Literature DB >> 7441551

Mechanisms of gastric acid secretion after pylorus and oesophagus ligation in the rat.

R Håkanson, J Hedenbro, G Liedberg, F Sundler, S Vallgren.   

Abstract

1. The effect of vagotomy on gastric acid secretion was studied in chronic gastric fistula rats at various times after denervation. In these rats basal and pentagastrin-induced acid output was permanently reduced. Thus, the magnitude of the acid response to pentagastrin in the conscious fistula rat is dependent upon an intact vagus. 2. The acid response to pylorus ligation in vagally intact rats was unaffected by drainage of the stomach and therefore not caused by distension. Bilateral vagotomy, performed simultaneously with the ligation, completely abolished acid secretion, while unilateral vagotomy reduced the acid output by half. Hence, in innervated rats, an intact vagal impulse flow appears to be essential for the acid response to pylorus ligation. When the pylorus ligation was performed 2-8 weeks after truncal vagotomy, the acid output showed a progressive return towards pre-denervation values. In the denervated rats the acid response to pylorus ligation was blocked by drainage of the stomach and therefore probably caused by distension, a mechanism which is independent of the vagal impulse flow. 3. The response to pylorus ligation in innervated rats was blocked by atropine and chlorisondamine but not by metiamide. In the denervated rats, the response to pylorus ligation was blocked by all three drugs. 4. Following ligation of both the pylorus and the oesophagus the acid response was poor. With drainage of the oesophagus the acid response was much enhanced, suggesting that oesophageal distension inhibits acid secretion. In the vagotomized rat the poor acid response to oesophageal + pyloric ligation could not be overcome by drainage of the oesophagus. In the innervated rat gastric distension could overcome the inhibition induced by oesophageal ligation. Also in chronically, but not in acutely vagotomized rats, gastric distension brought about a good acid response. Conceivably, gastric reflex mechanisms can activate acid secretion through vagal and/or intramural pathways. Both in innervated and denervated rats the response to gastric distension was inhibited by atropine, chlorisondamine and metiamide. 5. The results suggest that in the innervated rat vago-vagal reflexes are important for the gastric hypersecretion following ligation of the pylorus, and for the acid response to gastric distension following ligation of the pylorus and oesophagus. In the chronically vagotomized rat local intramural reflexes elicited by gastric distension are responsible for the acid response.

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Year:  1980        PMID: 7441551      PMCID: PMC1282964          DOI: 10.1113/jphysiol.1980.sp013355

Source DB:  PubMed          Journal:  J Physiol        ISSN: 0022-3751            Impact factor:   5.182


  15 in total

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5.  The mechanism of gastric hyperacidity produced by pylorus ligation in the rat.

Authors:  D A Brodie
Journal:  Am J Dig Dis       Date:  1966-03

6.  Mechanism of activation of rat stomach histidine decarboxylase after vagal denervation.

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Journal:  Eur J Pharmacol       Date:  1971-09       Impact factor: 4.432

7.  The effect of unilateral vagotomy on gastric secretion in the pylorus ligated rat.

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8.  The role of endogenous gastrin in the activation of gastric histidine decarboxylase in the rat. Effect of antrectomy and vagal denervation.

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9.  Effects of cimetidine, a histamine H2-receptor antagonist, on various experimental gastric and duodenal ulcers.

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10.  The mechanism of the inhibition of gastric secretion produced by esophageal ligation in the pylorus-ligated rat.

Authors:  D A Brodie; P G Knapp
Journal:  Gastroenterology       Date:  1966-06       Impact factor: 22.682

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