AI Article Synopsis

  • Metformin shows potential anti-cancer effects against inoperable pancreatic ductal adenocarcinoma (PDAC), particularly in patients without liver metastases, but can be affected by gastrointestinal issues and proton pump inhibitors (PPIs).
  • A review of patient records over two years identified 141 patients with PDAC, revealing that about 37.6% weren’t prescribed metformin at diagnosis, and a significant portion experienced nausea and vomiting (65.2%) or were on PPIs (46.2%).
  • The findings suggest that around a third of PDAC patients could participate in a future metformin trial, highlighting the need to manage side effects like nausea to reduce participant dropouts and to better understand how

Article Abstract

Purpose: Metformin has plausible direct and indirect anti-cancer properties against pancreatic adenocarcinoma cells. However, metformin may only be efficacious in patients with inoperable pancreatic ductal adenocarcinoma (PDAC) without liver metastases. Absorption may be decreased by gastrointestinal symptoms and proton pump inhibitors (PPIs). We aimed to justify and inform a future phase III trial of metformin versus placebo on survival in inoperable PDAC by documenting prevalence of patients meeting eligibility criteria, gastrointestinal symptoms and PPI use.

Methods: Patient notes with PDAC were reviewed at a large teaching hospital over 2 years. Study variables were obtained from multiple sources of information.

Results: 141 participants were identified (51.8% female), of which 37.6% were not prescribed metformin at diagnosis and had no radiological hepatic metastases. Characteristics were similar between non-metformin and metformin users. In eligible patients, 65.2% reported nausea and vomiting and 46.2% were prescribed PPIs.

Conclusion: Approximately, a third of all patients with inoperable PDAC are eligible for a future trial of metformin, allowing an estimate of the number of hospitals required for recruitment. Nausea and vomiting are common and should be managed effectively to prevent trial dropouts. PPI use is frequent and their influence on metformin's pharmacodynamic actions needs to be clarified.

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Source
http://dx.doi.org/10.1007/s00432-020-03177-yDOI Listing

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