Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study

Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study

Abstract Prescription of anti‐inflammatory drugs may be considered as a promising strategy in chronic wound healing where the inflammatory disturbance has delayed the healing process. It seems that hydrocortisone 17‐butyrate (HB17) would be promising in the form of a nano‐formulation to enhance drug...

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Autores principales: Reza Mombeiny, Shima Tavakol, Mostafa Kazemi, Mehdi Mehdizadeh, Akbar Hasanzadeh, Mohammad Karimi Babaahmadi, Ali Abedi, Peyman Keyhanvar
Formato: article
Lenguaje:EN
Publicado: Wiley 2021
Materias:
chronic wound healing
ethosome
hydrocortisone 17‐butyrate
nano‐carrier
nanoparticle
transdermal delivery
Biotechnology
TP248.13-248.65
Acceso en línea:https://doaj.org/article/76878550063642d19b9d9dbf357c082b
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spelling oai:doaj.org-article:76878550063642d19b9d9dbf357c082b2021-11-27T07:09:27ZAnti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study1751-875X1751-874110.1049/nbt2.12069https://doaj.org/article/76878550063642d19b9d9dbf357c082b2021-12-01T00:00:00Zhttps://doi.org/10.1049/nbt2.12069https://doaj.org/toc/1751-8741https://doaj.org/toc/1751-875XAbstract Prescription of anti‐inflammatory drugs may be considered as a promising strategy in chronic wound healing where the inflammatory disturbance has delayed the healing process. It seems that hydrocortisone 17‐butyrate (HB17) would be promising in the form of a nano‐formulation to enhance drug delivery efficacy. In the present study, transdermal delivery of nano‐HB17 in combination with iontophoresis was investigated ex vivo. Ethosomal‐HB17 was synthesised using lecithin, ethanol and cholesterol with a different ratio by hot method. The negative ethosomal‐HB17 particle size was around 244 ± 4.3 nm with high stability of up to 30 days. Additionally, evaluated entrapment efficiency of HB17 in ethosomes by high performance liquid chromatography was 40.6 ± 2.21%. Moreover, the permeation speed and amount of H17B in complete‐thickness rat skin in the presence and absence of iontophoresis showed that the penetration of free H17B and ethosomal‐H17B formulations were zero and 7.98 μg/cm2 in 120 min, respectively. Whereas in the case of applying iontophoresis, permeation amount obtained was zero and 19.69 μg/cm2 in 30 min in free H17B and ethosomal‐H17B formulations, respectively. It has been concluded that transdermal delivery of ethosomal‐H17B is an effective strategy to enhance drug delivery and it will be improved when it is combined with iontophoresis.Reza MombeinyShima TavakolMostafa KazemiMehdi MehdizadehAkbar HasanzadehMohammad Karimi BabaahmadiAli AbediPeyman KeyhanvarWileyarticlechronic wound healingethosomehydrocortisone 17‐butyratenano‐carriernanoparticletransdermal deliveryBiotechnologyTP248.13-248.65ENIET Nanobiotechnology, Vol 15, Iss 9, Pp 710-718 (2021)
institution DOAJ
collection DOAJ
language EN
topic chronic wound healing
ethosome
hydrocortisone 17‐butyrate
nano‐carrier
nanoparticle
transdermal delivery
Biotechnology
TP248.13-248.65
spellingShingle chronic wound healing
ethosome
hydrocortisone 17‐butyrate
nano‐carrier
nanoparticle
transdermal delivery
Biotechnology
TP248.13-248.65
Reza Mombeiny
Shima Tavakol
Mostafa Kazemi
Mehdi Mehdizadeh
Akbar Hasanzadeh
Mohammad Karimi Babaahmadi
Ali Abedi
Peyman Keyhanvar
Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study
description Abstract Prescription of anti‐inflammatory drugs may be considered as a promising strategy in chronic wound healing where the inflammatory disturbance has delayed the healing process. It seems that hydrocortisone 17‐butyrate (HB17) would be promising in the form of a nano‐formulation to enhance drug delivery efficacy. In the present study, transdermal delivery of nano‐HB17 in combination with iontophoresis was investigated ex vivo. Ethosomal‐HB17 was synthesised using lecithin, ethanol and cholesterol with a different ratio by hot method. The negative ethosomal‐HB17 particle size was around 244 ± 4.3 nm with high stability of up to 30 days. Additionally, evaluated entrapment efficiency of HB17 in ethosomes by high performance liquid chromatography was 40.6 ± 2.21%. Moreover, the permeation speed and amount of H17B in complete‐thickness rat skin in the presence and absence of iontophoresis showed that the penetration of free H17B and ethosomal‐H17B formulations were zero and 7.98 μg/cm2 in 120 min, respectively. Whereas in the case of applying iontophoresis, permeation amount obtained was zero and 19.69 μg/cm2 in 30 min in free H17B and ethosomal‐H17B formulations, respectively. It has been concluded that transdermal delivery of ethosomal‐H17B is an effective strategy to enhance drug delivery and it will be improved when it is combined with iontophoresis.
format article
author Reza Mombeiny
Shima Tavakol
Mostafa Kazemi
Mehdi Mehdizadeh
Akbar Hasanzadeh
Mohammad Karimi Babaahmadi
Ali Abedi
Peyman Keyhanvar
author_facet Reza Mombeiny
Shima Tavakol
Mostafa Kazemi
Mehdi Mehdizadeh
Akbar Hasanzadeh
Mohammad Karimi Babaahmadi
Ali Abedi
Peyman Keyhanvar
author_sort Reza Mombeiny
title Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study
title_short Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study
title_full Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study
title_fullStr Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study
title_full_unstemmed Anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: An ex vivo study
title_sort anti‐inflammatory ethosomal nanoformulation in combination with iontophoresis in chronic wound healing: an ex vivo study
publisher Wiley
publishDate 2021
url https://doaj.org/article/76878550063642d19b9d9dbf357c082b
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