Clinical pharmacology of etintidine in patients with duodenal ulcer |
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| Authors: | D. C. Brater W. M. Meyers Jr. K. A. Dandekar K. A. Pittman W. Peterson |
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| Affiliation: | (1) Departments of Pharmacology and Internal Medicine, Veterans Administration Hospital Center, The University of Texas Health Science Center at Dallas, Dallas, Texas;(2) Division of Drug Metabolism and Pharmacokinetics Bristol Laboratories, Syracuse, New York |
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| Abstract: | ![]()
Summary The gastric antisecretory activity of etintidine, a new histamine H2-receptor antagonist, was evaluated in 5 patients with quiescent duodenal ulcer disease. Meal-stimulated acid secretion was measured after 100 and 300 mg oral doses of etintidine, 100 and 300 mg oral doses of cimetidine, and placebo. Reductions from placebo in four-hour gastric acid secretion were 49, 65, 80, and 94%, with 100 mg cimetidine, 100 mg etintidine, 300 mg cimetidine, and 300 mg etintidine, respectively. Drug concentrations in plasma were determined by HPLC. The pharmacokinetics of the 2 drugs were similar. We analyzed sigmoid-shaped concentration-response curves to both agents; the concentrations causing 50% inhibition of meal-stimulated gastric acid secretion were 0.44±0.04 and 0.15±0.04 µg/ml for cimetidine and etintidine, respectively. However, characteristics of these curves were such that the potency difference diminished at higher concentrations. |
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| Keywords: | cimetidine etintidine duodenal ulcer histamine H2 antagonist gastric acidity pharmacodynamics |
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