Drug Use Clinical Trial
Official title:
Nordic Gastric and Esophageal Tumor Study
This is a population-based case-control study in all 5 Nordic countries from 1994 onwards. All cases with an esophageal or gastric tumor will be compared with 10 times as many population controls, frequency-matched by age, sex, and calendar year, country. This design offers excellent statistical power, length and completeness of follow-up, quality of data on exposures, outcomes and confounders, and control for confounding. The project will include a specific study entitled "Long-term medication with proton pump inhibitors and risk of gastric cancer", which is summarized here: Research question: Medication with proton pump inhibitors (PPI) (e.g., omeprazole and esomeprazole) is one of the most common long-term therapies globally, prompted by its high anti-acidic efficacy and good short-term safety profile. Gastric cancer is the 3rd leading cause of cancer-related mortality globally, responsible for 770,000 deaths each year. There are clear biological mechanisms linking long-term PPI-use with an increased risk of gastric cancer. However, existing research has not been able to provide a definite answer to whether long-term PPI-use is associated with an increased risk of gastric cancer. The reasons are that the literature is hampered by too short follow-up time to assess cancer development, and also insufficient statistical power, lack of population-based design and confounding. With the availability of nationwide complete medication registries in the Nordic countries, the firsts two starting already in 1994 (Denmark and Finland), we can now, by adding registry data from all Nordic countries together, conduct the first study providing a robust and valid answer to this research question. Overarching aim This project aims to clarify if (and if so to what extent) long-term PPI-therapy influences the risk of developing gastric adenocarcinoma. For validation reasons, we will also examine how long-term use of histamine-2-receptor blockers (H2RB) influences the risk of developing gastric adenocarcinoma. These analyses will validate that the findings are specific for PPIs. H2RB are used for the same indications as PPIs, but with a different biological mechanism. Hypothesis We plan to test the hypothesis that long-term use of PPI (but not H2RB) increases the risk of gastric adenocarcinoma. Prerequisites This will be the first project with all prerequisites to provide conclusive answers to the hypotheses above, i.e.: - Long follow-up (up to 28 years) - Complete follow-up (by virtue of the nationwide complete Nordic registries) - Population-based design (which rules out biased selection of cases or controls) - Superior statistical power (all five Nordic countries participate with nationwide data) - High-quality data on exposures, outcomes and confounders (thanks to well-maintained and complete nationwide Nordic health data registries) - Control for confounding factors (available for all participants, both cases and controls)
PROJECT DESCRIPTION Theory and method Study design We will conduct a nationwide and population-based multi-national case-control study in the five Nordic countries during the total study period from 1994 through 2022, thus allowing up to 28 years of follow-up. The start of the study period will vary between countries depending on when their national drug registries started, i.e. in 1994 (Denmark), 1994 (Finland), 2002 (Iceland), 2004 (Norway) and 2005 (Sweden). Participants The study will include all adult residents in Sweden, Denmark, Finland, Iceland and Norway with a first gastric adenocarcinoma diagnosed during the study period according to the national cancer registries. The control participants are selected from the general populations of the five countries and frequency-matched for age, sex, calendar year, and country. The index date for matching is the date of gastric adenocarcinoma diagnosis. For each case of gastric cancer, 10 control participants will be included. Because the controls are matched within each country by age and calendar year, the time-window used to ascertain the exposure will be the same in cases and controls. We will have the same detailed information on all study variables in cases and controls. Exposure The exposure is long-term PPI-use. Two definitions will be used. The first, high PPI-consumption, is defined as >180 defined daily doses (DDD) of PPI per year during the time from start of the drug registry or entry in the cohort until the index date. The second definition is cumulative exposure to PPI, defined by the total number of DDDs consumption during the time window of exposure. The DDDs are retrieved from the prescribed drug registries. From a Swedish cohort of 8,276,316 adult individuals of the general population that we use for research purposes, 496,579 (6.0%) were exposed to long-term PPI-use (>180 DDDs). The comparison exposure is long-term use of an H2RB (>180 DDDs), measured using the same two definitions described for PPI, i.e., high H2RB consumption and cumulative exposure. DDDs for H2RB are also retrieved from the prescribed drug registries. Outcome The study outcome will be gastric adenocarcinoma. Adenocarcinoma represents >95% of all gastric malignancies. We will not assess rare histologies of gastric malignancy because these have different aetiology, including the potential association with PPI-use. We will also conduct separately sub-analyses of cardia adenocarcinoma and non-cardia adenocarcinoma. Confounders A confounder is by definition associated with both the exposure and the outcome (and is not in the causal pathway between these).29 The main risk factor for gastric adenocarcinoma is 1) Helicobacter pylori-infection, but also other less strong risk factors might also have some confounding effects in this project, i.e., 2) age (as for most cancer types), 3) sex (a majority of patients with gastric adenocarcinoma are men), 4) calendar year (there have been changes in diagnostic ability of gastric adenocarcinoma), 5) country (there are some variations in incidence rates of gastric adenocarcinoma between the Nordic countries), 6) comorbidity (some severe diseases included in the Charlson comorbidity index might increase the risk of gastric adenocarcinoma), 7) long-term medication with aspirin or non-steroidal anti-inflammatory drugs (such medication may decrease the risk of gastric adenocarcinoma) and 8) long-term medication with statins (could also decrease this risk). All these 8 variables will be controlled for. Age, sex, calendar year, and country will be controlled for by matching. Helicobacter pylori, comorbidity, long-term medication (>180 defined DDDs per year) with aspirin or non-steroidal anti-inflammatory drugs and statins will be adjusted for using multivariable logistic regression. Regarding Helicobacter pylori, we will use treatment of this infection as a marker of infection, which is the most complete and valid way to assess presence of this infection in the dataset. For comorbidity we will use the most recent version of the well-validated Charlson comorbidity index.30 We have excellent data of both medication variables from the drug registries. Data sources For each participant, both cases and all controls, we will collect data from the following nationwide registries in all five countries: 1) Prescribed drug registries, 2) cancer registries, 3) patient registries, 4) cause of death registries and 5) registries of the total population. This will allow data on demographic characteristics (age, sex, calendar year, country), use of all relevant medications (including PPI, H2RB, Helicobacter pylori treatment, aspirin or non-steroidal anti-inflammatory drugs and statins with substance, brand name, ATC-code, formulation, package size, amount, dosage and dates for prescription and dispensation), comorbidity (all diagnoses and surgical procedures), and mortality. Project organisation Research team Ten people are directly involved in this project. The project originates and is organised from our research group at Karolinska Institutet (KI). The local team includes 7 people: The chief investigator Jesper Lagergren (main applicant), the biostatistician Giola Santoni, the statistician Jacinth Yan, the postdoctoral researcher Cecilia Radkiewicz, the PhD candidate we hope to recruit, and the administrator Giulia Marras. In addition, we have representatives of each of the four non-Swedish countries included in the project, i.e., associate professor My von Euler-Chelpin (Denmark), professor Joonas Kauppila (Finland), associate professor Helgi Birgisson (Iceland) and associate professor Eivind Ness-Jensen (Norway). The main roles of these team members are outlined here: 1. Jesper Lagergren will lead the work and the team conducting the work, be responsible for the progress of the project, and be supervisor of the postdoc and PhD candidate. 2. Giola Santoni will guide and supervise in the data complex data management and statistical analyses and co-supervise the PhD candidate. 3. Jacinth Yan will conduct complex data management and analyses. 4. Cecilia Radkiewicz will help with the planning and co-supervise the PhD candidate. 5. The PhD candidate will draft the detailed study protocol, do data management and statistical analyses with support of Giola Santoni, and draft the paper. 6. My von Euler-Chelpin is responsible for the Danish data collection. 7. Joonas Kauppila is responsible for the Finnish data collection. 8. Helgi Birgisson is responsible for the Icelandic data collection. 9. Eivind Ness-Jensen is responsible for the Norwegian data collection. 10. Giulia Marras will help organise the collaboration and administer the project. Data storage and management Because Danish law does not allow their data to leave the country, data will be stored at a safe server at the governmental agency Statistics Denmark, and managed by remote access. Giola Santoni is responsible for the data management and statistical analyses. Main applicant The main applicant, Jesper Lagergren, will spend approximately 10% of his work-time for this specific project. He is the chief investigator of this multi-national project. DATA ANALYSIS AND STATISTICS Design This will be a population-based case-control study with prospectively collected data on all variables for all cases and controls in the five Nordic countries. The data collection is prospective, which avoids recall bias and selection bias. For each case of gastric adenocarcinoma, 10 control participants from the general populations will be recruited. The control participants will be frequency-matched to the cases regarding age, sex, calendar year and country of residence. The additional possible confounders, i.e., Helicobacter pylori, comorbidity and medication with aspirin or non-steroidal anti-inflammatory drugs as well as statins will be adjusted for by modelling. Statistical analysis Conditional logistic regression will be used to estimate the relative risk of gastric adenocarcinoma comparing long-term PPI-users with non-users, providing odds ratios with 95% confidence intervals. Three models will be applied: 1) A crude model where only the matching variables are controlled for; 2) an adjusted model additionally adjusted for Helicobacter pylori, comorbidity and medication with aspirin or non-steroidal anti-inflammatory drugs as well as statins, and 3) a model with multivariable adjustment for all 8 confounders listed under 'Confounders' above, which will guarantee that these variables are completely adjusted for. We will also do stratified analyses for each of these 8 confounders. In addition, we will assess whether increased length of PPI-use (>10 years) among long-term users is associated with higher risk estimates, which would argue in favour of causality. Except for conventional confounding, confounding by indication (particularly protopathic bias) is a special threat to the validity of many pharmaco-epidemiological studies. However, long-term PPI-use is not an indication for gastric adenocarcinoma. Thus, this should not be a problem in the present project. Statistical power One of the advantages of the project is the excellent statistical power, which is due to inclusion of cases from five entire countries, long and complete follow-up and relatively high prevalence of long-term PPI-users. In order to further optimise the power, we include 10 controls per case, after which further controls will not improve power.31 The main analysis will include all approximately 47,000 cases and 470,000 controls, and sub-analyses of non-cardia adenocarcinoma will include 35,300 cases and 353,000 controls, while the sub-analysis of cardia adenocarcinoma will include 11,700 cases and 117,000 controls. The exposure prevalence of long-term PPI-use is 6% (and 2% for H2RB use). The main analysis has 100% power to verity an odds ratio already of 1.10, and we expect a much stronger association. For the analysis of cardia adenocarcinoma, the study has 94% power to verify an odds ratio of 1.15. ;
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