Clinoptilolite in Dextran Sulphate Sodium-Induced Murine Colitis: Efficacy and Safety of a Microparticulate Preparation

Author:

Nizet Stéphane1,Muñoz Eduardo2,Fiebich Bernd L3,Abuja Peter M4,Kashofer Karl4,Zatloukal Kurt4,Tangermann Simone5,Kenner Lukas56,Tschegg Cornelius1,Nagl Dietmar1,Scheichl Laurenz1,Meisslitzer-Ruppitsch Claudia1,Freissmuth Michael7,Berger Thomas1

Affiliation:

1. GLOCK Health, Science and Research GmbH, Deutsch-Wagram, Austria

2. Maimonides Biomedical Research Institute of Córdoba, Reina Sofía University Hospital, Department of Cell Biology, Physiology and Immunology, University of Córdoba, Córdoba, Spain

3. VivaCell Biotechnology GmbH, Denzlingen, Germany

4. Institute of Pathology, Medical University of Graz, Graz, Austria

5. Department of Experimental and Laboratory Animal Pathology, Medical University of Vienna, Austria

6. Ludwig Boltzmann Institute for Cancer Research (LBI-CR), Vienna, Austria

7. Institute of Pharmacology & Gaston H. Glock Research Laboratories for Exploratory Drug Development, Center for Physiology and Pharmacology, Medical University Vienna, Vienna, Austria

Abstract

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.

Publisher

Oxford University Press (OUP)

Subject

Gastroenterology,Immunology and Allergy

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