Amphotericin B loaded ethyl cellulose nanoparticles with magnified oral bioavailability for safe and effective treatment of fungal infection - 18/06/20
Benvenuto su EM|consulte, il riferimento dei professionisti della salute.
L'accesso al testo integrale di questo articolo richiede un abbonamento.
| pagine | 10 |
| Iconografia | 10 |
| Video | 0 |
| Altro | 0 |
Graphical abstract |
AmB-EC-NPs were synthesized using a high-pressure emulsification solvent evaporation and evaluated for in vitro and in vivo studies. This method yields small, monodisperse AmB-EC-NPs along with smooth surface morphology and improved encapsulation efficiency. AmB-EC-NPs could be effective, viable and a better alternative to currently existing iv formulations, for magnified oral delivery of AmB in the treatment of fungal infection without associated adverse effects.
Highlights |
• | Ethyl cellulose nanoparticles (EC-NPs) are used as a nanocarrier for magnified oral delivery of Amphotericin B (AmB). |
• | High pressure emulsification solvent evaporation (HPESE) method is used for the encapsulation of amphiphilic drugs. |
• | AmB loaded EC-NPs (AmB-EC-NPs) exhibited gastric and storage stability. |
• | AmB is present in monomeric form inside the biocompatible EC matrix, in contrast to aggregated form of AmB in Fungizone®. |
• | Antifungal activity is performed against C. albicans. |
• | The developed formulation shows reduced hemolytic toxicity, nephrotoxicity. |
Abstract |
Amphotericin B is a gold standard drug used in various fungal and parasitic infection treatment. Most of the marketed formulations are administered intravenously, but show dose-dependent adverse effects i.e., nephrotoxicity and hemolysis. Oral route eliminates the toxic concern but exhibits poor bioavailability. Therefore, ethylcellulose nanoparticles (EC-NPs) have been used for magnified oral delivery of AmB, where EC provides gastrointestinal stability. These nanoparticles were synthesized by high-pressure emulsification solvent evaporation (HPESE) method and evaluated for in vitro and in vivo studies. This method yields small, monodisperse AmB-EC-NPs along with smooth surface morphology and improved encapsulation efficiency. The developed formulation showed a sustained release pattern following Higuchi diffusion kinetics along with gastric and storage stability. Aggregation study revealed that AmB was present in its monomeric form inside the biocompatible EC matrix. The antifungal result demonstrated that the MIC of AmB-EC-NPs was reduced ∼1/3rd than AmB and Fungizone® at 24 h whereas it was observed ∼1/8th at 48 h. in vivo pharmacokinetic analysis demonstrated 1.3-fold higher AUC than Fungizone® even at a 4.5-time lesser dose via the oral route and a ∼15-fold rise in the bioavailability in contrast to the native AmB. The hemolytic study revealed that the developed formulation exhibited 8-fold lesser hemolysis than Fungizone®. Furthermore, the biosafety profile of AmB-EC-NPs was ensured by the significantly lesser level of blood urea nitrogen and plasma creatinine along with the normal pattern of renal tubules in comparison to AmB and Fungizone®. In conclusion, the results stipulated that the AmB-EC-NPs could be effective, viable and a better alternative to currently existing iv formulations, for magnified oral delivery of AmB in the treatment of fungal infection without associated adverse effects.
Il testo completo di questo articolo è disponibile in PDF.Keywords : Amphotericin B, Magnified oral delivery, Ethylcellulose, Antifungal activity, Pharmacokinetic, Nephrotoxicity, Hemolysis
Mappa
Vol 128
Articolo 110297- agosto 2020 Ritorno al numero
Articolo precedente
- Metal element alteration in the lung by cisplatin and CV247 administration
- Klára Szentmihályi, Anna Blázovics, Zoltán May, Miklós Mohai, Krisztina Süle, Mihály Albert, Gábor Szénási, Andor Sebestény, Csaba Máthé
- Anti-inflammatory and antixidant properties of blend formulated with compounds of Malpighia emarginata D.C (acerola) and Camellia sinensis L. (green tea) in lipopolysaccharide-stimulated RAW 264.7 macrophages
- Natália Cabral Souza, Eduardo Natan de Oliveira Nascimento, Iara Bezerra de Oliveira, Hugo Miguel Lisboa Oliveira, Eudeson Gustavo Paiva Santos, Mário Eduardo Rangel Moreira Cavalcanti Mata, Daniel Pens Gelain, José Cláudio Fonseca Moreira, Rodrigo Juliani Siqueira Dalmolin, Matheus Augusto de Bittencourt Pasquali
Benvenuto su EM|consulte, il riferimento dei professionisti della salute.
L'accesso al testo integrale di questo articolo richiede un abbonamento.
Già abbonato a @@106933@@ rivista ?