Clinical Trial Details
— Status: Recruiting
Administrative data
| NCT number |
NCT02047994 |
| Other study ID # |
12-36 |
| Secondary ID |
|
| Status |
Recruiting |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
March 2013 |
| Est. completion date |
December 2035 |
Study information
| Verified date |
March 2024 |
| Source |
International Agency for Research on Cancer |
| Contact |
Marcis Leja, MD, PhD |
| Phone |
+37 1 29 49 75 00 |
| Email |
marcis.leja[@]lu.lv |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Currently no ideal preventive modalities are available for reducing gastric-cancer caused
mortality in organized population-based application. The primary objective of the study is to
determine if H.pylori screening followed by eradication of positive subjects and endoscopic
follow-up of those with serological evidence of atrophic gastritis reduces mortality from
gastric cancer in middle-aged people in high-risk areas. The GISTAR study is a multicenter
randomized study of H.pylori eradication and pepsinogen testing for prevention of gastric
cancer mortality. Altogether 30.000 individuals aged 40-64 years will be enrolled, providing
90% study power to detect at least 35% reduction in gastric cancer mortality at 15 years of
follow-up. Participants will be randomly allocated to one of two groups. In the active
investigation/management group those positive for H.pylori will be offered eradication
therapy and individuals with decreased pepsinogen I/II ratio will be invited for endoscopy.
The control group will receive standard health care. The primary endpoint for this trial will
be the mortality difference from gastric cancer between the two groups at 15 years or when
enough cases accumulate to demonstrate a statistical difference. The study is expected to
provide valuable information on the utility for reduction in gastric cancer mortality of: 1)
H.pylori eradication in adults on a population-basis, including subjects who may already have
pre-malignant lesions; and 2) pepsinogen testing in screening settings. A pilot study of
3,455 individuals prior to the main trial was conducted from October 2013 to December 2016.
Description:
Gastric cancer is an important global public health issue in Eastern European regions, where
the burden of the disease is substantial. There is sufficient epidemiological and
experimental evidence that supports a causal link between H. pylori and gastric cancer.
However, there is still limited evidence from clinical trials to prove whether H. pylori
eradication with antimicrobial therapy is the approach of choice in entire infected
populations or only in selected groups to reduce the risk of gastric cancer and whether
eradication at advanced stages of atrophy is effective among these patients. The current
European and global guidelines are proposing screening with pepsinogen tests as the best
available tool to identify the individuals at increased risk for cancer development, yet
there is insufficient evidence available on how effective these tests are in organized cancer
screening settings.
We therefore propose to conduct a multi-center randomized trial in Latvia, Belarus and
Russia, areas with high burden of the disease, with the main objective of evaluating if H.
pylori screening followed by eradication in participants with positive result and endoscopy
of those with serological evidence of atrophic gastritis can reduce gastric cancer mortality.
The proposed trial will also investigate retrospectively if groups with chronic atrophic
gastritis can select subjects who require treatment to achieve comparable gastric cancer
reduction. Ultimately, this study will have the potential to find effective prevention
strategies through identifying appropriate target groups that could get most benefits from
the treatment.
The aim of this study is to search for new intervention strategies to decrease mortality from
gastric cancer in high-risk areas.
The primary objective of the study is to determine if H. pylori screening followed by
eradication of positive subjects and endoscopic follow-up of those with serological evidence
of atrophic gastritis reduces mortality from gastric cancer in a high risk population among
40-64 years old subjects.
The secondary objectives are:
1. To determine retrospectively if biomarkers of chronic atrophic gastritis or others can
select the group of subjects who require treatment to achieve gastric cancer reduction
comparable to the primary objective.
2. To evaluate the rationale for volatile marker testing in exhaled breath for early
identification of lesions in the stomach as well as other conditions related to
increased risk.
3. To evaluate the role of diet, lifestyle factors and environmental factors in the
development of gastric lesions.
4. To evaluate the impact of H. pylori eradication on selected medical conditions
potentially associated with the infection (e.g. obesity, inflammatory bowel disease,
dementia, circulatory diseases and esophageal diseases)
Methods: Approximately 30,000 men and women will be recruited into a randomized study.
Eligible subjects between 40-64 years of age at entry who are residents in high gastric
cancer incidence areas will be invited to participate in the trial by visiting one of the
study clinics set up specifically for this trial.
For eligible participants who agree to participate and sign informed consent, a risk factor
questionnaire will be administered and a complete medical evaluation will be performed at
baseline.
Participants will be randomly assigned to either Group 1 (50%) or Group 2 (50%). Among those
assigned to Group 1, H. pylori screening by detecting immunoglobulin G (IgG) group antibodies
in plasma/serum and pepsinogen test will be performed. According to the results of the tests,
participants will be assigned to H. pylori eradication treatment or upper endoscopy.
Participants with serological evidence of atrophic gastritis (low pepsinogen I/II ratio) will
undergo upper endoscopy with appropriate biopsy sampling as well as further follow-up with
endoscopy according to MAPS (Management of precancerous conditions and lesions in the
stomach) guidelines. H. pylori positive individuals will be offered standard eradication
treatment as appropriate. From subjects in this group, breath samples will also be collected
for volatile markers study by research nurses or junior physicians.
Participants assigned to Group 2 (50%) will constitute the control group, after having had a
medical evaluation at the time of recruitment. During the follow-up period this group will be
offered to consult a specialist when required due to clinical symptoms.
Both Group 1 and Group 2 will be offered fecal occult blood test (FOBT) as a benefit of study
participation. Any participants who show a positive FOBT result will be referred to
colonoscopy.
All the trial participants including Group 2 will be followed up at least for 15 years to
collect systematic information on medical conditions, in particular gastric cancer and cause
of death. A follow-up telephone call /alternative communication will be made every 5 years
for outcome assessment.
The general study is preceded by a pilot-study that was conducted from October 2013 to
December 2016 to test the assumptions as well as the tools and functionality of the study
infrastructure. According to the results of the pilot study, required infrastructure and
tools planned in the general study will be adapted accordingly.
Endpoints: The primary endpoint for our trial will be the mortality difference from gastric
cancer between Group 1 and Group 2 at 15 years or when enough cases accumulate to demonstrate
a statistical difference between the groups.
In addition to the mortality difference from gastric cancer between the two groups, other
endpoints required to achieve the secondary objectives are listed below:
- The difference in gastric cancer incidence between Group 1 and Group 2
- The all-cause mortality difference between Group 1 and Group 2
- The difference in incidence and mortality of medical conditions between Group 1 and
Group 2
- Sensitivity and specificity of pepsinogen tests to detect atrophy
- The proportion of gastric cancers arising in patients with non-atrophic vs. atrophic
gastritis
- The proportion of cancers arising in patients with atrophy, but negative for H. pylori
infection
- The difference in incidence of gastric cancer in the group with successful eradication
when compared to those refusing/failing eradication within Group I
- The proportion of gastric cancer cases being identified during scheduled follow-up
endoscopy out of the total number of cases in the follow-up group
- The differences in the test performance and disease prevalence between ethnic groups
- The performance (sensitivity, specificity, overall accuracy) of volatile marker testing
approach to diagnose gastric cancer as well as premalignant lesions in the stomach
A pilot study with 3,455 participants was started in October 2013 and completed in December
2016 in Latvia.
