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Inhibition of the enzymes in the leukotriene and prostaglandin pathways in inflammation by 3-aryl isocoumarins
Meera Ramanan, Shweta K. Sinha, Kasireddy Sudarshan, ,
Published in Elsevier Masson SAS
2016
PMID: 27597418
Volume: 124
   
Pages: 428 - 434
Abstract
The biosynthesis of leukotrienes in one of the arachidonic acid pathways and PGE2in the other by 5-LOX and mPGES1 respectively, play pivotal roles in augmenting inflammatory responses. PGE2is known to participate in cancer pathological processes as well. Isocoumarins are natural compounds with a wide range of biological activities. In this study, 3-aryl isocoumarin derivatives are synthesized and tested against 5-LOX enzyme in vitro and PGE2production in HeLa cells. Most of the compounds show high activity, and 1c is identified as a dual inhibitor with an IC50of 4.6 ± 0.26 μM and 6.3 ± 0.13 μM against 5-LOX and PGE2production respectively. Another compound 7f, exhibits an IC50of 12.4 ± 0.14 μM against 5-LOX. Further investigations reveal that the mechanism of action of 1c and 7f against 5-LOX is mixed and competitive modes of action respectively. Thunberginol (7c) exhibits IC50of 15.8 ± 0.03 μM against PGE2production. 1c and 7c inhibit the mRNA expression of mPGES1 and COX-2. The study has identified a novel scaffold, 1c with a dual inhibitory activity which can be further optimized to compete against Licofelone which is under clinical trials (with IC50of 6.0 μM for mPGES1 & 0.2 μM for 5-LOX). To conclude, 3-aryl isocoumarin derivatives appears as promising tools to fight against inflammatory diseases as well as cancer. © 2016 Elsevier Masson SAS
About the journal
JournalData powered by TypesetEuropean Journal of Medicinal Chemistry
PublisherData powered by TypesetElsevier Masson SAS
ISSN02235234
Open AccessNo
Concepts (59)
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    ARACHIDONATE 5 LIPOXYGENASE
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    Ascorbic acid
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    CYCLOOXYGENASE 1
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    CYCLOOXYGENASE 2
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    ISOCOUMARIN DERIVATIVE
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    LEUKOTRIENE
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    LICOFELONE
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    Messenger rna
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    Polycyclic aromatic hydrocarbon derivative
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    PROSTAGLANDIN
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    PROSTAGLANDIN E SYNTHASE 1
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    PROSTAGLANDIN E2
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    THUNBERGINOL
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    Unclassified drug
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    ZILEUTON
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    ARACHIDONATE 5 LIPOXYGENASE
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    ARACHIDONIC ACID
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    Cytokine
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    Free radical
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    ISOCOUMARIN DERIVATIVE
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    LEUKOTRIENE
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    Lipoxygenase inhibitor
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    PROSTAGLANDIN
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    PROSTAGLANDIN E2
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    Article
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    Controlled study
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    Drug mechanism
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    Drug synthesis
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    Enzyme inhibition
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    Gene expression
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    Hela cell line
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    IC50
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    In vitro study
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    Inflammation
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    Nonhuman
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    PROSTAGLANDIN SYNTHESIS
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    Biosynthesis
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    Chemistry
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    Drug effects
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    Enzymology
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    Gene expression regulation
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    Genetics
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    Human
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    Kinetics
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    Metabolism
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    Synthesis
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    ARACHIDONATE 5-LIPOXYGENASE
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    ARACHIDONIC ACID
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    Cytokines
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    DINOPROSTONE
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    Free radicals
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    Gene expression regulation, enzymologic
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    Hela cells
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    Humans
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    ISOCOUMARINS
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    LEUKOTRIENES
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    LIPOXYGENASE INHIBITORS
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    PROSTAGLANDINS
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    Rna, messenger