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Optimization and Characterization of Sodium Alginate Beads Providing Extended Release for Antidiabetic Drugs
by
Katona, Gábor
, Sipos, Bence
, Benei, Márk
, Csóka, Ildikó
in
antidiabetic
/ Antidiabetics
/ Comparative analysis
/ Diabetes
/ Drug delivery systems
/ Drugs
/ factorial design
/ Health products industry
/ Hypoglycemic agents
/ Instrument industry
/ nanomedicine
/ Nanoparticles
/ Optimization
/ Pharmaceuticals
/ polymeric micelle
/ Polymers
/ Product introduction
/ R&D
/ Research & development
/ Sodium
/ sodium alginate
/ Trends
/ Type 2 diabetes
/ Vehicles
2023
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Optimization and Characterization of Sodium Alginate Beads Providing Extended Release for Antidiabetic Drugs
by
Katona, Gábor
, Sipos, Bence
, Benei, Márk
, Csóka, Ildikó
in
antidiabetic
/ Antidiabetics
/ Comparative analysis
/ Diabetes
/ Drug delivery systems
/ Drugs
/ factorial design
/ Health products industry
/ Hypoglycemic agents
/ Instrument industry
/ nanomedicine
/ Nanoparticles
/ Optimization
/ Pharmaceuticals
/ polymeric micelle
/ Polymers
/ Product introduction
/ R&D
/ Research & development
/ Sodium
/ sodium alginate
/ Trends
/ Type 2 diabetes
/ Vehicles
2023
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Optimization and Characterization of Sodium Alginate Beads Providing Extended Release for Antidiabetic Drugs
by
Katona, Gábor
, Sipos, Bence
, Benei, Márk
, Csóka, Ildikó
in
antidiabetic
/ Antidiabetics
/ Comparative analysis
/ Diabetes
/ Drug delivery systems
/ Drugs
/ factorial design
/ Health products industry
/ Hypoglycemic agents
/ Instrument industry
/ nanomedicine
/ Nanoparticles
/ Optimization
/ Pharmaceuticals
/ polymeric micelle
/ Polymers
/ Product introduction
/ R&D
/ Research & development
/ Sodium
/ sodium alginate
/ Trends
/ Type 2 diabetes
/ Vehicles
2023
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Optimization and Characterization of Sodium Alginate Beads Providing Extended Release for Antidiabetic Drugs
Journal Article
Optimization and Characterization of Sodium Alginate Beads Providing Extended Release for Antidiabetic Drugs
2023
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Overview
The current research is aimed at investigating the relationship between the formulation components and conditions in the case of a binary drug delivery system, where antidiabetic drugs are co-formulated into polymeric micelles embedded in sodium alginate. Compared to chemical modifications of polymers with alginate, our development provides a simpler and scalable formulation process. Our results prove that a multi-level factorial design-based approach can ensure the development of a value-added polymeric micelle formulation with an average micelle size of 123.6 ± 3.1 nm and a monodisperse size distribution, showing a polydispersity index value of 0.215 ± 0.021. The proper nanoparticles were co-formulated with sodium alginate as a biologically decomposing and safe-to-administer biopolymer. The Box–Behnken factorial design ensured proper design space development, where the optimal sodium alginate bead formulation had a uniform, extended-release drug release mechanism similar to commercially available tablet preparations. The main conclusion is that the rapid-burst-like drug release can be hindered via the embedment of nanocarriers into biopolymeric matrices. The thermally stable formulation also holds the benefit of uniform active substance distribution after freeze-drying.
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