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Protective effect of resveratrol against methotrexate-induced oxidative stress in the small intestinal tissues of rats

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Date

2015

Author

Arslan, Aynur
Özçiçek, Fatih
Çimen, Ferda Keskin
Altuner, Durdu
Yaralı, Oğuzhan
Kurt, Nezahat
Tümkaya, Levent
Öztürk, Cengiz
Süleyman, Halis

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Arslan, A., Ozcicek, F., Keskin Cimen, F., Altuner, D., Yarali, O., Kurt, N., Tumkaya, L., Ozturk, C., & Suleyman, H. (2015). Protective effect of resveratrol against methotrexate-induced oxidative stress in the small intestinal tissues of rats. International journal of clinical and experimental medicine, 8(7), 10491–10500.

Abstract

The effect of resveratrol on the damage induced by methotrexate (MTX) in rat duodenum and jejunum tissue was investigated and evaluated in comparison with famotidine. the rats were divided into four groups as healthy group (HG), resveratrol+MTX (RMTX) group, famotidine+MTX (FMTX) group and the control group which received MTX (MTXC). RMTX group was given resveratrol 25 mg/kg and FMTX group famotidin 25 mg/kg, while MTXC and HG groups were orally administered distilled water once a day for 30 days. the rats in RMTX, FMTX and MTXC groups were given MTX of 5 mg/kg dose by the same way for 30 days. At the end of this period, amount of MDA, 8-OH/Gua and tGSH, and MPO gene expression were measured in the duodenal and jejunal tissues and the results were histopathologically evaluated. Resveratrol and famotidine were found to significantly prevent elevation of the MDA, 8-OH/Gua and MPO parameters with MTX and decrease of the levels of tGSH in the duodenal and jejunal tissues. Both drugs prevented severe damage to the villus and crypt epithelium in the duodenum and jejunum, congestion and hemorrhage, inflammatory cell infiltration and necrosis in the mucosa and submucosa due to MTX administration. Resveratrol could be considered in the clinical practice for treatment of the tissue damage in the intestines due to use of MTX, in comparison with famotidine. Resveratrol may be more advantageous than famotidine in long-term use against MTX toxicity since it does not inhibit gastric acid secretion.

Source

International Journal of Clinical and Experimental Medicine

Volume

8

Issue

7

URI

https://hdl.handle.net/11436/2953

Collections

  • PubMed İndeksli Yayınlar Koleksiyonu [2443]
  • Scopus İndeksli Yayınlar Koleksiyonu [6023]
  • TF, Temel Tıp Bilimleri Bölümü Koleksiyonu [700]
  • WoS İndeksli Yayınlar Koleksiyonu [5260]



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