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Development, optimization, and evaluation of PEGylated brucine-loaded PLGA nanoparticles
Faculty
Pharmacy
Year:
2020
Type of Publication:
ZU Hosted
Pages:
Authors:
Hanan Mohamed Mahmoud Mostafa Elnahas
Staff Zu Site
Abstract In Staff Site
Journal:
Drug Delivery Taylor & Francis
Volume:
Keywords :
Development, optimization, , evaluation , PEGylated brucine-loaded PLGA nanoparticles
Abstract:
The application of nanotechnology to drug delivery systems for cancer therapy has progressively received great attention. The most heavily investigated approach is the development of nanoparticles (NPs) utilizing biodegradable and biocompatible polymers such as poly (lactic-co-glycolic acid) (PLGA). These NPs could be further improved by surface modification utilizing a hydrophilic biodegradable polymer such as polyethylene glycol (PEG) to achieve passive targeting. Modified NPs can deliver drugs such as brucine (BRU), which has shown its potential in cancer therapy. The objective of the current investigation was to develop and evaluate the passive targeting of long-circulating PLGA NPs loaded with BRU. NPs were characterized in terms of drug-excipient compatibility studies, including FTIR and DSC; physicochemical evaluations including particle size, zeta potential, morphological evaluation, entrapment efficiency and percentage yield; total serum protein adsorbed onto NP surfaces; and in vitro release of the loaded drug. Factorial design was employed to attain optimal PLGA-loaded NPs. Finally, the in vivo anti-tumor activity of BRU-loaded PLGA NPs was evaluated in tumor-bearing mice. The NPs obtained had smooth surfaces with particle sizes ranged from 94 ± 3.05 to 253 ± 8.7nm with slightly positive surface charge ranged from 1.09 ± 0.15 to 3.71 ± 0.44 mV. Entrapment of BRU ranged between 37.5 ± 1.8% and 77 ± 1.3% with yields not less than 70.8%. Total protein adsorbed was less than 25.5 mg total protein/1mg NP. In vitro drug release was less than 99.1% at 168 h. Finally, significant reductions in tumor growth rate and mortality rate were observed for PEG PLGA NP formulations compared to both BRU solution and naked NPs.
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Hanan Mohamed Mahmoud Mostafa Elnahas, "Liposomal gel as Ocular Delivery System for Diclofenac sodium: In- Vitro and In-Vivo Studies", Egypt, 2012
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Hanan Mohamed Mahmoud Mostafa Elnahas, "FORMULATION AND EVALUATION OF CARBAMAZEPINE SOLID DISPERSIONS WITH POLYETHYLENE GLYCOL 6000 AND THEIR INCORPORATION INTO TABLETS", India, 2013
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Amr Selim Ahmed Ali Abu Lila, "Activation of TLR9 by incorporated pDNA within PEG-coated lipoplex enhances anti-PEG IgM production", nature, 2014
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