Chemoprevention in Barrett's oesophagus.
Study Goal
The researchers aimed to evaluate the potential of antioxidants, among other agents, in preventing the progression of Barrett's oesophagus to cancer.
Results Summary
The abstract mentions antioxidants as one of the suggested agents for chemoprevention but does not provide specific results regarding their effectiveness. The evidence for antioxidants is discussed, but no conclusive findings are highlighted.
Population
Patients with Barrett's oesophagus.
Effective Dosage
Not specified
Duration
Not specified
Interactions
None mentioned
| Intervention | Direction | Endpoint | Population | Dosage | Impact | Claim # |
|---|---|---|---|---|---|---|
Barrett's oesophagus | increase | cancer development | - | - | predisposes to | #1 |
Barrett's oesophagus | increase | oesophageal adenocarcinoma | Those with Barrett's | 40 fold | 40 fold increased risk of | #2 |
aspirin | decrease | prevention of progression to cancer | patients with Barrett's oesophagus | - | show promise | #3 |
proton pump inhibitors (PPIs) | decrease | prevention of progression to cancer | patients with Barrett's oesophagus | - | show promise | #4 |
green tea | decrease | prevention of progression to cancer | patients with Barrett's oesophagus | - | have been suggested | #5 |
berries | decrease | prevention of progression to cancer | patients with Barrett's oesophagus | - | have been suggested | #6 |
antioxidants | decrease | prevention of progression to cancer | patients with Barrett's oesophagus | - | have been suggested | #7 |
diet | decrease | prevention of progression to cancer | patients with Barrett's oesophagus | - | have been suggested | #8 |
Barrett's oesophagus normally affects the distal oesophagus when metaplastic columnar lined epithelium replaces stratified squamous epithelium which predisposes to cancer development. This develops as a consequence of chronic gastroesophageal reflux (GORD). Those with Barrett's have a 40 fold increased risk of oesophageal adenocarcinoma [1]. There are is still a lack of understanding of the natural history of the cell of origin. This does hamper research into this area. We accept that there is a limitation in testing of the pathogenesis of Barrett's oesophagus due to a lack of a universally accepted animal model. The major questions surrounding Barrett's oesophagus include validity of surveillance strategies, the optimal treatment and more importantly an agent that can prevent progression to cancer without unacceptable side effects. The main chemopreventative agents that show promise are aspirin and proton pump inhibitors (PPIs). There are other agents such as green tea, berries and antioxidants and diet that have been suggested; we discuss the evidence available for these strategies. We hope for continued improvement in the clinical trial infrastructure to facilitate testing of new pharmacological and endoscopic interventions for Barrett's oesophagus.