Effects of Pantoprazole on Stress-Induced Gastric Mucosal Lesions in Rats
10.3969/j.issn.0253-9896.2009.07.020
- VernacularTitle:泮托拉唑对应激损伤大鼠胃黏膜修复作用的研究
- Author:
Jianping HUA
;
Junmei LI
;
Guifeng MA
;
Zhijun LI
- Publication Type:Journal Article
- Keywords:
benzimidazoles;
peptides;
gastric mucosa;
stomach ulcer;
stress;
immunohistochemistry;
rat,Wistar
- From:
Tianjin Medical Journal
2009;37(7):589-591
- CountryChina
- Language:Chinese
-
Abstract:
Objective: To investigate the effects of Pantoprazole on the expression of TFF1 in stress-induced gastric mucosal lesions in rats, and the mechanism thereof. Methods: Fifty-six rats were randomly divided into seven groups, normal group, model groups (3 groups) and model therapy groups (3 groups). The rat model of water immersion- restraint stress (WRS) was established in model groups, model group1(the immediately after establishing models), model group 2 (4 h after establishing models) and model group 3(8 h after establishing models). The model therapy groups were divided into model therapy group 1 (immediately after establishing models), model therapy group 2 (4 h after establishing models), and model therapy group 3 (8 h after establishing models). The ulcer index (UI) and histological changes were observed after WRS in rats. The expression of TFF1 was detected by immunohistochemistry. Results: After WRS, the gastric mucosa was widely damaged in rats. UI were increased and the expression of TFF1 was decreased in model groups. After intervention with Pantoprazole, UI was lower in model therapy group than those in model groups (model group 1 vs model therapy group 1,69.13±1.97 vs 23.38±1.30, P < 0.01; model group 2 vs model therapy group 2, 57.50±8.81 vs 10.38±3.02, P < 0.01; model group 3 vs model therapy group 3, 43.50±6.76 vs 5.88±1.25, P < 0.01). The staining scores of TFF1 were increased (model group 1 vs model therapy group 1, 0.55±0.11 vs 0.92±O.15, P< 0.01; model group 2 vs model therapy group 2, 0.76±0.24 vs 1.36±0.21, P< 0.01; model group 3 vs model therapy group 3, 1.12±0.16 vs 1.65±0.11, P < 0.01). Conclusion: TFF1 may participate in the protection of gastric mucosa and promote ulcer recovery. Pantoprazole may participate in the defense of gastric mucosa through mediating the up-regulation of TFFI expression.
