1. Gene analysis indicated that soluble epoxide hydrolase 2 (sEH) was significantly upregulated in Nox4DN endothelial cells (EC). Inhibition of sEH activity in Nox4DN EC suppressed inflammation and macrophage adhesion to EC. PMID: 28185955
2. Estrogen/estrogen receptor-dependent methylation of the promoter region silences Ephx2 expression. PMID: 29295935
3. Data (including data from studies in knockout mice) suggest that expression of Ephx2 measured as mRNA, protein, and enzymatic activity is markedly up-regulated in corneal epithelium and retina in type 1 and type 2 diabetes; induction of Ephx2 may play roles in diabetic cataracts, diabetic retinopathy, and delayed wound healing. PMID: 29615440
4. These findings establish sEH in podocytes as a significant contributor to renal function under hyperglycemia. These data suggest that sEH is a potential therapeutic target for podocytopathies PMID: 28757338
5. Findings identify soluble epoxide hydrolase (sEH) in podocytes as a contributor to signaling events in acute renal injury and suggest that sEH inhibition may be of therapeutic value in proteinuria. PMID: 28485854
6. These data demonstrate that genetic deletion of sEH resulted in an altered oxylipin profile, which may have led to an enhanced CRH response. PMID: 27488890
7. Deficiency or pharmacological inhibition of sEH protected mice from the lipopolysaccharide-induced decrease in systemic arterial oxygen concentration. PMID: 27815261
8. Lungs of Ephx2(-/-) mice had a less pronounced inflammatory response and less autophagy with mild distal airspace enlargement accompanied by restored lung function and steady weight gain PMID: 28028752
9. over-expression of sEH enhances A1AR-dependent contraction and reduces KATP channel-dependent relaxation in MAs. These results suggest a possible interaction between sEH, A1AR, and KATP channels in regulating vascular tone. PMID: 27629787
10. we identified 31 significantly expressed proteins in mouse hippocampus using proteomics analysis and constructed a protein-protein interaction network associated with EPHX2 gene knockout PMID: 26722453
11. The role of soluble epoxide hydrolase in the pathophysiology of depression and resilience to repeated social defeat stress PMID: 26976569
12. CYP-eicosanoid profiling also revealed that renal, but not plasma and hepatic, 20-HETE levels were significantly increased in sEH-KO compared to WT mice PMID: 26727266
13. Dual inhibition of c-Raf and soluble epoxide hydrolase by t-CUPM prevents mutant KrasG12D-initiated murine pancreatic carcinoma growth. PMID: 26683769
14. sEH deficiency attenuated tyrosine hydroxylase-positive cell loss in a paraquat-induced mouse model of Parkinson's. PMID: 25128026
15. Simultaneous inhibition of sEH and c-RAF prevents chronic pancreatitis and murine pancreatic intraepithelial neoplasia in LSL-KrasG(1)(2)D/Pdx-1-Cre mice. PMID: 26722025
16. Suggest role for Ephx2 in vascular smooth muscle phenotypic modulation and migration in the development of atherosclerosis. PMID: 26453326
17. Sex-different regulation of sEH accounts for sex differences in flow-mediated dilation of microvessels in gonadally intact mice. PMID: 26453332
18. HS-induced contraction in A2AAR(-/-) mice was attenuated by sEH inhibitor.. the contribution of EETs, PPARgamma and KATP channels downstream of A2AAR to mediate enhanced vascular relaxation in response to HS diet PMID: 25739357
19. Suggest that sEH inhibition may be a promising strategy to treat atherosclerotic vascular disease. PMID: 25733327
20. Soluble epoxide hydrolase inhibition improves coronary endothelial function and prevents cardiac remodeling and diastolic dysfunction in obese insulin-resistant mice. PMID: 25724490
21. Compared with pharmacological inhibition of sEH, EPHX2 deletion caused the shift in arachidonic acid metabolism, which may led to pathological cardiac remodeling, especially cardiac fibrosis. PMID: 24718617
22. Soluble epoxide hydrolase inhibitor attenuates inflammation and airway hyperresponsiveness in mice. PMID: 24922186
23. Post-exposure administration of diazepam combined with soluble epoxide hydrolase inhibition stops seizures and modulates neuroinflammation in a murine model of acute TETS intoxication. PMID: 25448683
24. These results demonstrate a critical interaction of these two lipid metabolism pathways on tumorigenesis and suggest dual inhibition of COX-2 and sEH as a potential therapeutic strategy for cancer therapy. PMID: 25024195
25. These observations reveal that lipid electrophiles such as NO2-OA mediate antihypertensive signaling actions by inhibiting sEH and suggest a mechanism accounting for protection from hypertension afforded by the Mediterranean diet. PMID: 24843165
26. Increases in Ephx2 and antioxidative programming are key factors in the development of type 1 diabetic cardiomyopathy in Akita mice. PMID: 23848590
27. Ephx2 deficiency has significant contribution in coordination of ambulatory movements and working spatial memory in the mouse. PMID: 22922090
28. We conclude that type 1 diabetes mellitus upregulates soluble epoxide hydrolase mRNA and decreases concentrations of neuroprotective epoxyeicosatrienoic acids within the brain, leading to worse stroke outcome. PMID: 23899929
29. Chronic inhibition of Ephx2 lowers blood pressure in patients with renovascular hypertension. PMID: 22948718
30. Females are more susceptible to enhanced ischemic damage as a result of increased endothelial soluble epoxide hydrolase than males, especially in end-arteriolar striatal region. PMID: 23585883
31. Expression of Ephx2 appears cardioprotective; data from Ephx2 knockout mice suggest that synthesis of epoxyeicosatrienoic acids appear to prevent down-regulation of caveolin-1 from plasma membrane/caveolae/mitochondria in ischemia-reperfusion injury. PMID: 23403888
32. sEH is a physiological modulator of ER stress and a potential target for mitigating complications associated with obesity PMID: 23576437
33. demonstrated that potentiation of the cytochrome P450 (CYP) epoxy-genase pathway by either exogenous CYP-derived epoxyeicosatrienoic acids or sEH deletion significantly accelerated wound epithelialization in vivo PMID: 23122666
34. the importance of sEH in MCP-1-regulated monocyte chemotaxis PMID: 23160182
35. These results indicate that sEH gene deficiency or inhibition reduces inflammatory activities in the IL-10 (-/-) mouse model of inflammatory bowel disease. PMID: 22588244
36. investigation of role of cytoplasmic Ephx2 in diabetic nephropathy using gene disruption techniques: Streptozotocin-induced diabetic nephropathy is attenuated in Ephx2-deficient mice relative to wild-type controls. PMID: 22739108
37. Endothelial cells isolated from female cerebral microvessels are more resistant to ischemic injury, in part, because of lower sEH expression. PMID: 22723436
38. The results show that the soluble epoxide hydrolase can regulate mechanical hyperalgesia during inflammation by inactivating 8,9-EET, which sensitizes TRPA1-expressing nociceptors. PMID: 21970373
39. overexpressing the phosphatase domain of Ephx2 prevented the VEGF-mediated NO production and eNOS phosphorylation at Ser617, Ser635, and Ser1179 PMID: 22072631
40. ATF6 activation and DNA demethylation may coordinately contribute to Hcy-induced sEH expression and endothelial activation. PMID: 22354938
41. Data demonstrate that Ephx2 knockout improves endothelial function and reduces renal injury during diabetes. PMID: 21832210
42. Soluble epoxide hydrolase deficiency alters pancreatic islet size and improves glucose homeostasis in a model of insulin resistance PMID: 21571638
43. Mammalian soluble epoxide hydrolase is identical to liver hepoxilin hydrolase. PMID: 21217101
44. Redox regulation of soluble epoxide hydrolase by 15-deoxy-delta-prostaglandin J2 controls coronary hypoxic vasodilation. PMID: 21164107
45. These data demonstrate that potentiation of the CYP epoxygenase pathway by either increased endothelial EET biosynthesis or globally decreased EET hydrolysis attenuates NF-kappaB-dependent vascular inflammatory responses in vivo. PMID: 21059750
46. Promoter regions of Ephx2 are modified by soy estrogegns in prostate cancer cells. PMID: 20668305
47. Soluble epoxide hydrolase enzyme (SEH) inhibition or Ephx2 gene deletion antagonizes neointimal formation in vivo by mechanisms that are endothelium dependent. SEH inhibition may have therapeutic potential for flow-induced remodeling. PMID: 20035028
48. Inhibition of soluble epoxide hydrolase preserves cardiomyocytes in myocardial ischemic reperfusion injury. 14,15-EET-mediated protection is mediated in part by STAT3. PMID: 20008276
49. Total ovarian epoxide hydrolase activity increased following the induction of follicular development, and remained elevated through the periovulatory and postovulatory stages of a stimulated estrous cycle PMID: 15601917
50. Plasma levels of epoxy fatty acids were increased, and fatty acid diols levels were decreased, while measured levels of lipoxygenase- and cyclooxygenase-dependent oxylipins were unchanged in knockout mice. PMID: 17135253

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KEGG: mmu:13850

STRING: 10090.ENSMUSP00000069209

UniGene: Mm.15295