4.4 Article

A novel formulation of zolpidem for direct nose-to-brain delivery: synthesis, encapsulation and intranasal administration to mice

Journal

JOURNAL OF PHARMACY AND PHARMACOLOGY
Volume 70, Issue 9, Pages 1164-1173

Publisher

WILEY
DOI: 10.1111/jphp.12958

Keywords

anxiolytic effect; intranasal delivery; microcontainers; zolpidem

Funding

  1. Federal Agency of Scientific Organizations [007-Gamma3/3363/26]
  2. National Research Center Kurchatov Institute
  3. Russian Foundation for Basic Research
  4. Moscow city Government [15-33-70032 mol_a_mos]

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ObjectivesAnxiolytic drug zolpidem was incorporated into the microcontainers based on mesoporous calcium carbonate particles modified by diethylaminoethyl-dextran/hyaluronic acid shell. The release of zolpidem in saline solution and in polymer film modelling nasal mucosa was investigated. The anxiolytic effect of zolpidem upon intranasal administration of microcontainers and free medicine was determined by invivo experiments on mice. MethodsThe structures of all compounds during zolpidem synthesis were established using nuclear magnetic resonance spectroscopy. The loading efficacy and release kinetics of zolpidem were analysed by spectrophotometry. Surface morphology of formulation was investigated by scanning electron microscopy. To determine the effect of zolpidem-loaded containers administration by the intranasal route invivo experiments was carried out applying the open field test. Key findingsNasal administration of zolpidem in the form of the microcontainers based on mesoporous calcium carbonate particles modified by diethylaminoethyl-dextran/hyaluronic acid shell has a pronounced anxiolytic effect on the behaviour of the animals in the open field test. ConclusionsThe polyelectrolyte shell deposited together with zolpidem enhances the loading efficacy of the microcontainers. In vivo experiments on mice demonstrate increase in anxiolytic effect of zolpidem in microcontainers compared with upon intranasal administration of free medicine.

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