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Literature DB >> 5350103

Gastric acid secretion in patients with duodenal ulcer treated for one year with anticholinergic drugs.

M D Kaye, P Beck, J Rhodes, P M Sweetnam.

Abstract

Ninety patients with duodenal ulcer, divided randomly into three groups, were treated continuously for one year with either glycopyrronium, 1-hyoscyamine (as a sustained-release preparation) or inert tablets. Dosage with active tablets was so adjusted that the patient experienced definite but tolerable side-effects. Basal and maximal gastric acid secretion were measured immediately before and one week after cessation of treatment. There was no significant change in the means of these measurements in patients who received placebo or 1-hyoscyamine. In those given glycopyrronium, mean basal output was significantly increased. Mean maximal acid output in this group fell, but not significantly.Individual measurements of maximal acid output showed quite marked fluctuations in all groups. It is concluded that spontaneous changes in parietal cell mass may occur in patients with duodenal ulcer, and that prolonged anticholinergic therapy does not reduce parietal cell mass.

Entities: Chemical Disease Species

Mesh：

Substances：

Year: 1969 PMID： 5350103 PMCID： PMC1552990 DOI： 10.1136/gut.10.10.774

Source DB: PubMed Journal: Gut ISSN： 0017-5749 Impact factor: 23.059

20 in total

1. Long-continued inhibition of gastric secretion by poldine methosulphate in patients with peptic ulcer.

Authors: A H DOUTHWAITE; T H HILLS; J N HUNT
Journal: Br Med J Date: 1961-06-03

2. The effect of prolonged histamine stimulation on the parietal cell population and the secretory function of the guineapig stomach.

Authors: I N MARKS
Journal: Q J Exp Physiol Cogn Med Sci Date: 1957-04

3. Effect of large doses of histamine on gastric secretion of HCI; an augmented histamine test.

Authors: A W KAY
Journal: Br Med J Date: 1953-07-11

4. Effect of prolonged administration of an anticholinergic drug, propantheline bromide, on gastric histology and acid secretion.

Authors: M D Kaye; A Jacobs; H Ireson; D Trevett
Journal: Am J Dig Dis Date: 1968-11

5. Clinical evaluation of three long-acting anticholinergic compounds.

Authors: M D Kaye; J Rhodes; P M Sweetnam
Journal: Gut Date: 1968-10 Impact factor: 23.059

6. Gastric secretory patterns before and during treatment with 1-hyoscyamine.

Authors: P M Christiansen; P Rodbro
Journal: Scand J Gastroenterol Date: 1967 Impact factor: 2.423

7. Experimental achlorhydria: techniques of production with parietal cell antibody.

Authors: A I Walder
Journal: Surgery Date: 1968-07 Impact factor: 3.982

8. Comparative effect of long-term anticholinergic administration with glycopyrrolate and of vagotomy on parietal cell function, ultrastructure, and population.

Authors: E L Posey; R Elliott; B Shewmake; L Posey
Journal: Am J Dig Dis Date: 1968-06

Gastric acid secretion in patients with duodenal ulcer treated for one year with anticholinergic drugs.

1. Long-continued inhibition of gastric secretion by poldine methosulphate in patients with peptic ulcer.

2. The effect of prolonged histamine stimulation on the parietal cell population and the secretory function of the guineapig stomach.

3. Effect of large doses of histamine on gastric secretion of HCI; an augmented histamine test.

4. Effect of prolonged administration of an anticholinergic drug, propantheline bromide, on gastric histology and acid secretion.

5. Clinical evaluation of three long-acting anticholinergic compounds.

6. Gastric secretory patterns before and during treatment with 1-hyoscyamine.

7. Experimental achlorhydria: techniques of production with parietal cell antibody.

8. Comparative effect of long-term anticholinergic administration with glycopyrrolate and of vagotomy on parietal cell function, ultrastructure, and population.

9. Experimental alterations in gastric mucosal cellular population in dogs.

10. Long-term anticholinergic administration and gastric secretory function in dogs.

1. A controlled trial of glycopyrronium and l-hyoscyamine in the long-term treatment of duodenal ulcer.

2. Spontaneous and persisting decrease in maximal acid output.