| 27 Avril 2016
Regular use of aspirin was linked with a significantly reduced risk of  developing bile duct cancer, also called cholangiocarcinoma, in a recent  study. The findings, which are published in the journal  Hepatology, indicate that additional research on the potential of aspirin for preventing bile duct cancer is warranted. 
  Evidence has been accumulating that regular, long-term use of aspirin is  associated with decreased risks for several cancer types, especially  gastrointestinal cancers. To investigate the potential of aspirin for  preventing bile duct cancer, a team led by Jonggi Choi, MD, Roongruedee  Chaiteerakij, MD, PhD, and Lewis Roberts, MB ChB, PhD, of the Mayo  Clinic College of Medicine in Rochester, MN, conducted one of the  largest hospital-based case-control studies evaluating risk factors for  bile duct cancer in Western populations. Their study included 2395  patients with bile duct cancer who were seen at the Mayo Clinic from  2000 through 2014, and 4769 healthy controls who were matched with  patients by age, sex, race, and residence. A total of 591 (24.7 percent)  bile duct cancer patients and 2129 (44.6 percent) controls took  aspirin.  The researchers found that individuals who took aspirin had a 2.7-fold  to 3.6-fold reduced likelihood of having bile duct cancer compared with  those who did not take aspirin. In addition to finding an inverse  association between aspirin use and the presence of bile duct cancer,  the team discovered that primary sclerosing cholangitis (an inflammatory  condition that causes scars within the bile ducts), biliary tract  diseases, cirrhosis, hepatitis B virus infection, diabetes, and smoking  conferred risks of different magnitudes for the three different bile  duct cancer subtypes. This supports the hypothesis that bile duct cancer  subtypes are distinct diseases with their own risk factors.   “Chronic persistent inflammation is one of the key elements that  promotes cancer of the bile ducts, and well-known risk factors for bile  duct cancer have all been shown to increase the risk for bile duct  cancer by inducing chronic inflammation of the ducts,” explained Dr.  Choi. “Aspirin is an anti-inflammatory agent and may reduce the risk of  bile duct cancer by reducing inflammation through inhibition of the  cyclooxygenase enzyme. Previous studies have shown that aspirin also  blocks additional biological pathways that promote cancer development.”   Dr. Chaiteerakij noted that it remains to be seen whether aspirin is  safe and cost-effective for the purpose of protecting against bile duct  cancer. “Until now, there has been little evidence of a potential role  for aspirin in the prevention of bile duct cancer. Our study provides  the first evidence for this,” she said. Additional confirmatory results  are needed before aspirin can be recommended as a chemopreventive agent  for bile duct cancer, added Dr. Roberts. “The next steps should include  population-based studies examining the associations of aspirin use with  risk of bile duct cancer and also clinical trials, particularly in  populations at high-risk for bile duct cancer, to confirm the benefit of  aspirin for bile duct cancer prevention.” 
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