AI Article Synopsis

  • Clinoptilolite is a natural aluminum silicate with a unique structure that allows it to adsorb various harmful substances, and two different particle sizes (GHC1 and GHC2) were tested for their effects on recovery from intestinal inflammation in mice.
  • Mice received either GHC1 or GHC2 treatments, and results showed that GHC2, the smaller microparticulate preparation, was more effective in reducing inflammation compared to GHC1, and matched the efficacy of a known medication, 5-aminosalicylic acid.
  • The study concluded that GHC2 is both safe and effective for treating inflammatory bowel disease in mice, highlighting its potential therapeutic benefits due to its ability to

Article Abstract

Background: Clinoptilolite is an aluminium silicate of natural origin; the microporous structure and the net negative charge of its crystal lattice allows for adsorption of ions, toxins, inflammatory mediators, and some microorganisms. We generated 2 preparations of purified clinoptilolite, which differed by about 10-fold in particle size, ie, a standard powder (GHC1) and a microparticulate fraction (GHC2) with a size of 3.6 µm and 0.39 µm (d50) respectively. These were examined for their ability to accelerate the recovery of mice from DSS (dextran sulphate sodium)-induced intestinal inflammation.

Methods: Efficacy of clinoptilolite preparations was investigated by administering DSS-treated mice twice daily with 30 mg GHC2 or GHC1 for 5 consecutive days, followed by 5 days of recovery without DSS. To explore the safety of the microparticulate preparation (GHC2), mice were subjected to 4 cycles of DSS-exposure. We specifically verified that clinoptilolite microparticles were not systemically bioavailable by examining the gut tissue and the liver for the accumulation of microparticles by transmission electron microscopy.

Results: Treatment of mice with GHC2 was superior to GHC1 and as effective as the reference compound 5-aminosalicylic acid in ameliorating the damage induced by the exposure to DSS. In addition, no clinoptilolite particle was observed in the intestinal epithelial layer, gut-associated lymph follicles, or in the liver.

Conclusion: Our observations confirm that a microparticulate preparation of clinoptilolite is safe and effective in a murine model of inflammatory bowel disease and supports the hypothesis that the adsorptive capacity of clinoptilolite is of potential therapeutic relevance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6176897PMC
http://dx.doi.org/10.1093/ibd/izx042DOI Listing

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