1. Academic Validation
  2. Long-term administration of the fungus toxin, sterigmatocystin, induces intestinal metaplasia and increases the proliferative activity of PCNA, p53, and MDM2 in the gastric mucosa of aged Mongolian gerbils

Long-term administration of the fungus toxin, sterigmatocystin, induces intestinal metaplasia and increases the proliferative activity of PCNA, p53, and MDM2 in the gastric mucosa of aged Mongolian gerbils

  • Environ Health Prev Med. 2011 Jul;16(4):224-31. doi: 10.1007/s12199-010-0190-x.
Masahiro Kusunoki 1 Junichi Misumi Tatsuo Shimada Kazuo Aoki Noritaka Matsuo Hideaki Sumiyoshi Takeshi Yamaguchi Hidekatsu Yoshioka
Affiliations

Affiliation

  • 1 Department of Matrix Medicine, Faculty of Medicine, Oita University, Idaigaoka 1-1, Hasama-machi, Yufu, Oita, 879-5593, Japan. e21501@oita-u.ac.jp
Abstract

Objective: The causal agents of gastric Cancer could include fungus toxins. Sterigmatocystin (ST), a fungus toxin, is a risk factor of gastric Cancer. We investigated the effects of ST on the stomach tissues of Mongolian gerbils.

Methods: Seventy-five-week-old male Mongolian gerbils received ST ad libitum at a concentration of 0 ppb (non-treated, n = 11), 100 ppb (n = 7), or 1000 ppb (n = 13) dissolved in drinking water for a period of 24 weeks. After administration, we tested the histopathological changes and immunostaining for proliferating cell nuclear antigen (PCNA), p53, and MDM2 expression.

Results: We investigated the histopathological changes and determined the incidence of histopathological changes in Animals with various gastric diseases after ST administration at a dose of 0 ppb (non-treated control), 100, or 1,000 ppb as follows: firstly, indices for gastritis were 18.2, 100, and 100%, those for erosion events were 9.1, 100, and 92.3%, and those for polyps were 0, 71.4, and 61.5%, respectively. These incidences in the ST-administered groups (100 or 1000 ppb) showed significant increases compared with those in the non-treated control group. And, lastly, indices for intestinal metaplasia were 0, 100, and 15.4%, respectively. Furthermore, immunostaining for PCNA, p53, and MDM2 expression showed significantly greater rates in the ST-administered groups (100 or 1000 ppb) than in the non-treated control group.

Conclusion: The histopathological and immunohistopathological findings of this study indicate that ST exerts a marked influence on gastric mucus and gland cells, showing dominant gastritis, erosion events, polyps, and intestinal metaplasia in these Animals.

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