AI Article Synopsis

  • Aflatoxins (AFs) and fumonisins (FBs) are harmful toxins found in some foods that can lead to serious health issues like cancer.
  • A montmorillonite clay called UPSN was tested for its ability to bind these toxins in the gastrointestinal tract of Fischer 344 rats, showing a significant reduction in the excretion of AFM1 and FB1.
  • The study found that UPSN can effectively decrease the bioavailability of AFs and FBs, suggesting it could be a useful dietary supplement to lower toxin levels in food and minimize health risks.

Article Abstract

Aflatoxins (AFs) and fumonisins (FBs) can co-contaminate foodstuffs and have been associated with hepatocellular and esophageal carcinomas in humans at high risk for exposure. One strategy to reduce exposure (and toxicity) from contaminated foodstuffs is the dietary inclusion of a montmorillonite clay (UPSN) that binds AFs and FBs in the gastrointestinal tract. In this study, the binding capacity of UPSN was evaluated for AFB1, FB1 and a combination thereof in Fischer 344 rats. Rats were pre-treated with different dietary levels of UPSN (0.25% or 2%) for 1 week. Rats were gavaged with a single dose of either 0.125 mg AFB1 or 25 mg FB1 per kg body weight and a combination thereof in the presence and absence of an aqueous solution of UPSN. The kinetics of mycotoxin excretion were monitored by analyzing serum AFB1 -albumin, urinary AF (AFM1) and FB1 biomarkers over a period of 72 h. UPSN decreased AFM1 excretion by 88-97%, indicating highly effective binding. FB1 excretion was reduced, to a lesser extent, ranging from 45% to 85%. When in combination, both AFB1 and FB1 binding occurred, but capacity was decreased by almost half. In the absence of UPSN, the combined AFB1 and FB1 treatment decreased the urinary biomarkers by 67% and 45% respectively, but increased levels of AFB1 -albumin, presumably by modulating its cytochrome metabolism. UPSN significantly reduced bioavailability of both AFB1 and FB1 when in combination; suggesting that it can be utilized to reduce levels below their respective thresholds for affecting adverse biological effects.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4259160PMC
http://dx.doi.org/10.1002/jat.2942DOI Listing

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