O-prenylated 3-carboxycoumarins as a novel class of 15-LOX-1 inhibitors

Jabbari, Atena; Mousavian, Mina; Seyedi, Seyed Mohamad; Bakavoli, Mehdi; Sadeghian, Hamid

doi:10.1371/journal.pone.0171789

Cited by 11 publications

(13 citation statements)

References 26 publications

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“…Our latest research focuses on the design, synthesis, and bioactivity evaluation of a series of 3‐aryl coumarin analogues as well as a series of prenyloxy derivatives of the natural compound umbelliferone (e.g., auraptene) (Kavetsou et al, ; Roussaki et al, ; Roussaki et al, ). The promising results of these works in combination with the literature data (Dos Santos Nascimento et al, ; Ibrar, Shehzadi, Saeed, & Khan, ; Jabbari, Mousavian, Seyedi, Bakavoli, & Sadeghian, ), which reveal the role of the phenyl group at the prenylated coumarin's skeleton (Wiart, ), as well as the role of different substitutions on the phenyl group of an acetyloxy coumarin (Musa, Latinwo, Joseph, & Badisa, ), led us to design new series of coumarin analogues which combine the 3‐aryl substituent and acetyloxy‐/hydroxy‐ or geranyloxy moiety in order to investigate the effect of the presence of these groups on the biological activity (Scheme ).…”

Section: Resultsmentioning

confidence: 76%

Novel 3‐aryl‐5‐substituted‐coumarin analogues: Synthesis and bioactivity profile

Kavetsou

Katopodi

Argyri

et al. 2020

Drug Development Research

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Eighteen 3-aryl-5-substituted-coumarins-six 5-acetyloxy-derivatives, six 5-hydroxyderivatives, and six 5-geranyloxy-derivatives-were synthesized, structurally characterized and their antioxidant activity, lipoxygenase inhibitory ability, as well as their cytotoxic activity against human neuroblastoma SK-N-SH and HeLa adenocarcinoma cell lines were evaluated. The 5-acetyloxy-compounds 3a-3f were found to be the best cytotoxic agents among all the compounds studied. The bromo-substituted coumarins 3a and 3b were remarkably active against HeLa cell line showing IC 50 1.8 and 6.1 μM, respectively. Coumarin 5e possessing a geranyloxy-chain on position 5 of the coumarin scaffold presented dual bioactivity, while 5-geranyloxy-coumarin 5f was the most competent soybean lipoxygenase inhibitor of this series (IC 50 10 μM). As shown by in silico docking studies, the studied molecules present allosteric interactions with soybean lipoxygenases.

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Section: Resultsmentioning

confidence: 76%

Novel 3‐aryl‐5‐substituted‐coumarin analogues: Synthesis and bioactivity profile

Kavetsou

Katopodi

Argyri

et al. 2020

Drug Development Research

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“…This supports previous findings that the replacement of a phenyl group attached on the coumarin ring by a 2-pyridyl group or by a morpholinyl group decreased the inhibitory activity of 6- and 7-substituted coumarins against lipoxygenase [ 43 ]. Additionally, in the study of lipoxygenase inhibition by O -prenylated 3-carboxycoumarins, O -isopentenyl derivatives demonstrated no considerable lipoxygenase inhibition, while O -geranyl and O -farnesyl derivatives demonstrated potent inhibitory activity [ 44 ].…”

Section: Resultsmentioning

confidence: 99%

Lipoxygenase Inhibition Activity of Coumarin Derivatives—QSAR and Molecular Docking Study

et al. 2020

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Lipoxygenases (LOXs) are a family of enzymes found in plants, mammals, and microorganisms. In animals and plants, the enzyme has the capability for the peroxidation of unsaturated fatty acids. Although LOXs participate in the plant defense system, the enzyme’s metabolites can have numerous negative effects on human health. Therefore, many types of research are searching for compounds that can inhibit LOXs. The best quantitative structure–activity relationship (QSAR) model was obtained using a Genetic Algorithm (GA). Molecular docking was performed with iGEMDOCK. The inhibition of lipoxygenase was in the range of 7.1 to 96.6%, and the inhibition of lipid peroxidation was 7.0–91.0%. Among the synthesized compounds, the strongest inhibitor of soybean LOX-3 (96.6%) was found to be 3-benzoyl-7-(benzyloxy)-2H-chromen-2-one. A lipid peroxidation inhibition of 91.0% was achieved with ethyl 7-methoxy-2-oxo-2H-chromene-3-carboxylate. The docking scores for the soybean LOX-3 and human 5-LOX also indicated that this compound has the best affinity for these LOX enzymes. The best multiple linear QSAR model contains the atom-centered fragment descriptors C-06, RDF035p, and HATS8p. QSAR and molecular docking studies elucidated the structural features important for the enhanced inhibitory activity of the most active compounds, such as the presence of the benzoyl ring at the 3-position of coumarin’s core. Compounds with benzoyl substituents are promising candidates as potent lipoxygenase inhibitors.

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“…Enzyme preparation was down according to the pervious method which had been reported by Jabbari et al …”

Section: Methodsmentioning

confidence: 99%

“…More than 1,300 derivatives of coumarins, possessing anti‐inflammatory and anticancer properties, have been isolated from green plants, fungi, and bacteria . Several natural and synthetic derivatives of hydroxycoumarins have been reported as inhibitors of the lipo‐oxygenase pathways . Most of them inhibit the lipo‐oxygenase activity using redox mechanism with their hydroxyl groups .…”

Section: Introductionmentioning

confidence: 99%

A novel class of human 15‐LOX‐1 inhibitors based on 3‐hydroxycoumarin

et al. 2018

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Inflammations, sensitivities, and some cancers in mammals are intimately linked to the activity of lipo-oxygenase enzymes. Owing to the importance of these enzymes, mechanistic studies, product analysis, and synthesis of inhibitors have expanded. In this study, a series of hydroxycoumarins, methoxy-3-hydroxy coumarins, and 7-alkoxy-3-hydroxy coumarins were synthesized and evaluated as potential inhibitors of human 15-LOX-1. Among the synthetic coumarins, 7-methoxy-3-hydroxycoumarin derivative demonstrated potent inhibitory activity and the compound, 5f, showed the best result. Radical scavenging assessment, IC , HNMR, and DPPH bleaching results indicate that the electronic properties are the major factors for the lipo-oxygenase inhibition potency of the synthetic coumarins. Based on the theoretical studies, it was suggested that the mesomeric effect of the substituent at the seventh position of the benzene ring is one of the major factors in the stability of the oxy-radical intermediate.

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O-prenylated 3-carboxycoumarins as a novel class of 15-LOX-1 inhibitors

Cited by 11 publications

References 26 publications

Novel 3‐aryl‐5‐substituted‐coumarin analogues: Synthesis and bioactivity profile

Novel 3‐aryl‐5‐substituted‐coumarin analogues: Synthesis and bioactivity profile

Lipoxygenase Inhibition Activity of Coumarin Derivatives—QSAR and Molecular Docking Study

A novel class of human 15‐LOX‐1 inhibitors based on 3‐hydroxycoumarin

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