Your search keyword '"Prewett E."' showing total 5 results

1. The effect of GR122311X, a bismuth compound with H2-antagonist activity, on 24-hour intragastric acidity.

Author

Prewett EJ, Nwokolo CU, Hudson M, Sawyerr AM, Fraser A, and Pounder RE

Subjects

Adolescent, Adult, Bismuth pharmacology, Bismuth urine, Double-Blind Method, Humans, Male, Ranitidine pharmacology, Circadian Rhythm drug effects, Citrates pharmacology, Gastric Acid metabolism, Histamine H2 Antagonists pharmacology, Ranitidine analogs & derivatives

Abstract

GR122311X (ranitidine bismuth citrate Glaxo Group Research Ltd) is a bismuth compound with histamine H2-receptor antagonist activity. The gastric acid antisecretory activity of three oral dosage regimens of GR122311X was compared with placebo and 150 mg ranitidine b.d. The median 24-h integrated intragastric acidity was 38, 26 and 18% of the median placebo value during dosing with GR122311X 196, 391 and 782 mg b.d., respectively. The 24-h acid suppression with GR122311X 391 mg b.d. was not significantly different to that produced by 150 mg ranitidine b.d. (24% of placebo acidity). The median 24-h urinary bismuth excretion increased with rising dosage of GR122311X from 19.2 micrograms with 196 mg b.d., to 36.4 micrograms with 391 mg b.d., to 68.7 micrograms with 782 mg b.d. In conclusion, GR122311X is an effective antisecretory agent with modest systemic bismuth absorption.

Published

1991

2. Tolerance during 5 months of dosing with ranitidine, 150 mg nightly: a placebo-controlled, double-blind study.

Author

Nwokolo CU, Prewett EJ, Sawyerr AM, Hudson M, Lim S, and Pounder RE

Subjects

Adult, Double-Blind Method, Drug Administration Schedule, Drug Tolerance, Gastric Acidity Determination, Gastrins blood, Humans, Male, Prospective Studies, Ranitidine pharmacology, Time Factors, Ranitidine administration & dosage

Abstract

Repeated dosing with an H2-receptor antagonist results in a modest decrease in antisecretory potency termed "tolerance." The object of this prospective study was to determine whether tolerance is a progressive phenomenon or whether it levels off during prolonged dosing with a standard maintenance dose of an H2-antagonist. The effect of continuous dosing with ranitidine, 150 mg nightly, was compared with intermittent dosing (27 days of placebo each month) with active ranitidine, 150 mg nightly, only on the night of each experiment. Simultaneous 24-hour intragastric acidity and plasma gastrin concentration were measured monthly for 5 months in 17 healthy subjects (7 continuous and 10 intermittent dosing). In the intermittent-dosing group, the antisecretory response to ranitidine, 150 mg nightly, was preserved throughout the 141-day trial period; the median nocturnal integrated acidity decreased from 557 mmol.h/L (day 0) to 38 mmol.h/L on day 1 of dosing, and it ranged between 32 and 55 (median, 45) mmol.h/L during days 29-141. In the continuous-dosing group, there was a significant return of nocturnal intragastric acidity on days 29 and 85 compared with day 1 of dosing. The median nocturnal integrated acidity decreased in the continuous-dosing group from 554 mmol.h/L (day 0) to 87 mmol.h/L on the first day of dosing, and it ranged between 145 and 287 (median, 170) mmol.h/L during days 29-141. Either intermittent or continuous dosing with ranitidine was associated with an elevation of plasma gastrin concentration, which remained constant throughout the 5-month study. Tolerance does develop in healthy subjects during the first month of dosing with ranitidine, 150 mg nightly, but it is not a progressive phenomenon, and it is probably not of clinical relevance.

Published

1991

3. The effect of histamine H2-receptor blockade on bismuth absorption from three ulcer-healing compounds.

Author

Nwokolo CU, Prewett EJ, Sawyerr AM, Hudson M, and Pounder RE

Subjects

Adult, Double-Blind Method, Humans, Intestinal Absorption drug effects, Male, Organometallic Compounds pharmacokinetics, Placebos, Salicylates pharmacokinetics, Anti-Ulcer Agents pharmacokinetics, Bismuth pharmacokinetics, Ranitidine pharmacology, Receptors, Histamine H2 drug effects

Abstract

Twelve healthy male subjects were dosed with six regimens: ranitidine and De-Noltab (tripotassium dicitrato bismuthate; Gist-Brocades Ltd., Weybridge, England), placebo and De-Noltab, ranitidine and Pepto-Bismol liquid [bismuth salicylate; Procter & Gamble (Health and Beauty Care) Ltd., Egham, England], placebo and Pepto-Bismol, ranitidine and Roter tablets (bismuth subnitrate; Roter Pharma Ltd., Ashford, England), and placebo and Roter. Ranitidine, 300 mg, or placebo was administered at 10 PM (night before) and at 7 AM; at 9 AM, the oral dose of bismuth was either 2 De-Noltabs, 3 30-mL doses of Pepto-Bismol liquid, or 2 Roter tablets. When predosed with placebo, the median integrated 8-hour plasma bismuth concentration was significantly greater after dosing with De-Noltabs than after dosing with either Pepto-Bismol or Roter (61, 8, and 8 ng.h/mL, respectively), with a similar trend for 8-hour median urinary bismuth excretion (213, 40, and 6 micrograms, respectively). When predosed with ranitidine, only after De-Noltab administration were there significant increases in the 8-hour plasma bismuth concentration (147 ng.h/mL), and 8-hour urinary bismuth excretion (686 micrograms). Eliminating intragastric acidity may enhance bismuth absorption after oral dosing with De-Noltabs by maintaining intragastric tripotassium dicitrato bismuthate as a colloidal suspension.

Published

1991

4. The effect of ranitidine, cimetidine or famotidine on low-dose post-prandial alcohol absorption.

Author

Fraser AG, Prewett EJ, Hudson M, Sawyerr AM, Rosalki SB, and Pounder RE

Subjects

Adult, Cimetidine administration & dosage, Double-Blind Method, Eating, Ethanol blood, Famotidine administration & dosage, Humans, Male, Ranitidine administration & dosage, Cimetidine pharmacology, Ethanol metabolism, Famotidine pharmacology, Intestinal Absorption drug effects, Ranitidine pharmacology

Abstract

Plasma alcohol concentration following oral ingestion of 0.3 g/kg of alcohol (ethyl alcohol), one hour after an evening meal, was measured in four groups of 12 healthy subjects. Each group had a control study and a repeat study after 7 days dosing with either placebo or an H2-receptor antagonist (300 mg ranitidine nocte, 800 mg cimetidine nocte, or 40 mg famotidine nocte). There was no significant difference between the control and post-dosing studies in the integrated 4-h plasma alcohol concentration, peak plasma alcohol concentration, or time to reach peak alcohol concentration. This study shows that post-prandial alcohol absorption after 0.3 g/kg of alcohol is not affected by ranitidine, cimetidine or famotidine.

Published

1991

5. Nocturnal intragastric acidity during and after a period of dosing with either ranitidine or omeprazole.

Author

Prewett EJ, Hudson M, Nwokolo CU, Sawyerr AM, and Pounder RE

Subjects

Adult, Circadian Rhythm, Double-Blind Method, Humans, Hydrogen-Ion Concentration drug effects, Male, Omeprazole therapeutic use, Peptic Ulcer drug therapy, Ranitidine therapeutic use, Gastric Acid metabolism, Gastric Mucosa drug effects, Omeprazole pharmacology, Ranitidine pharmacology

Abstract

The magnitude and duration of changes in nocturnal intragastric acidity caused by 25 days of dosing with the antisecretory drugs ranitidine and omeprazole were investigated in a double-blind study of 22 healthy subjects. Nocturnal intragastric acidity was studied before (twice), during (on day 25), and after (every 3 days for 21 days) dosing with either 300 mg ranitidine at night or 40 mg omeprazole every morning. Three and six days after withdrawal of dosing with ranitidine, median integrated nocturnal intragastric acidity was increased significantly (17% and 14%, P = 0.01 and P = 0.05, respectively) compared with before dosing. Three days after withdrawal of dosing with omeprazole, median integrated nocturnal intragastric acidity was decreased significantly (-23%, P = 0.003). Compared with before dosing, no significant differences were seen in the ranitidine group between days 9 and 21 or the omeprazole group between days 6 and 21 after cessation of dosing. Fasting plasma gastrin concentration was measured on the morning of each study; compared with before treatment, the only significant elevations occurred on the last day of dosing with omeprazole (before, 4 pmol/L; during, 7 pmol/L). It is concluded that rebound intragastric hyperacidity after dosing with 300 mg ranitidine at night or sustained hypoacidity after dosing with 40 mg omeprazole every morning reflect transient disturbances of gastric function that are unlikely to be of clinical importance.

Published

1991