Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone

A two-component injectable hydrogel was suitably prepared for the encapsulation and prolonged release of tilorone which is an antimuscular atrophy drug. The rapid (7–45 s, depending on the polymer concentration) in situ solidifications of the hydrogel were evoked by the evolving Schiff-base bonds be...

Descripción completa

Detalles Bibliográficos
Autores principales: Abdelghafour, Mohamed M., Deák, Ágota, Kiss, Tamás, Budai-Szűcs, Mária, Katona, Gábor, Ambrus, Rita, Lőrinczi, Bálint, Keller-Pintér, Anikó, Szatmári, István, Szabó, Diána, Rovó, László, Janovák, László
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9782908/
https://www.ncbi.nlm.nih.gov/pubmed/36559217
http://dx.doi.org/10.3390/pharmaceutics14122723
_version_ 1784857451174035456
author Abdelghafour, Mohamed M.
Deák, Ágota
Kiss, Tamás
Budai-Szűcs, Mária
Katona, Gábor
Ambrus, Rita
Lőrinczi, Bálint
Keller-Pintér, Anikó
Szatmári, István
Szabó, Diána
Rovó, László
Janovák, László
author_facet Abdelghafour, Mohamed M.
Deák, Ágota
Kiss, Tamás
Budai-Szűcs, Mária
Katona, Gábor
Ambrus, Rita
Lőrinczi, Bálint
Keller-Pintér, Anikó
Szatmári, István
Szabó, Diána
Rovó, László
Janovák, László
author_sort Abdelghafour, Mohamed M.
collection PubMed
description A two-component injectable hydrogel was suitably prepared for the encapsulation and prolonged release of tilorone which is an antimuscular atrophy drug. The rapid (7–45 s, depending on the polymer concentration) in situ solidifications of the hydrogel were evoked by the evolving Schiff-base bonds between the aldehyde groups of modified PVA (4-formyl benzoate PVA, PVA-CHO, 5.9 mol% functionalization degree) and the amino groups of 3-mercaptopropionate chitosan (CHIT-SH). The successful modification of the initial polymers was confirmed by both FTIR and NMR measurements; moreover, a new peak appeared in the FTIR spectrum of the 10% w/v PVA-CHO/CHIT-SH hydrogel at 1647 cm(−1), indicating the formation of a Schiff base (–CH=N–) and confirming the interaction between the NH(2) groups of CHIT–SH and the CHO groups of PVA-CHO for the formation of the dynamic hydrogel. The reaction between the NH(2) and CHO groups of the modified biopolymers resulted in a significant increase in the hydrogel’s viscosity which was more than one thousand times greater (9800 mPa·s) than that of the used polymer solutions, which have a viscosity of only 4.6 and 5.8 mPa·s, respectively. Furthermore, the initial chitosan was modified with mercaptopropionic acid (thiol content = 201.85 ± 12 µmol/g) to increase the mucoadhesive properties of the hydrogel. The thiolated chitosan showed a significant increase (~600 mN/mm) in adhesion to the pig intestinal membrane compared to the initial one (~300 mN/mm). The in vitro release of tilorone from the hydrogel was controlled with the crosslinking density/concentration of the hydrogel; the 10% w/v PVA-CHO/CHIT-SH hydrogel had the slowest releasing (21.7 h(−1/2)) rate, while the 2% w/v PVA-CHO/CHIT-SH hydrogel had the fastest releasing rate (34.6 h(−1/2)). Due to the characteristics of these hydrogels, their future uses include tissue regeneration scaffolds, wound dressings for skin injuries, and injectable or in situ forming drug delivery systems. Eventually, we hope that the developed hydrogel will be useful in the local treatment of muscle atrophy, such as laryngotracheal atrophy.
format Online
Article
Text
id pubmed-9782908
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-97829082022-12-24 Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone Abdelghafour, Mohamed M. Deák, Ágota Kiss, Tamás Budai-Szűcs, Mária Katona, Gábor Ambrus, Rita Lőrinczi, Bálint Keller-Pintér, Anikó Szatmári, István Szabó, Diána Rovó, László Janovák, László Pharmaceutics Article A two-component injectable hydrogel was suitably prepared for the encapsulation and prolonged release of tilorone which is an antimuscular atrophy drug. The rapid (7–45 s, depending on the polymer concentration) in situ solidifications of the hydrogel were evoked by the evolving Schiff-base bonds between the aldehyde groups of modified PVA (4-formyl benzoate PVA, PVA-CHO, 5.9 mol% functionalization degree) and the amino groups of 3-mercaptopropionate chitosan (CHIT-SH). The successful modification of the initial polymers was confirmed by both FTIR and NMR measurements; moreover, a new peak appeared in the FTIR spectrum of the 10% w/v PVA-CHO/CHIT-SH hydrogel at 1647 cm(−1), indicating the formation of a Schiff base (–CH=N–) and confirming the interaction between the NH(2) groups of CHIT–SH and the CHO groups of PVA-CHO for the formation of the dynamic hydrogel. The reaction between the NH(2) and CHO groups of the modified biopolymers resulted in a significant increase in the hydrogel’s viscosity which was more than one thousand times greater (9800 mPa·s) than that of the used polymer solutions, which have a viscosity of only 4.6 and 5.8 mPa·s, respectively. Furthermore, the initial chitosan was modified with mercaptopropionic acid (thiol content = 201.85 ± 12 µmol/g) to increase the mucoadhesive properties of the hydrogel. The thiolated chitosan showed a significant increase (~600 mN/mm) in adhesion to the pig intestinal membrane compared to the initial one (~300 mN/mm). The in vitro release of tilorone from the hydrogel was controlled with the crosslinking density/concentration of the hydrogel; the 10% w/v PVA-CHO/CHIT-SH hydrogel had the slowest releasing (21.7 h(−1/2)) rate, while the 2% w/v PVA-CHO/CHIT-SH hydrogel had the fastest releasing rate (34.6 h(−1/2)). Due to the characteristics of these hydrogels, their future uses include tissue regeneration scaffolds, wound dressings for skin injuries, and injectable or in situ forming drug delivery systems. Eventually, we hope that the developed hydrogel will be useful in the local treatment of muscle atrophy, such as laryngotracheal atrophy. MDPI 2022-12-06 /pmc/articles/PMC9782908/ /pubmed/36559217 http://dx.doi.org/10.3390/pharmaceutics14122723 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/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 (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Abdelghafour, Mohamed M.
Deák, Ágota
Kiss, Tamás
Budai-Szűcs, Mária
Katona, Gábor
Ambrus, Rita
Lőrinczi, Bálint
Keller-Pintér, Anikó
Szatmári, István
Szabó, Diána
Rovó, László
Janovák, László
Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone
title Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone
title_full Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone
title_fullStr Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone
title_full_unstemmed Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone
title_short Self-Assembling Injectable Hydrogel for Controlled Drug Delivery of Antimuscular Atrophy Drug Tilorone
title_sort self-assembling injectable hydrogel for controlled drug delivery of antimuscular atrophy drug tilorone
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9782908/
https://www.ncbi.nlm.nih.gov/pubmed/36559217
http://dx.doi.org/10.3390/pharmaceutics14122723
work_keys_str_mv AT abdelghafourmohamedm selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT deakagota selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT kisstamas selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT budaiszucsmaria selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT katonagabor selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT ambrusrita selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT lorinczibalint selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT kellerpinteraniko selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT szatmariistvan selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT szabodiana selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT rovolaszlo selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone
AT janovaklaszlo selfassemblinginjectablehydrogelforcontrolleddrugdeliveryofantimuscularatrophydrugtilorone

Ejemplares similares