Coupling between Cyclooxygenase, Terminal Prostanoid Synthase, and Phospholipase A2

Ueno, Noriko; Murakami, Makoto; Tanioka, Toshihiro; Fujimori, Ko; Tanabe, Tadashi; Urade, Yoshihiro; Kudo, Ichiro

doi:10.1074/jbc.m100429200

Cited by 178 publications

(125 citation statements)

References 65 publications

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“…COX-1 appeared to be distributed rather uniformly throughout the ER membrane, whereas COX-2 was enriched in the perinuclear region. Similar locations of these enzymes were seen in HEK293 cells, as described previously (14,16).…”

Section: Mpges-2 and Pge 2 Productionsupporting

confidence: 51%

Cellular Prostaglandin E2 Production by Membrane-bound Prostaglandin E Synthase-2 via Both Cyclooxygenases-1 and -2

Murakami

Nakashima

Kamei

et al. 2003

Journal of Biological Chemistry

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313

308

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Current evidence suggests that two forms of prostaglandin (PG) E synthase (PGES), cytosolic PGES and membrane-bound PGES (mPGES) -1, preferentially lie downstream of cyclooxygenase (COX) -1 and -2, respectively, in the PGE 2 biosynthetic pathway. In this study, we examined the expression and functional aspects of the third PGES enzyme, mPGES-2, in mammalian cells and tissues. mPGES-2 was synthesized as a Golgi membrane-associated protein, and spontaneous cleavage of the N-terminal hydrophobic domain led to the formation of a truncated mature protein that was distributed in the cytosol with a trend to be enriched in the perinuclear region. In several cell lines, mPGES-2 promoted PGE 2 production via both COX-1 and COX-2 in the immediate and delayed responses with modest COX-2 preference. In contrast to the marked inducibility of mPGES-1, mPGES-2 was constitutively expressed in various cells and tissues and was not increased appreciably during tissue inflammation or damage. Interestingly, a considerable elevation of mPGES-2 expression was observed in human colorectal cancer. Collectively, mPGES-2 is a unique PGES that can be coupled with both COXs and may play a role in the production of the PGE 2 involved in both tissue homeostasis and disease.Biosynthesis of prostaglandin (PG) 1 E 2 , which is produced by a variety of cells and tissues and exhibits diverse bioactivities, is mediated by three enzymatic reactions involving phospholipase A 2 (PLA 2 ), cyclooxygenase (COX), and PGE synthase (PGES). In this biosynthetic pathway, arachidonic acid (AA) released from membrane phospholipids by cytosolic or secretory PLA 2 s is converted to PGH 2 by COX-1 or COX-2 and is then isomerized to PGE 2 by terminal PGES enzymes.The constitutive COX-1 mainly promotes immediate PG production elicited by agonists promptly mobilizing intracellular Ca 2ϩ , a situation in which a burst release of AA occurs (1-5).The inducible COX-2 is essential for delayed PG generation induced by proinflammatory stimuli, during which AA is gradually supplied over long periods, and also promotes immediate PG production if it already exists in cells primed by particular stimuli (1-5). Current studies employing isozyme-specific inhibitors and knockout mice have revealed that the two COXs play distinct roles in vivo (6 -10), and segregated utilization of these enzymes at the cellular level has been explained not only by their distinct expression profiles but also by subtle differences in their AA requirement, hydroperoxide sensitivity, and subcellular localization (4, 11-13). In addition, selective coupling with various terminal PG synthases has also been shown to influence crucially the utilization of the two COX isoforms during the different phases of cell activation (14 -16). PGES enzymes, which lie downstream of COXs, occur in multiple forms in mammalian cells (1). Among them, a perinuclear membrane-bound form of PGES belonging to the MAPEG (for membrane-associated proteins involved in eicosanoid and glutathione metabolism) family, which we herein cal...

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Section: Mpges-2 and Pge 2 Productionsupporting

confidence: 51%

Cellular Prostaglandin E2 Production by Membrane-bound Prostaglandin E Synthase-2 via Both Cyclooxygenases-1 and -2

Murakami

Nakashima

Kamei

et al. 2003

Journal of Biological Chemistry

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313

308

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“…Previous sketchy studies to focus on individual eicosanoids in EAE or MS patients have obvious limitations, as Ͼ20 different eicosanoids are produced by the concerted actions of cPLA 2 ␣ and downstream enzymes (Fig. S1) (16)(17)(18). To overcome such complexity and some controversy, we evaluated the cascade in the SCs of naive and EAE mice by the nonbiased top-down approach (AA cascade-targeted lipidomics and transcriptomics) and confirmed the results from knockout studies.…”

Section: Studies Of Experimental Autoimmune Encephalomyelitis (Eae) mentioning

confidence: 74%

“…By the AA cascadetargeted lipidomics approach, we found that the PGE 2 pathway is favored and the PGD 2 , PGI 2 , and 5-LO pathways are attenuated. Correlation analysis imply that the AA producing enzyme cPLA 2 ␣ possibly passes more AA to the COX than the 5-LO pathway in EAE, because the sequential actions of eicosanoidsynthesizing enzymes are regulated spatially and temporally in the cells, the so-called functional coupling (16)(17)(18). Likewise, PGH 2 , a common precursor of PGs, appears to be selectively consumed by the PGE 2 pathway rather than the PGI 2 and PGD 2 pathways, thereby producing PGE 2 in the SCs of EAE mice.…”

Section: Discussionmentioning

confidence: 99%

Targeted lipidomics reveals mPGES-1-PGE2 as a therapeutic target for multiple sclerosis

Kihara

Matsushita

Kita

et al. 2009

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

123

107

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The arachidonic acid (AA) cascade produces eicosanoids, such as prostaglandins (PGs), that regulate physiological and pathological functions. Although various nonsteroidal anti-inflammatory drugs have been developed, blocking upstream components (cyclooxygenase-1 and -2) of the AA cascade leads to severe side effects, including gastrointestinal ulcers and cardiovascular events, respectively, due to the complexity of the AA cascade. Here, using an AA cascade-targeted lipidomics approach, we report that microsomal PGE synthase 1 (mPGES-1) plays a key role in experimental autoimmune encephalomyelitis (EAE). Eicosanoids (mainly PGD 2) are produced constitutively in the spinal cord of naive mice. However, in EAE lesions, the PGE 2 pathway is favored and the PGD2, PGI2, and 5-lipoxygenase pathways are attenuated. Furthermore, mPGES-1 ؊/؊ mice showed less severe symptoms of EAE and lower production of IL-17 and IFN-␥ than mPGES-1 ؉/؉ mice. Expression of PGE2 receptors (EP1, EP2, and EP4) was elevated in EAE lesions and correlated with clinical symptoms. Immunohistochemistry on central nervous systems of EAE mice and multiple sclerosis (MS) patients revealed overt expression of mPGES-1 protein in microglia/macrophages. Thus, the mPGES-1-PGE 2-EPs axis of the AA cascade may exacerbate EAE pathology. Our findings have important implications for the design of therapies for MS.autoimmunity ͉ demyelination ͉ lipid mediator ͉ mass spectrometry ͉ Th17

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“…In contrast, R-flurbiprofen has similar Ab42 lowering activity to S-flurbiprofen, but much less potent COX inhibitory activity. (see for review Tegeder et al 2001b) Because HEK293 cells produce very low prostaglandin E 2 and have negligible activity of the enzymes involved in this cascade (Ueno et al 2001), the prostaglandin E 2 levels in our HEK293 culture were undetectable, although readily measured in CHO cells (data not shown). While we could not confirm the absence of COX inhibition by R-flurbiprofen in HEK293 cells, previous reports show the IC 50 for human COX-1 and COX-2 by R-flurbiprofen are more than 40 lM and 100 lM, while those of S-flurbiprofen are 0.03 lM and 0.9 lM, respectively (Geisslinger et al 2000; see for review Tegeder et al 2001b).…”

Section: Discussionmentioning

confidence: 97%

Selective inhibition of Aβ42 production by NSAID R‐enantiomers

Morita

Chu

Ubeda

et al. 2002

Journal of Neurochemistry

142

123

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Non-steroidal anti-inflammatory drugs (NSAIDs) have been associated with reduced risk for Alzheimer's disease (AD) and selected NSAIDs racemates suppress b-amyloid (Ab) accumulation in vivo and Ab42 production in vitro. Clinical use of NSAIDs for preventing or treating AD has been hampered by dose-limiting toxicity believed to be due to cyclooxygenase (COX)-inhibition that is reportedly not essential for selective Ab42 reduction. Profens have racemates and R-enantiomers were supposed to be inactive forms. Here we demonstrate that R-ibuprofen and R-flurbiprofen, with poor COX-inhibiting activity, reduce Ab42 production by human cells. Although these R-enantiomers inhibit nuclear factorjB (NF-jB) activation and NF-jB can selectively regulate Ab42, Ab42 reduction is not mediated by inhibition of NF-jB activation. Because of its efficacy at lowering Ab42 production and low toxicity profile, R-flurbiprofen is a strong candidate for clinical development.

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Coupling between Cyclooxygenase, Terminal Prostanoid Synthase, and Phospholipase A2

Cited by 178 publications

References 65 publications

Cellular Prostaglandin E2 Production by Membrane-bound Prostaglandin E Synthase-2 via Both Cyclooxygenases-1 and -2

Cellular Prostaglandin E2 Production by Membrane-bound Prostaglandin E Synthase-2 via Both Cyclooxygenases-1 and -2

Targeted lipidomics reveals mPGES-1-PGE2 as a therapeutic target for multiple sclerosis

Selective inhibition of Aβ42 production by NSAID R‐enantiomers

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