Literature DB >> 14687760

Additive pro-oxidative effects of methylmercury and ebselen in liver from suckling rat pups.

M Farina1, F A A Soares, G Zeni, D O Souza, J B T Rocha.   

Abstract

Oxidative stress has been pointed as an important molecular mechanism for liver injury in methylmercury (MeHg) poisoning. Ebselen, a seleno-organic compound that possesses anti-oxidant properties, is a useful therapeutic agent used in clinical situations involving oxidative stress. Here, we examined the possible in vivo protective effect of ebselen against the pro-oxidative effects of MeHg in liver from suckling rat pups. The effects of MeHg exposure (subcutaneous injections of methylmercury chloride: 2 mg/kg) on the hepatic levels of thiobarbituric acid reactive substances (TBARS) and non-ptotein thiols (NPSH), and on liver glutathione peroxidase (GSHPx) activity, as well as the possible antagonist effect of ebselen (10 mg/kg; subcutaneously) against MeHg effects, were evaluated during the post-natal period. In addition, the possible in vitro interaction between ebselen, glutathione (GSH) and MeHg was investigated by light/UV spectroscopy, with particular attention to the formation of complexes involving ebselen selenol intermediate and MeHg. After in vivo exposure, MeHg and ebselen alone increased hepatic TBARS levels. Moreover, simultaneous treatment with both compounds caused a higher increase in hepatic TBARS levels when compared to the treatments with individual compounds. Liver NPSH decreased after treatments with MeHg and ebselen alone. A significant negative correlation between hepatic TBARS and NPSH was observed. MeHg alone decreased liver GSHPx activity and ebselen, which did not affect this variable per se, reverted this inhibitory effect of MeHg. Light/UV spectroscopy showed that ebselen and GSH form a chemical intermediate that regenerates ebselen after MeHg addition. The presented results show that ebselen abolished the MeHg-induced inhibition on liver GSHPx activity, but did not prevent the oxidative effects of MeHg on liver lipids and NPSH. MeHg affects the in vitro interaction between ebselen and GSH and this phenomenon seems to be responsible for its inhibitory effect toward thiol-peroxidase activity. Additionally, ebselen presents pro-oxidative effects on rat liver, pointing to thiol depletion as a molecular mechanism related to ebselen-induced hepatotoxicity.

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Year:  2004        PMID: 14687760     DOI: 10.1016/j.toxlet.2003.10.001

Source DB:  PubMed          Journal:  Toxicol Lett        ISSN: 0378-4274            Impact factor:   4.372


  14 in total

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Journal:  Curr Protoc Nucleic Acid Chem       Date:  2011-12

2.  Modulation of methylmercury uptake by methionine: prevention of mitochondrial dysfunction in rat liver slices by a mimicry mechanism.

Authors:  Daniel Henrique Roos; Robson Luiz Puntel; Marcelo Farina; Michael Aschner; Denise Bohrer; João Batista T Rocha; Nilda B de Vargas Barbosa
Journal:  Toxicol Appl Pharmacol       Date:  2011-01-27       Impact factor: 4.219

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Journal:  Neurotox Res       Date:  2012-01-20       Impact factor: 3.911

Review 4.  Mechanisms of methylmercury-induced neurotoxicity: evidence from experimental studies.

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Journal:  Life Sci       Date:  2011-06-13       Impact factor: 5.037

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7.  Post-transcriptional defects of antioxidant selenoenzymes cause oxidative stress under methylmercury exposure.

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Journal:  J Biol Chem       Date:  2010-11-24       Impact factor: 5.157

8.  Sulforaphane Prevents Methylmercury-Induced Oxidative Damage and Excitotoxicity Through Activation of the Nrf2-ARE Pathway.

Authors:  Shu Feng; Zhaofa Xu; Fei Wang; Tianyao Yang; Wei Liu; Yu Deng; Bin Xu
Journal:  Mol Neurobiol       Date:  2016-01-07       Impact factor: 5.590

Review 9.  Mercury toxicity on sodium pump and organoseleniums intervention: a paradox.

Authors:  Ige Joseph Kade
Journal:  J Biomed Biotechnol       Date:  2012-08-14

Review 10.  Role of calcium and mitochondria in MeHg-mediated cytotoxicity.

Authors:  Daniel Roos; Rodrigo Seeger; Robson Puntel; Nilda Vargas Barbosa
Journal:  J Biomed Biotechnol       Date:  2012-07-03
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