Early effects of oral administration of lafutidine with mosapride compared with lafutidine alone on intragastric pH values

The ideal medication for gastric acid related diseases, especially for example hemorrhagic gastric ulcers and stress related gastric bleeding, should have a rapid onset of action to lower intragastric acidity, because in vitro studies have shown that blood coagulation and platelet aggregation are abolished at a pH less than 5.4 [1]. Medication for on-demand treatment also should have a rapid onset of action to assure that symptoms are controlled. Multiple agents including antacids, histamine H2 receptor antagonists (H2RAs) and proton pump inhibitors (PPIs) are currently available. PPIs are the most potent inhibitors of gastric acid secretion when used regularly [2]. However, no study has yet examined whether an H2RA with mosapride (orally ingested) more rapidly increases intragastric pH than the H2RA on its own. This crossover study was designed to compare the acute effect on the intragastric pH following administration of lafutidine 10 mg on its own, or lafutidine 10 mg with mosapride 5 mg.

All subjects completed the study. No adverse events were recorded during the study.

Mosapride citrate (mosapride) (4-amino-5-chloro-2-ethoxy-N-{[4-(4-fluorobenzyl)-2-morpholinyl]methyl} benzamide citrate) is a novel gastrokinetic agent that enhances gastrointestinal motility by stimulating the serotonin (5-HT4) receptor [3]. Mosapride stimulates acetylcholine release from cholinergic neurons in the gastrointestinal wall and may enhance upper gastrointestinal motor activity in the postprandial state in conscious dogs [4]. After oral administration, mosapride is absorbed in the small intestine in rats, rather than the stomach [5].

Mosapride accelerates gastric emptying in healthy adults. This study may indicate that mosapride accelerates the absorption of lafutidine. For example, mosapride accelerates the gastric emptying and completion rate of small bowel examinations in patients undergoing capsule endoscopy [6]. The time of gastric emptying time (GET) in the mosapride group was reduced and indicated the obvious effect of mosapride on shortening GET. Moreover, Preparation for barium enemas using mosapride before and after oral intestinal lavage solution (PEG-ELS) intake is more effective than the modified Brown's method that is commonly used in Japan [7]. Mosapride improves gastrointestinal motility and reduces gastric stasis or gastroesophageal reflux [8, 9]. Mosapride also alleviates gastrointestinal dysfunction.

Although many factors are implicated in the development of gastroesophageal reflux disease (GERD), acid reflux to the esophagus is considered to be the major causes of this disease. Treatment with PPIs to provide potent, long-term suppression of gastric acid is essential for disease management. On the other hand, the transient heartburn associated with mild GERD is attributed mainly to temporary, short-term gastric acid reflux. For example, water and antacid immediately increased gastric pH, while PPIs showed a delayed but prolonged effect compared to H2RAs [10].

Because lafutidine promptly suppressed gastric acid secrerion [11], it was orginally considered to be a useful drug for the on-demand treatment of mild GERD. Because mosapride accelerates gastric emptying, Lafutidine can pass from stomach to duodenum and be absorbed quickly. Lafutidine used with mosapride may cause the rapid onset of action, and may thus be more suitable for on-demand use.

The limitation of the present study is that the data were collected from healthy volunteers and not GERD patients requiring on-demand therapy. The clinical implications of our results remain unclear; however, our findings suggest that the orally administered combination of lafutidine 10 mg preceded by mosapride 5 mg tablets may be suitable for on-demand treatment in patients with GERD. Further studies are necessary to confirm this assumption.