A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design

The goal of this study was to develop and statistically optimize the metronidazole (MET), chitosan (CS) and alginate (Alg) nanoparticles (NP) nanocomposites (MET-CS-AlgNPs) using a (2(1) × 3(1) × 2(1)) × 3 = 36 full factorial design (FFD) to investigate the effect of chitosan and alginate polymer co...

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Autores principales: Sabbagh, Hazem Abdul Kader, Hussein-Al-Ali, Samer Hasan, Hussein, Mohd Zobir, Abudayeh, Zead, Ayoub, Rami, Abudoleh, Suha Mujahed
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7240564/
https://www.ncbi.nlm.nih.gov/pubmed/32244671
http://dx.doi.org/10.3390/polym12040772
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author Sabbagh, Hazem Abdul Kader
Hussein-Al-Ali, Samer Hasan
Hussein, Mohd Zobir
Abudayeh, Zead
Ayoub, Rami
Abudoleh, Suha Mujahed
author_facet Sabbagh, Hazem Abdul Kader
Hussein-Al-Ali, Samer Hasan
Hussein, Mohd Zobir
Abudayeh, Zead
Ayoub, Rami
Abudoleh, Suha Mujahed
author_sort Sabbagh, Hazem Abdul Kader
collection PubMed
description The goal of this study was to develop and statistically optimize the metronidazole (MET), chitosan (CS) and alginate (Alg) nanoparticles (NP) nanocomposites (MET-CS-AlgNPs) using a (2(1) × 3(1) × 2(1)) × 3 = 36 full factorial design (FFD) to investigate the effect of chitosan and alginate polymer concentrations and calcium chloride (CaCl(2)) concentration ondrug loading efficiency(LE), particle size and zeta potential. The concentration of CS, Alg and CaCl(2) were taken as independent variables, while drug loading, particle size and zeta potential were taken as dependent variables. The study showed that the loading efficiency and particle size depend on the CS, Alg and CaCl(2) concentrations, whereas zeta potential depends only on the Alg and CaCl(2) concentrations. The MET-CS-AlgNPs nanocomposites were characterized by X-ray diffraction (XRD), Fourier-transform infrared spectroscopy (FTIR), thermal gravimetric analysis (TGA), scanning electron microscopy (SEM) and in vitro drug release studies. XRD datashowed that the crystalline properties of MET changed to an amorphous-like pattern when the nanocomposites were formed.The XRD pattern of MET-CS-AlgNPs showed reflections at 2θ = 14.2° and 22.1°, indicating that the formation of the nanocompositesprepared at the optimum conditions havea mean diameter of (165±20) nm, with a MET loading of (46.0 ± 2.1)% and a zeta potential of (−9.2 ± 0.5) mV.The FTIR data of MET-CS-AlgNPs showed some bands of MET, such as 3283, 1585 and 1413 cm(−1), confirming the presence of the drug in the MET-CS-AlgNPs nanocomposites. The TGA for the optimized sample of MET-CS-AlgNPs showed a 70.2% weight loss compared to 55.3% for CS-AlgNPs, and the difference is due to the incorporation of MET in the CS-AlgNPs for the formation of MET-CS-AlgNPs nanocomposites. The release of MET from the nanocomposite showed sustained-release properties, indicating the presence of an interaction between MET and the polymer. The nanocomposite shows a smooth surface and spherical shape. The release profile of MET from its MET-CS-AlgNPs nanocomposites was found to be governed by the second kinetic model (R(2) between 0.956–0.990) with more than 90% release during the first 50 h, which suggests that the release of the MET drug can be extended or prolonged via the nanocomposite formulation.
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spelling pubmed-72405642020-06-11 A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design Sabbagh, Hazem Abdul Kader Hussein-Al-Ali, Samer Hasan Hussein, Mohd Zobir Abudayeh, Zead Ayoub, Rami Abudoleh, Suha Mujahed Polymers (Basel) Article The goal of this study was to develop and statistically optimize the metronidazole (MET), chitosan (CS) and alginate (Alg) nanoparticles (NP) nanocomposites (MET-CS-AlgNPs) using a (2(1) × 3(1) × 2(1)) × 3 = 36 full factorial design (FFD) to investigate the effect of chitosan and alginate polymer concentrations and calcium chloride (CaCl(2)) concentration ondrug loading efficiency(LE), particle size and zeta potential. The concentration of CS, Alg and CaCl(2) were taken as independent variables, while drug loading, particle size and zeta potential were taken as dependent variables. The study showed that the loading efficiency and particle size depend on the CS, Alg and CaCl(2) concentrations, whereas zeta potential depends only on the Alg and CaCl(2) concentrations. The MET-CS-AlgNPs nanocomposites were characterized by X-ray diffraction (XRD), Fourier-transform infrared spectroscopy (FTIR), thermal gravimetric analysis (TGA), scanning electron microscopy (SEM) and in vitro drug release studies. XRD datashowed that the crystalline properties of MET changed to an amorphous-like pattern when the nanocomposites were formed.The XRD pattern of MET-CS-AlgNPs showed reflections at 2θ = 14.2° and 22.1°, indicating that the formation of the nanocompositesprepared at the optimum conditions havea mean diameter of (165±20) nm, with a MET loading of (46.0 ± 2.1)% and a zeta potential of (−9.2 ± 0.5) mV.The FTIR data of MET-CS-AlgNPs showed some bands of MET, such as 3283, 1585 and 1413 cm(−1), confirming the presence of the drug in the MET-CS-AlgNPs nanocomposites. The TGA for the optimized sample of MET-CS-AlgNPs showed a 70.2% weight loss compared to 55.3% for CS-AlgNPs, and the difference is due to the incorporation of MET in the CS-AlgNPs for the formation of MET-CS-AlgNPs nanocomposites. The release of MET from the nanocomposite showed sustained-release properties, indicating the presence of an interaction between MET and the polymer. The nanocomposite shows a smooth surface and spherical shape. The release profile of MET from its MET-CS-AlgNPs nanocomposites was found to be governed by the second kinetic model (R(2) between 0.956–0.990) with more than 90% release during the first 50 h, which suggests that the release of the MET drug can be extended or prolonged via the nanocomposite formulation. MDPI 2020-04-01 /pmc/articles/PMC7240564/ /pubmed/32244671 http://dx.doi.org/10.3390/polym12040772 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
Sabbagh, Hazem Abdul Kader
Hussein-Al-Ali, Samer Hasan
Hussein, Mohd Zobir
Abudayeh, Zead
Ayoub, Rami
Abudoleh, Suha Mujahed
A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design
title A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design
title_full A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design
title_fullStr A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design
title_full_unstemmed A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design
title_short A Statistical Study on the Development of Metronidazole-Chitosan-Alginate Nanocomposite Formulation Using the Full Factorial Design
title_sort statistical study on the development of metronidazole-chitosan-alginate nanocomposite formulation using the full factorial design
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7240564/
https://www.ncbi.nlm.nih.gov/pubmed/32244671
http://dx.doi.org/10.3390/polym12040772
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