6533b828fe1ef96bd1288dd9

RESEARCH PRODUCT

Study of the potential toxicity of enniatins A, A(1), B, B(1) by evaluation of duodenal and colonic bioavailability applying an in vitro method by Caco-2 cells.

Maria Jose RuizJordi MañesGuillermina FontGiuseppe MecaGiuseppe Meca

subject

FusariumColonDuodenumBiological AvailabilityAbsorption (skin)PharmacologyToxicologyRisk AssessmentFusariumDepsipeptidesToxicity TestsmedicineHumansLarge intestineIncubationGastrointestinal tractbiologyChemistryMycotoxinsbiology.organism_classificationIn vitroBioavailabilitymedicine.anatomical_structureIntestinal AbsorptionCaco-2Caco-2 Cells

description

Abstract The bioavailability of the minor Fusarium mycotoxins enniatins (ENs) utilizing an in vitro method which allows the simulation of the small and large intestine tracts has been studied. This method, based on the application of the Caco-2 cells grown alone or in symbiosis with several strains characteristics of the gastrointestinal tract, has permitted to simulate the duodenal and colonic intestinal compartments, respectively. The duodenal bioavailability expressed as absorption value after 4 h of exposure, ranged from 57.7 to 76.8% for EN A, from 68.8 to 70.2% for EN A1, from 65.0 to 67.0% for EN B, and from 62.2 to 65.1% for EN B1. Colonic bioavailability after 48 h of incubation ranged from 17.3 to 33.3% for EN A, from 40.8 to 50.0% for EN A1, from 47.7 to 55.0% for EN B, and from 52.4 to 57.4% for En B1. The highest duodenal and colonic bioavailability was observed after Caco-2 cells exposed to EN A, ENs B and B1, respectively.

yearjournalcountryeditionlanguage
2010-11-25Toxicon : official journal of the International Society on Toxinology
10.1016/j.toxicon.2011.10.004https://pubmed.ncbi.nlm.nih.gov/22008903