Gastritis Clinical Trial
Official title:
Pharmacogenomics-Based Tailor-Made Strategy for Eradication of Helicobacter Pylori
The eradication rate of the standard H. pylori eradication therapy (such as the triple therapy with a proton pump inhibitor [PPI], amoxicillin and clarithromycin) depends on bacterial susceptibility to clarithromycin and genotypes of CYP2C19 in patients. The investigators intend to investigate whether the tailored therapy based on the two above-mentioned factors increases the cure rate of the initial eradication therapy.
Current treatment strategies for the eradication of H. pylori include a proton pump
inhibitor (PPI) and one or two anti-bacterial agents, such as amoxicillin, clarithromycin,
and metronidazole.
PPIs, such as lansoprazole and omeprazole, are mainly metabolized in the liver by a
genetically determined enzyme, S-mephenytoin 4'-hydroxylase (CYP2C19). Plasma concentrations
of PPIs and their activity for acid inhibition depend to a significant extent on the genetic
differences in the activity of this enzyme. The acid inhibition attained by the standard
dose of a PPI is sometimes therapeutically insufficient in individuals with the rapid
extensive metabolizer (RM) genotype of CYP2C19, whereas that in individuals with poor
metabolizer (PM) genotype of CYP2C19 is in most cases clinically sufficient. We have
reported that the CYP2C19 genotype status is one of the determinants of H. pylori
eradication therapy. In the triple therapy with a PPI, amoxicillin, and clarithromycin,
bacterial susceptibility to clarithromycin as well as the CYP2C19 genotype status was
significantly related to eradication rates of H. pylori. Therefore, the tailored treatment
based on these two factors is expected to increase the eradication rates of the initial
therapy.
Interestingly, both of CYP2C19 genotypes and bacterial susceptibility to clarithromycin can
be measured by the genetic test of the single nucleotide polymorphisms (SNPs) of the CYP2C19
gene and the 23S rRNA gene of H. pylori, respectively. We have recently developed the
inexpensive and reliable high-throughput method for measurement of such SNPs by the invader
assay. Polymorphisms of CYP2C19 of patients and mutations of 23S rRNA of H. pylori
associated with susceptibility to clarithromycin can be detected from the gastric tissue
samples infected with H. pylori, such as the gastric tissue sample already used for rapid
urease test (RUT).
Then, we treat H. pylori-positive patients by the tailored regimen based on genotypes of
CYP2C19 of patients and 23S rRNA of H. pylori or the standard regimen and test the
therapeutic efficacy of this pharmacogenomics-based tailored strategy in a prospective
manner.
Patients were randomly assigned to the standard or tailored regimen group with the use of a
computer-generated randomization list based on a blocked randomization method.
Patients assigned to the standard regimen group were treated with 30 mg of lansoprazole bid,
400 mg of clarithromycin bid, and 750 mg of amoxicillin bid for one week, which had been
approved under the Japanese formulary regulation regardless of any pharmacogenomic
backgrounds of H. pylori-infected peptic ulcer patients.
In the tailored regimen group, patients infected with a clarithromycin-sensitive strain of
H. pylori are treated with triple therapy consisting of clarithromycin 200 mg tid,
amoxicillin 500 mg tid and the individualized doses of lansoprazole dose (i.e., 30 mg tid in
RMs, 15 mg tid in IMs, and 15 mg bid in PMs) for one week, while patients infected with a
clarithromycin-resistant strain of H. pylori are treated with dual therapy consisting of
amoxicillin 500 mg qid and the individualzed dose of lansoprazole (i.e., 30 mg qid in RMs,
15 mg qid in IMs, and 15 mg bid in PMs) for two weeks.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Factorial Assignment, Masking: Open Label, Primary Purpose: Treatment
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