Does Proton Pump Inhibitor Increase the Clostridium difficile Infection Risk in the Treatment and Prophylaxis of Stress Ulcers than Histanime-2 Receptor Antagonist?

Clostridium difficile infection (CDI), most common cause of hospital acquired infectious diarrhea, has been reported to be increasing in incidence, severity, and mortality over the past several decades throughout the world. Several risk factors for CDI have been demonstrated including antibiotics exposure, old age, prolonged hospital and intensive care unit (ICU) stay, previous CDI episode, co-morbidities, and acid suppression therapy such as proton pump inhibitors (PPIs), and histamine 2 receptor antagonists (H2RAs), and so forth. Among them, acid suppression therapy has recently received an increased attention as a risk factor for CDI. Several epidemiologic studies have suggested increased CDI risk is associated with both PPIs and H2RAs.

Meanwhile, PPIs and H2RAs have been commonly used for prophylaxis and treatment of stress ulcers in critically ill patients. Several randomized controlled trials (RCTs) and meta-analyses demonstrated that PPIs were more effective than H2RA in preventing gastrointestinal (GI) bleeding, while others reported no significant difference between PPIs and H2RAs.1 Furthermore, some meta-analyses revealed no mortality benefit in patients with stress ulcer prophylaxis (SUP) than those without SUP.2 Although critically ill patients are at high risk of developing stress related ulcerations, the prevalence of overt GI bleeding in these patients has been reported to be relatively low, around 5%.

Several guidelines have recommended SUP just in patients with high risk factors for clinically important GI bleeding such as mechanical ventilation, coagulopathy, acute renal injury, and hepatic failure, and so forth. However, inappropriate use of gastric acid suppressants appear to be common in clinical practice. In some studies, 63% of ICU patients and 60% of hospitalized general ward patients, who prescribed SUP, had no appropriate indication and one-third of these patients were discharged without discontinuation of the medication.3,4

Several studies have demonstrated that both PPIs and H2RAs are associated with an increased risk of CDI occurrence. Although precise mechanisms of CDI occurrence by gastric acid suppression are not clear, loss of gastric acidic environment caused by PPIs or H2RAs has been suggested to induce bacterial overgrowth and altered distal gut microbiome with decreased bacterial diversity, which may contribute to CDI occurrence. The meta-analysis by Tleyjeh et al.,5 which included 35 observational studies with a total of 201,834 participants, demonstrated a relative risk of 1.44 (95% confidence interval, 1.22 to 1.70) for CDI occurrence among patients with H2RA therapy. On the contrary, several meta-analyses have showed pooled odds ratios of 1.65 to 2.15 for CDI occurrence among patients with PPIs therapy. In addition, U.S. Food and Drug Administration recently warned CDI can be associated with PPIs use.6–8 However, it is unclear whether the relation of gastric acid suppression (PPIs and H2RAs) and CDI occurrence is causal or mere association, suggesting that future well-organized prospective RCTs would be warranted.

To date, there has been little data of meta-analyses directly comparing CDI occurrence risk between PPIs and H2RA among patients with stress ulcer treatment and prevention. In this issue of Gut and Liver, Azab et al.9 investigated the comparative CDI risk of PPIs versus H2RAs in the prophylaxis and treatment of stress ulcers using a systematic review and meta-analysis. This meta-analysis, which included nine case-control and three cohort studies with a total of 74,132 patients, reported a pooled odds ratio of 1.386 (95% confidence interval, 1.152 to 1.668; p=0.001) for CDI occurrence among patients with PPIs use than those with H2RAs use. The results were consistent in the subgroup analyses of medication use purpose, study site, and study design. Therefore, current analysis suggest that PPIs use is associated with a higher risk of CDI occurrence by 38.6% in the prevention and treatment of stress ulcers compared to H2RAs use. This study, a first meta-analysis directly compared CDI risk between PPI versus H2RA during prevention and treatment of stress ulcers so far, provide clinicians with a valuable insight into the SUP strategy in real practice.

However, the results of this study does not conclude that clinicians would be better to choose H2RAs for prophylaxis and treatment of stress ulcers than PPIs. As the authors described, the quality of evidence of individual studies enrolled in this meta-analysis was low, implying that conclusions of this study must be interpreted cautiously. In addition, this meta-analysis could not analyze the potential impact of antibiotics use, the most important risk factor on CDI occurrence, because of natural limitation of the study design. To validate current meta-analysis findings and apply to clinical practice, further large-scaled prospective RCTs investigating the comparative efficacy of SUP, the potential influence on CDI occurrence, and the cost-effectiveness between PPIs and H2RAs use, should be needed among patients with high risk of overt GI bleeding.

In summary, currently available clinical data suggest relatively weak evidence that PPIs use seem to be more effective in preventing clinically overt GI bleeding and more risky for CDI occurrence compared to H2RA use. At present, considering the increasing incidence and clinical impact of CDI, and widespread use of PPIs and those potential serious side effects, clinicians should try to be confident that benefits of PPIs use always outweigh the harms for individual patients. In addition, SUP with PPIs or H2RA should be limited to critically ill patients at high risk for clinically important GI bleeding.