Rabeprazole: A Pharmacologic and Clinical Review For Acid-Related Disorders
Rabeprazole: A Pharmacologic and Clinical Review For Acid-Related Disorders
Rabeprazole: A Pharmacologic and Clinical Review For Acid-Related Disorders
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Rabeprazole: a pharmacologic
and clinical review for
acid-related disorders
1.
Introduction
2.
Pharmacology
3.
Drug safety
Temple University School of Medicine, Gastroenterology Section, Parkinson Pavilion, 8th Floor,
3401 North Broad Street, PA 19140, Philadelphia, USA
4.
Adverse events
5.
Laboratory abnormalities
6.
7.
8.
Expert opinion
1.
Introduction
Pharmacology
2.1
Pharmacodynamics
119
Rabeprazole
Histamine H2
receptor antagonists
Acetylcholine
Muscarinic
antagonists
Muscarinic
M3 receptor
Gastrin
Histamine
Histamine H2 receptor
CCK2 receptor
Ca2+dependent
pathway
cAMPdependent
pathway
+
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H+
Parietal
cell
K+
+ +
H K -ATPase
Rabeprazole
CI-
Acid (HCI)
Gastric gland
lumen
Figure 1. Model demonstrating rabeprazoles site of action at proton pump. Gastric acid is secreted by parietal cells of the
stomach in response to stimuli such as the presence of food in the stomach or intestine and the taste, smell, sight or thought of food.
Such stimuli result in the activation of histamine, acetylcholine or gastrin receptors (the H2, M3 and CCK2 receptors, respectively) located
in the basolateral membrane of the parietal cell, which initiates signal transduction pathways that converge on the activation of the
H+/K+-ATPase, the final step of acid secretion. Inhibition of this proton pump has the advantage that it will reduce acid secretion
independent of how secretion is stimulated, in contrast to other pharmacological approaches to the regulation of acid secretion; for
example, the inhibition of acid secretion by H2 receptor antagonists can be overcome by food-induced stimulation of acid secretion
through gastrin or acetylcholine receptors.
Reprinted from Nat Rev Drug Discov 2003;2:132-9.
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Pharmacokinetics
Clinical efficacy
Gastroesophageal reflux disease
2.3.1
121
Rabeprazole
Rabeprazole 20 mg
Lansoprazole 30 mg
Pantoprazole 40 mg
*
10
8.0
4.0
3.5
7.4
4.9
#
3.0
2.9
0.9
Omeprazole MUPS 20 mg
B.
3.4
Omeprazole 20 mg
Placebo
2.9
3.0
2.5
2.2
1.8
2.0
1.9
1.5
1.3
1.0
0.5
0
24 h
4.0
3.5
3.6
D.
3.3
3.0
#
2.5
4.0
3.5
2.2
2.1
1.8
2.0
1.5
1.3
1.0
Median gastric pH
C.
Median gastric pH
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Median gastric pH
A.
3.0
2.5
2.0
1.5
2.3
2.1
1.6
1.5
1.6
1.2
1.0
0.5
0.5
Night-time
Daytime
Figure 2. 24 h antisecretory activity of different proton-pump inhibitors in healthy volunteers. A. Time pH > 4 h; B. Median 24 h
pH. C. Median daytime pH. D. Median night-time pH.
Reprinted from Drugs 2003;63(24);2739-54 as extracted from [7].
*p 0.03 versus lansoprazole.
p 0.03 versus pantoprazole.
p 0.02 versus omeprazole.
p 0.04 versus omeprazole MUPS.
#p 0.04 versus placebo.
MUPS: Multiple unit pellet system.
2.5
Erosive oesophagitis
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2.5.1
Drug safety
3.1
Reproductive safety
Breast-feeding summary
123
Rabeprazole
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Adverse events
Laboratory abnormalities
Expert opinion
Declaration of interest
In co-administration clinical trials with rabeprazole plus
amoxicillin and clarithromycin (RAC) for H. pylori eradication,
no adverse events specifically related to these medications
were observed. In a multicenter trial of 803 patients, the
124
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125
Rabeprazole
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126
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Affiliation
Alia Dadabhai MD &
Frank K Friedenberg MD MS
Author for correspondence
Temple University Hospital,
Temple University School of Medicine,
Gastroenterology Section,
Parkinson Pavilion, 8th Floor,
3401 North Broad Street,
PA 19140, Philadelphia, USA
Tel: +1 215 707 3431; Fax: +1 215 707 2684;
E-mail: [email protected]