Archives of Medical Research
Volume 37, Issue 6 , Pages 717-722, August 2006

Ozone/Oxygen Mixture Modifies the Subcellular Redistribution of Bax Protein in Renal Tissue from Rats Treated with Cisplatin

  • Aluet Borrego

      Affiliations

    • National Laboratory for the Control of Drugs, Havana, Cuba
    • Corresponding Author InformationAddress reprint requests to: Mrs. Aluet Borrego, MSc, Researcher, Center for the Control and Development of Drugs (CECMED), Havana, Cuba;
  • ,
  • Zullyt Barbara Zamora

      Affiliations

    • Ozone Research Center, Center for the Control and Development of Drugs (CECMED), Havana, Cuba
  • ,
  • Ricardo González

      Affiliations

    • Ozone Research Center, Center for the Control and Development of Drugs (CECMED), Havana, Cuba
  • ,
  • Cheyla Romay

      Affiliations

    • Ozone Research Center, Center for the Control and Development of Drugs (CECMED), Havana, Cuba
  • ,
  • Silvia Menéndez

      Affiliations

    • Ozone Research Center, Center for the Control and Development of Drugs (CECMED), Havana, Cuba
  • ,
  • Frank Hernández

      Affiliations

    • Ozone Research Center, Center for the Control and Development of Drugs (CECMED), Havana, Cuba
  • ,
  • Jorge Berlanga

      Affiliations

    • Center for Genetic Engineering and Biotechnology, Biomedical Investigations Branch (CIGB), Havana, Cuba
  • ,
  • Teresita Montero

      Affiliations

    • Department of Histopathology, Dr. Luis Díaz Soto Hospital, Havana, Cuba

Received 9 August 2005; accepted 24 February 2006.

(ARCMED-D-05-00300)

Background

Cellular events in cisplatin-mediated nephrotoxicity include apoptosis induction, decreased protein synthesis, changes in the subcellular redistribution of Bax mitochondrial dysfunction, DNA injury, increased lipid peroxidation, depletion of glutathione and decrease in enzymatic activity of renal antioxidant enzymes. In previous papers we have shown that intra-rectal (ir) ozone/oxygen mixture protected and induced a significant recovery in cisplatin-induced renal damage and was related to a significant increase in the antioxidant system in renal tissue.

Methods

This study was undertaken to examine the effect of the ir applications of ozone/oxygen mixture in the renal expression pattern of Bax proteins in rats treated with cisplatin. A group of male Sprague-Dawley rats was pretreated with 15 ir applications of ozone/oxygen (1.1 mg/kg) before intraperitoneal injection of cisplatin (6 mg/kg). Another group was treated with five ir applications of ozone/oxygen mixture after cisplatin administration. Serum creatinine was measured thereafter. Subcellular distribution of Bax in renal tissue was analyzed by immunohistochemistry.

Results

Ozone pretreatment prevented the increase in serum creatinine levels and completely inhibited the acute tubular necrosis induced by cisplatin in renal tissue, diminishing the expression of Bax. Ozone treatment after cisplatin application reduced the increase in serum creatinine levels and the renal necrosis, inducing a lesser decrease of the Bax expression in cisplatin-treated kidneys.

Conclusions

Expression of Bax in renal tissue seems to play an important role in the protection and recovery in cisplatin-nephrotoxicity achieved by ozone/oxygen mixture.

Key Words: Ozone/oxygen mixture, Cisplatin-nephrotoxicity, Bax renal expression

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PII: S0188-4409(06)00097-X

doi:10.1016/j.arcmed.2006.02.008

Archives of Medical Research
Volume 37, Issue 6 , Pages 717-722, August 2006