Cytochrome P-450-dependent oxygenation of arachidonic acid to hydroxyicosatetraenoic acids.

Capdevila, Jorge H.; Marnett, Lawrence J.; Chacos, N.; Prough, Russell A.; Estabrook, Ronald W.

doi:10.1073/pnas.79.3.767

Cited by 141 publications

(62 citation statements)

References 23 publications

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“…The current results now suggest that AA conversion to products of the 12-LO pathway is a key step in All induced action in the adrenal gland. Our results showing no inhibition of 12-HETE with two structurally distinct cytochrome P450 inhibitors suggests that 12-HETE formation in the rat adrenal glomerulosa cell is not via the P450 epoxygenase system described by others in the kidney and liver (42)(43)(44). However, additional studies will be needed to fully clarify whether other AA metabolites such as epoxides play any role in aldosterone synthesis.…”

Section: Discussionmentioning

confidence: 82%

Specific action of the lipoxygenase pathway in mediating angiotensin II-induced aldosterone synthesis in isolated adrenal glomerulosa cells.

Nadler

Natarajan²,

Stern³

1987

J. Clin. Invest.

128

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Angiotensin II (All) in adrenal glomerulosa cells activates phospholipase C resulting in the formation of inositol phosphates and diacylglycerol rich in arachidonic acid (AA). Although glomerulosa cells can metabolize AA via cyclooxygenase (CO), this pathway plays little role in aldosterone synthesis. Recent evidence suggests that the lipoxygenase (LO) pathway may be important for hormonal secretion in endocrine tissues such as the islet of Langerhans. However, the capacity of the glomerulosa cell to synthesize LO products and their role in aldosterone secretion is not known. To study this, the effect of nonselective and selective LO inhibitors on All, ACTH, and potassium-induced aldosterone secretion and LO product formation was evaluated in isolated rat glomerulosa cells. BW755c, a nonselective LO inhibitor dose dependently reduced the AII-stimulated level of aldosterone without altering All binding (91±6 to 36±4 ng/106 cells/h 10-' M, P < 0.001). The same effect was observed with another nonselective LO blocker, phenidone, and a more selective 12-LO inhibitor, Baicalein. In contrast U-60257, a selective 5-LO inhibitor did not change the All-stimulated levels of aldosterone (208±11% control, All 10-9 M vs. 222±38%, All + U-60257). The LO blockers action was specific for All since neither BW755c nor phenidone altered ACTH or K+-induced aldosterone secretion. All stimulated the formation of the 12-LO product 12-hydroxyeicosatetraenoic acid as measured by ultraviolet detection and HPLC in AA loaded cells and by a specific RIA in unlabeled cells (501±50 to 990±10 pg/105 cells, P < 0.02). BW755c prevented the Allmediated rise in 12-HETE formation. In contrast, neither ACTH nor K+ increased 12-HETE levels. The addition of 12-HETE or its unstable precursor 12-HPETE (10-9 or 10' M) completely restored All action during LO blockade. All also produced an increase in 15-HETE formation, but the 15-LO products had no effect on aldosterone secretion. These studies suggest that the 12-LO pathway plays a key role as a new specific mediator of All-induced aldosterone secretion.

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Section: Discussionmentioning

confidence: 82%

Specific action of the lipoxygenase pathway in mediating angiotensin II-induced aldosterone synthesis in isolated adrenal glomerulosa cells.

Nadler

Natarajan²,

Stern³

1987

J. Clin. Invest.

128

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“…7 B; 8). Coinjection of an aliquot of the biological material with a known quantity of synthetic [5,6,8,9,11,12,14,1 5-2H] 14,1 5-EET-PFB shows the presence in the mixture of the EET-PFB-derived ion fragments at m/z 319, 303, and 301, and of an ion fragment at m/z 327, derived from the loss of PFB from the octadeuterated standard (Fig. 8 B).…”

Section: Methodsmentioning

confidence: 99%

“…AA can be metabolized by three distinct enzymatic pathways: (a) by cyclooxygenase to form biologically active PGs and TXs; (b) by lipoxygenases to form hydroperoxy fatty acids, monohydroxy fatty acids, and leukotrienes; and (c) by a recently described cytochrome P450 NADPH-dependent epoxygenase (5)(6)(7)(8)(9)(10). This third pathway of AA metabolism has been documented in the kidney (5,7,8).…”

Section: Introductionmentioning

confidence: 99%

Cytochrome P450 metabolites of arachidonic acid are potent inhibitors of vasopressin action on rabbit cortical collecting duct.

Hirt¹,

Capdevila²,

Falck³

et al. 1989

J. Clin. Invest.

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AA is metabolized by a cytochrome P450, NADPH-dependent epoxygenase to four regioisomeric epoxyeicosatrienoic acids (EETs). The EETs are further hydrated enzymatically to their respective diols, vic-dihydroxyeicosatrienoic acids (DHETs). We studied the effect of pretreatment with DHETs on 10 ,gU/cm2 arginine vasopressin (AVP)-stimulated hydraulic conductivity (Lp) (Lp X 10' cm/atm/s, mean±SE) in rabbit cortical collecting ducts (CCDs) perfused in vitro at 370C. At 10-6 M all four DHETs were potent inhibitors of the hydroosmotic effect of AVP. 14,15-DHET was the most potent isomer; it reduced AVP-induced Lp from a control value of 234.75±11.7, n = 17, to a value of 95.2±8.39, n = 5, P < 0.0001, a reduction of AVP-mediated water flow of 60%. The inhibitory effect of 14,15-DHET was dose dependent and significant to nanomolar concentrations. 14,15-DHET at 10-' M was as potent an inhibitor of AVP's activity as was 10-' M PGE2. AVP's hydroosmotic effect is mediated through its intracellular second messenger, cAMP. 8-p-ChlorophenylthiocAMP (CcAMP) at 10' M induced a peak Lp of 189.6±11.0, n = 8; pretreatment with 10-6 M 14,15-DHET reduced CcAMP-peak Lp to 132.0±13.4, n = 5, P < 0.01, demonstrating a post-cAMP effect. Gas chromatography/mass spectroscopy suggests that EETs are present in extracts purified from CCDs. We conclude that cytochrome P450 epoxygenase eicosanoids are potent inhibitors of the hydroosmotic effect of vasopressin and are endogenous constituents of normal CCDs, the major target tissue for AVP.

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“…Epoxyeicosatrienoic acids (EETs) are cytochrome P450 metabolites of arachidonic acid (1,2). Four regioisomeric EETs (14,15-, 11,12-, 8,9-and 5,6-EETs) are synthesized by cytochrome P450.…”

mentioning

confidence: 99%

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

Park

Herrnreiter

Pfister

et al. 2018

Journal of Biological Chemistry

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Endothelium-derived epoxyeicosatrienoic acids (EETs) have numerous vascular activities mediated by G protein-coupled receptors. Long-chain free fatty acids and EETs activate GPR40, prompting us to investigate the role of GPR40 in some vascular EET activities. 14,15-EET, 11,12-EET, arachidonic acid, and the GPR40 agonist GW9508 increase intracellular calcium concentrations in human GPR40-overexpressing HEK293 cells (EC 50 = 0.58 ± 0.08 µM, 0.91 ± 0.08 µM, 3.9 ± 0.06 µM and 19 ± 0.37 nM, respectively). EETs with cisand trans-epoxides had similar activities, whereas substitution of a thiirane sulfur for the epoxide oxygen decreased the activities. 8,9-EET, 5,6-EET, and the epoxide hydrolysis products 11,12-and 14,15-vicdihydroxyeicosatrienoic acids were less active than 11,12-EET. The GPR40 antagonist GW1100 and siRNA-mediated GPR40 silencing blocked the EET-and GW9508-induced calcium increases. EETs are weak GPR120 agonists. GPR40 expression was detected in human and bovine endothelial cells (ECs), smooth muscle cells, and arteries. 11,12-EET concentration-dependently relaxed preconstricted coronary arteries; however, these relaxations were not altered by GW1100. In human ECs, 11,12-EET increased MAP kinase-mediated ERK phosphorylation, phosphorylation and levels of connexin-43 (Cx43), and expression of cyclooxygenase-2 (COX-2), all of which were inhibited by GW1100 and the MAP kinase inhibitor U0126. Moreover, siRNA-mediated GPR40 silencing decreased 11,12-EETinduced ERK phosphorylation. These results indicated that GPR40 is a low-affinity EET receptor in vascular cells and arteries. We conclude that epoxidation of arachidonic acid to EETs enhances GPR40 agonist activity and that 11,12-EET stimulation of GPR40 increases Cx43 and COX-2 expression in ECs via ERK phosphorylation. INTRODUCTIONhttp://www.jbc.org/cgi

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Cytochrome P-450-dependent oxygenation of arachidonic acid to hydroxyicosatetraenoic acids.

Cited by 141 publications

References 23 publications

Specific action of the lipoxygenase pathway in mediating angiotensin II-induced aldosterone synthesis in isolated adrenal glomerulosa cells.

Specific action of the lipoxygenase pathway in mediating angiotensin II-induced aldosterone synthesis in isolated adrenal glomerulosa cells.

Cytochrome P450 metabolites of arachidonic acid are potent inhibitors of vasopressin action on rabbit cortical collecting duct.

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

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