Soluble epoxide hydrolase inhibition, epoxygenated fatty acids and nociception.
- Authors
- Wagner, Karen; Inceoglu, Bora; Hammock, Bruce D
- Year
- 2011
- Journal
- Prostaglandins & other lipid mediators
- PMID
- 21854866
- DOI
- 10.1016/j.prostaglandins.2011.08.001
- PMCID
- PMC3215909
The soluble epoxide hydrolase (sEH) enzyme regulates the levels of endogenous epoxygenated fatty acid (EFA) lipid metabolites by rapidly degrading these molecules. The EFAs have pleiotropic biological activities including the modulation of nociceptive signaling. Recent findings indicate that the EFAs, in particular the arachidonic acid (AA) derived epoxyeicosatrienoic acids (EETs), the docosahexaenoic acid (DHA) derived epoxydocosapentaenoic acids (EpDPEs) and eicosapentaenoic acid (EPA) derived epoxyeicosatetraenoic acids (EpETEs) are natural signaling molecules. The tight regulation of these metabolites speaks to their importance in regulating biological functions. In the past several years work on EFAs in regard to their activities in the nervous system evolved to demonstrate that these molecules are anti-inflammatory and anti-nociceptive. Here we focus on the recent advances in understanding the effects of sEH inhibition and increased EFAs on the nociceptive system and their ability to reduce pain. Evidence of their role in modulating pain signaling is given by their direct application and by inhibiting their degradation in various models of pain. Moreover, there is mounting evidence of EFAs role in the crosstalk between major nociceptive and anti-nociceptive systems which is reviewed herein. Overall the fundamental knowledge generated within the past decade indicates that orally bioavailable small molecule inhibitors of sEH may find a place in the treatment of a number of diverse painful conditions including inflammatory and neuropathic pain.
The Arachidonic Acid CascadeA simplified depiction of the formation of major metabolite families generated from arachidonic acid. AA is metabolized by cytochrome P450 enzymes into anti-inflammatory lipid mediators while the COX and LOX enzymes produce largely pro-inflammatory metabolites. The epoxyeicosatrienoic acids (EETs) are rapidly metabolized by the soluble epoxide hydrolase enzyme (sEH) to their corresponding diols the dihydroxyeicosatrienoic acids (DHETs). Inhibitors of sEH block this degradation and stabilize EET levels in vivo while reducing DHETs. The EETs suppress the transcription of the COX-2 isozyme and thus affect the AA cascade in an unexpected manner. Key cyclooxygenase metabolites include: (PGE2) prostaglandin E2, (PGD2) prostaglandin D2, (PGI2) prostaglandin I2 (prostacyclin), (TXA) thromboxane. Key lipoxygenase metabolites include: (5-HETE) 5-Hydroxyeicosatetraenoic acid, (12-HETE) 12-Hydroxyeicosatetraenoic acid, (LTB4) leukotriene B4. Other PUFAs can enter this pathway yielding among other metabolites, a variety of EFAs.
LLM interpretation
This figure is a biochemical pathway diagram illustrating the metabolism of Arachidonic Acid. It shows three primary enzymatic branches: Cyclooxygenase producing prostaglandins and thromboxane, Lipoxygenase producing HETEs and leukotrienes, and Cytochrome P450 producing EETs. The diagram further depicts the conversion of EETs to DHETs by the enzyme sEH, which is shown to be blocked by sEH inhibitors.
A dual sEH/COX-2 inhibitor efficiently blocks painA potent dual sEH/COX-2 inhibitor significantly alleviates intraplantar LPS induced allodynia measured by a von Frey mechanical nociception test (n=6 per group). The sEHI and co-administration of celecoxib and sEHI also attenuate the allodynia but not as effectively. Doses of celecoxib (CLX), sEHI (t-AUCB), or the dual inhibitor (10 mg/kg each s.c.) were compared to a combination of CLX + t-AUCB and an LPS control. The sEHI and combination treatment were significantly anti-allodynic when compared to the LPS control (P=0.02 and P<0.001 respectively). However the sEH/COX-2 dual inhibitor significantly (P<0.001) attenuated allodynia at both time points and was more effective than celecoxib or sEHI alone and the combination. Results are presented as percent of baseline mechanical withdrawal threshold on the y-axis.
LLM interpretation
This figure consists of a grouped bar chart and chemical structures for sEHI (t-AUCB), CLX (celecoxib), and a dual inhibitor. The bar chart measures the percent of baseline mechanical withdrawal response over time (Baseline, 2 hr, and 4 hr) across five groups: CTL, CLX, sEHI, CLX + sEHI, and Dual Inhibitor. At 2 and 4 hours, the Dual Inhibitor shows the highest response percentage, with statistical significance indicated by asterisks (*P < 0.05, **P < 0.01, ***P < 0.001) compared to the control.
EFAs and epoxyeicosatrienoic acid ethanolamides (EET-EAs) share structural featuresArachidonic acid is enzymatically converted to four regioisomers of epoxyeicosatrienoic acids (EETs) by cytochrome P450s. Here one regioisomer 11,12-EET is depicted. Arachidonic acid is a precursor in the synthesis of endogenous cannabinoids anandamide and 2-arachidonyl glycerol (not shown). Once synthesized from N-arachidonoyl phosphatidylethanolamine (NAPE) anandamide can be epoxygenated by cytochrome P450s to form regioisomers of EET-EAs which have similar functional properties with anandamide. Anandamide or 2-arachidonyl glycerol upon degradation by FAAH or MAGL releases arachidonic acid as a product which can act as substrate for cytochrome P450s to be converted to EETs.
LLM interpretation
This figure is a chemical diagram illustrating two parallel biosynthetic pathways. It shows the conversion of arachidonic acid to 11,12-EET and the conversion of anandamide to 11,12-EET ethanolamide, highlighting the structural similarities between the resulting epoxyeicosatrienoic acid (EET) and its ethanolamide derivative.
Cannabinoid receptors play a role in sEHI mediated anti-nociceptionThe soluble epoxide hydrolase inhibitor AEPU administered topically significantly attenuates thermal hyperalgesia when compared to control (CTL) LPS treated rats. Male Sprague Dawley rats (n=4 per group) were administered intraplantar 10ug/paw LPS in one hind paw followed by 10mg/rat AEPU and monitored using the modified Hargreavesβ thermal hyperalgesia test. This anti-hyperalgesic effect of the sEHI AEPU is blocked by a 2mg/rat topical administration of the selective CB2 receptor antagonist AM 630. However, the CB1 selective antagonist AM 251 displays no effect on sEHI mediated anti-hyperalgesia. Results are presented as percent of baseline thermal withdrawal latency on the y-axis.
LLM interpretation
This figure consists of a chemical structure of the sEHI AEPU and a grouped bar chart showing the percent of baseline thermal withdrawal response over time (Baseline, 2 hr, and 4 hr). The data compares four groups: CTL, AEPU (sEHI), AM630 (CB2 Antagonist), and AM251 (CB1 Antagonist). AEPU and AM251 maintain higher response percentages compared to CTL at 2 and 4 hours, while AM630 reduces the effect of AEPU; statistical significance is indicated by asterisks (*) for AEPU and AM251 at 2 hours, and AEPU at 4 hours.
| Name | Type |
|---|---|
| 11,12-EET local | drug |
| 14,15-EET-EA local | drug |
| 2-AG | drug |
| 5,6-EET-EA local | drug |
| 5,6EET regioisomer local | drug |
| 7,8-EpDPE local | drug |
| AA | cohort |
| acute pain threshold local | phenotype |
| adenylyl cyclase | drug |
| AEA | drug |
| algogenic lipids local | drug |
| Algogenic lipids local | drug |
| allodynia local | phenotype |
| Allodynia local | phenotype |
| allodynic local | phenotype |
| anandamide | drug |
| anti-hyperalgesia local | phenotype |
| Anti-hyperalgesic local | phenotype |
| anti-inflammatory local | phenotype |
| Anti-inflammatory local | phenotype |
| anti-inflammatory effect local | phenotype |
| anti-nociception local | phenotype |
| anti-nociceptive local | phenotype |
| Anti-nociceptive local | phenotype |
| anti-nociceptive effect | phenotype |
| arachidonic acid | drug |
| Arachidonic acid (AA) local | drug |
| arachidonic acid cascade local | drug |
| Arachidonic acid cascade local | drug |
| ATP-sensitive potassium channel local | drug |
| axonal region local | anatomy |
| Bioactive lipid metabolites local | drug |
| Bioactive lipids local | drug |
| BKCA channels local | drug |
| body temperature regulation local | phenotype |
| brain | anatomy |
| bulbospinal analgesia local | phenotype |
| Bulbospinal analgesia local | phenotype |
| cAMP | drug |
| cannabinoid analgesic system local | drug |
| cannabinoids | drug |
| carrageenan local | drug |
| Carrageenan local | drug |
| Carrageenan induced inflammatory pain local | phenotype |
| carrageenan model local | cohort |
| CB1 receptor | drug |
| CB1 receptor agonists local | drug |
| CB2 | drug |
| CB2 receptor agonists local | drug |
| celecoxib | drug |
| Cell phospholipids local | drug |
| Cellular membranes local | drug |
| central nervous system | anatomy |
| CNS | anatomy |
| CNS side effects local | phenotype |
| Conroy et al. local | cohort |
| COX local | drug |
| COX-2 local | drug |
| COX-2 inhibitor local | drug |
| COX-2 selective compounds local | drug |
| COX enzymes local | drug |
| COX inhibitors local | drug |
| COX inhibitor side effects local | phenotype |
| COX isozymes local | drug |
| CP 55940 local | drug |
| cyclooxygenase local | drug |
| Cyclooxygenase (COX) local | drug |
| cytochrome P450 | gene |
| Cytochrome P450 local | drug |
| Cytochrome P450 enzymes local | drug |
| Cytochrome P450 enzymes | gene |
| cytochrome P450 epoxygenases local | drug |
| cytochrome reductase local | gene |
| dendrites local | anatomy |
| Descending analgesic pathway local | phenotype |
| dexamethasone | drug |
| DHA | drug |
| DHA epoxides local | drug |
| DHETs local | drug |
| diabetic neuropathic pain local | phenotype |
| dihydroxy-fatty acid degradation products local | drug |
| diols local | drug |
| Diols of linoleate epoxides local | drug |
| docosahexaenoic acid (DHA) local | drug |
| D prostanoid receptor local | drug |
| dual sEH/COX-2 inhibitor local | drug |
| EET-AE local | drug |
| EET antagonists local | drug |
| EET mimetics local | drug |
| EETs local | drug |
| EFAs local | drug |
| Eicosapentaenoic acid local | drug |
| eicosapentaenoic acid (EPA) local | drug |
| endocannabinoids | drug |
| endogenous opioids | drug |
| enkephalin | drug |
| EPA local | drug |
| EPA epoxides local | drug |
| EpDPEs local | drug |
| EPHX2 local | gene |
| Epoxide hydrolase local | drug |
| epoxides of LA local | drug |
| Epoxyeicosatrienoic acids local | drug |
| epoxyeicosatrienoic acids (EETs) local | drug |
| Epoxyeicosatrienoic acids (EETs) local | drug |
| epoxy fatty acids local | drug |
| Epoxy fatty acids local | drug |
| Epoxy-fatty acids local | drug |
| EP receptors local | drug |
| E prostanoid receptor local | drug |
| Essential fatty acids local | drug |
| Essential fatty acids (EFAs) local | drug |
| FAAH | gene |
| Fatty acid binding protein local | gene |
| fatty acids | drug |
| GABA | phenotype |
| glial cells | anatomy |
| glutamate | drug |
| G protein-coupled receptor | drug |
| GΞ±s local | drug |
| hyperalgesia | phenotype |
| hyperalgesic local | phenotype |
| hypoalgesia local | phenotype |
| Indomethacin local | drug |
| Induced pain model local | phenotype |
| inflammation | phenotype |
| inflammatory conditions local | phenotype |
| inflammatory pain local | phenotype |
| leukotrienes local | drug |
| Leukotrienes local | drug |
| Linoleate epoxide diols local | drug |
| Linoleate epoxides local | drug |
| linoleic acid | drug |
| Linolenic acid | drug |
| lipolysis local | drug |
| lipoxygenase local | drug |
| Lipoxygenase (LOX) local | drug |
| Long-chain polyunsaturated fatty acids (PUFAs) local | drug |
| LOX local | drug |
| LOX | gene |
| LOX enzymes local | drug |
| LPS | drug |
| LPS induced inflammatory pain model local | cohort |
| MAGL | gene |
| mechanical allodynia | phenotype |
| Mechanical withdrawal behavior local | phenotype |
| mechanical withdrawal response local | phenotype |
| Membrane phosphoglyceride subclasses local | drug |
| methyl esters of EETs local | drug |
| morphine | drug |
| mouse brain | anatomy |
| mouse model of sepsis local | cohort |
| murine sepsis model local | cohort |
| NAPE local | drug |
| Narcotic agents local | drug |
| neuronal cells | phenotype |
| neuropathic pain | phenotype |
| neurosteroids | drug |
| NF-ΞΊB | gene |
| NFΞΊB pathway local | drug |
| NMDA antagonist | drug |
| nociception | phenotype |
| nociceptive behavior local | phenotype |
| nociceptive thresholds | phenotype |
| normal animals local | cohort |
| Normal rats local | cohort |
| NSAIDs | drug |
| opioid | drug |
| opioid agonists local | drug |
| Opioid agonists local | drug |
| opioid analgesic system local | drug |
| Opioid mediated analgesia local | phenotype |
| opioid receptor | drug |
| Oxylipins local | drug |
| P450 enzymes local | gene |
| pain | phenotype |
| pain not dependent on inflammation local | phenotype |
| pain related behavior local | phenotype |
| pain-related behavior local | phenotype |
| Pain-related behavior local | phenotype |
| PDE4 local | drug |
| PDE5 local | drug |
| PDEIs local | drug |
| PGE2 | drug |
| Phospholipase A2 | drug |
| phospholipids local | drug |
| picrotoxin | drug |
| PKA | drug |
| pro-inflammatory local | phenotype |
| Pro-inflammatory local | phenotype |
| pro-nociceptive local | phenotype |
| prostacyclin local | drug |
| prostaglandin E2 | drug |
| Prostaglandins | drug |
| prostanoids local | drug |
| Prostanoids local | drug |
| protein kinase A | drug |
| PTGS2 | gene |
| pyresis local | phenotype |
| rat model of inflammatory pain local | cohort |
| rats | cohort |
| rodent pain studies local | cohort |
| rodents | cohort |
| rofecoxib local | drug |
| rolipram | drug |
| sEH local | drug |
| sEH local | gene |
| sEH/COX-2 inhibitor local | drug |
| sEHI local | drug |
| sEHI+ rolipram combination local | drug |
| sEHIs local | drug |
| Selective COX inhibitors local | drug |
| sepsis | phenotype |
| signal transduction | phenotype |
| soluble epoxide hydrolase local | drug |
| soluble epoxide hydrolase inhibitor local | drug |
| soluble epoxide hydrolase inhibitors local | drug |
| soluble epoxide hydrolase (sEH) local | drug |
| spinal cord | anatomy |
| steroids local | drug |
| Steroids local | drug |
| Streptozocin local | drug |
| Terashvili et al. local | cohort |
| thermal tail flick latency local | phenotype |
| Thermal withdrawal behavior local | phenotype |
| thermal withdrawal response local | phenotype |
| thromboxane local | drug |
| Thromboxane local | drug |
| Thromboxane receptor local | drug |
| TRP channel local | drug |
| TrpV1 | gene |
| TRPV4 local | gene |
| type 1 diabetes | phenotype |
| ventrolateral periaqueductal gray local | anatomy |
| Win 55212-2 | drug |
| Ξ²-endorphin | drug |
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External
| Title | Authors | Journal | Year | Link |
|---|---|---|---|---|
| Discovery of Phenylacylpiperidine as Novel sEH Inhibitors through Scaffold Hopping of Natural Stilbene. | Ding J et al. | β | 2025 | β |
| Targeted lipidomic reveals dietary LA/n-3 PUFAs regulate inflammation and redox status via oxylipins in bivalves. | Zhu Y et al. | β | 2025 | β |
| Attenuation of Polycyclic Aromatic Hydrocarbon (PAH)-Induced Carcinogenesis and Tumorigenesis by Omega-3 Fatty Acids in Mice In Vivo. | Xia G et al. | β | 2024 | β |
| Challenges and opportunities of developing small-molecule therapies for age-related macular degeneration. | Fei X et al. | β | 2024 | β |
| Discovery of glycosidated glycyrrhetinic acid derivatives: Natural product-based soluble epoxide hydrolase inhibitors. | Liu Q et al. | β | 2024 | β |
| Exploring the Antiangiogenic and Anti-Inflammatory Potential of Homoisoflavonoids: Target Identification Using Biotin Probes. | Fei X et al. | β | 2024 | β |
| Associations between Plasma Lipid Mediators and Chronic Daily Headache Outcomes in Patients Randomized to a Low Linoleic Acid Diet with or without Added Omega-3 Fatty Acids. | Shen Q et al. | β | 2023 | β |
| HNF4Ξ± isoforms regulate the circadian balance between carbohydrate and lipid metabolism in the liver. | Deans JR et al. | β | 2023 | β |
| A Fast and Selective Approach for Profiling Vicinal Diols Using Liquid Chromatography-Post Column Derivatization-Double Precursor Ion Scanning Mass Spectrometry. | Wan D et al. | β | 2022 | β |
| Clinical and Preclinical Evidence for Roles of Soluble Epoxide Hydrolase in Osteoarthritis Knee Pain. | Gowler PRW et al. | β | 2022 | β |
| COX-2/sEH Dual Inhibitor Alleviates Hepatocyte Senescence in NAFLD Mice by Restoring Autophagy through Sirt1/PI3K/AKT/mTOR. | Zhang CY et al. | β | 2022 | β |
| Omega-6 Polyunsaturated Fatty Acids Enhance Tumor Aggressiveness in Experimental Lung Cancer Model: Important Role of Oxylipins. | Montecillo-Aguado M et al. | β | 2022 | β |
| Soluble epoxide hydrolase inhibitors: an overview and patent review from the last decade. | Iyer MR et al. | β | 2022 | β |
| 2-(Piperidin-4-yl)acetamides as Potent Inhibitors of Soluble Epoxide Hydrolase with Anti-Inflammatory Activity. | MartΓn-LΓ³pez J et al. | β | 2021 | β |
| EETs/sEHi alleviates nociception by blocking the crosslink between endoplasmic reticulum stress and neuroinflammation in a central poststroke pain model. | Liu T et al. | β | 2021 | β |
| Endocannabinoids and aging-Inflammation, neuroplasticity, mood and pain. | Park Y et al. | β | 2021 | β |
| Inhibition of the Soluble Epoxide Hydrolase as an Analgesic Strategy: A Review of Preclinical Evidence. | Wang Y et al. | β | 2021 | β |
| Longitudinal exposure to consumer product chemicals and changes in plasma oxylipins in pregnant women. | Welch BM et al. | β | 2021 | β |
| Pharmacology of the Equine Foot: Medical Pain Management for Laminitis. | Hopster K et al. | β | 2021 | β |
| Species Differences in Metabolism of Soluble Epoxide Hydrolase Inhibitor, EC1728, Highlight the Importance of Clinically Relevant Screening Mechanisms in Drug Development. | McReynolds CB et al. | β | 2021 | β |
| A large-scale genome-wide association study meta-analysis of cannabis use disorder. | Johnson EC et al. | β | 2020 | β |
| Cytochrome P450 Metabolism of Polyunsaturated Fatty Acids and Neurodegeneration. | Sarparast M et al. | β | 2020 | β |
| Epoxy Fatty Acids Are Promising Targets for Treatment of Pain, Cardiovascular Disease and Other Indications Characterized by Mitochondrial Dysfunction, Endoplasmic Stress and Inflammation. | McReynolds C et al. | β | 2020 | β |
| Small Molecule Soluble Epoxide Hydrolase Inhibitors in Multitarget and Combination Therapies for Inflammation and Cancer. | Das Mahapatra A et al. | β | 2020 | β |
| Yunnan Baiyao diminishes lipopolysaccharide-induced inflammation in osteoclasts. | Ren X et al. | β | 2020 | β |
| COX-2/sEH Dual Inhibitor PTUPB Potentiates the Antitumor Efficacy of Cisplatin. | Wang F et al. | β | 2018 | β |
| Design and Potency of Dual Soluble Epoxide Hydrolase/Fatty Acid Amide Hydrolase Inhibitors. | Kodani SD et al. | β | 2018 | β |
| Endocannabinoids, exercise, pain, and a path to health with aging. | Watkins BA | β | 2018 | β |
| Identification and optimization of soluble epoxide hydrolase inhibitors with dual potency towards fatty acid amide hydrolase. | Kodani SD et al. | β | 2018 | β |
| LC-MS/MS Analysis of the Epoxides and Diols Derived from the Endocannabinoid Arachidonoyl Ethanolamide. | Rand AA et al. | β | 2018 | β |
| Orally Available Soluble Epoxide Hydrolase/Phosphodiesterase 4 Dual Inhibitor Treats Inflammatory Pain. | BlΓΆcher R et al. | β | 2018 | β |
| Pharmacokinetics and antinociceptive effects of the soluble epoxide hydrolase inhibitor t-TUCB in horses with experimentally induced radiocarpal synovitis. | Guedes AGP et al. | β | 2018 | β |
| Basic/Translational Development of Forthcoming Opioid- and Nonopioid-Targeted Pain Therapeutics. | Knezevic NN et al. | β | 2017 | β |
| Modulation of innate immunity of patients with Alzheimer's disease by omega-3 fatty acids. | Fiala M et al. | β | 2017 | β |
| Pain Management in Horses. | Guedes A | β | 2017 | β |
| Soluble epoxide hydrolase activity and pharmacologic inhibition in horses with chronic severe laminitis. | Guedes A et al. | β | 2017 | β |
| Circulating levels of endocannabinoids and oxylipins altered by dietary lipids in older women are likely associated with previously identified gene targets. | Watkins BA et al. | β | 2016 | β |
| Genetic enhancement of microsomal epoxide hydrolase improves metabolic detoxification but impairs cerebral blood flow regulation. | Marowsky A et al. | β | 2016 | β |
| A multimodal disease modifying approach to treat neuropathic pain--inhibition of soluble epoxide hydrolase (sEH). | Pillarisetti S et al. | β | 2015 | β |
| Buthionine sulfoximine, an inhibitor of glutathione biosynthesis, induces expression of soluble epoxide hydrolase and markers of cellular hypertrophy in a rat cardiomyoblast cell line: roles of the NF-ΞΊB and MAPK signaling pathways. | Abdelhamid G et al. | β | 2015 | β |
| Cytochrome p450 enzymes in the bioactivation of polyunsaturated Fatty acids and their role in cardiovascular disease. | Westphal C et al. | β | 2015 | β |
| Cytochrome P450 epoxygenase pathway of polyunsaturated fatty acid metabolism. | Spector AA et al. | β | 2015 | β |
| Omeprazole increases the efficacy of a soluble epoxide hydrolase inhibitor in a PGEβ induced pain model. | Goswami SK et al. | β | 2015 | β |
| Oral treatment of rodents with soluble epoxide hydrolase inhibitor 1-(1-propanoylpiperidin-4-yl)-3-[4-(trifluoromethoxy)phenyl]urea (TPPU): Resulting drug levels and modulation of oxylipin pattern. | Ostermann AI et al. | β | 2015 | β |
| The 2014 Bernard B. Brodie award lecture-epoxide hydrolases: drug metabolism to therapeutics for chronic pain. | Kodani SD et al. | β | 2015 | β |
| A lipid gate for the peripheral control of pain. | Piomelli D et al. | β | 2014 | β |
| Stabilized epoxygenated fatty acids regulate inflammation, pain, angiogenesis and cancer. | Zhang G et al. | β | 2014 | β |
| Beneficial effects of inhibition of soluble epoxide hydrolase on glucose homeostasis and islet damage in a streptozotocin-induced diabetic mouse model. | Chen L et al. | β | 2013 | β |
| Impact of soluble epoxide hydrolase and epoxyeicosanoids on human health. | Morisseau C et al. | β | 2013 | β |
| Rationally designed multitarget agents against inflammation and pain. | Hwang SH et al. | β | 2013 | β |
| Role of epoxide hydrolases in lipid metabolism. | Morisseau C | β | 2013 | β |
| Soluble epoxide hydrolase: gene structure, expression and deletion. | Harris TR et al. | β | 2013 | β |
| Synthesis and biological activity of 4-substituted benzoxazolone derivatives as a new class of sEH inhibitors with high anti-inflammatory activity in vivo. | Tang L et al. | β | 2013 | β |
| Temporal changes of cytochrome P450 (Cyp) and eicosanoid-related gene expression in the rat brain after traumatic brain injury. | Birnie M et al. | β | 2013 | β |
| Therapeutic activity of inhibition of the soluble epoxide hydrolase in a mouse model of scrapie. | Poli G et al. | β | 2013 | β |
| Use of a soluble epoxide hydrolase inhibitor as an adjunctive analgesic in a horse with laminitis. | Guedes AG et al. | β | 2013 | β |