[HTML][HTML] Type 2 diabetes increases and metformin reduces total, colorectal, liver and pancreatic cancer incidences in Taiwanese: a representative population …

MS Lee, CC Hsu, ML Wahlqvist, HN Tsai, YH Chang… - BMC cancer, 2011 - Springer
MS Lee, CC Hsu, ML Wahlqvist, HN Tsai, YH Chang, YC Huang
BMC cancer, 2011Springer
Background Metformin protection against cancer risk in Orientals is uncertain. We examined
the possible metformin effect on total, esophageal, gastric, colorectal (CRC), hepatocellular
(HCC) and pancreatic cancers in a Taiwanese cohort. Methods A representative sample of
800,000 was drawn from the Taiwanese National Health Insurance data of 2000. A cohort of
480,984 participants 20 years or older, diabetes-cancer-free on 1st January 2000 was
formed and categorized as four groups by DM and metformin usage status. Eligible incident …
Background
Metformin protection against cancer risk in Orientals is uncertain. We examined the possible metformin effect on total, esophageal, gastric, colorectal (CRC), hepatocellular (HCC) and pancreatic cancers in a Taiwanese cohort.
Methods
A representative sample of 800,000 was drawn from the Taiwanese National Health Insurance data of 2000. A cohort of 480,984 participants 20 years or older, diabetes-cancer-free on 1st January 2000 was formed and categorized as four groups by DM and metformin usage status. Eligible incident cancer events had to occur one year after the index date until the end of 2007. The Cox proportional-hazards model evaluated relative risk of cancer for treated DM patients with or without metformin. The covariates included age, gender, other oral anti-hyperglycemic medication, Charlson comorbidity index (CCI) score and metformin exposure dosage and duration.
Results
With diabetes but no anti-hyperglycemic medication, cancer incidence density increased at least 2-fold for total, CRC and HCC. On metformin, total, CRC and HCC incidences decreased to near non-diabetic levels but to varying degrees depending on gender and cancer type (CRC in women, liver in men). Adjustment for other oral anti-hyperglycemic agents usage and CCI made the benefit of metformin more evident [hazard ratios (95% confidence intervals): total 0.12 (0.08-0.19), CRC 0.36 (0.13-0.98), liver 0.06 (0.02-0.16), pancreas 0.15 (0.03-0.79)]. There was a significant gender interaction with metformin in CRC which favored women. Metformin dosage for a significant decrease in cancer incidence was ≤500 mg/day.
Conclusions
Metformin can reduce the incidences of several gastroenterological cancers in treated diabetes.
Springer