We found 10 candidate EET receptors that are expressed in three EET-responsive cell lines, but not expressed in an EET-unresponsive line. Of these, only recombinant GPR132 showed EET-responsiveness in vitro, using a luminescence-based β-arrestin recruitment assay. Knockdown of zebrafish prevented EET-induced hematopoiesis, and marrow from GPR132 knockout mice showed decreased long-term engraftment capability. In contrast to high-affinity EET receptors, GPR132 is reported to respond to additional hydroxy-fatty acids in vitro, and we found that these same hydroxy-fatty acids enhance hematopoiesis in the zebrafish. We conducted structure-activity relationship analyses using both cell culture and zebrafish assays on diverse medium-chain fatty acids. Certain oxygenated, unsaturated free fatty acids showed high activation of GPR132, whereas unoxygenated or saturated fatty acids had lower activity. Absence of the carbon-1 position carboxylic acid prevented activity, suggesting that this moiety is required for receptor activation. GPR132 responds to a select panel of oxygenated polyunsaturated fatty acids to enhance both embryonic and adult hematopoiesis.

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Section: Discussionmentioning

confidence: 84%

Section: Discussionmentioning

confidence: 99%

Specific oxylipins enhance vertebrate hematopoiesis via the receptor GPR132

Lahvic

Ammerman

et al. 2018

Proc. Natl. Acad. Sci. U.S.A.

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“…Recently, GPR75 was proposed as a 20-HETE receptor (51) and GPR40 as a low-affinity EET receptor in vascular cells (94). If confirmed, these reports hold far-reaching significance and might portend a new golden age for the P450 eicosanoid field.…”

Section: Drug Development and Therapeutic Approachesmentioning

confidence: 98%

“…In contrast, after attempts by different groups, selective binding and trans-membrane signaling has been reported only for 14(R),15(S)-EET in guinea pig mononuclear and human U937 cells (95,96). G proteins, mitogenic kinases/phosphatases, cAMP-kinase A, prostanoids, PPAR nuclear receptors, and direct effects on ion-channel activity have been proposed as mediators of EET signaling (6,8,10,14,94); however, a membrane receptor capable of selective high-affinity EET binding and trans-membrane signaling has yet to be unequivocally identified. Complicating these efforts is the ready migration or transport of exogenously added EETs across cell membranes, as shown by their rapid esterification into cellular glycerolipids (39), raising the possibility that extracellular and/or intracellular events could mediate EET functional effects.…”

Section: The Characterization Of Mechanism(s) By Which the Aa Monooxymentioning

confidence: 99%

Thematic Review Series: Living History of Lipids The arachidonic acid monooxygenase: from biochemical curiosity to physiological/pathophysiological significance

Capdevila

Falck

2018

Journal of Lipid Research

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The initial studies of the metabolism of arachidonic acid (AA) by the cytochrome P450 (P450) hemeproteins sought to: ) elucidate the roles for these enzymes in the metabolism of endogenous pools of the FA,) identify the P450 isoforms involved in AA epoxidation and ω/ω-1 hydroxylation, and ) explore the biological activities of their metabolites. These early investigations provided a foundation for subsequent efforts to establish the physiological relevance of the AA monooxygenase and its contributions to the pathophysiology of, for example, cancer, diabetes, hypertension, inflammation, nociception, and vascular disease. This retrospective analyzes the history of some of these efforts, with emphasis on genetic studies that identified roles for the murine and genes in renal and vascular physiology and the pathophysiology of hypertension and cancer. Wide-ranging investigations by laboratories worldwide, including the authors, have established a better appreciation of the enzymology, genetics, and physiologic roles for what is now known as the third branch of the AA cascade. Combined with the development of analytical and pharmacological tools, including robust synthetic agonists and antagonists of the major metabolites, we stand at the threshold of novel therapeutic approaches for the treatment of renal injury, pain, hypertension, and heart disease.

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“…In order to test for more general functional differences between vascular cells, we examined the mRNA expression profile of mural and endothelial cells using the same single-cell mRNA dataset as above 11 across three broad categories associated with neurovascular function: contractile machinery, ion (potassium and calcium) channels and neurovascular signalling pathways (Supplementary Tables 4 & 5). The latter category included recently identified EET and 20-HETE receptors 16,17 and, given the recent finding that endothelial NMDA receptors can control vascular tone 18 , NMDA receptor subunits. Several genes showed differential expression between V1 and HC, all of which pointed to the vasculature in V1 being more contractile or responsive than in HC ( Supplementary Figure 3; Supplementary Tables 4 & 5).…”

Section: Functional Differences Between Vascular Cells In Hc and V1 Smentioning

confidence: 99%

Hippocampus has lower oxygenation and weaker control of brain blood flow than cortex, due to microvascular differences

Shaw

Bell

Boyd

et al. 2019

Preprint

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The hippocampus is essential for spatial and episodic memory but is damaged early in Alzheimer's disease and is very sensitive to hypoxia. Understanding how it regulates its oxygen supply is therefore key for designing interventions to preserve its function. However, studies of neurovascular function in the hippocampus in vivo have been limited by its relative inaccessibility.Here we compared hippocampal and visual cortical neurovascular function in awake mice, using two photon imaging of individual neurons and vessels and measures of regional blood flow and haemoglobin oxygenation. We show that blood flow, blood oxygenation and neurovascular coupling were decreased in the hippocampus compared to neocortex, because of differences in both the vascular network and pericyte and endothelial cell function. Modelling oxygen diffusion indicates that these features of the hippocampal vasculature could explain its sensitivity to damage during neurological conditions, including Alzheimer's disease, where the brain's energy supply is decreased.

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GPR40 is a low-affinity epoxyeicosatrienoic acid receptor in vascular cells

Cited by 51 publications

References 84 publications

Specific oxylipins enhance vertebrate hematopoiesis via the receptor GPR132

Specific oxylipins enhance vertebrate hematopoiesis via the receptor GPR132

Thematic Review Series: Living History of Lipids The arachidonic acid monooxygenase: from biochemical curiosity to physiological/pathophysiological significance

Hippocampus has lower oxygenation and weaker control of brain blood flow than cortex, due to microvascular differences

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