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Histopathological changes of gastric mucosa following oral administration of fumonisin B1 in mice
Authors:Abbas Tavasoly  Zahra Kamyabi-moghaddam  Alimohammad Alizade  Mohhmmadali Mohaghghi  Fatemeh Amininajafi  Alireza Khosravi  Maryam Rezaeian  Amirali Solati
Institution:1. Faculty of Veterinary Medicine, University of Tehran, Tehran, Iran
2. Cancer Research Center, Faculty of Medicine, University of Medical Science of Tehran, Tehran, Iran
3. Department of Veterinary Medicine, Islamic Azad University, Saveh Branch, Saveh, Iran
Abstract:Fumonisin B1 is a common secondary metabolite produced by Fusarium moniliforme that occurs in corn and corn-based foods. This mycotoxin is toxic to many species of laboratory and domestic animals and is known to induce a variety of diseases such as hepatic cancer and renal and hepatic dysfunction. The structure of fumonisin B1 (FB1) resembles sphingolipids so it can inhibit synthesis of ceramide, an enzyme in the sphingolipid biosynthetic pathway. This inhibition leads to the disruption of sphingolipid metabolism and increased levels of sphinganine and sphingosine (sphingoid bases) in the serum of treated animals. It is believed that the toxicity effect of fumonisin B1 is the result of these sphingoid bases. In the present research, mice were treated with FB1 to determine its pathological effects on gastric gland and gastric mucosa in the treated mice. For this purpose, the mice were randomly assigned into two groups, namely, control (n?=?14) and treatment (n?=?15). The treatment group was fed with prepared food containing FB1 (150 mg/kg) for a period of 4 months. One day after the last treatment, all animals in both groups were euthanized and their stomach were sampled and prepared for microscopic analysis. Histopathological analysis revealed a significant decrease in parietal cell number and a significant increase in the number of inflammatory cells in gastric mucosa. Also, atrophy of gastric glands was observed. The study confirmed that FB1 poisoning can have toxicopathological effects such as gastric gland atrophy and gastritis on mice gastric tissue.
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