Gastric acid secretion is lower and the rate of infection with Helicobacter pylori is higher in the Japanese population than in Europeans and Americans, and many such patients are
known to have hypochlorhydria caused by chronic atrophic gastritis.[19-21] Therefore, in KU-57788 mouse the Japanese population, an H2RA or a gastroprotective agent (GP) is presumed to have an effect equal to that of a powerful gastric secretion inhibitor such as a PPI, especially in the prevention and treatment of gastroduodenal mucosal injuries under use of LDA. But no report has yet described the effect of these drugs. We therefore conducted a study to compare teprenone (GP) and famotidine (H2RA) in Japanese patients taking LDA in order to evaluate their effects in the treatment of gastroduodenal mucosal injuries. Study subjects were patients who visited Osaka Medical College, Saga University, Kobe University, or facilities associated with
these schools between December 2007 and July 2012. Inclusion criteria were that patients required continuous medication with LDA (80–300 mg/day) for 12 weeks or longer after participation in the study, regardless of past LDA treatment, that they were aged 20 years or older, and that no peptic ulcer was detected on endoscopy at the start of treatment. Patients were included check details regardless of sex and whether or not they were outpatients. Exclusion criteria were as follows: (i) presence of peptic ulcer; (ii) previous gastrectomy or vagotomy; (iii) treatment with an H2RA or MCE公司 PPI within the 28 days (4 weeks) before the start of study medication administration; (iv) treatment with a non-steroidal anti-inflammatory drug (NSAID) within 28 days (4 weeks) before the start of study medication administration;
(v) a change in corticosteroid regimen (including dosage and administration, but excluding topical medication) within 14 days (2 weeks) before the start of study medication administration; (vi) serious liver disorder, serious renal disorder, serious cardiac disease, and/or serious blood dyscrasia; (vii) allergy or previous experience of an adverse reaction to famotidine or teprenone, which were scheduled to be administered; (viii) pregnancy or lactation, or an intention to become pregnant during the study period; or (ix) determination by an investigator or a sub-investigator that patient was ineligible. All subjects received oral and written explanations of the study prior to participation and gave written informed consent. The study was conducted in accordance with the Declaration of Helsinki (1995) after the protocol had been approved by the ethics review committee of each institution. We conducted a prospective, multicenter, randomized, open-label trial. After confirming the subjects had no peptic ulcer on endoscopy at the start of the study, we determined the Lanza score.
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