95 results on '"Karlstadt R"'
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2. MMX® mesalazine for the treatment of patients with ulcerative colitis: the impact of treatment on health related quality of life
3. MMX® mesalamine treatment for patients with mild-to-moderate ulcerative colitis: improvement in health-related quality of life
4. Evaluating induction and maintenance treatment with MMX mesalazine for patients with mild-to-moderate ulcerative colitis
5. Gastric pH control and pneumonia in the critically ill
6. PGI31 The Maintenance of Work-related Productivity During One Year of MMX Mesalamine Treatment for Patients with Quiescent Ulcerative Colitis
7. PGI28 Disease-Specific Health-related Quality of Life in Patients with Quiescent Ulcerative Colitis: Effects of one Year Maintenance Treatment with MMX Mesalamine
8. Induction of mucosal healing in mild-to-moderate ulcerative colitis in patients treated with MMX mesalamine: established versus newly diagnosed disease
9. Induction of clinical and endoscopic remission in mild-to-moderate ulcerative colitis in patients treated with MMX® mesalamine: established versus newly diagnosed disease
10. P200 - A phase I, age and gender stratified, open-label, parallel-group, single-dose study assessing pharmacokinetics (PK) of a single 4.8 g oral dose of MMX™ the mesalazine in healthy volunteers
11. Combining pharmacokinetic, scintigraphic and tablet dissolution analyses to investigate the drug release profiles of delayed-release mesalamine formulations
12. P040 ONCE-OR TWICE-DAILY MMX MESALAZINE (2.4G/DAY) IS EFFECTIVE FOR THE MAINTENANCE OF REMISSION OF MILD-TO-MODERATE ULCERATIVE COLITIS REGARDLESS OF THE MESALAZINE DOSE OR REGIMEN USED TO INDUCE REMISSION
13. P166 THE EFFICACY OF MMX™ MESALAZINE AS THE SOLE MEDICATION FOR THE INDUCTION AND MAINTENANCE OF REMISSION IN PATIENTS WITH MILD-TO-MODERATE ULCERATIVE COLITIS TREATED OVER 14-16 MONTHS
14. Maintenance therapy of duodenal ulcer with H2-receptor antagonists-a meta-analysis
15. Famotidine increases plasma alcohol concentration in healthy subjects
16. Efficacy and Safety Profile of Older Patients Using Oral INKP-102 as a Bowel Purgative Prior to Colonoscopy Compared to Visicol
17. Smaller, Microcrystalline Cellulose (MCC)-Free NaP 32 (INKP-102) Tabs Are Preferred by Patients (pts) for Future Colonoscopies vs. 40 Visicol® Tablets (V)
18. Clinical Laboratory Evaluation of 48 g Oral INKP-102 Compared to 60 g Visicol as a Bowel Purgative Prior to Colonoscopy
19. VOTE (Visicol Observational Tolerability & Experience) Registry Demonstrates Few Physician Calls, Good Patient (pt) Tolerance, and pt Preference for Visicol® Tablets (V) in Private Practice
20. New Microcrystalline Cellulose (MCC)- Free 32 NaP Tablet Prep (INKP-102) Comparable to 40 Tabs Visicol (V) for Overall Colon Cleansing (OCC) & Superior for Ascending Colon Cleansing (ACC)
21. Oral 48 g INKP-102 Has Improved Safety Profile over 60 g Sodium Phosphate Tablets as a Bowel Purgative Prior to Colonoscopy
22. Dose-Ranging Trial Comparing 6 Regimens of a New Microcrystalline Cellulose (MCC)-Free Formulation of Sodium Phosphate (NaP) Tablets (INKP-102) to Visicol® Tablets for Colon Cleansing
23. Letter to the editor
24. Pharmacokinetic comparison of proton pump inhibitors
25. The use of 20, 40 or 60mg/kg/day of continuously infused intravenous cimetidine (CI) in pediatric intensive care unit (PICU) patients
26. Correspondence
27. Intermittent intravenous pantoprazole and continuous cimetidine infusion: effect on gastric pH control in critically ill patients at risk of developing stress-related mucosal disease.
28. Risk factors for nosocomial pneumonia in intensive care
29. Famotidine increases plasma alcohol concentration in healthy subjects.
30. Maintenance therapy of duodenal ulcer with H2-receptor antagonists-a meta-analysis.
31. Acute treatment of benign gastric ulcer with once-daily bedtime dosing of cimetidine compared with placebo.
32. Parental Leave for Trainees in Gastroenterology.
33. Cimetidine and ranitidine on basal and ACTH-stimulated steroidogenesis.
34. Continuous intravenous cimetidine decreases stress-related upper gastrointestinal hemorrhage without promoting pneumonia.
35. Gastric pH improvement from NPO to enteral-fed period with intermittent intravenous (IV) pantoprazole (P) vs. continuously infused cimetidine (C)
36. Ability to predict gastroccult positivity based on presence of “coffee grounds”: a sub-analysis of preliminary data from the ICU pantoprazole study
37. Intermittent intravenous pantoprazole (P) maintains control of gastric pH in intensive care unit patients
38. Prophylaxis for stress-related gastric hemorrhage.
39. The effect of H2 receptor antagonists on intragastric pH in critically ill patients.
40. Impact of MMX® mesalamine on improvement and maintenance of health-related quality of life in patients with ulcerative colitis.
41. Gender-based biology and the gastrointestinal tract.
42. Gender differences--do they really count?
43. Intragastric pH and upper gastrointestinal bleeding in the ICU.
44. Cimetidine QID and BID in rapid heartburn relief and healing of lesions in gastroesophageal reflux disease.
45. Intragastric pH and upper gastrointestinal bleeding in the ICU.
46. Upper gastrointestinal bleeding in the critically ill.
47. Acid-suppression profile of two continuously infused intravenous doses of cimetidine.
48. Continuous infusion H2-receptor therapy.
49. Maintenance therapy of duodenal ulcer with H2-receptor antagonists--a meta-analysis.
50. H2 blockers in stress ulcer prophylaxis.
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