Helicobacter pylori (H. pylori) is a Gram-negative, microaerophilic bacterium that persistently colonizes the human stomach; more than half the human population is infected worldwide. H. pylori infection is a risk factor for the development of gastritis, peptic ulcer, gastric mucosa-associated lymphoid tissue lymphoma, and gastric cancer. The phaseⅠand Ⅱclinical trial of oral recombinant Helicobacter pylori vaccine had completed in Jiangsu Province in China. The data from phaseⅠand Ⅱclinical trial suggested that the oral recombinant Helicobacter pylori vaccine had a clinically acceptable safety and good immunogenicity for health adults and children. To further explore the safety and immunogenicity profile of this vaccine, a phase Ⅲ clinical trial was conducted.
Helicobacter pylori (H. pylori) is a Gram-negative, microaerophilic bacterium that persistently colonizes the human stomach; more than half the human population is infected worldwide. H. pylori infection is the major risk factor for the development of gastritis, peptic ulcer, gastric mucosa-associated lymphoid tissue lymphoma, and gastric cancer. At present, the main clinical treatment for H. pylori infection is the application of antibiotics and bismuth agent or H+ antagonists. Due to the widespread drug resistance, toxic side effects, high medical costs as well as poor patient compliance, it is unworkable to practice antibiotics therapy for H. pylori eradication on every patient. Vaccination is the most effective way for prevention H. pylori infection. Since H. pylori were found, great attention has been given to the H. pylori vaccine, scientists worldwide have made great efforts to develop both prophylactic and therapeutic H. pylori vaccine. Numerous H. pylori vaccine approaches have been studied, including inactivated whole cell H. pylori vaccine, genetic engineering subunit vaccine, live vector vaccines. Urease is considered to be an excellent candidate antigen for vaccine against H. pylori. However, no vaccine against H. pylori has been used in clinic. The phaseⅠand Ⅱclinical trial of oral recombinant Helicobacter pylori vaccine had completed in Jiangsu Province in China. The data from phaseⅠand Ⅱclinical trial suggested that the oral recombinant Helicobacter pylori vaccine had a clinically acceptable safety and good immunogenicity for children. To further explore the safety and immunogenicity profile of this vaccine, a phase Ⅲ clinical trial was conducted.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
PREVENTION
Masking
TRIPLE
Enrollment
4,464
Jiangsu Provincial Center for Diseases Control and Prevention
Nanjing, Jiangsu, China
The occurrence of Helicobacter pylori infection in participants one year after three-dose vaccinations.
Time frame: one year after the third dose
The immune response of anti-UreB IgG antibodies in serum after three-dose vaccinations in the immunogenicity subset of participants
seroconversion rates, GMTs, GMFI of anti-UreB IgG antibodies in serum after three-dose vaccinations in the immunogenicity subset of participants at month 1.
Time frame: 1 month after the third dose
The immune response of anti-UreB sIgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants
conversion rates, GMTs, GMFI of anti-UreB sIgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants at month 1
Time frame: 1 month after the third dose
The immune response of anti-UreB IgG antibodies in serum three-dose vaccinations in the immunogenicity subset of participants.
seroconversion rates, GMTs, GMFI of anti-UreB IgG antibodies in serum after three-dose vaccinations in the immunogenicity subset of participants at month 6
Time frame: 6 months after the third dose
The immune response of anti-UreB IgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants
To evaluate conversion rates, GMTs, GMFI of anti-UreB sIgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants at month 6
Time frame: 6 months after the third dose
The immune response of anti-UreB IgG antibodies in serum after three-dose vaccinations in the immunogenicity subset of participants
seroconversion rates, GMTs, GMFI of anti-UreB IgG antibodies in serum after three-dose vaccinations in the immunogenicity subset of participants at month 12
Time frame: 12 months after the third dose
The immune response of anti-UreB sIgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants
conversion rates, GMTs, GMFI of anti-UreB sIgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants at month 12
Time frame: 12 months after the third dose
Frequency of adverse reactions after taking the H. pylori vaccines in children
Frequency of adverse reactions within 3 days after taking the H. pylori vaccines in children
Time frame: within 3 days after each vaccination
Occurrence of serious adverse reactions after taking the H. pylori vaccines in children
Occurrence of serious adverse reactions within one year after the third dose in children
Time frame: From day 0 to One year after the third dose
Anti-UreB IgG antibodies persistency in serum after three-dose vaccinations in the immunogenicity subset of participants
seroconversion rates, GMTs, GMFI of anti-UreB IgG antibodies in serum after three-dose vaccinations in the immunogenicity subset of participants at month 24
Time frame: 24 months after the third dose
Anti-UreB IgA antibodies persistency in saliva after three-dose vaccinations in the immunogenicity subset of participants
conversion rates, GMTs, GMFI of anti-UreB sIgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants at month 24
Time frame: 24 months after the third dose
Anti-UreB IgG antibodies persistency in serum after three-dose vaccinations in the immunogenicity subset of participants
seroconversion rates, GMTs, GMFI of anti-UreB IgG antibodies in serum after three-dose vaccinations in the immunogenicity subset of participants at month 36
Time frame: 36 months after the third dose
Anti-UreB IgA antibodies persistency in saliva after three-dose vaccinations in the immunogenicity subset of participants
To evaluate conversion rates, GMTs, GMFI of anti-UreB sIgA antibodies in saliva after three-dose vaccinations in the immunogenicity subset of participants at month 36
Time frame: 36 months after the third dose
The occurrence of Helicobacter pylori infection in participants in the second year after three-dose vaccinations.
Time frame: in the second year after the third dose
The occurrence of Helicobacter pylori infection in participants in the third year after three-dose vaccinations.
Time frame: in the third year after the third dose.
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