Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damage

The hepatoprotective potential DTS (1.5 g/kg bw, Densh-ici-to-Chiusei, Kyotsu Jigyo, Tokyo, Japan) was evaluated against either toxic (1.5 g/kg bw) and sub-toxic (150 mg/kg bw) dosage of paracetamol-induced liver injury in Sprague-Dawley rat. Paracetamol intoxication caused a reduction of serum tota...

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Main Authors: Francesco Marotta, Prof., MD, PhD, Hariom Yadav, Upendra Gumaste, A.m.r. Helmy, Shalini Jain, Emilio Minelli
Format: Article
Language:English
Published: Elsevier 2009-01-01
Series:Annals of Hepatology
Subjects:
DTS
Online Access:http://www.sciencedirect.com/science/article/pii/S1665268119318113
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spelling doaj-857db60b435e4468867c611eff1876a62021-06-09T05:55:59ZengElsevierAnnals of Hepatology1665-26812009-01-01815056Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damageFrancesco Marotta, Prof., MD, PhD0Hariom Yadav1Upendra Gumaste2A.m.r. Helmy3Shalini Jain4Emilio Minelli5WHO-cntr for Biotech & Nat. Medicine, University of Milan, Italy; Address for correspondenceNIDDK, National Institutes of Health, Bethesda, USAAgharkar Research Institute, Pune, IndiaLiver Institute, Menoufyia University, Giza, EgyptDepartment of Food Science and Human Nutrition, University of Illinois, USAWHO-cntr for Biotech & Nat. Medicine, University of Milan, ItalyThe hepatoprotective potential DTS (1.5 g/kg bw, Densh-ici-to-Chiusei, Kyotsu Jigyo, Tokyo, Japan) was evaluated against either toxic (1.5 g/kg bw) and sub-toxic (150 mg/kg bw) dosage of paracetamol-induced liver injury in Sprague-Dawley rat. Paracetamol intoxication caused a reduction of serum total protein and increase levels of serum alkaline phosphatase (ALP), aspartate ami-notranferase (AST) and serum alanine aminotranferase (ALT) at higher extent in the toxic group. This phenomenon was paralleled by an impaired liver redox status (reduced glutathione (GSH), superoxide dismutase (SOD), glutathione peroxidase (GPx), and catalase (CAT) and increased MDA in both paracetamol-administered groups. Moreover, a marked reduction of AT-Pase and thiols together with DNA fragmentation occurred in liver tissue. Animals pretreated with DTS showed a marked mitigation of the severity of liver enzyme and of the impaired redox status of the liver. Moreover, DTS partly prevented the DNA fragmentation and the decline of liver tissue ATPase and protein thiol assay as compared with both groups treated with paracetamol alone. Although more detailed studies are awaited to ascertain the detailed mode of action of DTS, it wouls seem to be related to the prevention of formation of the reactive oxygen groups thereby preventing the damage on the hepatocytes and possibly modulating the genes responsible for synthesis of liver antioxidant enzymes thus providing marked DNA protection.http://www.sciencedirect.com/science/article/pii/S1665268119318113Paracetamoloxidative stressDNA fragmentationDTS
collection DOAJ
language English
format Article
sources DOAJ
author Francesco Marotta, Prof., MD, PhD
Hariom Yadav
Upendra Gumaste
A.m.r. Helmy
Shalini Jain
Emilio Minelli
spellingShingle Francesco Marotta, Prof., MD, PhD
Hariom Yadav
Upendra Gumaste
A.m.r. Helmy
Shalini Jain
Emilio Minelli
Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damage
Annals of Hepatology
Paracetamol
oxidative stress
DNA fragmentation
DTS
author_facet Francesco Marotta, Prof., MD, PhD
Hariom Yadav
Upendra Gumaste
A.m.r. Helmy
Shalini Jain
Emilio Minelli
author_sort Francesco Marotta, Prof., MD, PhD
title Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damage
title_short Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damage
title_full Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damage
title_fullStr Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damage
title_full_unstemmed Protective effect of a phytocompound on oxidative stress and DNA fragmentation against paracetamol-induced liver damage
title_sort protective effect of a phytocompound on oxidative stress and dna fragmentation against paracetamol-induced liver damage
publisher Elsevier
series Annals of Hepatology
issn 1665-2681
publishDate 2009-01-01
description The hepatoprotective potential DTS (1.5 g/kg bw, Densh-ici-to-Chiusei, Kyotsu Jigyo, Tokyo, Japan) was evaluated against either toxic (1.5 g/kg bw) and sub-toxic (150 mg/kg bw) dosage of paracetamol-induced liver injury in Sprague-Dawley rat. Paracetamol intoxication caused a reduction of serum total protein and increase levels of serum alkaline phosphatase (ALP), aspartate ami-notranferase (AST) and serum alanine aminotranferase (ALT) at higher extent in the toxic group. This phenomenon was paralleled by an impaired liver redox status (reduced glutathione (GSH), superoxide dismutase (SOD), glutathione peroxidase (GPx), and catalase (CAT) and increased MDA in both paracetamol-administered groups. Moreover, a marked reduction of AT-Pase and thiols together with DNA fragmentation occurred in liver tissue. Animals pretreated with DTS showed a marked mitigation of the severity of liver enzyme and of the impaired redox status of the liver. Moreover, DTS partly prevented the DNA fragmentation and the decline of liver tissue ATPase and protein thiol assay as compared with both groups treated with paracetamol alone. Although more detailed studies are awaited to ascertain the detailed mode of action of DTS, it wouls seem to be related to the prevention of formation of the reactive oxygen groups thereby preventing the damage on the hepatocytes and possibly modulating the genes responsible for synthesis of liver antioxidant enzymes thus providing marked DNA protection.
topic Paracetamol
oxidative stress
DNA fragmentation
DTS
url http://www.sciencedirect.com/science/article/pii/S1665268119318113
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