AI Article Synopsis

  • Mesalamine is the recommended first treatment for ulcerative colitis, and studies suggest it may help protect against colorectal cancer, although the exact reason for this protection is not yet clear.
  • Researchers found that when mesalamine interacts with copper, it can cause oxidative damage to DNA, indicating a potential mechanism for its anticancer effects.
  • The study identified that this reaction generates harmful hydroxyl radicals, leading to DNA strand breaks, highlighting how mesalamine's copper interaction could be both damaging and protective.

Article Abstract

Mesalamine is the first line pharmacologic intervention for patients with ulcerative colitis, and recent epidemiologic studies have demonstrated a protective association between therapeutic use of the drug and colorectal carcinoma. However, the mechanism by which this protection is afforded has yet to be elucidated. Because copper is found at higher than normal concentrations in neoplastic cell nuclei and is known to interact with phenolic compounds to generate reactive oxygen species, we investigated whether the reaction of mesalamine/copper was able to induce oxidative DNA strand breaks in φX-174 RF I plasmid DNA, and the various components of the mechanism by which the reaction occurred. Plasmid DNA strand breaks were induced by pharmacologically relevant concentrations of mesalamine in the presence of a micromolar concentration of Cu(II), and damage was inhibited by bathocuproinedisulfonic acid (BCS) and catalase. Further, we showed that the reaction of copper with mesalamine consumed molecular oxygen, which was inhibited by BCS. Electron paramagnetic resonance spectral analysis of the reaction of copper/mesalamine indicated the presence of the hydroxyl radical, which was inhibited by both BCS and catalase. This study demonstrates for the first time that through a copper-redox cycling mechanism, the copper-mediated oxidation of mesalamine is a pro-oxidant interaction that generates hydroxyl radicals which may participate in oxidative DNA damage. These results demonstrate a potential mechanism of the anticancer effects of mesalamine in patients with ulcerative colitis.

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Source
http://dx.doi.org/10.1016/j.tox.2010.11.009DOI Listing

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