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Celastrol modulates inflammation through inhibition of the catalytic activity of mediators of arachidonic acid pathway: Secretory phospholipase A2 group IIA, 5-lipoxygenase and cyclooxygenase-2
Chandrasekaran Ramakrishnan
Published in Academic Press
2016
PMID: 27597642
Volume: 113
   
Pages: 265 - 275
Abstract
Elevated production of arachidonic acid (AA)-derived pro-inflammatory eicosanoids due to the concerted action of secretory phospholipase A2 group IIA (sPLA2IIA), 5-lipoxygenase (5-LOX) and cyclooxygenase-2 (COX-2) is a common feature of many inflammatory disorders. Hence, modulation of the bioactivity of these 3 enzymes is an important strategy to control inflammation. However, the failure of drugs specific for an individual enzyme (sPLA2IIA-, 5-LOX- or COX-2) and the success of 5-LOX/COX-2 dual inhibitors in effectively controlling inflammation in clinical trials prompted us to evaluate a common inhibitor for sPLA2IIA, 5-LOX and COX-2 enzymes. Celastrol, a quinone methide triterpene, was selected in this regard through molecular docking studies. We provide the first evidence for celastrol's ability to inhibit the catalytic activity of sPLA2IIA, 5-LOX and COX-2 enzymes. Celastrol significantly inhibited the catalytic activity of sPLA2IIA (IC50 = 6 μM) in vitro, which is independent of substrate and calcium concentration. In addition, celastrol inhibited the catalytic activities of 5-LOX (IC50 = 5 μM) and COX-2 (IC50 = 20 μM) in vitro; sPLA2IIA-induced edema and carrageenan-induced edema in mice; and lipopolysaccharide-stimulated production of PGE2 in human neutrophils. Thus, celastrol modulates inflammatory responses by targeting multiple enzymes of AA pathway. © 2016 Elsevier Ltd
About the journal
JournalPharmacological Research
PublisherAcademic Press
ISSN10436618
Open AccessNo
Concepts (62)
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    ACETYLSALICYLIC ACID
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    ARACHIDONATE 5 LIPOXYGENASE
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    ARACHIDONIC ACID
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    ARISTOLOCHIC ACID
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    CELASTROL
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    Celecoxib
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    CYCLOOXYGENASE 2
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    Diclofenac
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    Ibuprofen
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    Lipopolysaccharide
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    NORDIHYDROGUAIARETIC ACID
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    PROSTAGLANDIN E2
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    SECRETORY PHOSPHOLIPASE A2
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    SECRETORY PHOSPHOLIPASE A2 GROUP IIA
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    Unclassified drug
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    ARACHIDONATE 5 LIPOXYGENASE
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    ARACHIDONIC ACID
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    Calcium
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    CYCLOOXYGENASE 2
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    CYCLOOXYGENASE 2 INHIBITOR
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    Lipoxygenase inhibitor
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    PHOSPHOLIPASE A2 GROUP II
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    PROSTAGLANDIN E2
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    TRIPTERINE
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    Triterpene
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    Animal experiment
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    Animal model
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    Antiinflammatory activity
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    Antioxidant activity
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    Article
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    Catalysis
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    Controlled study
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    Enzyme inhibition
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    Human
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    Human cell
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    In vitro study
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    Inflammation
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    Male
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    Mouse
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    Nonhuman
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    PAW EDEMA
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    Priority journal
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    Animal
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    Drug effects
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    Edema
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    Metabolism
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    Molecular docking
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    NEUTROPHIL
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    Animals
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    ARACHIDONATE 5-LIPOXYGENASE
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    ARACHIDONIC ACID
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    CYCLOOXYGENASE 2
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    CYCLOOXYGENASE 2 INHIBITORS
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    DINOPROSTONE
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    GROUP II PHOSPHOLIPASES A2
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    Humans
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    Lipopolysaccharides
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    LIPOXYGENASE INHIBITORS
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    Mice
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    Molecular docking simulation
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    NEUTROPHILS
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    Triterpenes