Abstract
Adverse effects of proton pump inhibitors (PPIs) have raised wide concerns. The association of PPIs with influenza is unexplored, while that with pneumonia or COVID-19 remains controversial. Our study aims to evaluate whether PPI use increases the risks of these respiratory infections. The current study included 160,923 eligible participants at baseline who completed questionnaires on medication use, which included PPI or histamine-2 receptor antagonist (H2RA), from the UK Biobank. Cox proportional hazards regression and propensity score-matching analyses were used to estimate the hazard ratios (HRs) and 95% confidence intervals (CIs). Comparisons with H2RA users were tested. PPI use was associated with increased risks of developing influenza (HR 1.32, 95%CI 1.12-1.56) and pneumonia (hazard ratio [HR] 1.42, 95% confidence interval [CI] 1.26-1.59). In contrast, the risk of COVID-19 infection was not associated with regular PPI use (HR 1.08, 95%CI 0.99-1.17), while the risks of severe COVID-19 (HR 1.19. 95%CI 1.11-1.27) and mortality (HR 1.37. 95%CI 1.29-1.46) were increased. However, when compared with H2RA users, PPI users were associated with a higher risk of influenza (HR 1.74, 95%CI 1.19-2.54), but not pneumonia or COVID-19-related outcomes. In conclusion, PPI users are associated with increased risks of influenza, pneumonia, as well as COVID-19 severity and mortality compared to non-users, while the effects on pneumonia or COVID-19-related outcomes under PPI use were attenuated when compared to the use of H2RAs. Appropriate use of PPIs based on comprehensive evaluation is required.
1. Introduction
Proton pump inhibitors (PPIs), as one of the most commonly used medications worldwide, have been utilized for treating various conditions related to excessive gastric acid secretion [1]. In the United States, the prescription of PPIs has doubled from 1999 to 2012, and the number of people taking PPIs is still increasing due to their availability over the counter [2]. However, concerns are being raised regarding the long-term and inappropriate use of PPIs, which have been linked to a wide range of adverse conditions, including osteoporotic fractures, renal failure, and vitamin deficiencies [3–5].
PPI-induced hypochlorhydria and gastrointestinal residence of pathogens might increase the risk of respiratory infections [6]. Cohort studies in the United Kingdom and the United States reveal the risks of developing community- and hospital-acquired pneumonia are increased by approximately 100% and 30%, respectively [7, 8]. In contrast, a nested case-control study based on the UK General Practice Research Database indicates long-term PPI therapy is not associated with increased risk for community-acquired pneumonia [9], and a retrospective cohort study involving 593 265 patients in Canada demonstrates no increased risk in developing pneumonia among PPI recipients [10]. Recently, attention has also been paid to the susceptibility to Coronavirus Disease 2019 (COVID-19) caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Based on 53,130 participants in the United States, a dose-dependent increased risk of COVID-19 positivity among PPI users is found [11]. Another Danish study also indicate a marginally increased risk of COVID-19 positivity [12], whereas studies based on the UK Biobank and a Korean cohort indicate nonsignificant association [13, 14]. Meta-analyses on the associations between the use of PPI and SARS-CoV-2 infection also demonstrate conflicting results [12, 15].
To date, the association between PPI and influenza remains unknown. The current evidence referring to PPI, pneumonia and COVID-19 is controversial. Previous studies had several limitations. For instance, the study based on the UK General Practice Research Database did not adjust for potential confounding variables for PPI indications [16]. Direct comparisons with histamine-2 receptor antagonist (H2RA) users were not conducted in previous studies to minimize confounding by indication. In addition, the findings by Almario et al. were based on patients with gastrointestinal symptoms, rather than the general population [11]. The previous UK Biobank study merely included participants tested for COVID-19 from March to June 2020 [13].
By leveraging the large-scale cohort and updated data in the UK Biobank, we aim to evaluate the associations between the regular use of PPIs and the susceptibility to respiratory infections, including influenza, pneumonia, and COVID-19.
2. Methods
2.1 Study population
The detailed information on study design for the UK Biobank was described previously [17]. Invitations were sent to about 9.2 million people who were aged 40-69, had capacity to consent, registered with the National Health Service (NHS), and lived within 25 miles of one of the assessment centers [18]. The participants were free to withdraw at any time [17]. Over 0.5 million participants were recruited from 22 assessment centers in Scotland, England, and Wales (specific locations of assessment centers are available at: https://biobank.ndph.ox.ac.uk/ukb/field.cgi?id=54) from 2006 to 2010. Information such as touch screen questionnaire, interview, blood pressure, eye measurements, physical measurements and so on was collected in the assessment centers (detailed content of assessments is available at: https://biobank.ndph.ox.ac.uk/ukb/refer.cgi?id=100241). Written informed consent was acquired from each participant, and ethical approval was obtained from the North West Multi-Center Research Ethics Committee (approval number: 11/NW/0382, 16/NW/0274, and 21/NW/0157). The current study has been approved under the UK Biobank project 83339. In this study, 11,171 participants with missing PPI medication data and 56,907 participants with missing covariate data were excluded, and we further restricted the cohort to the participants with available primary-care data. Among them, 1,298 participants without follow-up had been removed after initial exclusion. For the evaluation of associations with influenza, pneumonia, and other respiratory infections, those only with self-reported records and diagnoses were further excluded. For the COVID-19 infection and COVID-19-related outcomes, we excluded participants whose COVID-19 testing data were unavailable or who had died before the COVID-19 pandemic (Figure 1).
2.2 Definition of exposure
The exposure of interest was regular use of PPIs. Verbal interviews were conducted by a trained nurse if participants answered that they were regularly taking prescribed or over-the-counter medication on the touchscreen, in which ‘regular’ was defined as most days of the week for the last 4 weeks, and information on specific types of medications was further recorded, while no response to the question on the interview was considered missing data for PPI use. Short-term medications, for example, a 1-week course of antibiotics, were not recorded in the interview. Types of PPIs available in the UK Biobank included omeprazole, lansoprazole, esomeprazole, rabeprazole, and pantoprazole. The regular use of H2RAs was also defied by the above process. When comparing PPI users with H2RA users, participants who took both medications were excluded. Information on dose or duration of acid suppressant use was not available in the UK Biobank.
2.3 Definition of outcomes
The primary outcomes of interest were influenza, pneumonia, COVID-19 infections (Supplementary Table S1). Briefly, the first reported occurrences of respiratory system-related conditions within primary care data, the International Classification of Diseases (ICD)-10 codes were categorized by the UK Biobank (https://biobank.ndph.ox.ac.uk/showcase/label.cgi?id=2410). Influenza included those caused by identified influenza virus (J09-J10) and virus not identified (J11). Pneumonia was defined as that caused by viruses (J12), bacteria (J13-15), and other infectious organisms (J16-18).
COVID-19-related data in the UK Biobank (available from January 2020 to September 2021) based on follow-up of the participants was used [19]. COVID-19 infection mainly included information on positive COVID-19 tests, and patients with inpatient diagnoses or mortality due to COVID-19 were also regarded as having COVID-19 infection.
The secondary outcomes included other upper or lower respiratory infections, COVID-19 mortality, and COVID-19 severity. The definition of other upper respiratory infections contained acute nasopharyngitis, sinusitis, pharyngitis, tonsillitis, laryngitis, tracheitis, obstructive laryngitis, epiglottitis, or upper respiratory infections of multiple and unspecified sites (J00-J06). Other lower respiratory infections included acute bronchitis, bronchiolitis, and other unspecified ones (J20-J22). Severe COVID-19 cases were defined as being hospitalized for COVID-19. COVID-19 mortality was defined as the underlying recorded cause of death due to COVID-19 (ICD-10 U07.1 and U07.2).
2.4 Assessment of covariates
The covariates used for adjustments in our study were identified by a directed acyclic graph (DCA, Supplementary Figure 1) based on existing literature and expert knowledge. Baseline data on sociodemographic information (age, sex, ethnicity), socioeconomic status (deprivation index), alcohol consumption, smoking status, fresh fruit intake, multivitamin use, and body mass index (BMI) were collected from the UK Biobank, while physical activity was assessed using the International Physical Activity Questionnaire-Short Form. Gastroesophageal reflux disease (GERD), peptic ulcers, and upper gastrointestinal bleeding, were included as they are main indications for the use of PPIs. The comorbidities (hypertension, type 2 diabetes, renal failure, myocardial infarction, stroke, chronic obstructive pulmonary disease [COPD], asthma) were examined using self-reported data and adjusted due to their impact on the risk of respiratory infections. Since PPI and H2RA have highly similar indications, the use of H2RA was also adjusted. Data on medication use including aspirin, non-aspirin non-steroidal anti-inflammatory drugs (NSAIDS, including ibuprofen), and cholesterol-lowering medications were extracted and adjusted. For influenza and COVID-related outcomes, vaccinations were additionally adjusted.
2.5 CYP2C19 genetic variants
PPIs are mainly cleared by CYP2C19, and therefore their metabolism and effects are affected by different variants of CYP2C19. Genotyped genetic variant data after quality control was available for UK Biobank participants based on the Affymetrix Axiom UKB array and the Affymetrix UKBiLEVE array [20]. According to the Clinical Pharmacogenetics Implementation Consortium Guideline for CYP2C19 and Proton Pump Inhibitor Dosing [21], genotypic data of four CYP2C19 variants, including rs12248560 (CYP2C19*17), rs17884712 (CYP2C19*9), rs4986893 (CYP2C19*3), and rs4244285 (CYP2C19*2), were utilized to divide PPI users into three subgroups: (1) CYP2C19 rapid and ultrarapid metabolizers (carried 1 functional allele and 1 increased-function allele [*17]; or carried 2 increased-function alleles); (2) CYP2C19 normal metabolizers (carried 2 functional alleles); (3) CYP2C19 likely intermediate, intermediate and poor metabolizers (carried ≥ 1 alleles with no/decreased function [*2, *3, and *9]).
2.6 Statistical analysis
The baseline characteristics were demonstrated by percentages for categorical variables, and mean (standard deviation [SD]), or median (interquartile range [IQR]) for continuous variables according to the distribution of data after evaluating the data distribution.
Univariate and multivariate Cox proportional hazards regression models were utilized to assess the association between regular use of PPIs and the selected outcomes, and the results were presented as hazard ratios (HRs) with 95% confidence intervals (CIs). Multivariable model 1 included age and sex. Model 2 additionally contained other potential confounders selected a priori, including ethnicity, deprivation index, alcohol consumption, smoking, physical activity, BMI, fresh fruit intake, GERD, peptic ulcer, upper gastrointestinal bleeding, hypertension, type 2 diabetes, renal failure, myocardial infarction, stroke, COPD, asthma, aspirin, non-aspirin NSAIDS, H2RA, cholesterol-lowering medications, and multivitamin use. The reference group was participants without regular use of PPIs. Schoenfeld residuals tests were used to evaluate the proportional hazards assumptions, while no violation of the assumption was detected. Person-years were calculated from the number of participants and the date from Jan 2020 (for COVID-19-related outcomes) or recruitment (for other respiratory outcomes) to outcome diagnosis, last follow-up (September 2021 for COVID-19 infection and related outcomes; December 2021 for other outcomes), or death, whichever came first. Stratified analyses according to population characteristics, types of PPIs, and CYP2C19 metabolizers were performed using multivariable-adjusted models across subgroups of each stratifying variable, and the multiplicative interactions were evaluated using likelihood ratio tests
Quantitative bias analyses were performed to calculate e-values, which illustrates the strength of association between an unmeasured confounder and exposure or outcome, conditional on the measured covariates [22]. E-value is the smallest magnitude of risk estimates that an unmeasured confounder would need to have with the exposure and outcome to explain away an observed association [22]. The event-free probabilities were compared by Kaplan-Meier survival curves. In addition, we conducted additional analyses using multiple imputation by chained equations to include participants initially excluded due to missing ethnicity data using the “mice” package [23]. Moreover, propensity score-matching analysis was conducted. The same set of covariates was used to derive propensity scores, and the PPI users and non-users were matched with a ratio of 1:4 using the “MatchIT” package [24], which estimated the propensity scores in the background and matched observations based on the nearest neighbor method. The remaining imbalanced covariates (standardized mean difference ≥ 0.1) after propensity score matching were further adjusted by multivariate Cox regression models to calculate HRs and 95% CIs [25]. Furthermore, because PPI and H2RA share highly similar indications, we performed head-to-head comparisons between PPI and H2RA users to further minimize the protopathic bias [26, 27].
All statistical analyses were performed using R (version 4.2.0, https://www.r-project.org/). The significance level at α = 0.05 with two tails was used. Risk estimates were reported with 95% CIs.
3. Results
3.1 Study population
A total of 160,923 individuals aged 38 to 71 years who passed the initial selection criteria in the UK Biobank were included in this study (Table 1). The median follow-up was 7.1 (interquartile range [IQR] 6.2-8.5) years. The mean age of the included participants was 56.5 years, and 53.0% of them were women. Evidently, regular PPI users were characterized by higher rates of GERD (32.4% vs. 2.7%), peptic ulcer (5.6% vs. 0.9%), and upper gastrointestinal bleeding (0.2% vs. 0.03%) compared to non-regular PPI users. Higher burdens of comorbidities, as well as increased use of aspirin, H2RA, and cholesterol-lowering medications, were also observed in regular PPI users.
3.2 Proton pump inhibitor use and influenza, pneumonia, and COVID-19 infection
Increased risks of developing influenza, pneumonia, and other respiratory infections were identified in regular users of PPIs compared with non-regular users, and the risk remained raised after adjustments (Table 2). A 32% increased risk of developing influenza (aHR 1.32, 95% CI 1.12-1.56, P = 0.001; e-value 1.97) was observed among regular PPI users. In addition, regular use of PPIs was associated with a 42% increased risk of developing pneumonia (fully adjusted HR [aHR] 1.42, 95% CI 1.26-1.59, P < 0.001; e-value 2.19). Regular PPI users had lower event-free probabilities for influenza and pneumonia compared to those of non-users (Supplementary Figure 2 A-B). The association of PPI use with COVID-19 positivity was further evaluated in our study. Initially, in the non-adjusted model, the susceptibility to COVID-19 positivity was observed with a 18% increase (HR 1.18, 95% CI 1.09-1.26, P < 0.001 for non-adjusted model; Table 2) in participants with regular use of PPIs. However, full adjustments for covariates rendered the association nonsignificant (aHR 1.08, 95% CI 0.99-1.17, P = 0.101; Table 2).
3.3 Proton pump inhibitor use and other respiratory infections, COVID-19 severity, and COVID-19 morality
For other upper and lower respiratory infections, the risks among regular PPI users were increased by 19% (aHR 1.19, 95% CI 1.11-1.27, P < 0.001; e-value 1.67) and 37% (aHR 1.37, 95% CI 1.29-1.46, P < 0.001; e-value 2.08), respectively. In contrast, the risks of developing severe COVID-19 (aHR 1.33, 95% CI 1.09-1.61, P = 0.004; e value 1.99) and mortality due to COVID-19 (aHR 1.46, 95% CI 1.05-2.03, P = 0.024; e value 2.03) were significantly increased among PPI users compared to those among PPI non-users (Supplementary Table S2). PPI users had lower event-free probabilities for COVID-19 severity and mortality, but not COVID-19 positivity compared to those of non-users (Supplementary Figure 2 C-E).
3.4 Subgroup analysis
Stratified analyses were performed in the fully adjusted models for the main outcomes. Overall, no significant evidence of interactions was observed in the subgroup analyses referring to influenza (all P for interaction > 0.05, Figure 2). The subgroup analyses for other main outcomes were illustrated in Figure 2 and Supplementary Figure 3.
Among different types of PPIs, regular omeprazole or lansoprazole users were correlated with greater risks of respiratory infections(Supplementary Table S3). The risks of influenza were significant among CYP2C19 normal metabolizers, and the risk estimate increased among CYP2C19 likely intermediate, intermediate and poor metabolizers, while more information and larger sample sizes on PPI subtypes are still needed to increase the statistical power (Supplementary Table S4). The risks of COVID-19 severity and COVID-19 mortality were higher among CYP2C19 likely intermediate, intermediate and poor metabolizers (Supplementary Table S5). The risks of pneumonia were higher among CYP2C19 rapid and ultrarapid metabolizers (Supplementary Table S4).
3.5 Analysis by multiple imputation and propensity score-matching
After imputation of missing data, we found that individuals with regular use of PPIs were associated with similarly increased trends in the risks of influenza, pneumonia, other upper respiratory infections, and other lower respiratory infections (all P < 0.05) (Supplementary Table S6). The associations with COVID-19 severity and mortality were also significant (all P < 0.05) (Supplementary Table S7).
Matching of 9,910 regular PPI users and 39,760 non-regular users (1:4 by propensity scores) was also conducted, and the baseline characteristics were much more similar (Supplementary Table S8). The participants regularly exposed to PPIs were observed with increased risks for influenza, pneumonia, other upper respiratory infections, and other lower respiratory infections (all P < 0.05) (Supplementary Table S9), which were consistent with the results from Cox hazard proportional regression models. The associations with COVID-19 severity and mortality were also significant (all P < 0.05) (Supplementary Table S10).
3.6 Comparisons with H2RA users
To further confirm the results and reduce the effect of confounding by indications, we evaluated the risk of respiratory infections compared to the use of H2RAs, which is a less potent acid-suppressant and contains indications similar to PPI. When compared to regular H2RA users, participants with regular use of PPIs were also associated with an increased risk of influenza (HR 1.74, 95% CI 1.19-2.54, P = 0.004; e-value 2.87), other upper respiratory infection (HR 1.28, 95% CI 1.07-1.54, P = 0.008; e-value 1.88), and other lower respiratory infection (HR 1.33, 95% CI 1.18-1.50, P < 0.001; e-value 1.99) (Table 3). However, the associations with pneumonia (HR 1.22. 95% CI 0.96-1.54, P = 0.104),COVID-19 infection (HR 1.04. 95% CI 0.87-1.26, P = 0.629), COVID-19 severity (HR 0.91. 95% CI 0.64-1.30, P = 0.608), or COVID-19 mortality (HR 0.83. 95% CI 0.45-1.56, P = 0.745) were not significant (Supplementary Table S11).
4. Discussion
In this large-scale, population-based cohort with updated information, we identify that the use of PPIs is associated with incident influenza. In contrast, analyses of pneumonia, COVID-19 infection and related outcomes, reveal attenuated effects after being compared with H2RA users. The association with influenza remains robust across different subgroups stratified by population characteristics and CYP2C19 phenotypes.
The correlation between PPI use and the risk of influenza remains unexplored. For the past two decades, accumulating evidence indicates increased risks of pneumonia under the use of PPIs [7, 8, 28, 29], whereas others failed to show such associations [9, 10]. Conflicting findings also exist for studies referring to the risk of COVID-19 infection and related outcomes among PPI users, including several meta-analyses [11–15, 30–33]. Compared with existing studies, our study more comprehensively adjusts for a variety of critical covariates by utilizing the latest data from the UK Biobank. In addition, distinct from previous population-based studies, we compared the risks with H2RA users to further reduce protopathic and other unmeasured bias, since the users of acid suppressants, including PPIs and H2RAs, can have matched information on different characteristics, including indications. Although the risks of pneumonia were initially increased in Cox and propensity-score-matched analyses, direct comparison with H2RA users showed negative results, which indicates that previously observed associations could be due to unmeasured confounders.
Several proposed mechanisms can account for the association between the use of PPIs and respiratory tract infections. Since a low pH of gastric acid rapidly inactivates microorganisms, one critical issue is that reduced acidity induced by PPIs leads to the overgrowth of microorganisms, which can contribute to the development of infections in the respiratory tract through microaspiration[34]. Colonization and growth of pathogens under hypochlorhydria could increase the risk of respiratory infections. Although initial assessments indicated the use of PPIs might increase the risk of pneumonia, the head-to-head comparison with H2RAs yielded impacted effects. It could be due to the similar acid-suppressive effects of H2RAs and reduced sample size, which therefore warrants further investigations.
Concerns over protopathic bias due to non-specific and overlapping symptoms between influenza/pneumonia and acid-related diseases were raised [35]. Nevertheless, pneumonia and influenza often present with acute cough, and other concomitant symptoms distinct from acid-related diseases [36]. In contrast, patients with chronic cough are more commonly GERD-related [36]. The American College of Chest Physicians Clinical Practice Guidelines for Management of Reflux-Cough Syndrome also recommend against using PPI therapy alone for patients with chronic cough but without heartburn or regurgitation [37]. In our study, the use of PPIs is defined as taking the medication for most days of the week in the last 4 weeks, which is uncommon for acute cough. Although we cannot completely rule out protopathic bias, we have attempted to minimize it by adjusting for covariates including PPI indications, matching with propensity scores, and comparing with H2RA users.
For the risk of developing influenza, we analyzed the risks among different CYP2C19 metabolizers for the first time, and further observed a significant increase among CYP2C19 normal metabolizers compared to rapid and ultrarapid metabolizers. Although the risks of several outcomes, for example, influenza and pneumonia, for CYP2C19 likely intermediate, intermediate and poor metabolizers are not statistically significant, they could be due to the limited sample size, and the risk estimates are higher compared to those among other types of metabolizers. Intriguingly, the risks of developing influenza and pneumonia are higher among CYP2C19 rapid and ultrarapid metabolizers regularly taking PPIs compared to other types of metabolizers. Since our study exclusively involves participants with valid primary care data, such an increased risk might be to some extent contributed by the over-prescription or self-taking of PPIs under the undesired effects without following the proper strategy. Our findings are generally consistent with the assumption that slower metabolizers are associated with higher risks of adverse effects, while larger samples are needed to increase statistical power. Prescription of PPIs based on different CYP2C19 metabolism subtypes is therefore important to reduce the adverse effects.
Our study has several strengths. First, our study utilizes the updated large-sample data from the UK Biobank and exclusively includes participants with valid records from primary care, which reduces the information bias. Second, a variety of covariates, especially for the indications of PPIs and the use of aspirin, which might contribute to indication or protopathic bias, have been adjusted to enhance the robustness of our results. Third, genotypic data of metabolic enzymes has been integrated into our study. Fourth, propensity score-matching analysis reduces a greater portion of bias, and analyses by propensity-score matching or multiple imputation derive consistent results. Fifth, adjustments for vaccination for COVID-19 and influenza has been performed in our study to reduce the confounding effects by vaccination. Furthermore, the comparison with participants using H2RA, a less potent acid suppressant with similar indications, further reduces the confounding by indication. The findings on the risk of influenza remain highly consistent across different strata and sensitivity analyses.
Limitations exist in our study. Information on dose and duration of PPI use, different types of pneumonia, and pneumococcus vaccination is currently not available from the UK Biobank. It was possible that PPI use was misclassified during the follow-up in the UK Biobank since PPI use was mainly assessed at baseline. However, no effect moderation was observed in subgroup analyses for PPI users with indications (more likely to regularly use PPIs for a long period) compared to those without indications, indicating the risks remained increased among long-term PPI users. Additionally, PPIs are indicated for Helicobacter pylori (H. pylori) eradication, whereas the UK Biobank does not contain adequate data. Thus, the indication for eradicating H. pylori is not adjusted in this study. The data on different PPI subtypes and COVID-19 infection and related outcomes are relatively small, which limits their power and still needs further investigation. Moreover, residual confounding might still exist due to the observational nature, while the quantitative bias analysis indicated that our result was robust to unmeasured confounding. Residual genotyping impacts of other enzymes, although affecting the metabolism to a lesser extent, might also exist. Although no significant differences were found between PPIs and H2RAs regarding the association with pneumonia and COVID-19-related outcomes, this could be due to the reduced sample size and power, which require larger cohorts to validate the effects. Furthermore, the current study is principally based on white British ancestry in the United Kingdom, and future exploration of other ancestries with comparisons is warranted.
Our findings could have essential implications for the prevention of respiratory infections and the de-prescribing of PPIs in clinical practice. Administration of PPIs can rapidly increase intragastric pH to higher than 6 after 2-4 hours [38]. Emerging evidence has revealed the inappropriate prescription of PPIs in both the primary and secondary care settings, and 33-67% of the patients did not take the drug according to their countries’ criteria [39]. Similarly, the baseline characteristics of the included participants in our study demonstrate that approximately 60% of the regular PPI users do not have main indications. In addition, although influenza is usually self-limiting in healthy individuals, its risk of complications is significantly increased among pregnant women and people with immunosuppression or chronic diseases [40]. Therefore, comprehensive evaluation of PPI use is needed in clinical practice.
5. Conclusion
In conclusion, compared to non-users, people regularly taking PPIs are associated with increased susceptibility to influenza, pneumonia, as well as COVID-19 severity and mortality, while their association with pneumonia and COVID-19-related outcomes is attenuated after comparison with the use of H2RAs and remains to be further explored.
Data Availability
The UK Biobank data are available at https://www.ukbiobank.ac.uk/ after approval of application.
Conflict of Interest Statement
The authors declared no conflict of interest.
Declaration of generative AI in scientific writing
This study does not involve generative AI in scientific writing.
Acknowledgements
The authors are grateful to the UK Biobank for approval and access to data of the project, and this research has been conducted under Application Number 83339. We thank Dr. Qian Chen for her kind suggestions on statistical analyses.
Availability of Data and Materials
The UK Biobank data are available on application to the UK Biobank (www.ukbiobank.ac.uk).
Funding
This work is supported by the National Natural Science Foundation of China (82171698, 82170561, 81300279, 81741067, 82100238), the Program for High-level Foreign Expert Introduction of China (G2022030047L), the Natural Science Foundation for Distinguished Young Scholars of Guangdong Province (2021B1515020003), the Guangdong Basic and Applied Basic Research Foundation (2022A1515012081), the Foreign Distinguished Teacher Program of Guangdong Science and Technology Department (KD0120220129), the Climbing Program of Introduced Talents and High-level Hospital Construction Project of Guangdong Provincial People’s Hospital (DFJH201923, DFJH201803, KJ012019099, KJ012021143, KY012021183), and in part by VA Clinical Merit and ASGE clinical research funds (FWL).
Abbreviations
ACE2: angiotensin-converting enzyme 2
BMI: body mass index
CI: confidence interval
COVID-19: Coronavirus Disease 2019
DCA: directed acyclic graph
GERD: gastroesophageal reflux disease
H2RA: histamine-2 receptor antagonist
HR: hazard ratio
IQR: interquartile range
NSAIDS: non-aspirin non-steroidal anti-inflammatory drugs
PPI: proton pump inhibitor
SARS-CoV-2: severe acute respiratory syndrome coronavirus 2
SD: standard deviation.
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