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Development and Characterization of Citalopram-Loaded Thermosensitive Polymeric Micelles for Nasal Administration
by
Katona, Gábor
, Sipos, Bence
, Csóka, Ildikó
, Rajab, Fatima
in
Antidepressants
/ Bioavailability
/ Chromatography
/ Citalopram
/ Drug delivery systems
/ Drugs
/ Health aspects
/ intranasal
/ Mental depression
/ Molecular weight
/ Patient compliance
/ Permeability
/ Pharmaceuticals
/ Pluronic F127
/ Poloxamer 188
/ Polymer blends
/ polymeric micelle
/ Thermodynamics
/ thermosensitive
/ Vehicles
2025
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Development and Characterization of Citalopram-Loaded Thermosensitive Polymeric Micelles for Nasal Administration
by
Katona, Gábor
, Sipos, Bence
, Csóka, Ildikó
, Rajab, Fatima
in
Antidepressants
/ Bioavailability
/ Chromatography
/ Citalopram
/ Drug delivery systems
/ Drugs
/ Health aspects
/ intranasal
/ Mental depression
/ Molecular weight
/ Patient compliance
/ Permeability
/ Pharmaceuticals
/ Pluronic F127
/ Poloxamer 188
/ Polymer blends
/ polymeric micelle
/ Thermodynamics
/ thermosensitive
/ Vehicles
2025
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Development and Characterization of Citalopram-Loaded Thermosensitive Polymeric Micelles for Nasal Administration
by
Katona, Gábor
, Sipos, Bence
, Csóka, Ildikó
, Rajab, Fatima
in
Antidepressants
/ Bioavailability
/ Chromatography
/ Citalopram
/ Drug delivery systems
/ Drugs
/ Health aspects
/ intranasal
/ Mental depression
/ Molecular weight
/ Patient compliance
/ Permeability
/ Pharmaceuticals
/ Pluronic F127
/ Poloxamer 188
/ Polymer blends
/ polymeric micelle
/ Thermodynamics
/ thermosensitive
/ Vehicles
2025
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Development and Characterization of Citalopram-Loaded Thermosensitive Polymeric Micelles for Nasal Administration
Journal Article
Development and Characterization of Citalopram-Loaded Thermosensitive Polymeric Micelles for Nasal Administration
2025
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Overview
Background/Objectives: The intranasal (IN) route of administration is a promising non-invasive approach for brain targeting, bypassing the blood–brain barrier and enhancing bioavailability. Citalopram hydrobromide (CT), a widely prescribed sparingly water-soluble selective serotonin reuptake inhibitor (SSRI), faces challenges with oral and intravenous administration, including delayed onset, adverse effects, and patient compliance issues. Methods: This study aimed to develop a novel thermoresponsive polymeric micelle (PM) system based on Pluronic® copolymers (Pluronic F127 and Poloxamer 188) improving CT’s solubility, stability, and nasal permeability for enhanced antidepressant efficacy. A preliminary study was conducted to select the optimized formulation. The preparation process involved using the thin-film hydration method, followed by freeze-drying. Comprehensive evaluations of optimized formulation characteristics included Z-average, polydispersity index (PdI), thermal behavior (lower critical solution temperature, LCST), encapsulation efficiency, X-ray powder diffraction (XRPD), thermodynamic solubility, and biological stability. Additionally, in vitro CT release and CT permeability in nasal conditions were studied. Stability under storage was also evaluated. Results: The optimized CT-PM formulation showed nanoscale micelle size (Z-average of 31.41 ± 0.99 nm), narrow size distribution (polydispersity index = 0.241), and a suitable thermal behavior for intranasal delivery (lower critical solution temperature (LCST) ~31 °C). Encapsulation efficiency reached approximately 90%, with an amorphous structure confirmed via XRPD, leading to a 95-fold increase in CT solubility. The formulation demonstrated appropriate biological and physical stability. In vitro studies showed a 25-fold faster CT release from optimized formulation compared to the initial CT, while CT-PM permeability in nasal conditions increased four-fold. Conclusions: This novel nanoscale thermosensitive formulation is a value-added strategy for nasal drug delivery systems, offering enhanced drug solubility, rapid drug release, stability, and improved permeability. This smart nanosystem represents a promising platform to overcome the limitations of conventional CT administration, improving therapeutic outcomes and patient compliance in depression management.
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