Acid Secretory Capacity After Treatment with Omeprazole

Bhawna Sharma; Per Lundborg; R E Pounder; M Axelson; Miina K. Öhman; Iuri A. Santana; Monique Talbot; C. Cederberg

doi:10.3109/00365528609090920

Acid Secretory Capacity After Treatment with Omeprazole

Bhawna Sharma(University College London), Per Lundborg(University College London), R E Pounder(University College London), M Axelson(University College London), Miina K. Öhman(University College London), Iuri A. Santana(The Royal Free Hospital), Monique Talbot(The Royal Free Hospital), C. Cederberg(The Royal Free Hospital)

Scandinavian Journal of Gastroenterology

January 1, 1986

10.3109/00365528609090920

Cited by 19

Abstract

Omeprazole, an H+K+ATPase inhibitor, is a potent suppressor of gastric acid secretion. A dose of 30 mg/day caused a 97% decrease of mean 24-hour intragastric acidity in duodenal ulcer patients. Basal and postprandial plasma gastrin concentrations were increased during once daily omeprazole treatment, but were reversed after cessation of treatment. The object of this study was to investigate whether this omeprazole induced elevation of plasma gastrin has a trophic effect on the parietal cell mass in man.

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