The effect of chitosan on the bioaccessibility and intestinal permeability of acyclovir

6533b86efe1ef96bd12cbe7b

RESEARCH PRODUCT

The effect of chitosan on the bioaccessibility and intestinal permeability of acyclovir

Miriam Verwei Christian Heinen Heleen M. Wortelboer Patrick Augustijns Marlies Kubbinga Peter Langguth Mauricio A. García

subject

Swine Acyclovir Pharmaceutical Science Biocompatible Materials 02 engineering and technology Pharmacology 030226 pharmacology & pharmacy IN-VITRO EVALUATION Intestinal absorption Chitosan chemistry.chemical_compound 0302 clinical medicine Drug Interactions Pharmacology & Pharmacy General Medicine Permeation 021001 nanoscience & nanotechnology MOLECULAR-WEIGHT Jejunum 0210 nano-technology Life Sciences & Biomedicine Biotechnology Absorption (skin)Antiviral Agents Permeability 03 medical and health sciences Organ Culture Techniques In vivo medicine Animals Humans Biology ABSORPTION ENHANCERS Chitosan Science & Technology Intestinal permeability CACO-2 Caco-2 medicine.disease TRANSPORT Rats Bioavailability MODEL Intestinal Absorption chemistry COMMON EXCIPIENTS Caco-2 Intestinal tissue segments Caco-2 Cells TNO gastro-Intestinal Model (TIM-1)SYSTEM POORLY ABSORBABLE DRUGS TRACT

description

Chitosan is object of pharmaceutical research as a candidate permeability enhancer. However, chitosan was recently shown to reduce the oral bioavailability of acyclovir in humans. The effect of chitosan on two processes determining the oral bioavailability of acyclovir, bioaccessibility and intestinal absorption, was now investigated. Acyclovir's bioaccessibility was studied using the dynamic TNO gastro-Intestinal Model (TIM-1). Four epithelial models were used for permeability experiments: a Caco-2 cell model in absence and presence of mucus and both rat and porcine excised intestinal segments. Study concentrations of acyclovir (0.8 g/l) and chitosan (1.6 g/l and 4 g/l) were in line with those used in the aforementioned human study. No effect of chitosan was measured on the bioaccessibility of acyclovir in the TIM-1 system. The results obtained with the Caco-2 models were not in line with the in vivo data. The tissue segment models (rat and porcine intestine) showed a negative trend of acyclovir's permeation in presence of chitosan. The Ussing type chamber showed to be the most biopredictive, as it did point to an overall statistically significantly reduced absorption of acyclovir. This model thus seems most appropriate for pharmaceutical development purposes, in particular when interactions between excipients and drugs are to become addressed. ispartof: EUROPEAN JOURNAL OF PHARMACEUTICS AND BIOPHARMACEUTICS vol:136 pages:147-155 ispartof: location:Netherlands status: published

year	journal	country	edition	language
2019-03-01	European Journal of Pharmaceutics and Biopharmaceutics

https://doi.org/10.1016/j.ejpb.2019.01.021