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Role of Endothelins in Trinitrobenzene Sulfonic Acid-Induced Colitis in Rats
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To determine the role of endothelins (ET) on experimental colitis, following intracolonic trinitrobenzene sulfonic acid administration, rats were given orally either bosentan (BS), a nonselective ET receptor antagonist (100 mg/kg in 5% arabic gum), or arabic gum by gavage for 2 or 14 days. Macroscopic damage scores obtained in the vehicle (1.4 ± 0.4), acute (4.8 ± 0.6) and chronic (3.8 ± 0.3) colitis groups were significantly higher than in the control group (0). BS treatment reduced the scores in both acute (3 ± 0.5) and chronic (2.3 ± 0.5) colitis groups. Myeloperoxidase (MPO) activities of colonic tissues were elevated in acute and chronic colitis groups (325.1 ± 44.9 and 431.8 ± 54.6 U/g wet weight) as compared with the control group (73.6 ± 11 U/g wet weight). Plasma protein oxidation levels were found to be significantly increased in the chronic colitis group (1,158.1 ± 63.4 nmol/ml) compared with the control, ethanol and acute colitis groups (274.3 ± 23.1, 490 ± 52.2 and 422.2 ± 50.5 nmol/ml). BS treatment significantly reduced both the protein oxidation level (375.5 ± 46.9 nmol/ml) and MPO activity (167.5 ± 35.8 U/g wet weight). The results of the present study suggest the involvement of ETs in the pathogenesis of colonic injury in this animal model of colitis.
Title: Role of Endothelins in Trinitrobenzene Sulfonic Acid-Induced Colitis in Rats
Description:
To determine the role of endothelins (ET) on experimental colitis, following intracolonic trinitrobenzene sulfonic acid administration, rats were given orally either bosentan (BS), a nonselective ET receptor antagonist (100 mg/kg in 5% arabic gum), or arabic gum by gavage for 2 or 14 days.
Macroscopic damage scores obtained in the vehicle (1.
4 ± 0.
4), acute (4.
8 ± 0.
6) and chronic (3.
8 ± 0.
3) colitis groups were significantly higher than in the control group (0).
BS treatment reduced the scores in both acute (3 ± 0.
5) and chronic (2.
3 ± 0.
5) colitis groups.
Myeloperoxidase (MPO) activities of colonic tissues were elevated in acute and chronic colitis groups (325.
1 ± 44.
9 and 431.
8 ± 54.
6 U/g wet weight) as compared with the control group (73.
6 ± 11 U/g wet weight).
Plasma protein oxidation levels were found to be significantly increased in the chronic colitis group (1,158.
1 ± 63.
4 nmol/ml) compared with the control, ethanol and acute colitis groups (274.
3 ± 23.
1, 490 ± 52.
2 and 422.
2 ± 50.
5 nmol/ml).
BS treatment significantly reduced both the protein oxidation level (375.
5 ± 46.
9 nmol/ml) and MPO activity (167.
5 ± 35.
8 U/g wet weight).
The results of the present study suggest the involvement of ETs in the pathogenesis of colonic injury in this animal model of colitis.
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