Effects of pirenzepine on omeprazole-induced hypergastrinemia and acid suppression in peptic ulcer patients

Omeprazole effectively suppresses acid secretion, resulting in the long-term elevation of intragastric pH and serum gastrin level. Pirenzepine has been reported to inhibit gastrin secretion. This study was carried out to examine the effects of additional pirenzepine treatment on the hypergastrinemia...

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Bibliographic Details
Published in:Journal of gastroenterology 1996-04, Vol.31 (2), p.167-170
Main Authors: Tari, A, Hamada, M, Kamiyasu, T, Fukino, Y, Sumii, M, Haruma, K, Sumii, K, Inoue, M, Kajiyama, G
Format: Article
Language:English
Subjects:
Adult
Aged
Anti-Ulcer Agents - adverse effects
Anti-Ulcer Agents - therapeutic use
Drug Therapy, Combination
Duodenal Ulcer - drug therapy
Duodenal Ulcer - metabolism
Female
Gastric Acid - secretion
Gastrins - blood
Humans
Hydrogen-Ion Concentration
Male
Middle Aged
Omeprazole - adverse effects
Omeprazole - therapeutic use
Peptic Ulcer - drug therapy
Peptic Ulcer - metabolism
Pirenzepine - therapeutic use
Radioimmunoassay
Somatostatin - blood
Stomach Ulcer - drug therapy
Stomach Ulcer - metabolism
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Summary:Omeprazole effectively suppresses acid secretion, resulting in the long-term elevation of intragastric pH and serum gastrin level. Pirenzepine has been reported to inhibit gastrin secretion. This study was carried out to examine the effects of additional pirenzepine treatment on the hypergastrinemia and gastric acid suppression induced by omeprazole. Concentrations of serum gastrin and plasma somatostatin were measured in 28 peptic ulcer patients before treatment, after omeprazole treatment (20 mg/day) for 2 weeks, and after omeprazole and pirenzepine (100 mg/day) treatment for 2 weeks. The acid inhibitory effect of pirenzepine treatment in addition to omeprazole was evaluated by 24-h intragastric pH measurement in six healthy volunteers. Serum gastrin level was increased significantly, to 2.4-fold the pretreatment level, by omeprazole treatment. Additional treatment with pirenzepine suppressed serum gastrin level to 0.6-fold the omeprazole-treatment level. The serum somatostatin level was not altered significantly either by omeprazole treatment or by omeprazole and pirenzepine treatment. In healthy volunteers whose pH 3 holding time on 24-h intragastric pH monitoring was 70% by omeprazole treatment, omeprazole and pirenzepine treatment markedly increased the pH 3 holding time, to 89%. These findings suggest that pirenzepine is useful in reducing the undesirable effects of omeprazole-induced hypergastrinemia, i.e., the excessive trophic effect of omeprazole on the acid-secreting part of the stomach and the overstimulation of acid secretion. The additional pirenzepine treatment is also effective in suppressing acid secretion.
ISSN:0944-1174
1435-5922
DOI:10.1007/bf02389513