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Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment

Direct nose-to-brain delivery has been raised as a non-invasive powerful strategy to deliver drugs to the brain bypassing the blood-brain barrier (BBB). This study aimed at preparing and characterizing an innovative composite formulation, associating the liposome and hydrogel approaches, suitable fo...

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Autores principales: Adnet, Thomas, Groo, Anne-Claire, Picard, Céline, Davis, Audrey, Corvaisier, Sophie, Since, Marc, Bounoure, Frédéric, Rochais, Christophe, Le Pluart, Loïc, Dallemagne, Patrick, Malzert-Fréon, Aurélie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7151011/
https://www.ncbi.nlm.nih.gov/pubmed/32168767
http://dx.doi.org/10.3390/pharmaceutics12030251
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author Adnet, Thomas
Groo, Anne-Claire
Picard, Céline
Davis, Audrey
Corvaisier, Sophie
Since, Marc
Bounoure, Frédéric
Rochais, Christophe
Le Pluart, Loïc
Dallemagne, Patrick
Malzert-Fréon, Aurélie
author_facet Adnet, Thomas
Groo, Anne-Claire
Picard, Céline
Davis, Audrey
Corvaisier, Sophie
Since, Marc
Bounoure, Frédéric
Rochais, Christophe
Le Pluart, Loïc
Dallemagne, Patrick
Malzert-Fréon, Aurélie
author_sort Adnet, Thomas
collection PubMed
description Direct nose-to-brain delivery has been raised as a non-invasive powerful strategy to deliver drugs to the brain bypassing the blood-brain barrier (BBB). This study aimed at preparing and characterizing an innovative composite formulation, associating the liposome and hydrogel approaches, suitable for intranasal administration. Thermosensitive gel formulations were obtained based on a mixture of two hydrophilic polymers (Poloxamer 407, P407 and Poloxamer 188, P188) for a controlled delivery through nasal route via liposomes of an active pharmaceutical ingredient (API) of potential interest for Alzheimer’s disease. The osmolarity and the gelation temperature (T° sol-gel) of formulations, defined in a ternary diagram, were investigated by rheometry and visual determination. Regarding the issue of assays, a mixture composed of P407/P188 (15/1%, w/w) was selected for intranasal administration in terms of T° sol-gel and for the compatibility with the olfactory mucosal (280 ± 20 mOsmol, pH 6). Liposomes of API were prepared by the thin film hydration method. Mucoadhesion studies were performed by using mucin disc, and they showed the good natural mucoadhesive characteristics of in situ gel formulations, which increased when liposomes were added. The study demonstrated successful pharmacotechnical development of a promising API-loaded liposomes in a thermosensitive hydrogel intended for nasal Alzheimer’s disease treatment.
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spelling pubmed-71510112020-04-20 Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment Adnet, Thomas Groo, Anne-Claire Picard, Céline Davis, Audrey Corvaisier, Sophie Since, Marc Bounoure, Frédéric Rochais, Christophe Le Pluart, Loïc Dallemagne, Patrick Malzert-Fréon, Aurélie Pharmaceutics Article Direct nose-to-brain delivery has been raised as a non-invasive powerful strategy to deliver drugs to the brain bypassing the blood-brain barrier (BBB). This study aimed at preparing and characterizing an innovative composite formulation, associating the liposome and hydrogel approaches, suitable for intranasal administration. Thermosensitive gel formulations were obtained based on a mixture of two hydrophilic polymers (Poloxamer 407, P407 and Poloxamer 188, P188) for a controlled delivery through nasal route via liposomes of an active pharmaceutical ingredient (API) of potential interest for Alzheimer’s disease. The osmolarity and the gelation temperature (T° sol-gel) of formulations, defined in a ternary diagram, were investigated by rheometry and visual determination. Regarding the issue of assays, a mixture composed of P407/P188 (15/1%, w/w) was selected for intranasal administration in terms of T° sol-gel and for the compatibility with the olfactory mucosal (280 ± 20 mOsmol, pH 6). Liposomes of API were prepared by the thin film hydration method. Mucoadhesion studies were performed by using mucin disc, and they showed the good natural mucoadhesive characteristics of in situ gel formulations, which increased when liposomes were added. The study demonstrated successful pharmacotechnical development of a promising API-loaded liposomes in a thermosensitive hydrogel intended for nasal Alzheimer’s disease treatment. MDPI 2020-03-11 /pmc/articles/PMC7151011/ /pubmed/32168767 http://dx.doi.org/10.3390/pharmaceutics12030251 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Adnet, Thomas
Groo, Anne-Claire
Picard, Céline
Davis, Audrey
Corvaisier, Sophie
Since, Marc
Bounoure, Frédéric
Rochais, Christophe
Le Pluart, Loïc
Dallemagne, Patrick
Malzert-Fréon, Aurélie
Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment
title Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment
title_full Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment
title_fullStr Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment
title_full_unstemmed Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment
title_short Pharmacotechnical Development of a Nasal Drug Delivery Composite Nanosystem Intended for Alzheimer’s Disease Treatment
title_sort pharmacotechnical development of a nasal drug delivery composite nanosystem intended for alzheimer’s disease treatment
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7151011/
https://www.ncbi.nlm.nih.gov/pubmed/32168767
http://dx.doi.org/10.3390/pharmaceutics12030251
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