Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin

Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin

Context: Celecoxib (Cele), a nonsteroidal anti-inflammatory drug (NSAID) is linked with a spectrum of hepatotoxic influences, however the underlying mechanism (s) by which this drug induces liver damage is still unexplored. Aims: To demonstrate the hepatotoxic mechanism (s) of Cele in rats and th...

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Main Authors: Emtenan Sami Sulimani, Jehad Mustafa Yousef, Azza M. Mohamed
Format: Article
Language:English
Published: Academic Association of Pharmaceutical Sciences from Antofagasta (ASOCIFA) 2021-07-01
Series:Journal of Pharmacy & Pharmacognosy Research
Subjects:
celecoxib
inflammation
liver
melatonin
oxidative stress
quercetin
Online Access:https://jppres.com/jppres/pdf/vol9/jppres20.976_9.4.397.pdf
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spelling doaj-36d2cc26f7554168844cfbff6b1b37002021-04-16T03:40:21ZengAcademic Association of Pharmaceutical Sciences from Antofagasta (ASOCIFA)Journal of Pharmacy & Pharmacognosy Research0719-42502021-07-0194397408Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetinEmtenan Sami Sulimani0 Jehad Mustafa Yousef1Azza M. Mohamed2Department of Biochemistry, Faculty of Science, King Abdulaziz University, Jeddah, Saudi Arabia.Department of Biochemistry, College of Science, University of Jeddah, Jeddah, Saudi Arabia.Department of Biochemistry, College of Science, University of Jeddah, Jeddah, Saudi Arabia. Department of Therapeutic Chemistry, National Research Center, Cairo, Egypt.Context: Celecoxib (Cele), a nonsteroidal anti-inflammatory drug (NSAID) is linked with a spectrum of hepatotoxic influences, however the underlying mechanism (s) by which this drug induces liver damage is still unexplored. Aims: To demonstrate the hepatotoxic mechanism (s) of Cele in rats and the prophylactic roles of melatonin (Mel) and/or quercetin(Qr). Methods: Rats were divided into eight groups, GI, served as control group; GII, Mel (12 mg/kg/day) treated group; GIII, Qr (10 mg/kg/day) treated group; GIV, Mel and Qr treated group; GV, Cele (50 mg/kg/day) treated group; GVI, Cele treated group concurrently with Mel GVII, Cele treated group concurrently with Qr; GVIII, Cele treated group concurrently with the combination of the two agents. The efficiency of Mel and/or Qr on hepatic histomorphology was also investigated. Results: Cele significantly reduced hepatic succinate dehydrogenase and adenosine triphosphate and increased adenosine diphosphate versus the control group. Cele also caused rising in hepatic malondialdehyde, nitric oxide, tumor necrosis factor-α, transforming growth factor-β, caspase-3 and hydroxyproline as well as DNA damage along with depletion in catalase and glutathione reductase. Alteration in serum liver function markers and its histologic architecture were also observed in Cele treated group. Co-treatment of Cele treated rats with Mel and/or Qr, effectively ameliorated the deteriorations in the studied parameters as well as the histomorphologic liver pictures. Conclusions: Mel and/or Qr could protect the liver from Cele, toxicity, which was more pronounced in rats treated with the combination of the two agents.https://jppres.com/jppres/pdf/vol9/jppres20.976_9.4.397.pdfcelecoxibinflammationlivermelatoninoxidative stressquercetin
collection DOAJ
language English
format Article
sources DOAJ
author Emtenan Sami Sulimani
Jehad Mustafa Yousef
Azza M. Mohamed
spellingShingle Emtenan Sami Sulimani
Jehad Mustafa Yousef
Azza M. Mohamed
Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin
Journal of Pharmacy & Pharmacognosy Research
celecoxib
inflammation
liver
melatonin
oxidative stress
quercetin
author_facet Emtenan Sami Sulimani
Jehad Mustafa Yousef
Azza M. Mohamed
author_sort Emtenan Sami Sulimani
title Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin
title_short Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin
title_full Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin
title_fullStr Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin
title_full_unstemmed Molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin
title_sort molecular target mechanisms of celecoxib induced liver damage in rats and the potential prophylactic roles of melatonin and/or quercetin
publisher Academic Association of Pharmaceutical Sciences from Antofagasta (ASOCIFA)
series Journal of Pharmacy & Pharmacognosy Research
issn 0719-4250
publishDate 2021-07-01
description Context: Celecoxib (Cele), a nonsteroidal anti-inflammatory drug (NSAID) is linked with a spectrum of hepatotoxic influences, however the underlying mechanism (s) by which this drug induces liver damage is still unexplored. Aims: To demonstrate the hepatotoxic mechanism (s) of Cele in rats and the prophylactic roles of melatonin (Mel) and/or quercetin(Qr). Methods: Rats were divided into eight groups, GI, served as control group; GII, Mel (12 mg/kg/day) treated group; GIII, Qr (10 mg/kg/day) treated group; GIV, Mel and Qr treated group; GV, Cele (50 mg/kg/day) treated group; GVI, Cele treated group concurrently with Mel GVII, Cele treated group concurrently with Qr; GVIII, Cele treated group concurrently with the combination of the two agents. The efficiency of Mel and/or Qr on hepatic histomorphology was also investigated. Results: Cele significantly reduced hepatic succinate dehydrogenase and adenosine triphosphate and increased adenosine diphosphate versus the control group. Cele also caused rising in hepatic malondialdehyde, nitric oxide, tumor necrosis factor-α, transforming growth factor-β, caspase-3 and hydroxyproline as well as DNA damage along with depletion in catalase and glutathione reductase. Alteration in serum liver function markers and its histologic architecture were also observed in Cele treated group. Co-treatment of Cele treated rats with Mel and/or Qr, effectively ameliorated the deteriorations in the studied parameters as well as the histomorphologic liver pictures. Conclusions: Mel and/or Qr could protect the liver from Cele, toxicity, which was more pronounced in rats treated with the combination of the two agents.
topic celecoxib
inflammation
liver
melatonin
oxidative stress
quercetin
url https://jppres.com/jppres/pdf/vol9/jppres20.976_9.4.397.pdf
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AT jehadmustafayousef moleculartargetmechanismsofcelecoxibinducedliverdamageinratsandthepotentialprophylacticrolesofmelatoninandorquercetin
AT azzammohamed moleculartargetmechanismsofcelecoxibinducedliverdamageinratsandthepotentialprophylacticrolesofmelatoninandorquercetin
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